Safety and Efficacy of Ranibizumab and Luseogliflozin Combination Therapy in Patients with Diabetic Macular Edema: Protocol for a Multicenter, Open-Label Randomized Controlled Trial

The “Effectiveness and safety of Combination therapy of ranibizumab and luseOgliflozin in type 2 diabetes with diabetic Macular Edema, a parallel group comparison with the standard Treatment controlled by glimepiride, multicenter, randomized, open-label trial” (COMET Trial) was initiated in April 2018 and is set to finish in September 2023. Subjects were enrolled from April 2018 and enrollment will finish in September 2021. As shown in Fig. 1, subjects who are eligible for anti-VEGF agents are asked to participate in this study, and informed consent is sought prior to the screening test. If subjects meet the eligibility criteria of this study during the screening test, they are enrolled and randomized into a study agent treatment group or a control group.

The aim of this study is to enroll 60 subjects (30 for the study agent treatment group and 30 for the control group). Because no previous studies have evaluated the effects of combination therapy with anti-VEGF agents and SGLT2 inhibitors, we referred to the results of a clinical trial of combination therapy with intravitreal anti-VEGF injection and navigated laser photocoagulation (laser + anti-VEGF group) vs monotherapy of intravitreal anti-VEGF injection (anti-VEGF monotherapy group) to calculate the sample size [21], in which the number of intravitreal anti-VEGF injections from baseline to week 48 was 3.9 ± 1.3 in the laser + anti-VEGF group and 6.9 ± 2.3 in the anti-VEGF monotherapy group. We assumed that the effects in the control group in this study would be comparable to the anti-VEGF monotherapy group of the previous study, and the effects in the study agent treatment group in this study would be slightly less than the laser + anti-VEGF group in the previous study (although the study agent treatment may reduce the overall number of intravitreal anti-VEGF injections). We set that superiority is achieved if the intergroup difference in the number of intravitreal anti-VEGF injections was two or more. Assuming that the number of intravitreal anti-VEGF injections from baseline to week 48 was 4.9 in the study agent treatment group and 6.9 in the control group, with a standard deviation of 2.5, the minimum sample size required to achieve a significance of 0.05 from a two-sided test with a statistical power of 80% was determined to be 26 subjects for both groups (a total of 52 subjects). To allow for a 10% dropout rate, the planned enrollment was set at 60 subjects, with 30 in each group.

Patients with T2DM and the complication of DME are asked to participate in this study. The detailed inclusion criteria were as follows: (1) patients with T2DM between 20 and 80 years of age at consent; (2) patients with DME which affects the fovea, and with best corrected visual acuity (BCVA) of 0.05 or higher (BCVA converted to logarithm of minimum angle of resolution, logMAR, of 1.30 or less); (3) patients with a central retinal thickness (CRT) in the study eye of 350 μm or more (measured by optical coherence tomography, OCT) at the screening test (if the CRT values of both eyes are 350 μm or more, the eye with the thicker retina is defined as the study eye); (4) patients with HbA1c of 6.5% or higher and less than 12.0% at the screening test; (5) patients with body mass index (BMI) of 18.5 kg/m² or higher at the screening test; (6) patients with estimated glomerular filtration rate (eGFR) of 30 mL/min/1.73 m² or higher at the screening test; (7) patients for whom DM treatment has not been changed in the 8 weeks preceding the screening test; (8) patients who provide a written consent form to participate in this study after full explanation of the study.

The exclusion criteria were as follows: (1) patients with type 1 DM; (2) patients with a history of hypersensitivity against SGLT2 inhibitor or glimepiride; (3) patients with a history of metabolic acidosis, or coma or precoma due to DM or hypoglycemia within the 24 weeks preceding the screening test; (4) patients with severe infections, before or after surgery, or severe trauma which requires insulin treatment; (5) patients with severe renal dysfunction (eGFR < 30 mL/ min/1.73 m²), or patients who are undergoing dialysis (including peritoneal dialysis); (6) female patients who are pregnant, possibly pregnant, or plan to be pregnant or breast-feeding; (7) patients with urinary tract infection or dehydration, or patients who are prone to urinary tract infection or dehydration; (8) patients with positive urinary ketone body (urine qualitative of 2+ or higher); (9) patients with a history of leg amputation due to leg gangrene; (10) patients with a history of bone fracture due to osteoporosis; (11) patients who were treated by thiazolidine, SGLT2 inhibitors, sulfonylurea, or glinide within 8 weeks preceding the screening test; (12) patients who were treated with fibrate or diuretic agents and who changed the usage or dose of them within 8 weeks preceding the screening test; (13) patients who had received systemic administration of steroid within 8 weeks preceding the screening test; (14) patients with a history of cerebrovascular impairment or myocardial infarction within 48 weeks preceding the screening test; (15) patients with poorly controlled hypertension (clinic blood pressure measured in sitting position is 180 mmHg or higher in systolic blood pressure or 100 mmHg or higher in diastolic blood pressure); (16) patients with a history of vitrectomy or scleral buckling; (17) patients with a history of filtration surgery to the study eye for glaucoma treatment, or patients who are expected to require filtration surgery in the future; (18) patients with active proliferative diabetic retinopathy in the study eye; (19) patients with a history of idiopathic or autoimmune uveitis in the study eye; (20) patients with vitreomacular traction syndrome or epi-retinal membrane in the study eye (as measured by slit lamp microscope or OCT) which affects central visual acuity; (21) patients with iris neovascularization, vitreous hemorrhage, or traction retinal detachment in the study eye; (22) patients with epi-retinal fibrosis in the study eye, which affects macular area; (23) patients with morphological impairment at the central area of macula lutea in the study eye which can affect the improvement of visual acuity after the disappearance of macular edema (including those with atrophy of retinal pigment epithelium, fibrogenesis or scarring under the retina, severe retina ischemia or structural hard exudate); (24) patients with a history of cataract surgery or other intraocular surgeries to the study eye within 12 weeks preceding the screening test; (25) patients with a history of panretinal laser or macular photocoagulation to the study eye within 12 weeks preceding the screening test; (26) patients with history of yttrium–aluminum-garnet laser posterior capsulotomy to the study eye within 4 weeks preceding the screening test; (27) patients who received steroid to the study eye or the study eye surroundings within 16 weeks preceding the screening test; (28) patients who received angiogenic inhibitor (pegaptanib, bevacizumab, ranibizumab, aflibercept, and others) to any eyes within 12 weeks preceding the screening test; (29) patients in which the transparency of optic media in the study eye is insufficient to obtain fundus or OCT images; (30) patients who received systemic administration of angiogenic inhibitor within 24 weeks preceding the screening test; (31) patients with complications other than diabetic macular edema, which may cause worsening of visual acuity requiring surgical intervention during the study period, or which can affect the study endpoints; (32) patients with any signs of infectious blepharitis, keratitis, scleritis, or conjunctivitis in any eyes; (33) patients with a history of hypersensitivity against anti-VEGF agent or fluorescein; (34) patients who used kallidinogenase or sairei-to (Chinese medicinal herbal drugs) within 8 weeks preceding the screening test; (35) patients with other conditions that the investigator/researcher thinks inappropriate for the study.

The informed consent document is offered to subjects who are eligible for anti-VEGF agent to provide a comprehensive explanation of this study. Written consent is then obtained, after which the screening test is conducted to check the eligibility of the subject for this study. Subjects who meet all of the inclusion criteria and do not fail any of exclusion criteria are enrolled in this study.

After informed consent is obtained, eligible subjects are randomly assigned in an approximately 1:1 ratio to the study agent treatment group or the control group. The randomization sequence was generated using a computer-based dynamic allocation method with a minimization procedure to balance three allocation factors (HbA1c, urinary albumin, and BCVA).

All enrolled subjects receive an intravitreal injection of 0.5 mg anti-VEGF agent (ranibizumab) at the start of the study. Within 7 days after the initial intravitreal ranibizumab injection, subjects assigned to the study agent treatment group and the control group begin treatment with either the study agent (luseogliflozin) or control agent (glimepiride), respectively. Luseogliflozin (2.5 mg) is administered to the subjects in the study agent treatment group once daily before or after breakfast. Glimepiride (0.5 mg) is administered to the subjects in the control group once daily before or after breakfast. These luseogliflozin and glimepiride doses are maintained until week 4. If HbA1c is 7.0% or higher at week 4, the dose of luseogliflozin is maintained in the study agent treatment group, while the dose of glimepiride is increased to 1 mg/day in the control group. If hypoglycemia (symptomatic hypoglycemia or plasma glucose of less than 70 mg/dL measured by self-measurement of blood glucose, SMBG) is observed from baseline to week 4, glimepiride is not increased. If HbA1c is 8.5% or higher at weeks 24–48, the dose of luseogliflozin is increased to 5 mg/day in the study agent treatment group, while the dose of glimepiride is increased to 2 mg/day in the control group. If hypoglycemia is observed during weeks 4 and 24, luseogliflozin and glimepiride are not increased. The dose of luseogliflozin or glimepiride can be reduced if researchers decide that a dose reduction is required because of the occurrence of hypoglycemia or other adverse events. All study subjects are observed every 4 weeks by an ophthalmologist.

Additional intravitreal ranibizumab injections are carried out if the subjects meet the following criteria: (1) CRT measured by OCT is more than 350 μm; (2) CRT measured by OCT increases more than 100 μm from the reference CRT obtained after enrollment to the study; (3) CRT measured by OCT increases relative to the previous observation point, and BCVA converted to logMAR decreases by 0.2 from the BCVA obtained after enrollment to the study. If the subjects meet any of the aforementioned criteria, ranibizumab is injected at a minimum of 3-week intervals. The combination therapy of ranibizumab and luseogliflozin/ glimepiride is continued to week 48. From week 48 to 52 (the post-observation period), the ranibizumab and luseogliflozin/glimepiride therapies are both discontinued. Observations are made at the time of screening (for the baseline) and then every 4 weeks until week 52 (after the initial intravitreal ranibizumab injection). Table 1 shows the schedule of assessments performed at each observation point, including mandatory and optional assessments.

The primary endpoint of this study is an intergroup difference in the number of intravitreal anti-VEGF injections to the study eye from baseline to week 48. Secondary and exploratory endpoints include ophthalmologic and internal medical clinical parameters. The details of the secondary and exploratory endpoints are summarized in Table 2.

A case report form is used for data collection. A central registration number is used to identify the subjects for anonymization.

Data collection and management is carried out by third-party entities to avoid bias. Data management is performed by Soiken Inc. Data Management Group (the data center). To manage and ensure quality, the study is monitored by the Soiken Inc. Monitoring Group. For additional data quality management, the principal investigator and Central Committee confirm the progress of the study as necessary through the Soiken Inc. Data Management Group to ensure conformance with the protocol and the Ethical Guidelines for Medical and Health Research Involving Human Subjects (Dec. 22, 2014; Ministry of Education, Culture, Sports, Science and Technology/Ministry of Health, Labour and Welfare) and the Clinical Trials Act (April. 14, 2017; Ministry of Education, Culture, Sports, Science and Technology/Ministry of Health, Labour and Welfare).

During this study, the investigators constantly monitor any adverse events (AEs) through regular medical checkups. All related AEs, not only side effects to the drugs but also abnormal clinical laboratory test values and any untoward medical occurrence, are reported and documented. Adverse events are followed up until normalization or recovery to a level not considered to be an adverse event, or until 4 weeks after the end of the pre-observation period or study discontinuation.

Primary, secondary, and exploratory efficacy endpoints will be analyzed using the full analysis set (FAS), and will include all subjects in each of the intervention groups. However, subjects with a severe protocol violation, such as registration without consent, or registration out of the enrollment period, or subjects without any baseline data, will be excluded from the FAS. Analysis using per protocol set (PPS) is to be conducted, if necessary, but will exclude subjects with a protocol violation, such as violation of eligibility criteria, use of prohibited or restricted concomitant drugs, or poor adherence to study agent or control agent (less than 75%). A safety analysis will be conducted on the safety analysis population, which will include all subjects in each of the intervention groups who received at least one dose of study agent or control agent.

No patients nor the general public will be involved in the planning, execution, analysis, and evaluation of the study.