1. Introduction

Low-Grade Serous Ovarian Cancer (LGSOC) is a rare histological subtype of epithelial ovarian cancer. Approximately 90% of serous carcinomas are high-grade, and only 10% will be low-grade. For example, there are only around 560 cases of low-grade serous carcinomas diagnosed in the UK each year. Ref. [1] LGSOC is a distinct pathological and clinical entity and appears to exist on a continuum with their likely precursor lesions, the serous borderline tumors. It is characterized by a more indolent biological behavior and lower sensitivity to traditional chemotherapy (response rates of approximately 5%) when compared to high-grade serous ovarian cancer (HGSOC) [2].

Maximal effort cytoreductive surgery aimed at reduction of tumor load is the cornerstone of treatment for women with LGSOC. Attributed to its decreased chemosensitivity, debulking even to a residual disease less than 1 cm has been demonstrated to also be beneficial in those patients where total macroscopic clearance cannot be obtained [3]. For that reason, the value of neoadjuvant chemotherapy in LGSOC is not as well defined as in HGSOC [4].

Despite its indolent behavior, 70% of women with advanced stage LGSOC will experience a disease recurrence [5,6]. For that reason, NCCN [7] and ESMO [8] guidelines endorse therapeutic options that include systemic carboplatin and paclitaxel, either alone or with endocrine agents as maintenance in stage II–IV disease. Endocrine therapy alone, most commonly with an aromatase inhibitor, has also been considered. Currently, national guidelines and standards of practice vary broadly and personal preferences and views of the individual treating teams, often shape patients’ journeys without adequate evidence. Novel agents, such as MEK inhibitors, have shown significant promise, but funding and availability/licensing issues provide a significant obstacle to their wide incorporation into routine clinical care [2].

In the present work, we performed a literature review and, subsequently, a meta-analysis to evaluate the efficacy of traditional (i.e., cytotoxic and antihormonal) postoperative treatment options in patients with LGSOC.

2. Materials and Methods

2.1. Data Sources and Study Selection

A comprehensive, systematic computer literature search on PubMed was performed using the following Medical Subject Headings (MeSH) terms: “low grade serous ovarian cancer” AND/OR “adjuvant treatment” AND/OR “recurrent” AND/OR “chemotherapy” AND/OR “hormonal therapy”.

Separate searches were performed with MeSH terms on MEDLINE and EMBASE to extract all relevant literature available.

2.2. Study Selection

Inclusion criteria were studies published in English between September 2000 and June 2021. All types of meta-analyses, prospective, retrospective, and systematic reviews were eligible for inclusion in the current review and all retrieved studies were evaluated for eligibility by two authors (R.M. and E.M.)

The population of this study includes patients with histologically confirmed stage II–IV LGSOC who have undergone primary cytoreduction. We included studies that reported data about traditional adjuvant treatment approaches: cytotoxic chemotherapy, antihormonal agents, or a combination of both. Options of antihormonal agents included: aromatase inhibitors, tamoxifen, and LH-HR analogues.

2.3. We Excluded Studies That

• Did not report specific information about type of adjuvant treatment;

• Did not include survival data;

• Included patients who did receive neoadjuvant treatment;

• Included other new targeted therapies: Poly-ADP ribose polymerase (PARP) inhibitors, MEK inhibitors, and antiangiogenics;

• Included patients who received intraperitoneal chemotherapy;

• Grey Literature was not considered—case reports, letters, and comments were excluded.

Our Systematic review was submitted to the PROSPERO register and published in the database with the registration number: CRD42021277026.

2.4. Statistical Analysis

Age and follow-up time were expressed in mean or median depending on the study.

Survival was expressed as median time to recurrence, % patients, PFS or OS in 2, 3 or 5 years and HR for PFS and/or OS. This heterogeneity to describe survival made the data difficult to analyze.

Descriptive statistics were used to describe the treatments employed for the qualitative analysis, with median PFS and OS measurements reported individually along with their respective 95% CI.

After study selection and application of the exclusion criteria, we stratified studies included in the meta-analysis to systemic chemotherapy versus no treatment and to hormonal treatment after systemic chemotherapy versus systemic chemotherapy only. We could not identify any relevant literature evaluating antihormonal treatment alone versus no systemic treatment, nor any literature about chemotherapy versus antihormonal treatment. We used the R software version 3.6 with the metafor and the meta packages. For all the studies, we reported hazard ratios (HR) and we pooled the HR for OS and PFS using the inverse variance method (the weight given to each study being the inverse of the variance) and the random effects model to account for heterogeneity. We used the Sidik–Johnkman estimator for tau and Chi-squared and Cochrane Q-tests to quantify heterogeneity across studies by computing the I² for each endpoint. All 95% CIs were two-sided.

2.5. Quality Assessment of Studies

The methodological quality of cohort studies was evaluated using the “Quality Assessment Tools of the National Heart, Lung, and Blood Institute” (NHLBI) [9].

3. Results

3.1. Evidence Acquisition

Searching in the Literature with MeSH terms we found 1690 articles. After the exclusion of Grey Literature, i.e., case reports, letters, and comments, and non-English paper, 205 records were selected. After reading the abstracts, 108 were excluded as per the aforementioned exclusion criteria. We assessed 97 full articles for eligibility and identified only 12 studies eligible for inclusion in the qualitative analysis (Figure 1). The other 85 articles did not provide survival data of the therapeutic strategy target of our study.

3.2. Study Characteristics

In the 12 studies eligible for inclusion, 9 concerned patients in the first line setting (Primary treatment) and 3 concerned patients with recurrent disease.

Except one phase II trial [10] all other studies were of retrospective nature. Two of the studies had a prospective part in addition to the retrospective analysis [11,12].

The baseline characteristics of the 12 included studies are shown in Table 1 (Primary treatment) and Table 2 (Recurrence).

Overall, 1892 patients were included from all studies: 1734 in the first-line setting and 158 in recurrent disease.

3.3. Qualitative Synthesis

First-Line Setting (Primary Treatment)

Nine studies were included in this group. The type of treatment was antihormonal therapy alone in one study [19] and a combination of chemotherapy and antihormonal therapy in three studies [11,12,15], whereas two studies compared chemotherapy alone vs just watch and wait [13,14].

Three studies reported descriptive analysis data of patients treated with only chemotherapy [16,17,18].

In four these nine studies, only a descriptive analysis of treatments was done (three for cytotoxic chemotherapy, one for antihormonal treatment) without any control group and did not report any survival results for adjuvant treatment with HR [16,17,18,19]. As they also did not consistently report survival, these studies were not included in the meta-analysis.

The five remaining studies that were ultimately included in the present meta-analysis evaluated the following regimens: three studies compared cytotoxic chemotherapy alone vs chemotherapy followed by maintenance antihormonal therapy [11,12,15] and two studies compared chemotherapy vs no adjuvant treatment at all [13,14]. We report in more detail the three studies that evaluated cytotoxic chemotherapy alone vs chemotherapy followed by maintenance antihormonal therapy below.

Schlumbrecht et al. (2011) divided antihormonal therapy into two categories. The first category, named “Consolidation therapy”, included patients without radiological or clinical evidence of residual disease at the end of their first-line chemotherapy, who then received antihormonal treatment. The second category, named “Maintenance therapy”, included patients who had persistent but stable disease after adjuvant chemotherapy, who then received antihormonal treatment. We opted to include only the data of patients in the category “Consolidation therapy”, to be consistent with the rest of the included patients in this meta-analysis that had undergone complete cytoreduction. In total, 95.8% of the patients were treated with platinum-based chemotherapy [15].

Gershenson et al. (2017) evaluated patients who underwent primary cytoreductive surgery followed by platinum-based chemotherapy and observation versus antihormonal therapy (as per the physician’s choice) starting within 3 months of completion of postoperative chemotherapy. In total, 54.3% of the patients received Letrozole [11].

A previous study conducted by Gershenson et al. in 2015 included a subgroup of 287 patients who had undergone primary cytoreductive surgery followed by platinum-based chemotherapy. In total, 50 of these patients also received maintenance hormonal therapy, which we also included in the present analysis [12].

The studies and their regimens are presented in Table 3.

3.4. Recurrent Setting

Only three case studies were identified and included in this group: 36 patients reported by Tang et al. (2019) [10], 64 patients by Gershenson et al. (2012) [20], and 58 by Gershenson et al. (2009) [6].

The types of applied treatments were antihormonal treatment alone in two studies (Tang et al., 2019, Gershenson et al., 2012) [10,20] and chemotherapy alone in one study (Gershenson 2009) [6]. These three studies were only descriptive and did not provide any comparative data with a control group. None of these studies included HR in their results.

In the PARAGON phase II study (Tang et al., 2019) anastrozole given for at least 6 months was associated with a clinical benefit rate of 61% in patients with recurrent ER- and/or PR-positive low-grade ovarian cancer or serous ovarian borderline tumors. The toxicity profile reported was acceptable toxicity. Median PFS was 11.1 months (95% CI: 3.2–11.9) [10].

In a further retrospective study by Gershenson et al. (2012) evaluating 64 patients with histologically confirmed, recurrent low-grade serous ovarian/peritoneal carcinoma who received hormonal therapy at their institution between 1989 and 2009 showed an overall response rate of only 9%. In total, 61% of the patient regimens resulted in a progression-free survival duration of at least 6 months. Patient regimens involving ER+/PR+ disease produced a longer median time to disease progression (8.9 months) than patient regimens involving ER+/PR- disease did (median = 6.2 months; p = 0.053). This antitumor activity was considered as moderate by the authors and appealed for further studies to determine whether ER/PR expression status may be used as a predictive biomarker for low-grade disease [20].

In 2009, Gershenson et al. performed a descriptive analysis of 58 patients with recurrent LGSOC, who received 108 combinations of different chemotherapy regimens (“patient regimens”); 60.6% were platinum-based. Stable disease was observed in 65 patients (60.2%). The overall response rate for the platinum-sensitive cohort was 4.9%, and 2.1% for the platinum-resistant cohort. The median overall survival was 87.1 months and the median time to progression was 29.0 weeks (34.7 weeks for platinum-sensitive cohort and 26.4 weeks for platinum-resistant cohort) (p = 0.32) [6].

With only three studies in this group, a valid meta-analysis was not feasible. Thus, we only included first-line treatment data in this meta-analysis.

3.5. Quantitative Synthesis

For the primary patients who were included in the present meta-analysis, median OS for those treated with systemic chemotherapy alone ranged between 88.2 and 106.8 months, whereas for those patients who were additionally treated with antihormonal treatment as a maintenance, the median OS ranged between 100.9 and 115.7 months and the median PFS between 25.9 and 76.4 months. Median PFS was 25.9 and 76.4 months, respectively.

Forest plots summarizing the efficacy of the various treatment approaches are presented in Figure 2. The pooled HR analyzes did not reveal any statistically significant PFS or OS benefit associated with the addition of antihormonal treatment after completion of systemic first-line chemotherapy in LGSOC patients who had undergone complete cytoreduction when compared to systemic chemotherapy alone: for PFS, pooled HR = 0.59, 95% CI [0.33, 1.04]), I² = 77% (Figure 2c), and for OS, pooled HR = 0.83, 95% CI [0.50, 1.39], I² = 46% (Figure 2b).

Moreover, systemic chemotherapy also failed to significantly improve OS when compared to no treatment at all after successful cytoreduction (pooled HR = 1.01, 95% CI [0.79, 1.29], I² = 0%, Figure 2a). No PFS data were reported for the studies with chemotherapy alone.

3.6. Quality Assessments

The quality of 11 retrospective studies and of the prospective study were assessed using the NHLBI study quality assessment tool and were rated as “fair” in all cases. The most common biases were the absence of sample size justification and the missed measurement of confounding variables. Table 4

4. Discussion

To our knowledge, this is the first comprehensive systematic review and meta-analysis to assess the potential survival impact of antihormonal maintenance treatment or even cytotoxic first-line chemotherapy in patients who had undergone successful cytoreduction for advanced stage LGSOC. Analyzed evidence failed to demonstrate a survival benefit through the addition of antihormonal agents after completion of first-line chemotherapy compared to chemotherapy alone in completely cytoreduced LGSOC patients. Equally, chemotherapy alone was not associated with any significant improvement in survival compared to watch and wait strategies.

These data give a clear signal of the necessity of overcoming conventional ways of thinking for the management of LGSOC. It is prime time for traditional cytotoxic and antihormonal agents to give their place to novel targeted approaches, especially developed for these rare neoplasms in an overall scheme of individualization of treatment.

Chemosensitivity in LGSOC is being increasingly disputed [17,21]. Conventional chemotherapy studies for advanced ovarian cancer used to include all histological subtypes, i.e., both low and high grade, without specific differentiation. However, in accordance with the universal trends in oncology to individualize care, systemic studies also in ovarian cancer have started stratifying patients according to their tumor biology and even the development of umbrella studies aimed at recruiting across various organs by equivalent histology.

In surgical studies, such a differentiation is more challenging due to the well-defined difficulties of objectively performed high quality surgical studies. For example, the prospective phase III randomized GOG 0213 trial included only seven patients with LGSC [22]. Similarly, the European study DESKTOP III also recruited only 10 LGSC patients [23].

Antihormonal treatment in ovarian cancer has been part of the treatment armamentarium for years, even for high-grade histology. For example, Tamoxifen has been broadly accepted as an alternative to non-platinum monotherapy for palliative relapsed patients [24]. Patients with LGSOC with higher estrogen receptor (ER) expression appear to benefit from such an approach even in earlier treatment settings [25]. Still, solid data from prospective randomized clinical trials of antihormonal treatment versus cytotoxic chemotherapy are lacking and broad national and international variations in practice exist regarding their clinical utilization. For example, in a German survey, 43% of physicians (gynecologists, gynecologic oncologists, and oncologists) did not consider antihormonal therapy as a treatment option [26].

Studies of the molecular biology of LGSOC have identified a high frequency of estrogen and progesterone expression, but also the important role of the mitogen-activated protein kinase (MAPK) signaling pathway on its pathogenesis. KRAS mutations occur in 16% to 44% of LGSOCs, BRAF mutations in 2% to 20%, and NRAS mutations in up to 26%. This differentiates LGSOC from HGSOC, the latter being associated with ubiquitous p53 mutations, copy number abnormalities, and DNA repair defects [27].

MEK inhibitors are orally bioavailable, small-molecule inhibitors of MEK1/2. An initial phase II trial examined selumetinib in recurrent LGSOC and demonstrated objective response rates of 15% and a median PFS of 11.0 months. No correlation between response and mutational status was found [28].

Two large randomized clinical trials of MEK inhibitors in recurrent LGSOC followed this initial study. GOG 0281 was a phase II/III trial comparing trametinib with the physician’s choice of pegylated liposomal doxorubicin or weekly paclitaxel, topotecan, letrozole, or tamoxifen [29]. MILO/ENGOT-ov11 compared binimetinib with the physician’s choice [30].

On the basis of an interim analysis of 303 patients, enrolment in MILO was discontinued following an interim analysis as the PFS HR crossed the predefined futility boundary. In an updated analysis, median PFS times were 10.4 for binimetinib and 11.5 months for the physician’s choice (HR, 1.15; p = 0.748). However, GOG 0281 successfully met its primary end point, with a median PFS of 13.0 months for trametinib and 7.2 months for the physician’s choice (HR, 0.48; p < 0.001) and ORRs of 26% and 6.2% for trametinib and the physician’s choice, respectively. In England, trametinib is currently funded via the Cancer Drugs Fund for patients with recurrent LGSOC who have progressive disease following platinum-based chemotherapy and who have exhausted all endocrine therapy. Data to support the use of MEK inhibitors in the first-line setting are still lacking and further studies are required. Furthermore, studies of MEK inhibitors in combination with other targeted therapies such as BRAF inhibitors are showing promise in LGSOC [30,31].

The strength of our work is that it is the first meta-analysis in the literature about systematic adjuvant treatment in LGSOC, but there are several limitations to our study. The most important is that very few studies are available, and the heterogeneity among these studies limits a uniform interpretation of the results and the inclusion of the data in quantitative analyses. More data are now needed to confirm that hormonal treatment after systemic chemotherapy in LGSOC does not lead to any benefit for OS or for PSF and to determine the best way to combine these two therapies, if applicable.

In this context, the multicenter prospective randomized phase III trial NRG-GY-019, which started recruiting in mid-2019, randomizes newly diagnosed stage II–IV LGSOC-patients following initial debulking surgery to adjuvant platinum/taxane chemotherapy followed by maintenance letrozole vs letrozole alone [32]. However, more randomized trials are necessary to have scientific evidence about the best approach in this subgroup of patients.

5. Conclusions

Our data reinforce current evidence that future treatment trends are clearly pointing towards the omission of traditional systemic approaches in, at least optimally cytoreduced, LGSOC patients. This approach would spare unnecessary toxicity for many patients. Our focus should concentrate on the development of especially targeted agents and their broad implementation, even in restricted settings.

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Enlarge this image.

Figure 1. PRISMA Flow Diagram.

Enlarge this image.

Figure 2. Meta-analysis for: (a) OS in patients with systemic chemotherapy alone, (b) for OS and (c) PFS for patients treated with additional antihormonal maintenance treatment after completion of systemic chemotherapy.

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