Correspondence to Dr René Rodríguez-Gutiérrez; [email protected]
Strengths and limitations of this study
In the design of the search strategy, we employed a previously published filter for studies evaluating values and preferences.
Risk of bias assessment of included studies was performed in accordance with a specific tool for assessing values and preferences studies.
The GRADE approach was employed to evaluate the certainty of our results.
Results are mostly based on studies graded at high risk of bias.
We did not found studies evaluating preferences for initiation of sodium-glucose cotransporter-2 inhibitors.
Background
The American Diabetes Association and the European Association for the Study of Diabetes have highlighted the importance of providing a patient-centred approach in patients with type 2 diabetes.1 To support clinicians in providing holistic care, it is important to understand the values and preferences that are considered by patients when choosing a particular treatment option.2 More specifically, evidence on how patients weigh the balance of benefits, harms and burden of treatment can inform patient-centred practice.
Glucagon-like peptide-1 receptor agonists (GLP-1 RA) and sodium-glucose cotransporter-2 inhibitors (SGLT-2i) are two new drug classes of medications to treat type 2 diabetes that are rapidly changing clinical practice because of demonstrable reductions in cardiovascular and kidney outcomes, without increasing hypoglycaemic.3–10 These drugs have notable differences in their benefits and harms and how patients are required to administer them. While GLP-1 RA are mostly injected, SGLT-2i are taken orally. The extent to which these treatments impact patients and carers (treatment burden) is often ignored both in the clinical decision-making process and clinical practice guidelines. Moreover, understanding the values and preferences that patients consider in the process of initiating either of both therapies is still inconclusive, and a thorough and integrative analysis of the available evidence could assist both patients and clinicians in the integral management of the disease.11
As a result of the aforementioned, we performed this systematic review to inform a clinical practice guideline (BMJ Rapid Recommendation) on the values and preferences that patients consider in the process of initiating GLP-1 RA and SGLT-2i when compared with each other or other drug treatments for type 2 diabetes (box 1). The goal of the BMJ Rapid Recommendations project is to create rapid and trustworthy recommendations regarding medical topics of interest by identifying relevant studies which might change practice and are of interest to readers.12 These guidelines were also informed by a linked systematic review and network meta-analysis on effectiveness and a systematic review on risk prediction models. Together these reviews confirmed, with overall high certainty evidence, benefits of SGLT-2i and GLP-1 RA while demonstrating that absolute benefits differ across patients with different risks for cardiovascular and renal outcomes. In this context, our systematic review was performed to inform judgements on the values that patients consider when balancing benefits, harms and burdens of treatment for SGLT-2i and GLP-1 RA.
Box 1Linked resources in the BMJ rapid recommendations cluster
Reference to this values and preferences systematic review here.
Reference to guideline paper37
Reference to prognostic systematic review38
Reference to systematic review and network meta-analysis for SGLT-2i and GLP-1 receptor agonists for type 2 diabetes39
Reference to MAGICapp public guideline: to appear at www.magicapp.org
Reference to MAGIC multiple comparisons evidence summaries and decision aids: www.magicevidence.org/match-it
Methods
We followed the Preferred Reporting Items for Systematic Reviews and Meta-Analyses checklist for writing this review.13
Eligibility criteria
We included any study design using quantitative or qualitative analysis to report values and preferences held by patients with type 2 diabetes mellitus when initiating GLP-1 RA or SGLT-2i treatments or alternative glucose-lowering therapy. We excluded: (1) cost-effectiveness studies (as preferences are not directly assessed), (2) studies that report data that is not patient-reported (as they do not reflect the overall patient perspective), (3) studies assessing patient satisfaction on a specific treatment rather than preferences for it when compared with other choices, (4) studies that elicited or explored treatment preferences without reporting the process or factors considered in the decision (as results could be biased due to lack of assessment of values driving the preference), (5) studies of patients with a previously stated preference for GLP-1 RA or SGLT-2i (as results can be biased toward one treatment choice due to previous experience with it) and (6) randomised clinical trials that evaluated patient preferences of a given intervention over a previous treatment (due to possible differences in experiencing each treatment).
Search strategy
A systematic search strategy was performed on MEDLINE, Scopus, EMBASE, Web of Science and the Cochrane Central Register of Controlled Trials from inception until May 2020. An experienced search specialist designed and conducted the search strategy using a combination of keywords and Medical Subject Headings terms related to values and preferences considered by patients with type 2 diabetes mellitus for initiating GLP-1 RA or SGLT-2i (online supplemental material 1). A previously published filter for studies regarding values and preferences was added to narrow the obtained studies.14
Study selection
After excluding duplicated studies, three reviewers independently and in duplicate screened the title and abstract of retrieved records. Potentially eligible reports were then reviewed in full text. Differences were reconciled by either consensus or discussion with a third reviewer. To ensure an adequate inter-rater agreement, the investigators performed calibration exercises until acceptable agreement was achieved with Cohen’s kappa coefficient >0.7. Study selection process was performed in the Distiller Systematic Review Software (Evidence Partners DistillerSR, Ottawa, Canada).
Data collection
A web-based extraction form for data collection was used following piloting to ensure adequate inter-rater agreement and later modifications according to reviewers’ input. Paired data extractors worked independently to abstract study characteristics, participants’ baseline characteristics, methods used to measure values and preferences, and number and percentage of patients who chose to take the medication according to their values and preferences. Disagreements in the data collection process were resolved by either consensus or arbitration by a third reviewer.
Outcome definition
The term ‘values and preferences’ was defined according to the Grading of Recommendations, Assessment, Development and Evaluation (GRADE) working group definition: ‘the process that individuals use in considering the potential benefits, harms, costs, limitations and inconvenience of the management options in relation to one another’.15 In order to broaden our scope, the following definition was also considered: ‘given a choice, the selection of one alternative a priori’.16 We considered reporting of the following attributes: benefits, harms, costs, limitations or inconvenience related to available treatment options.
Risk of bias assessment
Two independent reviewers working in duplicate adjudicated risks of bias in individual studies based on our main outcome, using a tool proposed by the GRADE working group. It evaluates the following four domains: selection of participants into the study, completeness of data measurement instrument and data analysis.17 Disagreements were resolved by consensus or arbitration by a third reviewer.
Certainty of evidence assessment
To assess the certainty of evidence for the different drug profile comparisons that were included in this review, we followed the constructs proposed by the GRADE working group which are: study design, risk of bias, inconsistency, indirectness, imprecision and other methodological considerations. An overall certainty of evidence grade was then obtained (very low, low, low-moderate, high).18
Data synthesis
Due to the nature of the research question and design of the included studies, our results are reported as a narrative synthesis since a pooled analysis is not feasible.
Patient and public involvement
Patients or members of the public were not involved with the design of this study.
Results
Search strategy and study selection
A total of 11 162 records were retrieved in the search and screened using the title and abstract. (figure 1) From these, 86 full-text articles were assessed for eligibility and 17 studies comprising 7296 patients were included in this review19–35 (table 1). We did not identify studies reported values and preferences of SGLT-2i and all eligible studies evaluated GLP-1 RA.
Enlarge this image.Figure 1. Study selection flow diagram. GLP-1 RA, glucagon-like peptide-1 receptor agonists; SGLT-2i, sodium-glucose cotransporter-2 inhibitors.
Demographic and study characteristics
| Author, year | Country | N | Injection experience | Age (years) | Female (%) | Race (%) | BMI | HbA1c | Years of diagnosis | Assessment approach | Drugs evaluated |
| Boye et al24 2019 | Italy | 216 | M | 60.5 (9.9)* | 42.1 | White: 98.60 Other: 0.9 | ND | ND | ND | TTO | Dulaglutide QW Semaglutide QW |
| Brooks et al25 2019 | Japan | 161 | N | 55 (48–63)‡ | 16 | ND | 25.9 (23.9-28.9)‡ | 8.3 (7.4-9.1)‡ | <1 year: 1% 1–5 years: 24% 5–10 years: 38%>10 yrs: 37% | DCE | Dulaglutide QW Semaglutide QW |
| Dibonaventura et al19 2010 | International | 1340 | N | 55.3 (12.1)* | 46.8 | White: 90.5 Other:9.5 | ND | ND | 6.2 (5.9)* | Online survey | Sitagliptin Liraglutide QD |
| Evans et al20 2013 | UK | 188 | M | 63.9 (5.9)* | 42.8 | ND | 36.7 (5.9)* | 8.9 (1.1)* | 8.5 (3.3)* | Case-note survey | Sitagliptin Liraglutide QD |
| Gelhorn et al27 2015 | UK | 243 | N | 60.5 (10.9)* | 23.9 | White: 72 Asian: 15.2 | 29.8 (5.4)* | <7%: 28.8% 7.1%–8%: 25.5% 8.1%–9%:11.1%>9%: 6.6% NR: 28% | <1 year: 5.8% 1–5 years: 35.8% 5–10 years: 34.6%>10 yrs: 23.9% | DCE | Liraglutide QD Dulaglutide QW |
| Gelhorn et al28 2016 | Japan | 182 | N | 58.9 (10)* | 35.7 | ND | 26.1 (5)* | <7%: 53.3% 7.1%–8%: 31.3% 8.1–9: 8.8%>9 %: 6.6% | <1 year: 3.9%<1–5 years: 32.4% 5–10 years: 29.1%>10 yrs: 34.6% | DCE | Dulaglutide QW Liraglutide QD |
| Hauber et al26 2015 | USA | 643 | M | 52.7 (15)* | 48.3 | ND | ND | <7%: 34.5% 7%–9%: 44.1%>9%: 12.8% | ND | DCE | GLP-1 RA in general |
| Jendle et al21 2012 | Sweden | 840 | M | ND | ND | ND | ND | ND | ND | WTP via DCE | Liraglutide QD Rosiglitazone Glimepiride Insulin glargine Exenatide Twice daily |
| Lüdemann et al22 2015 | Germany | 62 | E | 60.3 (11.1)* | 53.2 | White: 98.4 Others: 1.6 | 31.2 (3.5)* | 7.4 (0.5)* | 7.5 (6.3)* | Cross-over trial | Vildagliptin Liraglutide QD |
| Matza et al29 2017 | UK | 209 | M | 60.4 (8.9)* | 42.6 | White: 86.6 Other: 14.4 | ND | ND | ND | TTO | QW GLP-1 RA injection devices |
| Matza et al31 2018a | Italy | 238 | M | 60.2 (9.3)* | 41.2 | White:100 | ND | ND | ND | TTO | QW GLP-1 RA injection devices |
| Matza et al30 2018b | USA | 404/58§ | E | 60.7 (11.4)* | 54 | White: 78 African/American: 14.6 | ND | ND | 13.7 (9.0)* | Questionnaire | Liraglutide QD Dulaglutide QW |
| Matza et al32 2020 | USA | 310 | N | 60 (10.8)* | 48.4 | White: 50 Black/African american: 33.9 | ND | 7.29 (1.4)* | 8.06 (6.7)* | Cross-over trial | Dulaglutide QW Semaglutide QW |
| Polsteret al33 2010 | USA | 382 | M | 52.7 (8.8)* | 52 | White: 89.2 | ND | 7.3 (no SD) | 7.6 (5.3)* | TTO | Liraglutide QD Exenatide Twice daily |
| Poon et al23 2018 | UK | 232 | N | 61.8 (10.8)* | 25.9 | White: 78 Asian: 13.8 | 29.8 (6.1)* | <7%: 30.6% 7.1%–8%: 22% 8.1%–9%: 12.5%>9% : 4.7% NR : 30.2% | < 1 year: 7.3%, 1–5 years: 36.6% 5–10 years:28.9%>10 years: 27.2% | DCE | Dulaglutide QW Insulin glargine |
| Qin et al34 2017a | Germany and UK | 510 | E | 57 (11)* | 48.6 | White: 93.5 Asian/Asian British: 3.3 | 34.2 (7.5)* | 7.4 (1.9)* | 7.2 (5.9)* | DCE | Liraglutide QD Exenatide QW |
| Qin et al35 2017b | International | 1482 | N | 56 (11.4)* | 32 | White: 51.60 Asian: 40.7 | ND | 7.4 (2.3)* | 7 (0.5–61.9)† | DCE | Liraglutide QD Exenatide QW |
*Mean/SD.
†Range.
‡Median/IQR.
§Demographic characteristics shown for full sample; only 58 participants were included in the preferences analysis.
BID, twice daily administration; BMI, body mass index; DCE, discrete choice experiment; E, Injection experienced; GLP-1 RA, glucagon-like peptide-1 receptor agonists; HbA1c, Glycosilated hemoglobin; M, mixed; N, injection naïve; ND, no data; QD, once daily administration; QW, once weekly administration; TTO, time trade-off; WTP, willingness-to-pay.
Study characteristics
All studies employed quantitative methods to assess outcomes of interest. Five studies comprising a total of 2662 patients evaluated preferences for GLP-1 RA versus other glucose-lowering drugs.19–23 Furthermore, 12 studies comprising a total of 4634 patients evaluated preferences between, at least, two different GLP-1 RA medications or related injection devices, taking into account clinical attributes and/or device-related ones such as dosing, application frequency or characteristics of the application device.24–35 Mean age of participants in the included studies ranged between 52.7 and 63.9 years. Most studies reporting duration of diabetes and included patients at least 1 year after diagnosis.
Employed methodologies to elicit values and preferences
The most frequently employed methodology to elicit patients’ preferences was discrete choice experiment (DCE) (eight studies) where utilities, relative importance (RI) or ORs where used as units of measurement to quantify values and preferences.21 23 25–28 34 35 The next most frequent methodology was the time-trade-off (TTO) approach in four studies.24 29 31 33 Utilities, health state disutilities and RI were the units of measurement in these studies. Other methodologies employed were willingness to pay,21 online surveys,19 questionnaires,30 crossover trials22 32 and case-note surveys20 (table 1).
Risk of bias and certainty of evidence assessment
Overall, 12 studies were found at high-risk of bias due to the usage of non-validated instruments for eliciting preferences and invalid representation of efficacy and safety of the drug profiles.19–22 24–28 30 33 34 Only five studies were found at low risk of bias, these studies used a previously validated survey to measure preferences between different GLP-1 RA on both injection naïve and experienced patients23 29 31 32 35 (figure 2).
We evaluated the certainty of evidence regarding the following drug profile comparisons: GLP-1 RA versus dypeptil peptidase-4 inhibitors (DPP-4i), insulin glargine and other glucose-lowering therapies, liraglutide versus exenatide and dulaglutide, dulaglutide versus semaglutide and studies evaluating attributes of GLP-1RA injection devices. The certainty of evidence was judged to be very low in all cases due to concerns regarding study design, risk of bias and imprecision in all cases. In addition, concerns regarding inconsistency and indirectness were identified in most of the evidence for the different drug profile comparisons (table 2).
Table 2GRADE assessment of the certainty of evidence
| Certainty assessment | |||||||||
| No of studies | Study design | Risk of bias | Inconsistency | Indirectness | Imprecision | Other considerations | Impact | Certainty | Importance |
| GLP-1 RA (liraglutide) compared with DPP-4i (sitagliptin, vildagliptin) | |||||||||
| 3 | Observational studies* | Very serious† | Serious‡ | Very serious§ | Serious¶ | None | Higher preference for DPP-4i over liraglutide was observed in two out of three studies. | ⨁◯◯◯ VERY LOW | |
| GLP-1 RA (liraglutide, dulaglutide) compared with Insulin Glargine | |||||||||
| 2 | Observational studies | Serious** | Not serious | Very serious§ | Serious¶ | None | Higher preference for GLP-1 RA was observed in both studies. | ⨁◯◯◯ VERY LOW | |
| Other glucose-lowering treatments compared with GLP-1 RA | |||||||||
| 1 | Observational studies | Very serious†† | Not serious‡‡ | Very serious§ | Serious¶ | None | GLP-1 RA were preferred over other study drugs. (rosiglitazone, glimepiride) | ⨁◯◯◯ VERY LOW | |
| Liraglutide vs exenatide | |||||||||
| 4 | Observational studies | Very serious§§ | Not serious | Very serious§,¶¶ | Serious¶ | None | Liraglutide was preferred over twice-daily exenatide; however, once weekly exenatide was preferred over liraglutide. | ⨁◯◯◯ VERY LOW | |
| Liraglutide versus dulaglutide | |||||||||
| 3 | observational studies | very serious*** | not serious | very serious§,††† | serious¶ | none | In all three studies, a preference for dulaglutide over liraglutide was shown. | ⨁◯◯◯ VERY LOW | |
| Dulaglutide versus semaglutide | |||||||||
| 3 | Observational studies | Very serious‡‡‡ | Very serious§§§ | Very serious§,¶¶¶ | Serious¶ | None | A strong preference for dulaglutide was observed in two studies; however, these studies only presented injection attributes to participants. In the other study, a strong preference for semaglutide was observed where not only injection attributes but also clinical attributes of each drug profile were presented. | ⨁◯◯◯ VERY LOW | |
| Studies evaluating attributes of GLP-1 RA injection devices | |||||||||
| 3 | Observational studies | Serious**** | Not serious | Not serious | Serious¶ | None | As administration requirements for GLP-1 RA injection devices increase, preferences decrease. Patients strongly prefer weekly over daily injection devices. | ⨁◯◯◯ VERY LOW | |
*One study presented a cross-overdesign.
†Two studies presented a high risk of bias in the attrition item. One of the studies presented a high risk of bias in the item of instrument validity and reliability (1340 participants) which was the biggest one. The three studies presented a high risk of bias in two out of six items assessed (representation of the outcome and understanding of the tool by study participants). Therefore, we judged the trials to have very serious methodological limitations.
‡Two of the studies included patients naive to injectable medications and demonstrated a preference for DPP-4i over liraglutide. In another study, more participants preferred liraglutide over vildagliptin and included patients naive to injectable medications. The harms and benefits presented for patient‘sdecisions differed between studies (liraglutide weight reduction effect was omitted in the study where patients preferred sitagliptin). None of the included studies reported CIs of the point estimate neither statistical hypothesis tests to further assess inconsistency. We judged the evidence to have serious inconsistency.
§Drug profile did not fully represent the best available evidence now.
¶Although the evaluated sample size was optimal, the Cl of the point of estimate was not reported. We judge serious imprecision in the evidence.
**One of two studies was judged as overall low risk of bias (232 patients). The other study was at high risk in the attrition domain, representation of outcomes and understanding of the tool by study participants. (840 patients). We judge risk of bias to be serious for this outcome.
††The study was classified overall high risk of bias due to concerns regarding the attrition rate, representation of the outcome and understanding of the tool by study participants.
‡‡Since no further evidence is presented, it is not feasible to classify inconsistency.
§§One out of four studies presented low risk of bias in all the evaluated items (1482 patients). The other three studies (510, 382, 840 patients) presented a high risk of bias in the items of attrition, representation of the outcome and understanding the tool by study participants. We judge the evidence to have serious methodological limitations.
¶¶In all studies, medication profiles were presented with varying benefits and harms which were not based on the best available evidence now.
***Two of the three studies were at high risk of bias due to concerns regarding selection of participants and evaluation of the outcomes.
†††Serious concerns on indirectness are present due to heterogeneity among populations, where two of them were injection naive and another one was injection experienced. Furthermore, two studies presented drug profiles with only clinical variables and the other presented drug profiles with only device characteristics.
‡‡‡Two studies were classified as high risk of bias due to concerns regarding attrition rate and instrument validity and reliability for evaluating patient preferences.
§§§The direction of patient preferences tended to vary across studies wherein two of them, strong preferences for semaglutide were observed. However, in the other study, strong preference for dulaglutide was reported.
¶¶¶Two studies presented only device attributes as part of the treatment profile. However, the third study also added clinical attributes to the drug profile. This difference could have altered the direction of results across studies.
****Two of the three studies were classified as overall low risk of bias and the other one as high risk of bias due to concerns regarding selection of participants, attrition rate and representation of the outcome and understanding of the tool by study participants.
DPP-4i, dypeptil peptidase-4 inhibitors; GLP-1 RA, Glucagon-like peptide-1 receptor agonists.
Preferences for GLP-1 RA versus other types of glucose-lowering medications
Overall, five studies evaluated preferences for a GLP-1 RA versus other treatments of type 2 diabetes, such as insulin glargine,23 sitagliptin,19 20 vildagliptin,22 rosiglitazone and glimepiride.21 From these, one study was found to be at low risk of bias.23 Two studies were performed on the injection-naïve population,19 23 one on injection-experienced22 and the remaining two on a mixed population.20 21 Among the studies which presented drug profiles as part of their methodology, all studies described efficacy (defined as a change in glycosilated hemoglobin [HbA1c]), proportion of side effects, weight change, dosing frequency and delivery system. Four studies described hypoglycaemic risk,19–21 23 and three included blood pressure change in the studied drugs profile.19–21 From the five studies, two described the all above-mentioned attributes on their drug profiles20 21 (table 3). Shown below is a subdivision of the drug comparisons that were assessed in these studies.
Table 3Drug evidence profiles presented to participants in studies comparing GLP-1 RA to other glucose-lowering therapies
| Author, year | Preferred therapy | Change in HbA1c | Adverse Effects (%) | Weight change (kg) | Hypoglycaemic (%) | Blood pressure changes (mmHg) | Dosing Frequency | Type of delivery system | Population experience |
| Dibonaventura et al19 2010 | SG | SG: −1.4% LG: −2.4% | LG: Nausea 11%–19%, Vomit 5%–7%, Diarrhoea 8%–15% SG: No adverse effects | SG: 0 LG: −3.5 | SG: Low risk LG: Low risk | SG: 0 LG: −2 to –3 | SG: QD LG. QD | SG: Oral LG: Injected | Injection naive |
| Evans et al20 2013 | LG | LG: −1 to −1.5% SG: −0.5 to 1% | LG: 10%–15% feelings of sickness, 8%–15% diarrhea SG: No side effects | LG: −3.4 SG: No effect | LG: Low risk SG: Low risk | LG: Small reduction SG: No effect | LG: QD SG: QD | LG: Injected SG: Oral | Mixed |
| Jendle et al21 2012* | LG | LG: −1.1% RGL: −0.3% GLM: −0.7% INS: −0.9% EXN: −0.8% | LG: 4.1% RGL: 0.2% GLM: 0.8% INS: 0.1% EXN: 12.2% | LG: −1.5 RGL:+1.9 GLM:+1.04 INS:+1.5 EXN: −2.2 | LG: 0.2 RGL: 0.1 GLM: 1.3 INS: 1.4 EXN: 2.6 | LD: −2.5 RGL: −0.3 GLM:+0.41 INS:+1.6 EXN: −3.8 | LD: QD EX: Twice daily GL: OD RS: OD INS:MD | LD: Injected RGL: Oral GLM: Oral EXN: Injected INS: Injected | Mixed |
| Lüdemann et al22 2015† | VG | VG: −0.3% LG: −0.5% | VG: 15% LG: 37.5% | VG: −0.1 LG: −2.2 | ND | ND | VG: QD LG: QD | VG: Oral LG: Injected | Injection experienced |
| Poon et al23 2018 | DG | DG: 53.2% achieve HbA1c goal INS: 30.9% achieve HbA1c goal. | DG: Nausea 15.4% Pancreatitis 0.7% in first 18 months INS: Nausea 1.5%, Pancreatitis 0% | DG: −1.87 INS:+1.44 | DG: 5 events in 1 year INS: 8 events in 1 year | ND | DG: QW INS: MD | DG: Single prefilled pen ready. INS: Multiple dose prefilled pens, titration required. | Injection naive |
*Only listed nausea as an adverse effect, blood pressure change assessed as systolic blood pressure change.
†Attribute values are results from the cross-over trial.
BID, twice daily; DG, dulaglutide; EXN, exenatide; GLM, glimepiride; GLP-1 RA, glucagon-like peptide-1 receptor agonists; INS, insulin; LG, liraglutide; MD, multiple daily; ND, no data; OD, once daily; QD, once daily; QW, once weekly; RGL, rosiglitazone; SG, sitagliptin; VG, vildagliptin.
Glp-1 RA compared with DPP-4i
Three studies evaluated preferences between orally administered DPP-4i (sitagliptin and vildagliptin) and GLP-1 RA (liraglutide).19 20 22 Preference for DPP-4i in both injection naïve and experienced patients was observed in two out of three studies.19 22 Attributes ranked as the most important for choosing a DPP-4i over GLP-1 RA were its oral administration route and lesser frequency of side effects. For patients choosing GLP-1 RA, the most important attributes were blood sugar/HbA1c lowering effect and weight loss effect (table 4).
Table 4Drug preferences and attributes leading to preference among included studies
| Author, year | Drug preference (as measured) | Unit of measurement for drug attribute assessment | Scale | Attributes (attribute weight) |
| Boye et al24 2019 | Dulaglutide: 88.4% Semaglutide: 11.6% | Utility (95% CI) | 0–1 0=death 1=full health | Oral : 0.9 (0.89–0.91) oral+dulaglutide device : 0.89 (0.88–0.9) oral+semaglutide device : 0.88 (0.87–0.89) |
| Brooks et al25 2019 | Dulaglutide: 20% Semaglutide: 80% | Utility coefficient (SE) | 0 No Limit | Cardiovascular disease reduction: 1.08 (0.05) HbA1c reduction: 0.60 (0.07) avoidance of nausea: 0.55 (0.08) Method of administration: 0.05 (0.05) |
| Dibonaventura et al19 2010 | Sitagliptin: 84.4% Liraglutide: 15.6% | Ranked importance (SD) | 0 No limit | Effectiveness of medication (0.6% difference in HBA1c): 4.49 (0.84) Experience of prescribing Physician with medication: 4.11 (0.96) side effects: 3.92 (1.17) method of administration (oral vs injectable): 3.86 (1.23) Out-of-pocket costs of medication: 3.42 (1.43) |
| Evans et al20 2013 | Liraglutide: 62.5% Sitagliptin: 37.5% | Most important attribute according to preferred drug | 0%–100% | Liraglutide: weight loss, 61% sitagliptin: oral administration, 66% |
| Gelhorn et al27 2015 | Dulaglutide: 83.1% Liraglutide: 16.9% | Relative importance | 0%–100% | Dosing frequency: 41.6% type of delivery system: 35.5% frequency of nausea: 10.4% wt change: 5.9% HbA1c change: 3.6% low blood sugar events (hypoglycaemic): 3.0% |
| Gelhorn et al28 2016 | Dulaglutide: 94.5% Liraglutide: 5.5% | Relative importance | 0%–100% | Dosing frequency: 44.1%, type of delivery system: 26.3% frequency of nausea: 15.1% frequency of hypoglycaemic: 7.4% wt change: 6.2% HbA1c change: 1.0% |
| Hauber et al26 2015 | NA | Relative importance | 0 No limit | Weekly injection frequency (vs daily) shorter and thinner needle (vs longer and thicker) eliminating injection site reactions |
| Jendle et al21 2012 | Overall participants were willing to pay more for liraglutide compared with all other drugs. (twice daily EXN, RGL, GLI, INS) | Prepared to pay an extra Î/day for liraglutide | 0 No limit | Change in body weight RGL: 2.7, INS: 2.35, GLI: 1.87, EXN: −0.46 method of administration EXN:1.04, INS: 0.0, RGL: −1.3, GLI: −0.82 change in HBA1c RGL: 0.95, GLI: 0.43, EXN: 0.27, INS: 0.04 change in systolic BP: INS: 0.65, GLI: 0.46, RGL: 0.34, EXN: −0.2 nausea EXN: 0.08, GLI: −0.03, RGL: −0.04, INS: −0.04 hypoglycaemic rate: EXN: 0.07, GLI: 0.03, INS: 0.03, RGL: 0.0 |
| Lüdemann et al 22 2015 | Vildagliptin: 51.7% Liraglutide: 48.3% | Patient preference according to drug choice | 0% to 100% (Important and Very important.)§ | How you take the medication: VG: 71%, LG: 44.8% Side effects (nausea, vomiting and diarrhoea): VG: 67.8%, LG: 41.4% blood sugar lowering: VG: 77.4%, LG: 75.9% wt loss and blood pressure decrease: VG: 64.6%, LG: 65.5% |
| Matza et al29 2017 | NA | Health-State utility* | 0–1 0=death 1=full health | A: 0.88; B: 0.85; C: 0.86; D: 0.86; E: 0.87; F: 0.87; G: 0.87 |
| Matza et al31 2018a | NA | Health-State utility* | 0–1 0=death 1=full health | A: 0.9; B: 0.86; C: 0.87; D: 0.87; E: 0.88; F: 0.88; G: 0.8 |
| Matza et al30 2018b | Dulaglutide: 70.7%‡ Liraglutide: 22.4% ‡ | DID-PQ scores | Prefer/strongly prefer drug percentage 0% to 100% | Ease of fitting the injection: 72.1% DG ease preparing injection: 67.2% DG time to prepare: 67.2% DG confidence of using correctly: 65.5% DG ease of bringing injection device: 63.8% DG confidence injection: 60.3% DG needle size: 60.4% DG |
| Matza et al32 2020 | Dulaglutide: 84.2% Semaglutide: 12.3% | Patient preference | 0%–100% | Dulaglutide preference: device's ease of use 92.7%, reasons related to the needle 33.3%, ease of learning to use the device 17.6% liraglutide preference: device can be used multiple times 39.5%, ease of use 26.3%, less generation of plastic waste 26.3% |
| Polster et al33 2010 | Liraglutide: 0.97 (CI 0.96 to 0.98) Exenatide Twice daily: 0.94 (CI 0.92 to 0.955) | Relative Importance† (Health Utility) | 0%–100% | Efficacy: 39% (0.016) nausea: 30% (0.011) hypoglycaemic: 17% (0.006) dosing schedule: 14% (0.005) |
| Poon et al23 2018 | Dulaglutide: 75% Insulin glargine: 25% | Relative Importance | 0%–100% | Delivery system: 19.8 % GI effects: 18.2% dosing frequency: 17.7% wt change: 15.6% HbA1change: 14.2% frequency of pancreatitis: 12.3% frequency of hypoglycaemic: 2.2% |
| Qin et al34 2017a | Exenatide QW: 78.60% Liraglutide: 21.40% | OR (95% CI) | 0 No limit | Less side effects: 2.66 (2.51–2.82) Efficacy (<1.5 pts HbA1c): 2.57 (2.36–2.804) Once weekly dosing frequency: 2.25 (2.13–2.38) multiuse pen: 1.709 (1.55–1.88) needle size, device size and titration were not significant in patient’s preference |
| Qin et al35 2017b | Liraglutide: 21.40% Exenatide QW: 78.60% | OR (95% CI) | 0 No limit | Less side effects: 2.66 efficacy (<1.5 Hba1c): 2.57 weekly dosing frequency: 2.25 multiuse pen: 1.709 |
*VG: preferred vildagliptin; LG: preferre dliraglutide
†Definition of relative importance relativeimportance is calculated by dividing the difference in the average TTO utilityfor the best and worst levels for each attribute across all possible scenarios and across all respondents by the sum of those mean differences
‡Preference for overall ease of use
§Health state A: oral treatment only; health state B: reconstitution, waiting, needle handling; health state C: reconstitution,waiting; health state D: reconstitution, needle handling; health state E: reconstitution; health state F: needle handling; health state G: no inconveniences
¶
**Risk of pancreatitis considered in study profile for GLP-1 RA, we advise to take results with caution
BID, twice daily; DID-EQ, Diabetes Injection Device Experience Questionnaire; EXN, exenatide; GLI, glimepiride; INS, insulin glargine; QW, once weekly; RGL, rosiglitazone.
Insulin glargine compared with GLP-1 RA
Two studies evaluated preferences between liraglutide or dulaglutide and insulin glargine, both of them showed preference for GLP-1 RA.21 23 The first study found that 75% of participants preferred a dulaglutide profile when compared with insulin glargine where among patients who preferred the former, the most important reasons were type of delivery system and dosing frequency, with RI (proportion of the variance in the medication decision accounted by each attribute) of 24.5% and 19.2% for each attribute, respectively. Moreover, in patients who preferred insulin, most important reasons for choice were lesser frequency of gastrointestinal adverse effects (RI: 45.3%) and pancreatitis (RI: 26.5%).23 (table 4)
In the second study (willingness-to pay-analysis), participants were prepared to pay an extra €3.36/day for liraglutide over insulin glargine where weight change was the most important attribute leading to liraglutide preference (€2.35/day). In this study, liraglutide was presented as the best profile among all subdomains.21 The risk for hypoglycaemic was not an important attribute for patients’ preference in both studies.
Other glucose-lowering treatments compared with GLP1-RA
One study evaluated the preference for liraglutide and other oral treatments, including rosiglitazone and glimepiride. Participants were prepared to pay an extra €2.64 and €1.94/day for liraglutide over rosiglitazone and glimepiride, respectively. The main component for preference of liraglutide over both drugs was its weight loss effect. The only attribute which leads participants to pay more for rosiglitazone and glimepiride over liraglutide was the oral administration route.21
Different GLP-1 RA medications
Twelve studies evaluating preferences between different GLP-1 RA medications were included. Attributes that were included in these were related to dosing frequency and device type, but some also included efficacy, safety, and price as attributes. Drug profiles examined in these studies were extended release (weekly) and twice daily exenatide, once daily liraglutide and once weekly semaglutide and dulaglutide. Six of them were DCEs25–28 34 35 and four were TTOs.24 29 31 33 The remaining two were a questionnaire30 and a cross-over trial.32
Liraglutide versus exenatide
Four studies evaluated this comparison.21 33–35 Overall, participants preferred once daily liraglutide compared with twice daily exenatide. However, they preferred once weekly exenatide compared with once daily liraglutide.
One survey found that 96% of included participants preferred once daily liraglutide over twice daily exenatide, where liraglutide also was presented as the drug having better efficacy, less rates of nausea and hypoglycaemic.33 Two other surveys (one on injection naïve and the other on injection experienced users) reported that when assuming equal efficacy within both profiles (1.2 decreases in HbA1c), 78.6% of injection experienced users preferred once weekly exenatide compared with a profile matching liraglutide.34 Among injection-naïve participants, 77% preferred the profile matching exenatide.35 In both studies, attributes determining preference were better efficacy, lesser frequency of side effects and weekly dosing frequency. Moreover, even when efficacy was assumed to be better for liraglutide (1.2 vs 0.8 decrease in HbA1c), patients still preferred a weekly exenatide matching profile. (table 4) A willingness-to-pay analysis demonstrated that participants were willing to pay an extra €0.81/day for once daily liraglutide over twice daily exenatide where once daily administration (lesser dosing frequency) was the main component driving the preference (€1.04/day).21
Liraglutide versus dulaglutide
Three studies evaluated this comparison, one of them only compared device characteristics.27 28 30 A preference for dulaglutide was observed in all three.
In two studies, one in Japan and the other in the UK most of the population preferred the profile representing dulaglutide (94.5% and 83.1% for Japanese and UK population, respectively). Its profile consisted of a once weekly injection with a single-use prefilled pen compared with a once daily application with a multiuse pen that required dose titration for liraglutide. Slightly greater efficacy (reported difference in proportions of patients reaching treatment goals across groups was <3%), greater weight loss effect, and lesser frequency of nausea and hypoglycaemic were also attributes included on the dulaglutide profile. In both samples, the most important attributes for choosing a medication were dosing frequency (RI: 41.6%, 44.1% for the UK and Japanese population, respectively) and type of delivery system (RI: 35.5%, 26.3% for the UK and Japanese population, respectively)27 28 (table 4). In the third one, a survey comparing medication devices was applied on patients experienced to both treatments and revealed a preference for the dulaglutide device (table 4). In this case, participants’ preference was chosen based on their own experience.30
Dulaglutide versus semaglutide
Three studies evaluated this comparison where two of them evaluated device attributes24 32 and the other added clinical attributes to the drug profiles.25 Overall, among devices, participants preferred the one accompanying dulaglutide. When clinical attributes when considered in the drug profile, participants preferred semaglutide.
In a survey comparing device characteristics by providing hypothetical health states with each one, 88% of participants preferred the health state with the dulaglutide device over the semaglutide device, as the first one was considered ‘less complicated’ and ‘quicker’. Considering that the study exclusively analysed preferences regarding injection devices, no information regarding efficacy, side effects and price was assessed on either of the health states, assuming that they were all equal regarding these characteristics. Dulaglutide consisted of a one-dose injection with no needle handling and no dose adjustment. Patients who preferred semaglutide profile considered that a one-dose injection would make them ‘buy too many pens’.24 A cross-over trial comparing both injection devices found that 84.2% of participants preferred the dulaglutide profile, mainly due to its ‘ease of use’.32
In contrast, one study comparing both drugs using five attributes (method of administration, HbA1c change, reduction in cardiovascular (CV) risk, weight change and common side effects) reported that 80% of participants preferred the semaglutide profile, which was presented as the more efficient (1.9% vs 1.4% reduction in HbA1c), with greater weight loss effect, greater rate of nausea, 26% CV risk reduction (vs no risk reduction for dulaglutide), and with a multidose prefilled pen with dose adjustment (vs a single-dose prefilled pen with no dose adjustment representing dulaglutide). CV risk reduction followed by HBA1c reduction and rate of side effects were the most important attributes leading to their choice based on coefficient utilities25 (table 4).
Studies evaluating attributes of GLP-1 RA injection devices and administration regimes
Three studies fell into this category, none of which evaluated a specific drug profile; conversely, these studies evaluated patients’ preferences for injection devices based on different device attributes (table 4). One found that among a mixed population of injection naïve and injection experienced patients, changing injection frequency from daily to weekly was the most important attribute for choice of treatment.26 The other two found consistent main findings; each administration requirement (needle handling, reconstitution and waiting) was associated with higher disutilities when compared with an oral health state.29 31
Discussion
In this systematic review, we found no direct evidence to inform judgements about how patients with type 2 diabetes considering SGLT-2i and GLP-1 RA value established benefits on cardiovascular and kidney outcomes, weighed against harms and burdens of treatments. Taking this into account, several evidence evaluating preferences for GLP-1 RA was found where patients consistently showed resistance to injectables and complicated devices, preferring oral medications or weekly injected devices, which reflects on potential burdens of treatment likely to impact their treatment choices. However, these results demonstrate a major shortcoming of our systematic review; none of the studies presented patients with best current evidence on benefits and harms of these drugs, making any inferences about values and preferences of highly limited value as analysing the state of evidence on a certain medication at a specific point in time does not necessarily reflect the state of the same in the future with respect to it, therefore, treatment profiles could vary depending on the year in which the preference study was performed. Furthermore, studies defined efficacy of different drugs based on their glucose-lowering potential and for almost all did not assess patient-important microvascular or macrovascular outcomes.36
The evidence on burden of treatment serves as a reminder to guideline panels often restricting judgements of values and preferences to benefits and harms and clinicians leaving this factor out of the equation in assisting patients in making well-informed treatment choices.2 Indeed, the BMJ Rapid Recommendations put great emphasis on this evidence, directly impacting recommendations favouring SGLT-2i over GLP-1 RA.
This review has multiple strengths. We used of a previously validated search strategy to perform systematic reviews and meta-analysis of patients’ preferences studies. Additionally, we followed high methodological standards in conducting the review and evaluated each study’s quality with a specialised tool for patients’ preference studies and performed a further comprehensive analysis of the certainty of evidence by following the GRADE working group constructs. Finally, we considered the consistency of the evidence presented in the included studies to elicit patients’ preferences with the current best available evidence when drawing conclusions. This approach emphasised issues about the applicability of findings of this review to the BMJ Rapid Recommendations (Box 1).
We acknowledge there are several important limitations in our study. Our results are based mostly on studies graded at high risk of bias due to important methodological concerns. As a result, when assessing the certainty of evidence, all preferences in each drug comparison are graded at a very low certainty. More importantly, most of the included studies drew conclusions that could be influenced by conflict of interest. Moreover, there was no information regarding other important second-line treatments for diabetes such as SGLT-2i, therefore, we could not directly establish preferences between SGLT-2i and GLP-1 RA which would be very important due to both drugs’ increasing popularity among patients and clinicians. Some explanations on the absence of studies evaluating preferences for and among SGLT-2i could be that they are relatively new when compared with GLP-1 RA (the first SGLT-2i to be approved by the Food and Drug Administration was canagliflozin in 2013, compared with exenatide in 2005) and that as GLP-1 RA tend to have similar efficacy profiles, industry-based studies could have been carried out to assess preferences between treatments based on other attributes.
Overall, there is still not enough evidence to demonstrate a patient preference tendency between GLP-1 RA and SGLT-2i. Clinicians should individualise the use of these medications to each patient individual context, taking into consideration the best current evidence on efficacy and side effects all the while considering treatment burden, patient preferences, among other factors in the process of shared decision making. Furthermore, when opting to use GLP-1 RA, it would be optimal to consider weekly versions due to higher preferences observed for these in the present study.
Further studies are needed to elicit patients’ values and preferences among wider spectrum of oral and injectable diabetes treatments. There is a specific and urgent need to assess patient’s values and preferences between weekly injected GLP-1 RAs and all other classes of oral glucose-lowering medications including SGLT-2i. Furthermore, our review highlights the need for information about treatment efficacy based on systematic reviews rather than single studies. Additionally, our review findings emphasise the importance of standardising the way in which drug profiles are presented in values and preferences studies, where we suggest that attributes such as efficacy, side effects, mode of administration and dosage, cost, among other important variables to be constantly included in the building of drug profiles so that precise and trustworthy results are ensured.
Data availability statement
No additional data available.
Ethics statements
Patient consent for publication
Not required.
Contributors Conceiving of the research idea: JGG-G, RR-G, LL, RAM, SP, SL, QH and PV; First draft of the research protocol: JGG-G, ADG-C, JMM-A, RCS, NA-V, RR-G; Final version of the research protocol: all authors; Search strategy design: NA-V; Study selection process: JGG-G, ADG-C, JMM-A and RCS; Data extraction process: JGG-G, ADG-C, JMM-A and RCS; Data synthesis: JGG-G, ADG-C, JMM-A and RCS; First draft of the manuscript: JGG-G, ADG-C, JMM-A, RCS and RR-G; Final version of the manuscript: all authors.
Funding The authors have not declared a specific grant for this research from any funding agency in the public, commercial or not-for-profit sectors.
Competing interests All authors have completed the ICMJE uniform disclosure form at www.icmje.org/coi_disclosure.pdf and declare: JGG-G, ADG-C, JMM-A, LL, RCS, RAM, SP, SL, QH, NA-V, PV, RR-G: no support from any organisation for the submitted work; no financial relationships with any organisations that might have an interest in the submitted work in the previous three years. SL was supported by grants from the National Natural Science Foundation of China (grant number 21534008), Sichuan Science and Technology Program (grant number 2019YFH0150), and 1.3.5 Project for Disciplines of Excellence, West China Hospital, Sichuan University (grant number ZYGD18022 and 2020HXF011). But none of the grant contributes to this work.
Patient and public involvement statement The paper informs a Rapid Recommendation on the use of SGLT-2 inhibitors and GLP-1 receptor agonists that will be released on a digital platform (www.magicproject.org) and made available to organisations to adapt for their own materials and purposes.
Provenance and peer review Not commissioned; externally peer reviewed.
Supplemental material This content has been supplied by the author(s). It has not been vetted by BMJ Publishing Group Limited (BMJ) and may not have been peer-reviewed. Any opinions or recommendations discussed are solely those of the author(s) and are not endorsed by BMJ. BMJ disclaims all liability and responsibility arising from any reliance placed on the content. Where the content includes any translated material, BMJ does not warrant the accuracy and reliability of the translations (including but not limited to local regulations, clinical guidelines, terminology, drug names and drug dosages), and is not responsible for any error and/or omissions arising from translation and adaptation or otherwise.
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Details
; Lytvyn, Lyubov 3 ; Solis, Ricardo Cesar 2
; Mustafa, Reem A 4 ; Palmer, Suetonia C 5 ; Li, Sheyu 6 ; Qiukui Hao 7
; Alvarez-Villalobos, Neri Alejandro 2 ; Vandvik, Per Olav 8 ; Rodríguez-Gutiérrez, René 1
1 Plataforma INVEST Medicina UANL-KER Unit Mayo Clinic (KER Unit Mexico), Universidad Autonoma de Nuevo Leon Facultad de Medicina, Monterrey, Nuevo León, Mexico; Endocrinology Division, Department of Internal Medicine, Hospital Universitario Dr José Eleuterio González, Monterrey, Nuevo León, Mexico
2 Plataforma INVEST Medicina UANL-KER Unit Mayo Clinic (KER Unit Mexico), Universidad Autonoma de Nuevo Leon Facultad de Medicina, Monterrey, Nuevo León, Mexico
3 Department of Health Research Methods, Evidence, and Impact, McMaster University, Hamilton, Ontario, Canada
4 Internal Medicine, Division of Nephrology and Hypertension, University of Kansas Medical Center, Kansas City, Kansas, USA
5 Department of Medicine, University of Otago, Christchurch, Christchurch, New Zealand
6 Department of Endocrinology and Metabolism, West China Hospital, Sichuan University, Chengdu, Sichuan, China; Division of Population Health and Genomics, Ninewells Hospital and School of Medicine, University of Dundee, Dundee, UK
7 The center of Gerontology and Geriatrics, National Center for Geriatric Clinical Research, Sichuan University, Chengdu, Sichuan, China
8 Department of Medicine, Lovisenberg Diakonale Hospital, Oslo, Norway