About the Authors:
James Mattina
Roles Data curation, Formal analysis, Methodology, Writing - original draft, Writing - review & editing
Affiliation: Studies of Translation, Ethics and Medicine (STREAM), Biomedical Ethics Unit, McGill University, Montréal, Quebec, Canada
Benjamin Carlisle
Roles Data curation, Formal analysis, Methodology, Software, Writing - original draft, Writing - review & editing
Affiliation: Studies of Translation, Ethics and Medicine (STREAM), Biomedical Ethics Unit, McGill University, Montréal, Quebec, Canada
Yasmina Hachem
Roles Data curation, Formal analysis, Writing - original draft, Writing - review & editing
Affiliation: Studies of Translation, Ethics and Medicine (STREAM), Biomedical Ethics Unit, McGill University, Montréal, Quebec, Canada
Dean Fergusson
Roles Conceptualization, Data curation, Formal analysis, Methodology, Writing - original draft, Writing - review & editing
Affiliation: Department of Clinical Epidemiology, Ottawa Hospital Research Institute, Ottawa, Ontario, Canada
Jonathan Kimmelman
Roles Conceptualization, Formal analysis, Funding acquisition, Methodology, Project administration, Supervision, Visualization, Writing - original draft, Writing - review & editing
* E-mail: [email protected]
Affiliation: Studies of Translation, Ethics and Medicine (STREAM), Biomedical Ethics Unit, McGill University, Montréal, Quebec, Canada
ORCID http://orcid.org/0000-0003-1614-6779Abstract
Failure in cancer drug development exacts heavy burdens on patients and research systems. To investigate inefficiencies and burdens in targeted drug development in cancer, we conducted a systematic review of all prelicensure trials for the anticancer drug, sorafenib (Bayer/Onyx Pharmaceuticals). We searched Embase and MEDLINE databases on October 14, 2014, for prelicensure clinical trials testing sorafenib against cancers. We measured risk by serious adverse event rates, benefit by objective response rates and survival, and trial success by prespecified primary endpoint attainment with acceptable toxicity. The first two clinically useful applications of sorafenib were discovered in the first 2 efficacy trials, after five drug-related deaths (4.6% of 108 total) and 93 total patient-years of involvement (2.4% of 3,928 total). Thereafter, sorafenib was tested in 26 indications and 67 drug combinations, leading to one additional licensure. Drug developers tested 5 indications in over 5 trials each, comprising 56 drug-related deaths (51.8% of 108 total) and 1,155 patient-years (29.4% of 3,928 total) of burden in unsuccessful attempts to discover utility against these malignancies. Overall, 32 Phase II trials (26% of Phase II activity) were duplicative, lacked appropriate follow-up, or were uninformative because of accrual failure, constituting 1,773 patients (15.6% of 11,355 total) participating in prelicensure sorafenib trials. The clinical utility of sorafenib was established early in development, with low burden on patients and resources. However, these early successes were followed by rapid and exhaustive testing against various malignancies and combination regimens, leading to excess patient burden. Our evaluation of sorafenib development suggests many opportunities for reducing costs and unnecessary patient burden in cancer drug development.
Author Summary
Numerous research subjects are exposed to unsafe and/or ineffective treatments in unsuccessful drug development programs. Yet, even successful drug development programs can involve heavy burdens for research subjects. In this manuscript, we measure risks and benefits for research subjects participating in the successful development of the anticancer drug sorafenib (first approved by the United States Food and Drug Administration in 2005). After discovering the first two cancer types responding to sorafenib, drug developers and researchers tested sorafenib against many other cancer types and in combination with many other drugs. We find that researchers were able to discover the utility of sorafenib for the first two cancer types quickly and with very little patient burden. Thereafter, attempts to extend the clinical application of sorafenib to other cancers and drug combinations involved many patients and adverse events and were mostly fruitless. We also find that many studies pursued after the first approval of sorafenib returned limited scientific information because they were duplicative or insufficiently informative. Our findings suggest that even successful drug development programs can entail substantial patient burden; they also point to ways that regulators, researchers, and policymakers can improve the risk-benefit ratio for research subjects.
Citation: Mattina J, Carlisle B, Hachem Y, Fergusson D, Kimmelman J (2017) Inefficiencies and Patient Burdens in the Development of the Targeted Cancer Drug Sorafenib: A Systematic Review. PLoS Biol 15(2): e2000487. doi:10.1371/journal.pbio.2000487
Academic Editor: Lisa Bero, University of Sydney, Australia
Received: July 5, 2016; Accepted: January 6, 2017; Published: February 3, 2017
Copyright: © 2017 Mattina et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Data Availability: All relevant data are within the paper and its Supporting Information files.
Funding: Canadian Institutes of Health Research (grant number EOG111391). The funder had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Competing interests: The authors have declared that no competing interests exist.
Abbreviations: AERO, Accumulation of Evidence and Research Organization; HCC, hepatocellular carcinoma; NSCLC, non-small-cell lung carcinoma; ORR, objective response rate; OS, overall survival; RCC, renal cell carcinoma; TTSP, time to symptomatic progression
Introduction
In cancer, only 1 in 20 new drugs introduced to clinical development receives approval from the United States Food and Drug Administration (FDA) [1]. This high rate of attrition imposes burdens and opportunity costs on research subjects. It also consumes scarce human and material resources. Numerous studies have identified various sources of inefficiency in research, including poor priority setting, [2] biased study design, [3] underpowering, [4] and incomplete reporting [5]. Eliminating such inefficiencies holds promise for improving human protections and the social return on research investments.
Targeted therapies offer great promise for improving efficiencies and reducing burdens in cancer drug development. Indeed, targeted drugs like imatinib, sunitinib, or crizotinib have been approved for marketing on the basis of a small number of trials. Yet, little is known about total research activities and burdens for targeted drugs--especially those occurring after a drug receives its first regulatory approval. To quantify the patient burden and examine inefficiencies in cancer drug development, we undertook a systematic review of all published clinical trials for the drug sorafenib for which there was no FDA label at the time of trial launch (hereafter called "prelicensure trials").
Sorafenib (Bayer/Onyx Pharmaceuticals) is the first multikinase inhibitor targeting RAF serine/threonine kinases and tumour vasculature [6]. Sorafenib was approved by the FDA for renal cell carcinoma (RCC) in 2005, [7] hepatocellular carcinoma (HCC) in 2007, [8] and radioactive iodine-refractory differentiated thyroid cancer in 2013 [9] and remains a current standard of care for each. In 2013, total sales were approximately [euro]771 million [10]. Sorafenib has also frequently been used off-label, especially in patients whose tumours show alterations in relevant gene targets [11,12]. Our selection of sorafenib enabled us to capture trial activities for a novel targeted drug over 15 y, including almost a decade since initial FDA approval.
Methods
Literature Search
We searched Embase and MEDLINE databases on October 14, 2014, using the following search terms: "sorafenib" or "Nexavar" or variations of "BAY 43-9006," and MeSH terms including variations of "clinical trial" or "randomized controlled trial" or other keywords associated with clinical trial design. No date restrictions were applied. Our complete search strategy can be found in the supplementary materials (see S1 Text).
Study Eligibility
We applied the following inclusion criteria: (1) primary data, (2) full-text publication, (3) English language, (4) final report, (5) interventional trials, and (6) administered sorafenib as monotherapy or in a combination treatment regimen in (7) patients with a cancer diagnosis. We excluded articles that reported the following: (1) laboratory study of ex vivo human tissues, (2) case reports, (3) expansion cohorts of previously published trials, (4) adjuvant or maintenance therapy trials (these were excluded because the main measure of benefit used in our study, objective tumour response, is inapplicable), (5) expanded access, and (6) FDA on-label studies in which enrolment began after regulatory approval for the same indication and treatment regimen. For the purposes of this study, "on label" was defined on the basis of cancer site.
Data Extraction
We extracted articles using a previously described template [13] that captures the following fields: (1) purpose and investigator conclusions, (2) study design and funding, (3) patient characteristics, (4) treatment procedures and duration, and (5) measures of patient risk and benefit--including response, survival, and adverse events. Trials were extracted independently by two coders using Numbat meta-analysis management software, [14] and disagreements were resolved by discussion. When data were not reported, we emailed corresponding authors. The response rate for missing data queries was 58% (19/33).
The duration of treatment was determined by the period between first drug exposure and the primary endpoint. For example, if a study used progression-free survival at 6 mo (PFS6) for the primary endpoint, duration of treatment was scored as 6 mo. For all other endpoints, we imputed duration of treatment by multiplying the median number of cycles administered by cycle length. The objective response rate (ORR) was defined as the proportion of confirmed complete and partial responses according to Response Evaluation Criteria In Solid Tumours (RECIST) or alternative response criteria if RECIST response was absent. We excluded haematological malignancies from all response analyses, since response evaluation criteria are noncomparable with solid tumours.
Treatment-related grade 3 to 5 adverse events (G3-5 AEs) according to the National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE) were captured. Safety reporting was highly variable from one trial to another. To standardize the safety data across trials, we captured the most frequent treatment-related grade 3-4 adverse event reported. Grade 5 events were captured separately. Safety data were expressed as a percentage of patients with a grade 3-5 adverse event who received at least one dose of sorafenib.
A trial was categorized as "positive" if the primary efficacy endpoint demonstrated a statistically significant positive effect and the authors reported acceptable toxicity. When primary endpoints were not declared, or if results were inconclusive according to prespecified criteria or a trial had multiple primary efficacy endpoints with conflicting outcomes, trials were scored as inconclusive. A trial was deemed "negative" if it failed to reach its primary endpoint with statistical significance (i.e., null result) or had an author assessment of unacceptable toxicity. For hybrid trials (e.g., Phase I-II trials), the primary endpoint was extracted and the trial outcome was scored from the higher phase component.
We deemed trials to have "limited value" when they were (1) duplicative Phase II, (2) not appropriately followed up, or (3) had recruitment failure. All criteria for limited value were specified before analysis. We considered a Phase II trial to be potentially duplicative if it matched a previous Phase II trial in its phase, patient characteristics (based on indication, histopathology/subtype, biomarker eligibility, number of prior therapies, types of prior therapies, response to prior therapies, and disease stage), and treatment regime (dose and combination drug). We restricted this to Phase II trials only, since these trials are aimed primarily at generating hypotheses that can be tested in more rigorous randomized trials, and they do not generally use clinical endpoints (hence, pooling of multiple small studies would not enable a more precise estimate of clinical utility). Our criteria for a trial that lacked follow-up included any Phase II trial that met its primary efficacy endpoint with a recommendation from the authors to pursue further testing that we were unable to identify a follow-up randomized trial using survival endpoints in the ClinicalTrials.gov or World Health Organization (WHO) clinical trial registries as of at least 3 y since trial close. We considered these trials to have limited value because they have delivered a signal of clinical promise but their hypotheses regarding clinical value remain unresolved and thus are inadequate for guiding practice. Recruitment failure was defined as any trial (Phase I through III) that failed to reach at least 85% of its targeted enrolment for reasons other than futility or benefit, based on trial report or registration. All trials were assessed independently by two coders for "limited value" status; raw agreement was 88%. All differences were resolved by discussion [15].
The above methods were published in a previous report [13]. However, the following methodological refinements were made in analysis stages because we believed they better captured the most relevant dynamics of efficiency and patient burden: (a) all figures involving time were presented by enrolment date rather than publication date, (b) criteria for studies of limited value were more stringent, (c) we included combination trials in our analysis, (d) we probed for trends in risk and benefit of trials using cumulative meta-analysis.
Analysis and Statistics
Objective response rate and serious adverse event proportions with 95% confidence intervals were calculated with R version 3.2.3 [16]. Pooling of objective response rates and serious adverse event rates was done using the meta package for R, [17] using the DerSimonian and Laird random-effects method [18].
The differences in our analysis of risk (grade 3-5 adverse event rate) and benefit (objective response rate) between industry and nonindustry trial subgroups and between Phase I and Phase II trial subgroups were analysed in R version 3.2.3 [16] using a weighted regression analysis. We tested whether industry-funded studies had more favourable outcomes on the hypothesis that companies have more complete and timely access to preclinical and clinical evidence and that companies might be motivated to fund only those studies likely to produce a license. The individual trial results were weighted by the inverse variance of the rate estimate. For all inferential testing, we defined p < 0.05 to be statistically significant. As all inferential testing was exploratory, we did not adjust for statistical multiplicity.
To show how risks and benefits evolved during sorafenib development, we plotted cumulative rates of grade 3-5 adverse events and overall responses by trial phase. Cumulative effect estimates were calculated using the DerSimonian and Laird random-effects method.
To determine where burdens are most concentrated and to probe for research inefficiencies, we plotted Accumulation of Evidence and Research Organization (AERO) diagrams representing indication in the vertical axis and year of first patient enrolment in the horizontal. Each node represents a clinical trial categorized by trial phase (node shape) and primary endpoint attainment (node colour).
Survival data were collected from experiments with any nonsorafenib comparator arm in which survival endpoints included all patients. Hazard ratios were either reported in the study or were calculated from summary time-to-event data using formulas from Tierney et al [19].
Patient Involvement
No patients were involved in setting the research question or the outcome measures, nor were they involved in the design or implementation of the study. Since we used data from previous clinical trials, we are unable to disseminate the results of the research to study participants directly.
Results
Study Characteristics
Our search captured 203 clinical trials, of which 74 administered sorafenib as monotherapy [20-93] and 132 tested sorafenib in combination with another anticancer therapy; [43,55,66,94-190] 3 trials tested sorafenib as both monotherapy and in a combination regimen [43,55,66]. As a whole, 11,355 patients were exposed to sorafenib in prelicensure trials in 26 malignancies, with an estimated 3,928 patient-years of involvement over a period of 13.2 y. A total of 4,988 patients received sorafenib as monotherapy, and 6,367 patients received sorafenib in combination therapy. The properties of trials in our sample are listed in Table 1, and a PRISMA flow diagram can be found in S1 Fig.
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Table 1. Properties of extracted trials in our sample.
Note that three trials [43,55,66] tested sorafenib as both monotherapy and in a combination regimen.
http://dx.doi.org/10.1371/journal.pbio.2000487.t001
Patient Benefit and Burden of Sorafenib Exposure
In total, 1,486 patients receiving sorafenib experienced objective tumour response (12.1%, 95% CI 10.4% to 14.1%), and 108 died from drug-related toxicities (2.2%, 95% CI 1.9% to 2.5%). A minimum of 2,618 patients experienced grade 3-4 drug-related serious adverse events (24.1%, 95% CI 21.7% to 26.6%).
For monotherapy, 281 patients showed objective tumour response (6.8%, 95% CI 5.2% to 8.7%), and 23 patients died from drug-related toxicities (1.4%, 95% CI 1.1% to 1.8%); a minimum of 748 patients experienced grade 3-4 drug-related toxicities (15.3%, 95% CI 13% to 17.9%). In combination therapy, 1,205 patients experienced objective tumour response (17.0%, 95% CI 14.5% to 19.8%), and 85 patients died from treatment-related toxicity (2.6%, 95% CI 2.2% to 3.1%). A minimum of 1,870 patients experienced grade 3-4 drug-related toxicities (30.5%, 95% CI 27.2% to 34.0%).
Clinical Development Trajectory
To show how risks and benefits evolved during sorafenib development, we plotted cumulative rates of grade 3-5 adverse events and objective responses for monotherapy (Fig 1) and combination therapy (Fig 2), by trial phase. Risk-benefit ratios remained relatively stable over the course of development in both monotherapy and combination therapy. We plotted AERO diagrams to show trial activities as a function of time and malignancy for monotherapy (Fig 3) and combination therapy (Fig 4). The apparent tapering of activities after year 2009 actually reflects that many trials now initiated have not yet published results and thus do not appear on the AERO diagram (on average, the interval between trial initiation and publication was 5 y). Optimal dose and schedule were identified in the earliest Phase I trials initiated in 2000 [20-23]. Initiation of two Phase II monotherapy trials occurred in 2002, each identifying an indication (renal cell carcinoma [40] and hepatocellular carcinoma [33]) that went on to receive licensure. At this time, sorafenib testing had accrued 5 drug-related deaths (4.6% of 108 total) and 93 total patient-years of involvement (2.4% of 3,928 total).
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 1. Cumulative risk (grade 3-5 serious adverse events [G3-5 AEs], in red) and benefit (overall response rate, in black) trends for sorafenib monotherapy.
(A) Phase I, (B) Phase II, and (C) Phase III trials, ordered by enrolment date. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g001
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 2. Cumulative risk (grade 3-5 serious adverse events [G3-5 AEs], in red) and benefit (overall response rate, in black) trends for sorafenib combination therapy.
(A) Phase I, (B) Phase II, and (C) Phase III trials, ordered by enrolment date. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g002
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 3. Accumulation of Evidence and Research Organization (AERO) diagram of sorafenib monotherapy trials, arranged by enrolment date.
Rectangular nodes indicate Phase I trials, circular nodes indicate Phase II trials, and triangular nodes indicate Phase III trials. Green nodes indicate studies that reached their primary endpoint with acceptable toxicity (positive trials), yellow nodes indicate an inconclusive study, and red nodes indicate a failure to reach the primary endpoint or unacceptable toxicity (negative trials). White nodes are trials with nonefficacy primary endpoints. Bold denotes FDA-approved indications and corresponding years of licensure. Numbers in nodes represent the reference numbers of each trial. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g003
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 4. Accumulation of Evidence and Research Organization (AERO) diagram of sorafenib combination therapy trials, arranged by enrolment date.
Rectangular nodes indicate Phase I trials, circular nodes indicate Phase II trials, and triangular nodes indicate Phase III trials. Green nodes indicate studies that reached their primary endpoint with acceptable toxicity (positive trials), yellow nodes indicate an inconclusive study, and red nodes indicate a failure to reach the primary endpoint or unacceptable toxicity (negative trials). White nodes are trials with nonefficacy primary endpoints. Numbers in nodes represent the reference numbers of each trial. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g004
With the pivotal renal cell carcinoma trial underway, the exploration of new indications surged in 2004 and 2005--with 27 Phase II trials launched across 14 new indications (Figs 3 and 4)--and diminished thereafter. Two of these "exploratory" studies achieved statistical significance on their primary efficacy endpoint [53,61], one of which recommended further investigation of sorafenib monotherapy in non-small-cell lung carcinoma (NSCLC) [61]. From 2006 onwards, the majority of new trials investigated sorafenib in a combination regimen, with especially intensive investigation (>5 efficacy trials) of 5 indications: melanoma, ovarian cancer, breast cancer, non-small-cell lung carcinoma, and pancreatic cancer. Testing in these 5 indications comprised 56 drug-related deaths (51.8% of 108 total) and 1,155 patient-years (29.4% of 3,928 total) of burden in unsuccessful attempts to discover clinical utility. In total, sorafenib was tested in 26 indications and 67 drug combinations. Currently, sorafenib has not received an FDA label for any combination therapy, consistent with the unsuccessful Phase III trials in Fig 4. Fig 5 shows adverse events and number of patients enrolled as a function of time with landmark events.
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 5. Cumulative treatment-related grade 3-5 adverse events (G3-5 AEs) (light red) and cumulative patients enrolled (dark red) in trials of sorafenib monotherapy and combination therapy over time with landmark events.
Dates are based on first patient enrolment. Blue line segments indicate start and primary completion dates for pivotal trials in approved indications, and blue diamonds indicate new drug application (NDA) submissions leading to approval within 6 mo. RCC = renal cell carcinoma; HCC = hepatocellular carcinoma. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g005
The pivotal RCC Phase III trial [41] did not demonstrate a statistically significant advantage on its prespecified primary endpoint of overall survival (OS). This might have been due to early crossover; sorafenib was licensed on the basis of a significant progression-free survival advantage.
In HCC, the pivotal trial [35] identified coprimary endpoints of overall survival and time to symptomatic progression (TTSP). However, only overall median survival met the prespecified criteria for statistical significance, and the trial was represented as inconclusive with respect to the primary endpoint in Fig 3. The parallel Phase III study, designed for regulatory submissions in Asia [36], explicitly excluded a primary endpoint from the protocol and was also scored inconclusive on the AERO diagram (Fig 3). This study also reached statistical significance for overall survival but not time to symptomatic progression.
The most recent FDA approval occurred in November 2013 for metastatic differentiated thyroid cancer refractory to radioactive iodine treatment [9]. This was on the basis of a successful Phase III trial showing improved progression-free survival over placebo [74]; this trial did not demonstrate a statistically significant survival advantage.
Analysis of overall survival revealed significant benefit against comparators in hepatocellular carcinoma in one monotherapy [35] and one combination trial [126] (Fig 6). For all other indications and combinations, exposure to sorafenib was neither demonstrably advantageous nor disadvantageous for patients, according to prespecified thresholds of significance. There was no obvious trend towards sorafenib disadvantage.
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 6. Hazard ratios (HRs) of overall median survival (OS) comparing monotherapy and combination therapy trials, arranged by trial initiation date (publication date shown).
Asterisks indicate significant survival benefit according to prespecified statistical thresholds. RCC = renal cell carcinoma; HCC = hepatocellular carcinoma; NSCLC = non-small-cell lung carcinoma. Per-trial data are available in our supplementary materials (see S1 Data).
http://dx.doi.org/10.1371/journal.pbio.2000487.g006
Patterns of Research and Limited Value Studies
There was a significant improvement in objective response rate between Phase I and Phase III trials testing sorafenib in a combination regimen (15.5% and 22.4%, respectively; p < 0.05). Phase III trials testing sorafenib monotherapy reported a significantly lower grade 3-5 adverse event rate than Phase II trials (10.4% versus 16.7%, respectively; p < 0.05). All other analyses of objective response rate and grade 3-5 adverse events by funding source or trial phase were not significantly different between subgroups (Fig 7).
Download:
*
PPT
PowerPoint slide
*
PNG
larger image
*
TIFF
original image
Fig 7. Pooled estimates and 95% CI for subgroup analyses.
(A) objective response rate (ORR) and (B) grade 3-5 adverse events (G3-5 AEs) by therapy, funding source, and phase number. Asterisks indicate statistical significance (p < 0.05).
http://dx.doi.org/10.1371/journal.pbio.2000487.g007
In total, 32 Phase II trials of limited value were identified (26% of Phase II trials), representing 1,773 patients and 701 y of patient involvement (15.6% and 17.8% of total prelicensure trial activity, respectively). In these trials, there were 367 grade 3-4 sorafenib-related adverse events and 9 patient deaths (14.0% of 2,618 adverse events and 8.3% of 108 deaths in sorafenib testing, respectively). Among the 1,717 patients in these studies evaluable for response in solid tumours, 269 achieved objective tumour response (18.1% of 1,486 responses in sorafenib testing).
Out of 124 Phase II studies, 10 were deemed potentially duplicative (8.1%) (S2 Table). In 14 instances, Phase II trials with a positive primary efficacy endpoint and author recommendation for further testing were not followed up in randomized trials testing survival (11.3%). Ten Phase II studies failed to accrue a sample sufficient to address the primary objectives of the study (8.1%; see S2 Text for details).
Discussion
In this study, we extend our previous work exploring efficiency and burden in drug development. Consistent with our earlier reports looking at the anticancer drug sunitinib [13], we find that drug developers identified useful dosing, scheduling, and responding indications in a short amount of time with only a minimal number of trials, adverse events, or patient years. This suggests that drug developers can be highly effective at detecting signals of clinical promise using preclinical and preliminary clinical evidence--especially when there is a strong market incentive for efficiency.
However, once indications responding to sorafenib were identified, many indications and combination regimes were tested in rapid succession, leading to an accumulation of burden with greatly diminished return, as measured by FDA label revisions or confirmed clinical value. Cumulative risk and benefit analyses showed that in over a decade of drug development, the risk-benefit ratio remained relatively stable. This suggests that patients were not necessarily exposed to more unfavourable conditions with persistent testing but also that drug developers and clinical research groups were not able to mitigate risk or hone their ability to unlock greater clinical utility. Our analysis also found that patients allocated to sorafenib arms in randomized trials were generally neither advantaged nor disadvantaged in terms of survival (note that our pooled estimate may somewhat underestimate survival advantage because of crossover in HCC and RCC studies). This suggests that patient burdens entailed by this pattern of rapid-fire exploration are at least not associated with survival disadvantage for patients receiving sorafenib.
Implications for Drug Developers
Our results also suggest that, while drug developers are adept at identifying and confirming correct hypotheses about clinical utility, researchers are slow to curtail attempts to discover new responding indications or to abandon hypotheses that flag in testing. Regarding the former, attempting to extend the label of a drug seems appropriate--especially where a drug has shown activity against two discrete malignancies. Elsewhere, we have argued that translation trajectories must contain at least some negative trials in order to furnish health care systems with adequate evidence [223]; not testing sorafenib against other plausible malignancies would have left oncologists uncertain about additional applications of the drug. However, our findings suggest that researchers were unable to join preclinical evidence together with a rapidly expanding clinical evidence base to extend the label of sorafenib. For a systematic review of preclinical evidence relating to monotherapy trials in this paper, see Mattina et al. 2016 [224]. It is possible that new adaptive trial designs might offer more efficient ways of ruling out nonresponding indications.
Reluctance to abandon hypotheses is illustrated by the highly perseverant and, until now, futile attempts to apply sorafenib to indications like non-small-cell lung carcinoma, breast cancer, and glioma. One potential explanation for such perseverance is clinical demand. Treatment of glioma has improved little in the last decade, and researchers might be willing to launch new glioma trials even if their confidence in promise is meagre. A second possibility is market demand: if the potential commercial returns are sufficiently large, drug companies may be willing to pursue trials that have marginal prospects of success. Third, seeming perseverance may reflect that many researchers test nearly identical hypotheses simultaneously, thus limiting the ability of researchers to build on insights. Favouring this interpretation is the fact that the periods of clinical testing for all trials deemed duplicative in our analysis overlapped. On the other hand, many trial activities for highly tested indications such as breast cancer did not overlap in terms of time period. Last, researchers may be prone to cognitive biases by which evidence confirming a molecular hypothesis is given greater weight than evidence disconfirming it. Sorafenib was tested against melanoma, generally on the conviction that sorafenib can interrupt disease progression through the MAPK pathway. However, seven trials that were founded on this premise had negative outcomes, resulting in potentially excess exposures [46,48,160,161,165,168,169]. The pattern of testing we observed is consistent with a dynamic in which researchers embrace findings when they support a pathophysiological premise but doubt their veracity when results conflict with favoured pathophysiological premises. The possible effects of cognitive biases on clinical development decisions deserves further exploration.
Our analysis raises a natural question: at what point should researchers discontinue attempts to extend a drug's label to other indications and drug combinations? Reasonable people might disagree. The fact that cancer is a life-threatening illness would favour the kind of exhaustive testing we observed, as would the prospect that a novel multikinase inhibitor like sorafenib might show activity against a variety of malignancies. Under conditions of high uncertainty, it could make sense to launch many "hypothesis-generating" Phase II trials [225]. In our view, however, several points would caution against the extensive and perseverant testing we observed after licensure. First, the nontrivial toxicities associated with sorafenib--especially when combined with other drugs--would demand grounding any new trial in a good evidentiary rationale. Second, the fact that sorafenib is a targeted drug and that drug developers were so adept at selecting viable hypotheses early on should favour a higher proportion of successes in extending the label of sorafenib. Third, further testing of a drug ties up human and material resources that might be applied to other research programs. In a realm like cancer, where there is a dense pipeline of novel drug candidates and pressing clinical need, these opportunity costs should encourage judicious launch of new trials [225].
Our findings identify other opportunities to decrease patient burden and improve research efficiency. According to the criteria we used, 26% of prelicensure Phase II trials of sorafenib had limited value because they were duplicative, not followed up as appropriate, or unable to recruit a critical mass of subjects. To be sure, that a study is destined to have "limited value" is not always knowable at trial outset. Yet, knowing the volume of studies that--in retrospect--had limited value can motivate development of mechanisms and practices that reduce their occurrence. For instance, duplicative trials were always conducted during overlapping time periods; researchers, ethics committees, and data safety monitoring bodies should monitor trial registries for identical studies that have already started recruitment, and reevaluate risk and benefit when there is duplication. Others have observed that many positive, exploratory studies are not followed up with rigorous testing--particularly in combination trials [226]. It may seem counterintuitive to label any "positive" trial as having "limited value." However, a large percentage of drug prescriptions in cancer are off-label, [227,228] and in numerous cases, positive surrogate responses that have not been promptly followed up with rigorous testing have led to adoption of treatments that were later shown ineffective and harmful [229-231]. Less duplication and better follow up of promising findings might be achieved by improving the flow of information and coordination among research teams. Trials with unsuccessful accrual are less likely to meet the statistical power needed to answer their primary question and impose unnecessary burden on patients and resources in the process. Ethics committees, investigators, and data safety monitoring bodies should closely monitor the design, recruitment, and feasibility of meeting accrual goals throughout a trial to mitigate risks from slow accrual [15].
Study Limitations
Our findings should be interpreted in light of the following limitations. First, this analysis focused solely on published trial reports and is thus susceptible to the effects of publication bias. Because of labour limitations, for example, we did not search clinical trial registries for completed but unpublished studies. However, incorporating unpublished studies would not be expected to improve the favourability of risk-benefit ratios or to alter the temporal dynamics we observed. Second, this analysis used objective response rate in solid tumours as a proxy for benefit and treatment-related serious adverse events as a proxy for patient burden. We used response because it allows comparison of benefit across solid tumours and trial phases. However, response is a surrogate endpoint. Moreover, sorafenib is cytostatic in many malignancies, and clinical benefit may not be reflected in objective response rate. Treatment-related adverse events were also inconsistently reported--many studies only reported adverse events occurring in over a certain percentage of patients. Our measure of risk likely underestimates the real estimates. Third, some might question our criteria for "limited value" trials. Our definition of duplication probably excluded trials that many would consider duplicative or overlapping or that a meta-analyst would consider similar enough to aggregate. Indeed, several studies we classified as distinct using our criteria would almost certainly be viewed by many oncologists as substantially overlapping if not identical (see S2 Text). On the other hand, there may be grounds for believing some studies we classified as duplicative are distinct because they enrolled different demographic groups. As well, we note that even studies deemed to have "limited value" yield some information. For example, studies that are underpowered because of recruitment failure might be combined with similar studies in a meta-analysis. However, this places the onus of deriving scientific insights on meta-analyses that might or might not materialize; the important question is whether the value of this information is sufficient to purchase their patient burden and opportunity costs. Also, studies that have "limited value" might sometimes be beyond the control of sponsors or research teams. If the standard of care shifts radically, studies might close for low recruitment or positive Phase II studies might not have follow-up. It is therefore impossible to exclude that some studies classified as having limited value reflect dynamism elsewhere in cancer drug development. Last, the ethical implications of our findings need to be interpreted against the fact that the vast majority of trials in our sample enrolled patients with refractory disease. Nothing in our analysis would suggest such patients were deprived of standard of care or that enrolment was associated with survival disadvantage. Nevertheless, even when patients have advanced disease, the imposition of burdens like side effects and time commitment should be grounded in a compelling biological rationale.
Conclusions
Our findings--when interpreted alongside the other drug development trajectory we analysed--suggest that drug developers can marshal preclinical and early trial evidence to discover a drug's utility very efficiently. Inefficiencies, costs, and burdens accumulate later in drug development, and the majority of patient burden--however measured--accumulates after successful interventional strategies have been discovered. The patterns we observe suggest that a combination of commercial considerations, poor coordination, time pressures, and cognitive biases may distort trial decision making, resulting in substantial excess burdens and resource demands.
Supporting Information
S1 Fig. PRISMA flow diagram.
(TIFF)
S2 Fig. Forest plot of objective response rates (ORR) per trial, by funding source, for monotherapy trials.
There was no significant difference in objective response rate (p > 0.05) between trials with industry-only funding and trials with at least one non-industry funding source.
(PDF)
S3 Fig. Forest plot of treatment-related grade 3-5 adverse events per trial, by funding source, for monotherapy trials.
There was no significant difference in grade 3-5 serious adverse event rate (p > 0.05) between trials with industry-only funding and trials with at least one non-industry funding source.
(PDF)
S4 Fig. Forest plot of objective response rates (ORR) per trial, by phase, for monotherapy trials.
There was no significant difference in objective response rate (p > 0.05) between phase I, phase II and phase III trials.
(PDF)
S5 Fig. Forest plot of treatment-related grade 3-5 adverse events per trial, by phase, for monotherapy trials.
There was a significant improvement in grade 3-5 serious adverse event rate (p < 0.05) between phase II and phase III trials. No other comparisons showed significance (p > 0.05).
(PDF)
S6 Fig. Forest plot of objective response rates (ORR) per trial, by funding source, for combination therapy trials.
There was no significant difference in objective response rate (p > 0.05) between trials with industry-only funding and trials with at least one non-industry funding source.
(PDF)
S7 Fig. Forest plot of treatment-related grade 3-5 adverse events per trial, by funding source, for combination therapy trials.
There was no significant difference in grade 3-5 serious adverse event rate (p > 0.05) between trials with industry-only funding and trials with at least one non-industry funding source.
(PDF)
S8 Fig. Forest plot of objective response rates (ORR) per trial, by phase, for combination therapy trials.
There was a significant improvement in objective response rate (p < 0.05) between phase I and phase III trials. No other comparisons showed significance (p > 0.05).
(PDF)
S9 Fig. Forest plot of treatment-related grade 3-5 adverse events per trial, by phase, for combination therapy trials.
There was no significant difference in grade 3-5 serious adverse event rate (p > 0.05) between phase I, phase II and phase III trials.
(PDF)
S1 Table. PRISMA research checklist.
(DOC)
S2 Table. Substantially overlapping trials by eligibility criteria.
(DOCX)
S1 Text. Embase and MEDLINE search strategy.
(DOCX)
S2 Text. Citations of limited value trials by prespecified criteria.
(DOCX)
S3 Text. Research protocol adapted from a previous report [13].
(DOCX)
S4 Text. Codebook for extraction of information from clinical trials.
(DOCX)
S1 Data. Dataset of clinical trials.
(XLSX)
Acknowledgments
We acknowledge the contributions of the Studies of TRanslation, Ethics And Medicine (STREAM) research group--in particular, Esther Vinarov.
Contopoulos-Ioannidis DG, Alexiou GA, Gouvias TC, Ioannidis J. Life cycle of translational research for medical interventions. Science. 2008;321(5894):1298-1299. doi: 10.1126/science.1160622. pmid:18772421
Chalmers I, Bracken MB, Djulbegovic B, Garattini S, Grant J, Gülmezoglu AM, et al. How to increase value and reduce waste when research priorities are set. The Lancet. 2014;383(9912):156-165
Ioannidis JP, Greenland S, Hlatky MA, Khoury MJ, Macleod MR, Moher D, et al. Increasing value and reducing waste in research design, conduct, and analysis. The Lancet. 2014;383(9912):166-175
Keen HI, Pile K, Hill CL. The prevalence of underpowered randomized clinical trials in rheumatology. The Journal of rheumatology. 2005;32(11):2083-2088. pmid:16265683
Hakala A, Kimmelman J, Carlisle B, Freeman G, Fergusson D. Accessibility of trial reports for drugs stalling in development: a systematic assessment of registered trials. BMJ. 2015;350:h1116. doi: 10.1136/bmj.h1116. pmid:25752879
Wilhelm S, Carter C, Lynch M, Lowinger T, Dumas J, Smith RA, et al. Discovery and development of sorafenib: a multikinase inhibitor for treating cancer. Nature reviews Drug discovery. 2006;5(10):835-844. doi: 10.1038/nrd2130. pmid:17016424
US Food and Drug Administration C. Sorafenib NDA approval letter; 2005. http://www.accessdata.fda.gov/drugsatfda_docs/appletter/2005/021923ltr.pdf
US Food and Drug Administration C. Sorafenib labeling revision; 2007. http://www.accessdata.fda.gov/drugsatfda_docs/label/2007/021923s004s005s006s007lbl.pdf
US Food and Drug Administration C. Sorafenib labeling revision; 2013. http://www.accessdata.fda.gov/drugsatfda_docs/label/2013/021923s016lbl.pdf
Nasdaq. Bayer/Amgen's Nexavar Fails in Late-Stage Study--Analyst Blog; 2014. http://www.nasdaq.com/article/bayeramgens-nexavar-fails-in-late-stage-study-analyst-blog-cm334828
Giri S, Hamdeh S, Bhatt VR, Schwarz JK. Sorafenib in relapsed AML with FMS-like receptor tyrosine kinase-3 internal tandem duplication mutation. Journal of the National Comprehensive Cancer Network. 2015;13(5):508-514. pmid:25964636
Le Tourneau C, Delord JP, Gonçalves A, Gavoille C, Dubot C, Isambert N, et al. Molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer (SHIVA): a multicentre, open-label, proof-of-concept, randomised, controlled phase 2 trial. The Lancet Oncology. 2015;16(13):1324-1334. doi: 10.1016/S1470-2045(15)00188-6. pmid:26342236
Carlisle B, Demko N, Freeman G, Hakala A, MacKinnon N, Ramsay T, et al. Benefit, risk, and outcomes in drug development: a systematic review of sunitinib. Journal of the National Cancer Institute. 2016;108(1):djv292. doi: 10.1093/jnci/djv292. pmid:26547927
Carlisle BG. Numbat Meta-Analysis Extraction Manager; 2015. https://github.com/bgcarlisle/Numbat
Carlisle B, Kimmelman J, Ramsay T, MacKinnon N. Unsuccessful trial accrual and human subjects protections: An empirical analysis of recently closed trials. Clinical Trials. 2015;12(1):77-83. doi: 10.1177/1740774514558307. pmid:25475878
R Core Team. R: a language and environment for statistical computing. Vienna, Austria; 2015. https://www.R-project.org/
Schwarzer G. Meta: general package for meta-analysis; 2015. R package version 4.2-0. https://github.com/guido-s/meta
DerSimonian R, Laird N. Meta-analysis in clinical trials. Controlled clinical trials. 1986;7(3):177-188. pmid:3802833
Tierney JF, Stewart LA, Ghersi D, Burdett S, Sydes MR. Practical methods for incorporating summary time-to-event data into meta-analysis. Trials. 2007;8(1):16
Strumberg D, Richly H, Hilger RA, Schleucher N, Korfee S, Tewes M, et al. Phase I clinical and pharmacokinetic study of the Novel Raf kinase and vascular endothelial growth factor receptor inhibitor BAY 43-9006 in patients with advanced refractory solid tumors. Journal of clinical oncology. 2005;23(5):965-972. pmid:15613696
Moore M, Hirte H, Siu L, Oza A, Hotte S, Petrenciuc O, et al. Phase I study to determine the safety and pharmacokinetics of the novel Raf kinase and VEGFR inhibitor BAY 43-9006, administered for 28 days on/7 days off in patients with advanced, refractory solid tumors. Annals of oncology. 2005;16(10):1688-1694. doi: 10.1093/annonc/mdi310. pmid:16006586
Awada A, Hendlisz A, Gil T, Bartholomeus S, Mano M, De Valeriola D, et al. Phase I safety and pharmacokinetics of BAY 43-9006 administered for 21 days on/7 days off in patients with advanced, refractory solid tumours. British Journal of Cancer. 2005;92(10):1855-1861. doi: 10.1038/sj.bjc.6602584. pmid:15870716
Clark JW, Eder JP, Ryan D, Lathia C, Lenz HJ. Safety and pharmacokinetics of the dual action Raf kinase and vascular endothelial growth factor receptor inhibitor, BAY 43-9006, in patients with advanced, refractory solid tumors. Clinical Cancer Research. 2005;11(15):5472-5480. doi: 10.1158/1078-0432.CCR-04-2658. pmid:16061863
Minami H, Kawada K, Ebi H, Kitagawa K, Kim Yi, Araki K, et al. Phase I and pharmacokinetic study of sorafenib, an oral multikinase inhibitor, in Japanese patients with advanced refractory solid tumors. Cancer science. 2008;99(7):1492-1498. doi: 10.1111/j.1349-7006.2008.00837.x. pmid:18477034
Miller AA, Murry DJ, Owzar K, Hollis DR, Kennedy EB, Abou-Alfa G, et al. Phase I and pharmacokinetic study of sorafenib in patients with hepatic or renal dysfunction: CALGB 60301. Journal of Clinical Oncology. 2009;27(11):1800-1805. doi: 10.1200/JCO.2008.20.0931. pmid:19255312
Tolcher AW, Appleman LJ, Shapiro GI, Mita AC, Cihon F, Mazzu A, et al. A phase I open-label study evaluating the cardiovascular safety of sorafenib in patients with advanced cancer. Cancer chemotherapy and pharmacology. 2011;67(4):751-764. doi: 10.1007/s00280-010-1372-3. pmid:20521052
Widemann BC, Kim A, Fox E, Baruchel S, Adamson PC, Ingle AM, et al. A phase I trial and pharmacokinetic study of sorafenib in children with refractory solid tumors or leukemias: a Children's Oncology Group Phase I Consortium report. Clinical Cancer Research. 2012;18(21):6011-6022. doi: 10.1158/1078-0432.CCR-11-3284. pmid:22962440
Semrad TJ, Eddings C, Pan CX, Lau DH, Gandara D, Beckett L, et al. Feasibility study of intra-patient sorafenib dose-escalation or re-escalation in patients with previously treated advanced solid tumors. Investigational new drugs. 2012;30(5):2001-2007. doi: 10.1007/s10637-011-9761-y. pmid:22015991
Crump M, Hedley D, Kamel-Reid S, Leber B, Wells R, Brandwein J, et al. A randomized phase I clinical and biologic study of two schedules of sorafenib in patients with myelodysplastic syndrome or acute myeloid leukemia: a NCIC (National Cancer Institute of Canada) Clinical Trials Group Study. Leukemia & lymphoma. 2010;51(2):252-260
Pratz KW, Cho E, Levis MJ, Karp JE, Gore SD, McDevitt M, et al. A pharmacodynamic study of sorafenib in patients with relapsed and refractory acute leukemias. Leukemia. 2010;24(8):1437-1444. doi: 10.1038/leu.2010.132. pmid:20535150
Borthakur G, Kantarjian H, Ravandi F, Zhang W, Konopleva M, Wright JJ, et al. Phase I study of sorafenib in patients with refractory or relapsed acute leukemias. Haematologica. 2011;96(1):62-68. doi: 10.3324/haematol.2010.030452. pmid:20952518
Man CH, Fung TK, Ho C, Han HH, Chow HC, Ma AC, et al. Sorafenib treatment of FLT3-ITD+ acute myeloid leukemia: favorable initial outcome and mechanisms of subsequent nonresponsiveness associated with the emergence of a D835 mutation. Blood. 2012;119(22):5133-5143. doi: 10.1182/blood-2011-06-363960. pmid:22368270
Abou-Alfa GK, Schwartz L, Ricci S, Amadori D, Santoro A, Figer A, et al. Phase II study of sorafenib in patients with advanced hepatocellular carcinoma. Journal of Clinical Oncology. 2006;24(26):4293-4300. doi: 10.1200/JCO.2005.01.3441. pmid:16908937
Furuse J, Ishii H, Nakachi K, Suzuki E, Shimizu S, Nakajima K. Phase I study of sorafenib in Japanese patients with hepatocellular carcinoma. Cancer science. 2008;99(1):159-165. doi: 10.1111/j.1349-7006.2007.00648.x. pmid:17953709
Llovet JM, Ricci S, Mazzaferro V, Hilgard P, Gane E, Blanc JF, et al. Sorafenib in advanced hepatocellular carcinoma. New England Journal of Medicine. 2008;359(4):378-390. doi: 10.1056/NEJMoa0708857. pmid:18650514
Cheng AL, Kang YK, Chen Z, Tsao CJ, Qin S, Kim JS, et al. Efficacy and safety of sorafenib in patients in the Asia-Pacific region with advanced hepatocellular carcinoma: a phase III randomised, double-blind, placebo-controlled trial. The lancet oncology. 2009;10(1):25-34. doi: 10.1016/S1470-2045(08)70285-7. pmid:19095497
Yau T, Chan P, Ng KK, Chok SH, Cheung TT, Fan ST, et al. Phase 2 open-label study of single-agent sorafenib in treating advanced hepatocellular carcinoma in a hepatitis B--endemic Asian population. Cancer. 2009;115(2):428-436. doi: 10.1002/cncr.24029. pmid:19107763
Wörns MA, Weinmann A, Pfingst K, Schulte-Sasse C, Messow CM, Schulze-Bergkamen H, et al. Safety and efficacy of sorafenib in patients with advanced hepatocellular carcinoma in consideration of concomitant stage of liver cirrhosis. Journal of clinical gastroenterology. 2009;43(5):489-495. doi: 10.1097/MCG.0b013e31818ddfc6. pmid:19247201
Pressiani T, Boni C, Rimassa L, Labianca R, Fagiuoli S, Salvagni S, et al. Sorafenib in patients with Child-Pugh class A and B advanced hepatocellular carcinoma: a prospective feasibility analysis. Annals of oncology. 2013;24(2):406-411. doi: 10.1093/annonc/mds343. pmid:23041587
Ratain MJ, Eisen T, Stadler WM, Flaherty KT, Kaye SB, Rosner GL, et al. Phase II placebo-controlled randomized discontinuation trial of sorafenib in patients with metastatic renal cell carcinoma. Journal of Clinical Oncology. 2006;24(16):2505-2512. pmid:16636341
Escudier B, Eisen T, Stadler WM, Szczylik C, Oudard S, Siebels M, et al. Sorafenib in advanced clear-cell renal-cell carcinoma. New England Journal of Medicine. 2007;356(2):125-134. doi: 10.1056/NEJMoa060655. pmid:17215530
Akaza H, Tsukamoto T, Murai M, Nakajima K, Naito S. Phase II study to investigate the efficacy, safety, and pharmacokinetics of sorafenib in Japanese patients with advanced renal cell carcinoma. Japanese journal of clinical oncology. 2007;37(10):755-762. doi: 10.1093/jjco/hym095. pmid:17951335
Jonasch E, Corn P, Pagliaro LC, Warneke CL, Johnson MM, Tamboli P, et al. Upfront, randomized, phase 2 trial of sorafenib versus sorafenib and low-dose interferon alfa in patients with advanced renal cell carcinoma. Cancer. 2010;116(1):57-65. doi: 10.1002/cncr.24685. pmid:19862815
Escudier B, Szczylik C, Hutson TE, Demkow T, Staehler M, Rolland F, et al. Randomized phase II trial of first-line treatment with sorafenib versus interferon Alfa-2a in patients with metastatic renal cell carcinoma. Journal of clinical oncology. 2009;27(8):1280-1289. doi: 10.1200/JCO.2008.19.3342. pmid:19171708
Amato R, Zhai J, Willis J, Saxena S, DeFoe M. A phase II trial of intrapatient dose-escalated sorafenib in patients with metastatic renal cell carcinoma. Clinical genitourinary cancer. 2012;10(3):153-158. doi: 10.1016/j.clgc.2012.03.001. pmid:22551785
Eisen T, Ahmad T, Flaherty K, Gore M, Kaye S, Marais R, et al. Sorafenib in advanced melanoma: a Phase II randomised discontinuation trial analysis. British journal of cancer. 2006;95(5):581-586. doi: 10.1038/sj.bjc.6603291. pmid:16880785
Flaherty KT, Lathia C, Frye RF, Schuchter L, Redlinger M, Rosen M, et al. Interaction of sorafenib and cytochrome P450 isoenzymes in patients with advanced melanoma: a phase I/II pharmacokinetic interaction study. Cancer chemotherapy and pharmacology. 2011;68(5):1111-1118. doi: 10.1007/s00280-011-1585-0. pmid:21350850
Ott PA, Hamilton A, Min C, Safarzadeh-Amiri S, Goldberg L, Yoon J, et al. A phase II trial of sorafenib in metastatic melanoma with tissue correlates. PLoS ONE. 2010;5(12):e15588. doi: 10.1371/journal.pone.0015588. pmid:21206909
Elser C, Siu LL, Winquist E, Agulnik M, Pond GR, Chin SF, et al. Phase II trial of sorafenib in patients with recurrent or metastatic squamous cell carcinoma of the head and neck or nasopharyngeal carcinoma. Journal of Clinical Oncology. 2007;25(24):3766-3773. pmid:17704426
Williamson SK, Moon J, Huang CH, Guaglianone PP, LeBlanc M, Wolf GT, et al. Phase II evaluation of sorafenib in advanced and metastatic squamous cell carcinoma of the head and neck: Southwest Oncology Group Study S0420. Journal of Clinical Oncology. 2010;28(20):3330-3335. doi: 10.1200/JCO.2009.25.6834. pmid:20498388
Safarinejad MR. Safety and efficacy of sorafenib in patients with castrate resistant prostate cancer: a phase II study. Urologic Oncology: Seminars and Original Investigations. 2010;28(1):21-27. doi: 10.1016/j.urolonc.2008.06.003. pmid:18789732
Chi K, Ellard S, Hotte S, Czaykowski P, Moore M, Ruether J, et al. A phase II study of sorafenib in patients with chemo-naive castration-resistant prostate cancer. Annals of Oncology. 2007;19(4):746-51. pmid:18056648
Steinbild S, Mross K, Frost A, Morant R, Gillessen S, Dittrich C, et al. A clinical phase II study with sorafenib in patients with progressive hormone-refractory prostate cancer: a study of the CESAR Central European Society for Anticancer Drug Research-EWIV. British journal of cancer. 2007;97(11):1480-1485. doi: 10.1038/sj.bjc.6604064. pmid:18040273
Dahut WL, Scripture C, Posadas E, Jain L, Gulley JL, Arlen PM, et al. A phase II clinical trial of sorafenib in androgen-independent prostate cancer. Clinical Cancer Research. 2008;14(1):209-214. doi: 10.1158/1078-0432.CCR-07-1355. pmid:18172272
Schwandt A, von Gruenigen VE, Wenham RM, Frasure H, Eaton S, Fusco N, et al. Randomized phase II trial of sorafenib alone or in combination with carboplatin/paclitaxel in women with recurrent platinum sensitive epithelial ovarian, peritoneal, or fallopian tube cancer. Investigational new drugs. 2014;32(4):729-738. doi: 10.1007/s10637-014-0078-5. pmid:24619298
Matei D, Sill MW, Lankes HA, DeGeest K, Bristow RE, Mutch D, et al. Activity of sorafenib in recurrent ovarian cancer and primary peritoneal carcinomatosis: a gynecologic oncology group trial. Journal of Clinical Oncology. 2011;29(1):69-75. doi: 10.1200/JCO.2009.26.7856. pmid:21098323
Bodnar L, Górnas M, Szczylik C. Sorafenib as a third line therapy in patients with epithelial ovarian cancer or primary peritoneal cancer: a phase II study. Gynecologic oncology. 2011;123(1):33-36. doi: 10.1016/j.ygyno.2011.06.019. pmid:21723597
Bianchi G, Loibl S, Zamagni C, Salvagni S, Raab G, Siena S, et al. Phase II multicenter, uncontrolled trial of sorafenib in patients with metastatic breast cancer. Anti-cancer drugs. 2009;20(7):616-624. pmid:19739318
Moreno-Aspitia A, Morton RF, Hillman DW, Lingle WL, Rowland KM, Wiesenfeld M, et al. Phase II trial of sorafenib in patients with metastatic breast cancer previously exposed to anthracyclines or taxanes: North Central Cancer Treatment Group and Mayo Clinic Trial N0336. Journal of Clinical Oncology. 2009;27(1):11-15. doi: 10.1200/JCO.2007.15.5242. pmid:19047293
Blumenschein GR, Gatzemeier U, Fossella F, Stewart DJ, Cupit L, Cihon F, et al. Phase II, multicenter, uncontrolled trial of single-agent sorafenib in patients with relapsed or refractory, advanced non-small-cell lung cancer. Journal of Clinical Oncology. 2009;27(26):4274-4280. doi: 10.1200/JCO.2009.22.0541. pmid:19652055
Wakelee HA, Lee JW, Hanna NH, Traynor AM, Carbone DP, Schiller JH. A double-blind randomized discontinuation phase II study of sorafenib (BAY 43-9006) in previously treated non-small cell lung cancer patients: Eastern Cooperative Oncology Group study E2501. Journal of thoracic oncology: official publication of the International Association for the Study of Lung Cancer. 2012;7(10):1574
Dy GK, Hillman SL, Rowland KM, Molina JR, Steen PD, Wender DB, et al. A front-line window of opportunity phase 2 study of sorafenib in patients with advanced nonsmall cell lung cancer. Cancer. 2010;116(24):5686-5693. doi: 10.1002/cncr.25448. pmid:21218460
Kelly RJ, Rajan A, Force J, Lopez-Chavez A, Keen C, Cao L, et al. Evaluation of KRAS Mutations, Angiogenic Biomarkers, and DCE-MRI in Patients with Advanced Non-Small-Cell Lung Cancer Receiving Sorafenib. Clinical Cancer Research. 2011;17(5):1190-1199. doi: 10.1158/1078-0432.CCR-10-2331. pmid:21224376
Kim ES, Herbst RS, Wistuba II, Lee JJ, Blumenschein GR, Tsao A, et al. The BATTLE trial: personalizing therapy for lung cancer. Cancer discovery. 2011;1(1):44-53. doi: 10.1158/2159-8274.CD-10-0010. pmid:22586319
Dingemans AMC, Mellema WW, Groen HJ, Van Wijk A, Burgers SA, Kunst PW, et al. A phase II study of sorafenib in patients with platinum-pretreated, advanced (stage IIIb or IV) non-small cell lung cancer with a KRAS mutation. Clinical Cancer Research. 2013;19(3):743-751. doi: 10.1158/1078-0432.CCR-12-1779. pmid:23224737
El-Khoueiry A, Ramanathan R, Yang D, Zhang W, Shibata S, Wright J, et al. A randomized phase II of gemcitabine and sorafenib versus sorafenib alone in patients with metastatic pancreatic cancer. Investigational new drugs. 2012;30(3):1175-1183. doi: 10.1007/s10637-011-9658-9. pmid:21424698
Kloos RT, Ringel MD, Knopp MV, Hall NC, King M, Stevens R, et al. Phase II trial of sorafenib in metastatic thyroid cancer. Journal of Clinical Oncology. 2009;27(10):1675-1684. doi: 10.1200/JCO.2008.18.2717. pmid:19255327
Savvides P, Nagaiah G, Lavertu P, Fu P, Wright JJ, Chapman R, et al. Phase II trial of sorafenib in patients with advanced anaplastic carcinoma of the thyroid. Thyroid. 2013;23(5):600-604. doi: 10.1089/thy.2012.0103. pmid:23113752
Gupta-Abramson V, Troxel AB, Nellore A, Puttaswamy K, Redlinger M, Ransone K, et al. Phase II trial of sorafenib in advanced thyroid cancer. Journal of Clinical Oncology. 2008;26(29):4714-4719. doi: 10.1200/JCO.2008.16.3279. pmid:18541894
Lam ET, Ringel MD, Kloos RT, Prior TW, Knopp MV, Liang J, et al. Phase II clinical trial of sorafenib in metastatic medullary thyroid cancer. Journal of Clinical Oncology. 2010;28(14):2323-2330. doi: 10.1200/JCO.2009.25.0068. pmid:20368568
Chen L, Shen Y, Luo Q, Yu Y, Lu H, Zhu R. Response to sorafenib at a low dose in patients with radioiodine-refractory pulmonary metastases from papillary thyroid carcinoma. Thyroid. 2011;21(2):119-124. doi: 10.1089/thy.2010.0199. pmid:21186953
Ahmed M, Barbachano Y, Riddell A, Hickey J, Newbold KL, Viros A, et al. Analysis of the efficacy and toxicity of sorafenib in thyroid cancer: a phase II study in a UK based population. European Journal of Endocrinology. 2011;165(2):315-322. doi: 10.1530/EJE-11-0129. pmid:21566072
Hoftijzer H, Heemstra KA, Morreau H, Stokkel MP, Corssmit EP, Gelderblom H, et al. Beneficial effects of sorafenib on tumor progression, but not on radioiodine uptake, in patients with differentiated thyroid carcinoma. European journal of endocrinology. 2009;161(6):923-931. doi: 10.1530/EJE-09-0702. pmid:19773371
Brose MS, Nutting CM, Jarzab B, Elisei R, Siena S, Bastholt L, et al. Sorafenib in radioactive iodine-refractory, locally advanced or metastatic differentiated thyroid cancer: a randomised, double-blind, phase 3 trial. The Lancet. 2014;384(9940):319-328
Dubey S, Jänne PA, Krug L, Pang H, Wang X, Heinze R, et al. A phase II study of sorafenib in malignant mesothelioma: results of CALGB 30307. Journal of thoracic oncology: official publication of the International Association for the Study of Lung Cancer. 2010;5(10): 1655-61
Papa S, Popat S, Shah R, Prevost AT, Lal R, McLennan B, et al. Phase 2 study of sorafenib in malignant mesothelioma previously treated with platinum-containing chemotherapy. Journal of Thoracic Oncology. 2013;8(6):783-787. doi: 10.1097/JTO.0b013e31828c2b26. pmid:23571475
Nabors L, Supko J, Rosenfeld M, Chamberlain M, Phuphanich S, Batchelor T, et al. Phase I trial of sorafenib in patients with recurrent or progressive malignant glioma. Neuro-oncology. 2011;13(12):1324-30. doi: 10.1093/neuonc/nor145. pmid:21954442
Nimeiri HS, Oza AM, Morgan RJ, Huo D, Elit L, Knost JA, et al. A phase II study of sorafenib in advanced uterine carcinoma/carcinosarcoma: a trial of the Chicago, PMH, and California Phase II Consortia. Gynecologic oncology. 2010;117(1):37-40. doi: 10.1016/j.ygyno.2010.01.013. pmid:20117828
Gitlitz BJ, Moon J, Glisson BS, Reimers HJ, Bury MJ, Floyd JD, et al. Sorafenib in Patients with Platinum Treated Extensive Stage Small Cell Lung Cancer (SCLC): A Southwest Oncology Group (SWOG 0435) Phase II Trial. Journal of thoracic oncology: official publication of the International Association for the Study of Lung Cancer. 2010;5(11):1835
Sridhar SS, Winquist E, Eisen A, Hotte SJ, McWhirter E, Tannock IF, et al. A phase II trial of sorafenib in first-line metastatic urothelial cancer: a study of the PMH Phase II Consortium. Investigational new drugs. 2011;29(5):1045-1049. doi: 10.1007/s10637-010-9408-4. pmid:20191303
Dreicer R, Li H, Stein M, DiPaola R, Eleff M, Roth BJ, et al. Phase 2 trial of sorafenib in patients with advanced urothelial cancer. Cancer. 2009;115(18):4090-4095. doi: 10.1002/cncr.24467. pmid:19536901
Maki RG, D'Adamo DR, Keohan ML, Saulle M, Schuetze SM, Undevia SD, et al. Phase II study of sorafenib in patients with metastatic or recurrent sarcomas. Journal of Clinical Oncology. 2009;27(19):3133-3140. doi: 10.1200/JCO.2008.20.4495. pmid:19451436
von Mehren M, Rankin C, Goldblum JR, Demetri GD, Bramwell V, Ryan CW, et al. Phase 2 Southwest Oncology Group-directed intergroup trial (S0505) of sorafenib in advanced soft tissue sarcomas. Cancer. 2012;118(3):770-776. doi: 10.1002/cncr.26334. pmid:21751200
Santoro A, Comandone A, Basso U, Parra HS, De Sanctis R, Stroppa E, et al. Phase II prospective study with sorafenib in advanced soft tissue sarcomas after anthracycline-based therapy. Annals of oncology. 2013;24(4):1093-1098. pmid:23230134
Grignani G, Palmerini E, Dileo P, Asaftei S, D'Ambrosio L, Pignochino Y, et al. A phase II trial of sorafenib in relapsed and unresectable high-grade osteosarcoma after failure of standard multimodal therapy: an Italian Sarcoma Group study. Annals of Oncology. 2011;23(2):508-16. doi: 10.1093/annonc/mdr151. pmid:21527590
Ray-Coquard I, Italiano A, Bompas E, Le Cesne A, Robin YM, Chevreau C, et al. Sorafenib for patients with advanced angiosarcoma: a phase II Trial from the French Sarcoma Group (GSF/GETO). The oncologist. 2012;17(2):260-266. doi: 10.1634/theoncologist.2011-0237. pmid:22285963
El-Khoueiry AB, Rankin CJ, Ben-Josef E, Lenz HJ, Gold PJ, Hamilton RD, et al. SWOG 0514: a phase II study of sorafenib in patients with unresectable or metastatic gallbladder carcinoma and cholangiocarcinoma. Investigational new drugs. 2012;30(4):1646-1651. doi: 10.1007/s10637-011-9719-0. pmid:21748296
Bengala C, Bertolini F, Malavasi N, Boni C, Aitini E, Dealis C, et al. Sorafenib in patients with advanced biliary tract carcinoma: a phase II trial. British journal of cancer. 2010;102(1):68-72. doi: 10.1038/sj.bjc.6605458. pmid:19935794
Greenwald DR, Li H, Luger SM, Go RS, King D, Patel T, et al. A phase II study of sorafenib (BAY 43-9006) in recurrent diffuse large B cell lymphoma: an eastern cooperative oncology group study (E1404). J Hematol Oncol. 2013;6:46. doi: 10.1186/1756-8722-6-46. pmid:23829878
Guidetti A, Carlo-Stella C, Locatelli SL, Malorni W, Pierdominici M, Barbati C, et al. Phase II study of sorafenib in patients with relapsed or refractory lymphoma. British journal of haematology. 2012;158(1):108-119. doi: 10.1111/j.1365-2141.2012.09139.x. pmid:22571717
Yordanova A, Hose D, Neben K, Witzens-Harig M, Gütgemann I, Raab MS, et al. Sorafenib in patients with refractory or recurrent multiple myeloma. Hematological oncology. 2013;31(4):197-200. doi: 10.1002/hon.2043. pmid:23494836
Chevreau C, Le Cesne A, Ray-Coquard I, Italiano A, Cioffi A, Isambert N, et al. Sorafenib in patients with progressive epithelioid hemangioendothelioma. Cancer. 2013;119(14):2639-2644. doi: 10.1002/cncr.28109. pmid:23589078
Park S, Ryu M, Ryoo B, Im S, Kwon H, Lee S, et al. Sorafenib in patients with metastatic gastrointestinal stromal tumors who failed two or more prior tyrosine kinase inhibitors: a phase II study of Korean gastrointestinal stromal tumors study group. Investigational new drugs. 2012;30(6):2377-2383. doi: 10.1007/s10637-012-9795-9. pmid:22270258
Flaherty KT, Schiller J, Schuchter LM, Liu G, Tuveson DA, Redlinger M, et al. A phase I trial of the oral, multikinase inhibitor sorafenib in combination with carboplatin and paclitaxel. Clinical Cancer Research. 2008;14(15):4836-4842. doi: 10.1158/1078-0432.CCR-07-4123. pmid:18676756
Siu LL, Awada A, Takimoto CH, Piccart M, Schwartz B, Giannaris T, et al. Phase I trial of sorafenib and gemcitabine in advanced solid tumors with an expanded cohort in advanced pancreatic cancer. Clinical cancer research. 2006;12(1):144-151. doi: 10.1158/1078-0432.CCR-05-1571. pmid:16397036
Mross K, Steinbild S, Baas F, Gmehling D, Radtke M, Voliotis D, et al. Results from an in vitro and a clinical/pharmacological phase I study with the combination irinotecan and sorafenib. European Journal of Cancer. 2007;43(1):55-63. doi: 10.1016/j.ejca.2006.08.032. pmid:17095207
Awada A, Gil T, Whenham N, Hamme J, Besse-Hammer T, Brendel E, et al. Safety and pharmacokinetics of sorafenib combined with capecitabine in patients with advanced solid tumors: results of a phase 1 trial. The Journal of Clinical Pharmacology. 2011;51(12):1674-1684. doi: 10.1177/0091270010386226. pmid:21209247
Escudier B, Lassau N, Angevin E, Soria JC, Chami L, Lamuraglia M, et al. Phase I trial of sorafenib in combination with IFN [alpha] -2a in patients with unresectable and/or metastatic renal cell carcinoma or malignant melanoma. Clinical Cancer Research. 2007;13(6):1801-1809. doi: 10.1158/1078-0432.CCR-06-1432. pmid:17363536
Azad NS, Posadas EM, Kwitkowski VE, Steinberg SM, Jain L, Annunziata CM, et al. Combination targeted therapy with sorafenib and bevacizumab results in enhanced toxicity and antitumor activity. Journal of Clinical Oncology. 2008;26(22):3709-3714. doi: 10.1200/JCO.2007.10.8332. pmid:18669456
Vaishampayan UN, Burger AM, Sausville EA, Heilbrun LK, Li J, Horiba MN, et al. Safety, efficacy, pharmacokinetics, and pharmacodynamics of the combination of sorafenib and tanespimycin. Clinical Cancer Research. 2010;16(14):3795-3804. doi: 10.1158/1078-0432.CCR-10-0503. pmid:20525756
Brendel E, Ludwig M, Lathia C, Robert C, Ropert S, Soria JC, et al. Pharmacokinetic results of a phase I trial of sorafenib in combination with dacarbazine in patients with advanced solid tumors. Cancer chemotherapy and pharmacology. 2011;68(1):53-61. doi: 10.1007/s00280-010-1423-9. pmid:20821331
Duran I, Hotté SJ, Hirte H, Chen EX, MacLean M, Turner S, et al. Phase I targeted combination trial of sorafenib and erlotinib in patients with advanced solid tumors. Clinical Cancer Research. 2007;13(16):4849-4857. doi: 10.1158/1078-0432.CCR-07-0382. pmid:17699864
Kupsch P, Henning BF, Passarge K, Richly H, Wiesemann K, Hilger RA, et al. Results of a phase I trial of sorafenib (BAY 43-9006) in combination with oxaliplatin in patients with refractory solid tumors, including colorectal cancer. Clinical colorectal cancer. 2005;5(3):188-196. pmid:16197622
Hong DS, Sebti SM, Newman RA, Blaskovich MA, Ye L, Gagel RF, et al. Phase I trial of a combination of the multikinase inhibitor sorafenib and the farnesyltransferase inhibitor tipifarnib in advanced malignancies. Clinical Cancer Research. 2009;15(22):7061-7068. doi: 10.1158/1078-0432.CCR-09-1241. pmid:19903778
Kumar SK, Jett J, Marks R, Richardson R, Quevedo F, Moynihan T, et al. Phase 1 study of sorafenib in combination with bortezomib in patients with advanced malignancies. Investigational new drugs. 2013;31(5):1201-1206. doi: 10.1007/s10637-013-0004-2. pmid:23887852
Richly H, Henning B, Kupsch P, Passarge K, Grubert M, Hilger R, et al. Results of a Phase I trial of sorafenib (BAY 43-9006) in combination with doxorubicin in patients with refractory solid tumors. Annals of Oncology. 2006;17(5):866-873. doi: 10.1093/annonc/mdl017. pmid:16500908
Schultheis B, Kummer G, Zeth M, Brendel E, Xia C, Kornacker M, et al. Phase IB study of sorafenib in combination with gemcitabine and cisplatin in patients with refractory solid tumors. Cancer chemotherapy and pharmacology. 2012;69(2):333-339. doi: 10.1007/s00280-011-1685-x. pmid:21735354
Rosen LS, Puzanov I, Friberg G, Chan E, Hwang YC, Deng H, et al. Safety and pharmacokinetics of ganitumab (AMG 479) combined with sorafenib, panitumumab, erlotinib, or gemcitabine in patients with advanced solid tumors. Clinical Cancer Research. 2012;18(12):3414-3427. doi: 10.1158/1078-0432.CCR-11-3369. pmid:22510349
Monk P, Lam E, Mortazavi A, Kendra K, Lesinski GB, Mace TA, et al. A phase I study of high-dose interleukin-2 with sorafenib in patients with metastatic renal cell carcinoma and melanoma. Journal of immunotherapy (Hagerstown, Md: 1997). 2014;37(3):180
Desar I, Timmer-Bonte J, Burger D, van der Graaf W, van Herpen C. A phase I dose-escalation study to evaluate safety and tolerability of sorafenib combined with sirolimus in patients with advanced solid cancer. British journal of cancer. 2010;103(11):1637-1643. doi: 10.1038/sj.bjc.6605777. pmid:21045832
Davies JM, Dhruva NS, Walko CM, Socinski MA, Bernard S, Hayes DN, et al. A phase I trial of sorafenib combined with cisplatin/etoposide or carboplatin/pemetrexed in refractory solid tumor patients. Lung Cancer. 2011;71(2):151-155. doi: 10.1016/j.lungcan.2010.05.022. pmid:20580118
Infante JR, Jones SF, Bendell JC, Greco FA, Yardley DA, Lane CM, et al. A drug interaction study evaluating the pharmacokinetics and toxicity of sorafenib in combination with capecitabine. Cancer chemotherapy and pharmacology. 2012;69(1):137-144. doi: 10.1007/s00280-011-1674-0. pmid:21626051
LoConte NK, Holen KD, Schelman WR, Mulkerin DL, Deming DA, Hernan HR, et al. A phase I study of sorafenib, oxaliplatin and 2 days of high dose capecitabine in advanced pancreatic and biliary tract cancer: a Wisconsin oncology network study. Investigational new drugs. 2013;31(4):943-948. doi: 10.1007/s10637-012-9916-5. pmid:23263993
Dasari A, Gore L, Messersmith W, Diab S, Jimeno A, Weekes C, et al. A phase I study of sorafenib and vorinostat in patients with advanced solid tumors with expanded cohorts in renal cell carcinoma and non-small cell lung cancer. Investigational new drugs. 2013;31(1):115-125. doi: 10.1007/s10637-012-9812-z. pmid:22415798
Simonelli M, Zucali PA, Lorenzi E, Rubino L, De Vincenzo F, De Sanctis R, et al. Phase I pharmacokinetic and pharmacodynamic study of lapatinib in combination with sorafenib in patients with advanced refractory solid tumors. European Journal of Cancer. 2013;49(5):989-998. doi: 10.1016/j.ejca.2012.10.016. pmid:23146956
Ganesan P, Piha-Paul S, Naing A, Falchook G, Wheler J, Fu S, et al. Phase I clinical trial of lenalidomide in combination with sorafenib in patients with advanced cancer. Investigational new drugs. 2014;32(2):279-286. doi: 10.1007/s10637-013-9966-3. pmid:23756764
Gangadhar TC, Cohen EE, Wu K, Janisch L, Geary D, Kocherginsky M, et al. Two drug interaction studies of sirolimus in combination with sorafenib or sunitinib in patients with advanced malignancies. Clinical Cancer Research. 2011;17(7):1956-1963. doi: 10.1158/1078-0432.CCR-10-2061. pmid:21447721
Awada A, Hendlisz A, Christensen O, Lathia CD, Bartholomeus S, Lebrun F, et al. Phase I trial to investigate the safety, pharmacokinetics and efficacy of sorafenib combined with docetaxel in patients with advanced refractory solid tumours. European journal of cancer. 2012;48(4):465-474. doi: 10.1016/j.ejca.2011.12.026. pmid:22285181
Shacham-Shmueli E, Geva R, Figer A, Bulocinic S, Nalbandyan K, Shpigel S, et al. Phase I Trial of Sorafenib in Combination With 5-Fluorouracil/Leucovorin in Advanced Solid Tumors. The Journal of Clinical Pharmacology. 2012;52(5):656-669. doi: 10.1177/0091270011404027. pmid:22232731
Navid F, Baker SD, McCarville MB, Stewart CF, Billups CA, Wu J, et al. Phase I and clinical pharmacology study of bevacizumab, sorafenib, and low-dose cyclophosphamide in children and young adults with refractory/recurrent solid tumors. Clinical Cancer Research. 2013;19(1):236-246. doi: 10.1158/1078-0432.CCR-12-1897. pmid:23143218
Serve H, Krug U, Wagner R, Sauerland MC, Heinecke A, Brunnberg U, et al. Sorafenib in combination with intensive chemotherapy in elderly patients with acute myeloid leukemia: results from a randomized, placebo-controlled trial. Journal of Clinical Oncology. 2013;31(25):3110-3118. doi: 10.1200/JCO.2012.46.4990. pmid:23897964
Macdonald DA, Assouline SE, Brandwein J, Kamel-Reid S, Eisenhauer EA, Couban S, et al. A phase I/II study of sorafenib in combination with low dose cytarabine in elderly patients with acute myeloid leukemia or high-risk myelodysplastic syndrome from the National Cancer Institute of Canada Clinical Trials Group: trial IND. 186. Leukemia & lymphoma. 2013;54(4):760-766
Ravandi F, Cortes JE, Jones D, Faderl S, Garcia-Manero G, Konopleva MY, et al. Phase I/II study of combination therapy with sorafenib, idarubicin, and cytarabine in younger patients with acute myeloid leukemia. Journal of Clinical Oncology. 2010;28(11):1856-1862. doi: 10.1200/JCO.2009.25.4888. pmid:20212254
Inaba H, Rubnitz JE, Coustan-Smith E, Li L, Furmanski BD, Mascara GP, et al. Phase I pharmacokinetic and pharmacodynamic study of the multikinase inhibitor sorafenib in combination with clofarabine and cytarabine in pediatric relapsed/refractory leukemia. Journal of Clinical Oncology. 2011;29(24):3293-3300. doi: 10.1200/JCO.2011.34.7427. pmid:21768474
Ravandi F, Alattar ML, Grunwald MR, Rudek MA, Rajkhowa T, Richie MA, et al. Phase 2 study of azacytidine plus sorafenib in patients with acute myeloid leukemia and FLT-3 internal tandem duplication mutation. Blood. 2013;121(23):4655-4662. doi: 10.1182/blood-2013-01-480228. pmid:23613521
Abou-Alfa GK, Johnson P, Knox JJ, Capanu M, Davidenko I, Lacava J, et al. Doxorubicin plus sorafenib vs doxorubicin alone in patients with advanced hepatocellular carcinoma: a randomized trial. Jama. 2010;304(19):2154-2160. doi: 10.1001/jama.2010.1672. pmid:21081728
Petrini I, Lencioni M, Ricasoli M, Iannopollo M, Orlandini C, Oliveri F, et al. Phase II trial of sorafenib in combination with 5-fluorouracil infusion in advanced hepatocellular carcinoma. Cancer chemotherapy and pharmacology. 2012;69(3):773-780. doi: 10.1007/s00280-011-1753-2. pmid:22033636
Cabrera R, Pannu D, Caridi J, Firpi R, Soldevila-Pico C, Morelli G, et al. The combination of sorafenib with transarterial chemoembolisation for hepatocellular carcinoma. Alimentary pharmacology & therapeutics. 2011;34(2):205-213
Hsu CH, Shen YC, Lin ZZ, Chen PJ, Shao YY, Ding YH, et al. Phase II study of combining sorafenib with metronomic tegafur/uracil for advanced hepatocellular carcinoma. Journal of hepatology. 2010;53(1):126-131. doi: 10.1016/j.jhep.2010.01.035. pmid:20416968
Dufour JF, Hoppe H, Heim MH, Helbling B, Maurhofer O, Szucs-Farkas Z, et al. Continuous administration of sorafenib in combination with transarterial chemoembolization in patients with hepatocellular carcinoma: results of a phase I study. The oncologist. 2010;15(11):1198-1204. doi: 10.1634/theoncologist.2010-0180. pmid:21036880
Del Prete S, Montella L, Caraglia M, Maiorino L, Cennamo G, Montesarchio V, et al. Sorafenib plus octreotide is an effective and safe treatment in advanced hepatocellular carcinoma: multicenter phase II So. LAR. study. Cancer chemotherapy and pharmacology. 2010;66(5):837-844. doi: 10.1007/s00280-009-1226-z. pmid:20041325
Srimuninnimit V, Sriuranpong V, Suwanvecho S. Efficacy and safety of sorafenib in combination with gemcitabine in patients with advanced hepatocellular carcinoma: A multicenter, open-label, single-arm phase II study. Asia-Pacific Journal of Clinical Oncology. 2014;10(3):255-260. doi: 10.1111/ajco.12191. pmid:24810940
Chow P, Poon D, Khin MW, Singh H, Han HS, Goh A, et al. Multicenter phase II study of sequential radioembolization-sorafenib therapy for inoperable hepatocellular carcinoma. PLoS ONE. 2014;9(3):e90909. doi: 10.1371/journal.pone.0090909. pmid:24614178
Yang Y, Lu Y, Wang C, Bai W, Qu J, Chen Y, et al. Cryotherapy is associated with improved clinical outcomes of sorafenib therapy for advanced hepatocellular carcinoma. Cell biochemistry and biophysics. 2012;63(2):159-169. doi: 10.1007/s12013-012-9353-2. pmid:22477032
Naqi N, Ahmad S, Murad S, Khattak J. Efficacy and safety of sorafenib--gemcitabine combination therapy in advanced hepatocellular carcinoma: An open-label Phase II feasibility study. Hematology/oncology and stem cell therapy. 2014;7(1):27-31. doi: 10.1016/j.hemonc.2013.11.003. pmid:24333135
Sieghart W, Pinter M, Reisegger M, Müller C, Ba-Ssalamah A, Lammer J, et al. Conventional transarterial chemoembolisation in combination with sorafenib for patients with hepatocellular carcinoma: a pilot study. European radiology. 2012;22(6):1214-1223. doi: 10.1007/s00330-011-2368-z. pmid:22215073
Finn RS, Poon RT, Yau T, Klümpen HJ, Chen LT, Kang YK, et al. Phase I study investigating everolimus combined with sorafenib in patients with advanced hepatocellular carcinoma. Journal of hepatology. 2013;59(6):1271-1277. doi: 10.1016/j.jhep.2013.07.029. pmid:23928403
Hagihara A, Ikeda M, Ueno H, Morizane C, Kondo S, Nakachi K, et al. Phase I study of combination chemotherapy using sorafenib and transcatheter arterial infusion with cisplatin for advanced hepatocellular carcinoma. Cancer science. 2014;105(3):354-358. doi: 10.1111/cas.12353. pmid:24438504
Pawlik TM, Reyes DK, Cosgrove D, Kamel IR, Bhagat N, Geschwind JFH. Phase II trial of sorafenib combined with concurrent transarterial chemoembolization with drug-eluting beads for hepatocellular carcinoma. Journal of Clinical Oncology. 2011;29(30):3960-3967. doi: 10.1200/JCO.2011.37.1021. pmid:21911714
Abou-Alfa GK, Chan SL, Lin CC, Chiorean EG, Holcombe RF, Mulcahy MF, et al. PR-104 plus sorafenib in patients with advanced hepatocellular carcinoma. Cancer chemotherapy and pharmacology. 2011;68(2):539-545. doi: 10.1007/s00280-011-1671-3. pmid:21594722
Park JW, Koh YH, Kim HB, Kim HY, An S, Choi JI, et al. Phase II study of concurrent transarterial chemoembolization and sorafenib in patients with unresectable hepatocellular carcinoma. Journal of hepatology. 2012;56(6):1336-1342. doi: 10.1016/j.jhep.2012.01.006. pmid:22314421
Lee SJ, Lee J, Park SH, Park JO, Park YS, Kang WK, et al. Phase 1 trial of S-1 in combination with sorafenib for patients with advanced hepatocellular carcinoma. Investigational new drugs. 2012;30(4):1540-1547. doi: 10.1007/s10637-011-9706-5. pmid:21695438
Ooka Y, Chiba T, Ogasawara S, Arai K, Suzuki E, Tawada A, et al. A phase I/II study of S-1 with sorafenib in patients with advanced hepatocellular carcinoma. Investigational new drugs. 2014;32(4):723-728. doi: 10.1007/s10637-014-0077-6. pmid:24599799
Kelley R, Nimeiri H, Munster P, Vergo M, Huang Y, Li CM, et al. Temsirolimus combined with sorafenib in hepatocellular carcinoma: a phase I dose-finding trial with pharmacokinetic and biomarker correlates. Annals of oncology. 2013;24(7):1900-1907. doi: 10.1093/annonc/mdt109. pmid:23519998
Chen SW, Lin LC, Kuo YC, Liang JA, Kuo CC, Chiou JF. Phase 2 study of combined sorafenib and radiation therapy in patients with advanced hepatocellular carcinoma. Int J Radiat Oncol Biol Phys. 2014;88(5):1041-1047. doi: 10.1016/j.ijrobp.2014.01.017. pmid:24661657
Ryan CW, Goldman BH, Lara PN, Mack PC, Beer TM, Tangen CM, et al. Sorafenib with interferon alfa-2b as first-line treatment of advanced renal carcinoma: a phase II study of the Southwest Oncology Group. Journal of clinical oncology. 2007;25(22):3296-3301. doi: 10.1200/JCO.2007.11.1047. pmid:17664477
Gollob JA, Rathmell WK, Richmond TM, Marino CB, Miller EK, Grigson G, et al. Phase II trial of sorafenib plus interferon alfa-2b as first-or second-line therapy in patients with metastatic renal cell cancer. Journal of Clinical Oncology. 2007;25(22):3288-3295. doi: 10.1200/JCO.2007.10.8613. pmid:17664476
Tagawa ST, Milowsky MI, Jeske S, Mazumdar M, Kung S, Sung M, et al. A phase I trial of sorafenib plus gemcitabine and capecitabine for patients with advanced renal cell carcinoma: New York Cancer Consortium Trial NCI 6981. American journal of clinical oncology. 2011;34(5):443-448. doi: 10.1097/COC.0b013e3181e9c0d7. pmid:20881475
Bracarda S, Porta C, Boni C, Santoro A, Mucciarini C, Pazzola A, et al. Could interferon still play a role in metastatic renal cell carcinoma? A randomized study of two schedules of sorafenib plus interferon-alpha 2a (RAPSODY). European urology. 2013;63(2):254-261. doi: 10.1016/j.eururo.2012.08.027. pmid:22964169
Maroto J, Del Muro X, Mellado B, Perez-Gracia J, Andrés R, Cruz J, et al. Phase II trial of sequential subcutaneous interleukin-2 plus interferon alpha followed by sorafenib in renal cell carcinoma (RCC). Clinical and Translational Oncology. 2013;15(9):698-704. doi: 10.1007/s12094-012-0991-z. pmid:23359179
Hong DS, Gordon MS, Samlowski WE, Kurzrock R, Tannir N, Friedland D, et al. A phase I, open-label study of trebananib combined with sorafenib or sunitinib in patients with advanced renal cell carcinoma. Clinical genitourinary cancer. 2014;12(3):167-177. doi: 10.1016/j.clgc.2013.11.007. pmid:24365125
Procopio G, Verzoni E, Bracarda S, Ricci S, Sacco C, Ridolfi L, et al. Sorafenib with interleukin-2 vs sorafenib alone in metastatic renal cell carcinoma: the ROSORC trial. British journal of cancer. 2011;104(8):1256-1261. doi: 10.1038/bjc.2011.103. pmid:21448165
Bellmunt J, Trigo JM, Calvo E, Carles J, Pérez-Gracia JL, Rubió J, et al. Activity of a multitargeted chemo-switch regimen (sorafenib, gemcitabine, and metronomic capecitabine) in metastatic renal-cell carcinoma: a phase 2 study (SOGUG-02-06). The lancet oncology. 2010;11(4):350-357. doi: 10.1016/S1470-2045(09)70383-3. pmid:20163987
Amato RJ, Flaherty AL, Stepankiw M. Phase I trial of everolimus plus sorafenib for patients with advanced renal cell cancer. Clinical genitourinary cancer. 2012;10(1):26-31. doi: 10.1016/j.clgc.2011.11.002. pmid:22169794
Hainsworth JD, Waterhouse DM, Penley WC, Shipley DL, Thompson DS, Webb CD, et al. Sorafenib and everolimus in advanced clear cell renal carcinoma: a phase I/II trial of the SCRI oncology research consortium. Cancer investigation. 2013;31(5):323-329. doi: 10.3109/07357907.2013.789900. pmid:23614653
Rini B, Szczylik C, Tannir NM, Koralewski P, Tomczak P, Deptala A, et al. AMG 386 in combination with sorafenib in patients with metastatic clear cell carcinoma of the kidney. Cancer. 2012;118(24):6152-6161. doi: 10.1002/cncr.27632. pmid:22692704
Larkin JM, Ferguson T, Pickering L, Edmonds K, James M, Thomas K, et al. A phase I/II trial of sorafenib and infliximab in advanced renal cell carcinoma. British journal of cancer. 2010;103(8):1149-1153. doi: 10.1038/sj.bjc.6605889. pmid:20842130
Niwakawa M, Hashine K, Yamaguchi R, Fujii H, Hamamoto Y, Fukino K, et al. Phase I trial of sorafenib in combination with interferon-alpha in Japanese patients with unresectable or metastatic renal cell carcinoma. Investigational new drugs. 2012;30(3):1046-1054. doi: 10.1007/s10637-010-9630-0. pmid:21246251
Harzstark AL, Small EJ, Weinberg VK, Sun J, Ryan CJ, Lin AM, et al. A phase 1 study of everolimus and sorafenib for metastatic clear cell renal cell carcinoma. Cancer. 2011;117(18):4194-4200. doi: 10.1002/cncr.25931. pmid:21387258
Eisen T, Marais R, Affolter A, Lorigan P, Robert C, Corrie P, et al. Sorafenib and dacarbazine as first-line therapy for advanced melanoma: phase I and open-label phase II studies. British journal of cancer. 2011;105(3):353-359. doi: 10.1038/bjc.2011.257. pmid:21750549
McDermott DF, Sosman JA, Gonzalez R, Hodi FS, Linette GP, Richards J, et al. Double-blind randomized phase II study of the combination of sorafenib and dacarbazine in patients with advanced melanoma: a report from the 11715 Study Group. Journal of Clinical Oncology. 2008;26(13):2178-2185. doi: 10.1200/JCO.2007.14.8288. pmid:18445842
Hauschild A, Agarwala SS, Trefzer U, Hogg D, Robert C, Hersey P, et al. Results of a phase III, randomized, placebo-controlled study of sorafenib in combination with carboplatin and paclitaxel as second-line treatment in patients with unresectable stage III or stage IV melanoma. Journal of Clinical Oncology. 2009;27(17):2823-2830. doi: 10.1200/JCO.2007.15.7636. pmid:19349552
Amaravadi RK, Schuchter LM, McDermott DF, Kramer A, Giles L, Gramlich K, et al. Phase II trial of temozolomide and sorafenib in advanced melanoma patients with or without brain metastases. Clinical Cancer Research. 2009;15(24):7711-7718. doi: 10.1158/1078-0432.CCR-09-2074. pmid:19996224
Flaherty KT, Lee SJ, Zhao F, Schuchter LM, Flaherty L, Kefford R, et al. Phase III trial of carboplatin and paclitaxel with or without sorafenib in metastatic melanoma. Journal of Clinical Oncology. 2013;31(3):373-379. doi: 10.1200/JCO.2012.42.1529. pmid:23248256
Bhatia S, Moon J, Margolin KA, Weber JS, Lao CD, Othus M, et al. Phase II Trial of Sorafenib in Combination with Carboplatin and Paclitaxel in Patients with Metastatic Uveal Melanoma: SWOG S0512. PLoS ONE. 2012;7(11):e48787. doi: 10.1371/journal.pone.0048787. pmid:23226204
Mahalingam D, Malik L, Beeram M, Rodon J, Sankhala K, Mita A, et al. Phase II study evaluating the efficacy, safety, and pharmacodynamic correlative study of dual antiangiogenic inhibition using bevacizumab in combination with sorafenib in patients with advanced malignant melanoma. Cancer chemotherapy and pharmacology. 2014;74(1):77-84. doi: 10.1007/s00280-014-2479-8. pmid:24817603
Beasley G, Coleman A, Raymond A, Sanders G, Selim M, Peterson B, et al. A phase I multi-institutional study of systemic sorafenib in conjunction with regional melphalan for in-transit melanoma of the extremity. Annals of surgical oncology. 2012;19(12):3896-3905. doi: 10.1245/s10434-012-2373-8. pmid:22549288
Egberts F, Gutzmer R, Ugurel S, Becker J, Trefzer U, Degen A, et al. Sorafenib and pegylated interferon-[alpha] 2b in advanced metastatic melanoma: a multicenter phase II DeCOG trial. Annals of oncology. 2011;22(7):1667-1674. doi: 10.1093/annonc/mdq648. pmid:21220519
Margolin KA, Moon J, Flaherty LE, Lao CD, Akerley WL, Othus M, et al. Randomized phase II trial of sorafenib with temsirolimus or tipifarnib in untreated metastatic melanoma (S0438). Clinical Cancer Research. 2012;18(4):1129-1137. doi: 10.1158/1078-0432.CCR-11-2488. pmid:22228638
Davies MA, Fox PS, Papadopoulos NE, Bedikian AY, Hwu WJ, Lazar AJ, et al. Phase I study of the combination of sorafenib and temsirolimus in patients with metastatic melanoma. Clinical Cancer Research. 2012;18(4):1120-1128. doi: 10.1158/1078-0432.CCR-11-2436. pmid:22223528
Xue C, Huang Y, Huang P, Yu Q, Pan J, Liu L, et al. Phase II study of sorafenib in combination with cisplatin and 5-fluorouracil to treat recurrent or metastatic nasopharyngeal carcinoma. Annals of oncology. 2013;24(4):1055-1061. doi: 10.1093/annonc/mds581. pmid:23172635
Mardjuadi F, Medioni J, Kerger J, D'Hondt L, Canon JL, Duck L, et al. Phase I study of sorafenib in combination with docetaxel and prednisone in chemo-naïve patients with metastatic castration-resistant prostate cancer. Cancer chemotherapy and pharmacology. 2012;70(2):293-303. doi: 10.1007/s00280-012-1914-y. pmid:22752248
Nabhan C, Villines D, Valdez T, Tolzien K, Lestingi T, Bitran J, et al. Phase I study investigating the safety and feasibility of combining imatinib mesylate (Gleevec) with sorafenib in patients with refractory castration-resistant prostate cancer. British journal of cancer. 2012;107(4):592-597. doi: 10.1038/bjc.2012.312. pmid:22805325
Beardsley EK, Hotte SJ, North S, Ellard SL, Winquist E, Kollmannsberger C, et al. A phase II study of sorafenib in combination with bicalutamide in patients with chemotherapy-naive castration resistant prostate cancer. Investigational new drugs. 2012;30(4):1652-1659. doi: 10.1007/s10637-011-9722-5. pmid:21785998
Welch SA, Hirte HW, Elit L, Schilder RJ, Wang L, MacAlpine K, et al. Sorafenib in combination with gemcitabine in recurrent epithelial ovarian cancer: a study of the Princess Margaret Hospital Phase II Consortium. International Journal of Gynecological Cancer. 2010;20(5):787-793. doi: 10.1111/IGC.0b013e3181e273a8. pmid:20847613
Pölcher M, Eckhardt M, Coch C, Wolfgarten M, Kübler K, Hartmann G, et al. Sorafenib in combination with carboplatin and paclitaxel as neoadjuvant chemotherapy in patients with advanced ovarian cancer. Cancer chemotherapy and pharmacology. 2010;66(1):203-207. doi: 10.1007/s00280-010-1276-2. pmid:20204367
Ramasubbaiah R, Perkins S, Schilder J, Whalen C, Johnson C, Callahan M, et al. Sorafenib in combination with weekly topotecan in recurrent ovarian cancer, a phase I/II study of the Hoosier Oncology Group. Gynecologic oncology. 2011;123(3):499-504. doi: 10.1016/j.ygyno.2011.08.033. pmid:21955480
Isaacs C, Herbolsheimer P, Liu MC, Wilkinson M, Ottaviano Y, Chung GG, et al. Phase I/II study of sorafenib with anastrozole in patients with hormone receptor positive aromatase inhibitor resistant metastatic breast cancer. Breast cancer research and treatment. 2011;125(1):137-143. doi: 10.1007/s10549-010-1226-z. pmid:20976541
Gradishar WJ, Kaklamani V, Sahoo TP, Lokanatha D, Raina V, Bondarde S, et al. A double-blind, randomised, placebo-controlled, phase 2b study evaluating sorafenib in combination with paclitaxel as a first-line therapy in patients with HER2-negative advanced breast cancer. European Journal of Cancer. 2013;49(2):312-322. doi: 10.1016/j.ejca.2012.08.005. pmid:22954665
Schwartzberg LS, Tauer KW, Hermann RC, Makari-Judson G, Isaacs C, Beck JT, et al. Sorafenib or Placebo with Either Gemcitabine or Capecitabine in Patients with HER-2-Negative Advanced Breast Cancer That Progressed during or after Bevacizumab. Clinical Cancer Research. 2013;19(10):2745-2754. doi: 10.1158/1078-0432.CCR-12-3177. pmid:23444220
Baselga J, Segalla JGM, Roché H, del Giglio A, Pinczowski H, Ciruelos EM, et al. Sorafenib in combination with capecitabine: an oral regimen for patients with HER2-negative locally advanced or metastatic breast cancer. Journal of clinical oncology. 2012;30(13):1484-1491. doi: 10.1200/JCO.2011.36.7771. pmid:22412143
Mina LA, Yu M, Johnson C, Burkhardt C, Miller KD, Zon R. A phase II study of combined VEGF inhibitor (bevacizumab+ sorafenib) in patients with metastatic breast cancer: Hoosier Oncology Group Study BRE06-109. Investigational new drugs. 2013;31(5):1307-1310. doi: 10.1007/s10637-013-9976-1. pmid:23812905
Loibl S, Rokitta D, Conrad B, Harbeck N, Wüllner M, Warm M, et al. Sorafenib in the Treatment of Early Breast Cancer: Results of the Neoadjuvant Phase II Study-SOFIA*. Breast Care. 2014;9(3):2-2
Luu T, Frankel P, Chung C, Chow W, Mortimer J, Hurria A, et al. Phase I/II trial of vinorelbine and sorafenib in metastatic breast cancer. Clinical breast cancer. 2014;14(2):94-100. doi: 10.1016/j.clbc.2013.10.013. pmid:24370210
Adjei AA, Molina JR, Mandrekar SJ, Marks R, Reid JR, Croghan G, et al. Phase I Trial of Sorafenib in Combination with Gefitinib in Patients with Refractory or Recurrent Non-Small Cell Lung Cancer. Clinical Cancer Research. 2007;13(9):2684-2691. doi: 10.1158/1078-0432.CCR-06-2889. pmid:17473200
Scagliotti G, Novello S, von Pawel J, Reck M, Pereira JR, Thomas M, et al. Phase III study of carboplatin and paclitaxel alone or with sorafenib in advanced non-small-cell lung cancer. Journal of Clinical Oncology. 2010;28(11):1835-1842. doi: 10.1200/JCO.2009.26.1321. pmid:20212250
Paz-Ares LG, Biesma B, Heigener D, von Pawel J, Eisen T, Bennouna J, et al. Phase III, randomized, double-blind, placebo-controlled trial of gemcitabine/cisplatin alone or with sorafenib for the first-line treatment of advanced, nonsquamous non-small-cell lung cancer. Journal of Clinical Oncology. 2012;30(25):3084-3092. doi: 10.1200/JCO.2011.39.7646. pmid:22851564
Gridelli C, Morgillo F, Favaretto A, De Marinis F, Chella A, Cerea G, et al. Sorafenib in combination with erlotinib or with gemcitabine in elderly patients with advanced non-small-cell lung cancer: a randomized phase II study. Annals of oncology. 2011;22(7):1528-1534. doi: 10.1093/annonc/mdq630. pmid:21212155
Lind JS, Dingemans AMC, Groen HJ, Thunnissen FB, Bekers O, Heideman DA, et al. A multicenter phase II study of erlotinib and sorafenib in chemotherapy-naive patients with advanced non-small cell lung cancer. Clinical Cancer Research. 2010;16(11):3078-3087. doi: 10.1158/1078-0432.CCR-09-3033. pmid:20395213
Spigel DR, Burris HA, Greco FA, Shipley DL, Friedman EK, Waterhouse DM, et al. Randomized, double-blind, placebo-controlled, phase II trial of sorafenib and erlotinib or erlotinib alone in previously treated advanced non-small-cell lung cancer. Journal of clinical oncology. 2011;29(18):2582-2589. doi: 10.1200/JCO.2010.30.7678. pmid:21576636
Okamoto I, Miyazaki M, Morinaga R, Kaneda H, Ueda S, Hasegawa Y, et al. Phase I clinical and pharmacokinetic study of sorafenib in combination with carboplatin and paclitaxel in patients with advanced non-small cell lung cancer. Investigational new drugs. 2010;28(6):844-853. doi: 10.1007/s10637-009-9321-x. pmid:19760364
Kindler HL, Wroblewski K, Wallace JA, Hall MJ, Locker G, Nattam S, et al. Gemcitabine plus sorafenib in patients with advanced pancreatic cancer: a phase II trial of the University of Chicago Phase II Consortium. Investigational new drugs. 2012;30(1):382-386. doi: 10.1007/s10637-010-9526-z. pmid:20803052
Chiorean EG, Schneider BP, Akisik FM, Perkins SM, Anderson S, Johnson CS, et al. Phase 1 pharmacogenetic and pharmacodynamic study of sorafenib with concurrent radiation therapy and gemcitabine in locally advanced unresectable pancreatic cancer. Int J Radiat Oncol Biol Phys. 2014;89(2):284-291. doi: 10.1016/j.ijrobp.2014.02.024. pmid:24726286
Gonçalves A, Gilabert M, François E, Dahan L, Perrier H, Lamy R, et al. BAYPAN study: a double-blind phase III randomized trial comparing gemcitabine plus sorafenib and gemcitabine plus placebo in patients with advanced pancreatic cancer. Annals of oncology. 2012;23(11):2799-2805. pmid:22771827
Cascinu S, Berardi R, Sobrero A, Bidoli P, Labianca R, Siena S, et al. Sorafenib does not improve efficacy of chemotherapy in advanced pancreatic cancer: A GISCAD randomized phase II study. Digestive and Liver Disease. 2014;46(2):182-186. doi: 10.1016/j.dld.2013.09.020. pmid:24189171
Aparicio J, García-Mora C, Martín M, Petriz ML, Feliu J, Sánchez-Santos ME, et al. A Phase I, Dose-Finding Study of Sorafenib in Combination with Gemcitabine and Radiation Therapy in Patients with Unresectable Pancreatic Adenocarcinoma: A Grupo Español Multidisciplinario en Cáncer Digestivo (GEMCAD) Study. PLoS ONE. 2014;9(1):e82209. doi: 10.1371/journal.pone.0082209. pmid:24416138
Cardin DB, Goff L, Li CI, Shyr Y, Winkler C, DeVore R, et al. Phase II trial of sorafenib and erlotinib in advanced pancreatic cancer. Cancer medicine. 2014;3(3):572-579. doi: 10.1002/cam4.208. pmid:24574334
Lee EQ, Kuhn J, Lamborn KR, Abrey L, DeAngelis LM, Lieberman F, et al. Phase I/II study of sorafenib in combination with temsirolimus for recurrent glioblastoma or gliosarcoma: North American Brain Tumor Consortium study 05-02. Neuro-oncology. 2012;14(12):1511-8. doi: 10.1093/neuonc/nos264. pmid:23099651
Peereboom DM, Ahluwalia MS, Ye X, Supko JG, Hilderbrand SL, Phuphanich S, et al. NABTT 0502: a phase II and pharmacokinetic study of erlotinib and sorafenib for patients with progressive or recurrent glioblastoma multiforme. Neuro-oncology. 2013;15(4):490-496. doi: 10.1093/neuonc/nos322. pmid:23328813
Reardon DA, Vredenburgh JJ, Desjardins A, Peters K, Gururangan S, Sampson JH, et al. Effect of CYP3A-inducing anti-epileptics on sorafenib exposure: results of a phase II study of sorafenib plus daily temozolomide in adults with recurrent glioblastoma. Journal of neuro-oncology. 2011;101(1):57-66. doi: 10.1007/s11060-010-0217-6. pmid:20443129
Den RB, Kamrava M, Sheng Z, Werner-Wasik M, Dougherty E, Marinucchi M, et al. A phase I study of the combination of sorafenib with temozolomide and radiation therapy for the treatment of primary and recurrent high-grade gliomas. Int J Radiat Oncol Biol Phys. 2013;85(2):321-328. doi: 10.1016/j.ijrobp.2012.04.017. pmid:22687197
Zustovich F, Landi L, Lombardi G, Porta C, Galli L, Fontana A, et al. Sorafenib plus daily low-dose temozolomide for relapsed glioblastoma: a phase II study. Anticancer research. 2013;33(8):3487-3494. pmid:23898124
Galanis E, Anderson SK, Lafky JM, Uhm JH, Giannini C, Kumar SK, et al. Phase II study of bevacizumab in combination with sorafenib in recurrent glioblastoma (N0776): a north central cancer treatment group trial. Clinical Cancer Research. 2013;19(17):4816-4823. doi: 10.1158/1078-0432.CCR-13-0708. pmid:23833308
Hottinger A, Aissa A, Espeli V, Squiban D, Dunkel N, Vargas M, et al. Phase I study of sorafenib combined with radiation therapy and temozolomide as first-line treatment of high-grade glioma. British journal of cancer. 2014;110(11):2655-2661. doi: 10.1038/bjc.2014.209. pmid:24786603
Sharma N, Pennell N, Nickolich M, Halmos B, Ma P, Mekhail T, et al. Phase II trial of sorafenib in conjunction with chemotherapy and as maintenance therapy in extensive-stage small cell lung cancer. Investigational new drugs. 2014;32(2):362-368. doi: 10.1007/s10637-013-0061-6. pmid:24420556
Krege S, Rexer H, Dorp F, Geeter P, Klotz T, Retz M, et al. Prospective randomized double-blind multicentre phase II study comparing gemcitabine and cisplatin plus sorafenib chemotherapy with gemcitabine and cisplatin plus placebo in locally advanced and/or metastasized urothelial cancer: SUSE (AUO-AB 31/05). BJU international. 2014;113(3):429-436. doi: 10.1111/bju.12437. pmid:24053564
Martín-Liberal J, López-Pousa A, Broto JM, Cubedo R, Gallego O, Brendel E, et al. Phase I trial of sorafenib in combination with ifosfamide in patients with advanced sarcoma: a Spanish group for research on sarcomas (GEIS) study. Investigational new drugs. 2014;32(2):287-294. doi: 10.1007/s10637-013-9989-9. pmid:23801301
Canter RJ, Borys D, Olusanya A, Li CS, Lee LY, Boutin RD, et al. Phase I trial of neoadjuvant conformal radiotherapy plus sorafenib for patients with locally advanced soft tissue sarcoma of the extremity. Annals of surgical oncology. 2014;21(5):1616-1623. doi: 10.1245/s10434-014-3543-7. pmid:24554062
Meyer JM, Perlewitz KS, Hayden JB, Doung YC, Hung AY, Vetto JT, et al. Phase I trial of preoperative chemoradiation plus sorafenib for high-risk extremity soft tissue sarcomas with dynamic contrast-enhanced MRI correlates. Clinical Cancer Research. 2013;19(24):6902-6911. doi: 10.1158/1078-0432.CCR-13-1594. pmid:24132922
Lee J, Capanu M, O'Reilly E, Ma J, Chou J, Shia J, et al. A phase II study of gemcitabine and cisplatin plus sorafenib in patients with advanced biliary adenocarcinomas. British journal of cancer. 2013;109(4):915-919. doi: 10.1038/bjc.2013.432. pmid:23900219
El-Khoueiry A, Rankin C, Siegel A, Iqbal S, Gong I, Micetich K, et al. S0941: a phase 2 SWOG study of sorafenib and erlotinib in patients with advanced gallbladder carcinoma or cholangiocarcinoma. British journal of cancer. 2014;110(4):882-887. doi: 10.1038/bjc.2013.801. pmid:24423918
Azad N, Dasari A, Arcaroli J, Taylor GE, Laheru DA, Carducci MA, et al. Phase I pharmacokinetic and pharmacodynamic study of cetuximab, irinotecan and sorafenib in advanced colorectal cancer. Investigational new drugs. 2013;31(2):345-354. doi: 10.1007/s10637-012-9820-z. pmid:22615057
Galal K, Khaled Z, Mourad AM, et al. Role of cetuximab and sorafenib in treatment of metastatic colorectal cancer. Indian journal of cancer. 2011;48(1):47. doi: 10.4103/0019-509X.75825. pmid:21248446
Samalin E, Bouche O, Thézenas S, Francois E, Adenis A, Bennouna J, et al. Sorafenib and irinotecan (NEXIRI) as second-or later-line treatment for patients with metastatic colorectal cancer and KRAS-mutated tumours: a multicentre Phase I/II trial. British journal of cancer. 2014;110(5):1148-1154. doi: 10.1038/bjc.2013.813. pmid:24407191
Tabernero J, Garcia-Carbonero R, Cassidy J, Sobrero A, Van Cutsem E, Köhne CH, et al. Sorafenib in combination with oxaliplatin, leucovorin, and fluorouracil (modified FOLFOX6) as first-line treatment of metastatic colorectal cancer: the RESPECT trial. Clinical Cancer Research. 2013;19(9):2541-2550. doi: 10.1158/1078-0432.CCR-13-0107. pmid:23532888
Sun W, Powell M, O'Dwyer PJ, Catalano P, Ansari RH, Benson AB. Phase II study of sorafenib in combination with docetaxel and cisplatin in the treatment of metastatic or advanced gastric and gastroesophageal junction adenocarcinoma: ECOG 5203. Journal of Clinical Oncology. 2010;28(18):2947-2951. doi: 10.1200/JCO.2009.27.7988. pmid:20458043
Kim C, Lee JL, Choi YH, Kang BW, Ryu MH, Chang HM, et al. Phase I dose-finding study of sorafenib in combination with capecitabine and cisplatin as a first-line treatment in patients with advanced gastric cancer. Investigational new drugs. 2012;30(1):306-315. doi: 10.1007/s10637-010-9531-2. pmid:20839031
Yamada Y, Kiyota N, Fuse N, Kato K, Minami H, Hashizume K, et al. A phase I study of sorafenib in combination with S-1 plus cisplatin in patients with advanced gastric cancer. Gastric Cancer. 2014;17(1):161-172. doi: 10.1007/s10120-013-0247-9. pmid:23532594
Martin-Richard M, Gallego R, Pericay C, Foncillas JG, Queralt B, Casado E, et al. Multicenter phase II study of oxaliplatin and sorafenib in advanced gastric adenocarcinoma after failure of cisplatin and fluoropyrimidine treatment. A GEMCAD study. Investigational new drugs. 2013;31(6):1573-1579. doi: 10.1007/s10637-013-0020-2. pmid:24077981
Castellano D, Capdevila J, Sastre J, Alonso V, Llanos M, García-Carbonero R, et al. Sorafenib and bevacizumab combination targeted therapy in advanced neuroendocrine tumour: a phase II study of Spanish Neuroendocrine Tumour Group (GETNE0801). European Journal of Cancer. 2013;49(18):3780-3787. doi: 10.1016/j.ejca.2013.06.042. pmid:24012098
Chan JA, Mayer RJ, Jackson N, Malinowski P, Regan E, Kulke MH. Phase I study of sorafenib in combination with everolimus (RAD001) in patients with advanced neuroendocrine tumors. Cancer chemotherapy and pharmacology. 2013;71(5):1241-1246. doi: 10.1007/s00280-013-2118-9. pmid:23475104
Berruti A, Sperone P, Ferrero A, Germano A, Ardito A, Priola AM, et al. Phase II study of weekly paclitaxel and sorafenib as second/third-line therapy in patients with adrenocortical carcinoma. European Journal of Endocrinology. 2012;166(3):451-458. doi: 10.1530/EJE-11-0918. pmid:22189997
London AJ, Kimmelman J. Why clinical translation cannot succeed without failure. Elife. 2015;4:e12844. doi: 10.7554/eLife.12844. pmid:26599839
Mattina J, MacKinnon N, Henderson VC, Fergusson D, Kimmelman J. Design and Reporting of Targeted Anti-Cancer Preclinical Studies: A Meta-Analysis of Animal Studies Investigating Sorafenib Antitumor Efficacy. Cancer research. 2016;76(16):4627-36. doi: 10.1158/0008-5472.CAN-15-3455. pmid:27261504
Hey SP, Kimmelman J. Ethics, error, and initial trials of efficacy. Science translational medicine. 2013;5(184):184fs16-184fs16. doi: 10.1126/scitranslmed.3005684. pmid:23658242
Maitland ML, Hudoba C, Snider KL, Ratain MJ. Analysis of the yield of phase II combination therapy trials in medical oncology. Clinical Cancer Research. 2010;16(21):5296-5302. doi: 10.1158/1078-0432.CCR-10-0669. pmid:20837695
Mullins CD, Montgomery R, Abernethy AP, Hussain A, Pearson SD, Tunis S. Recommendations for clinical trials of off-label drugs used to treat advanced-stage cancer. Journal of Clinical Oncology. 2012;30(6):661-666. doi: 10.1200/JCO.2011.35.5198. pmid:22253467
Eaton AA, Sima CS, Panageas KS. Prevalence and Safety of Off-Label Use of Chemotherapeutic Agents in Older Patients With Breast Cancer: Estimates From SEER-Medicare Data. Journal of the National Comprehensive Cancer Network. 2016;14(1):57-65. pmid:26733555
Rettig RA, Jacobson PD, Farquhar CM, Aubry WM. False Hope: Bone Marrow Transplantation for Breast Cancer. Oxford University Press; 2007
Miller K, Wang M, Gralow J, Dickler M, Cobleigh M, Perez EA, et al. Paclitaxel plus bevacizumab versus paclitaxel alone for metastatic breast cancer. New England Journal of Medicine. 2007;357(26):2666-2676. doi: 10.1056/NEJMoa072113. pmid:18160686
Stadtmauer EA, O'Neill A, Goldstein LJ, Crilley PA, Mangan KF, Ingle JN, et al. Conventional-dose chemotherapy compared with high-dose chemotherapy plus autologous hematopoietic stem-cell transplantation for metastatic breast cancer. New England Journal of Medicine. 2000;342(15):1069-1076. doi: 10.1056/NEJM200004133421501. pmid:10760307
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer
© 2017 Public Library of Science. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited: Mattina J, Carlisle B, Hachem Y, Fergusson D, Kimmelman J (2017) Inefficiencies and Patient Burdens in the Development of the Targeted Cancer Drug Sorafenib: A Systematic Review. PLoS Biol 15(2): e2000487. doi:10.1371/journal.pbio.2000487
Abstract
Failure in cancer drug development exacts heavy burdens on patients and research systems. To investigate inefficiencies and burdens in targeted drug development in cancer, we conducted a systematic review of all prelicensure trials for the anticancer drug, sorafenib (Bayer/Onyx Pharmaceuticals). We searched Embase and MEDLINE databases on October 14, 2014, for prelicensure clinical trials testing sorafenib against cancers. We measured risk by serious adverse event rates, benefit by objective response rates and survival, and trial success by prespecified primary endpoint attainment with acceptable toxicity. The first two clinically useful applications of sorafenib were discovered in the first 2 efficacy trials, after five drug-related deaths (4.6% of 108 total) and 93 total patient-years of involvement (2.4% of 3,928 total). Thereafter, sorafenib was tested in 26 indications and 67 drug combinations, leading to one additional licensure. Drug developers tested 5 indications in over 5 trials each, comprising 56 drug-related deaths (51.8% of 108 total) and 1,155 patient-years (29.4% of 3,928 total) of burden in unsuccessful attempts to discover utility against these malignancies. Overall, 32 Phase II trials (26% of Phase II activity) were duplicative, lacked appropriate follow-up, or were uninformative because of accrual failure, constituting 1,773 patients (15.6% of 11,355 total) participating in prelicensure sorafenib trials. The clinical utility of sorafenib was established early in development, with low burden on patients and resources. However, these early successes were followed by rapid and exhaustive testing against various malignancies and combination regimens, leading to excess patient burden. Our evaluation of sorafenib development suggests many opportunities for reducing costs and unnecessary patient burden in cancer drug development.
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer