Title
Evaluation of Superiority of Valsartan+Celecoxib+Metformin Over Metformin Alone in Type 2 Diabetes Patients
A 26-week Single Site, Randomized, Double-blind, Active-controlled, Parallel Group, Human PoC Study to Evaluate Superiority of RK-01, Valsartan Plus Celecoxib Addon to Metformin Versus Metformin Alone in Type 2 Diabetes Patients
Phase
Phase 1/Phase 2Lead Sponsor
ARKAY TherapeuticsStudy Type
InterventionalStatus
Not yet recruitingIndication/Condition
Type 2 Diabetes High Blood Pressure Arthritis ObesityIntervention/Treatment
Metformin Val, Cel and Met XR Low [metformin (724), celecoxib (69001), valsartan (61401)] Val, Cel and Met XR High [metformin (724), valsartan (61401), celecoxib (69001)]Study Participants
115Evaluation of safety, tolerability and superiority of RK-01, a valsartan plus celecoxib dual add-on to metformin-HCL XR over metformin in newly diagnosed and obese adult type 2 diabetes patients with high blood pressure, arthritis and inadequate glycemic control with metformin monotherapy, diet and exercise over 26 weeks of treatment.
Objective: To assess effect of RK-01 on HbA1c levels, beta cell function and insulin resistance with co-administration of valsartan, celecoxib and metformin-HCl XR relative to metformin monotherapy.
Hypothesis: After 26 weeks of treatment with valsartan, celecoxib and metformin-HCl XR provides greater improvements in glycemic, inflammatory and atherogenic parameters compared to metformin monotherapy.
PRIMARY:
In patients with type 2 diabetes with inadequate glycemic control with metformin monotherapy:
Objective: To assess effect of RK-01 on HbA1c levels, beta cell function and insulin resistance with co-administration of valsartan, celecoxib and metformin-HCl XR relative to metformin monotherapy. Improvements in glycemic, inflammatory and atherogenic parameters including beta cell function relative to adult healthy volunteers with normal glucose tolerance (NGT) treated with placebo for 26 weeks will also be assessed. An interim study assessment will also be performed after 12 weeks of treatment.
Hypothesis: After 26 weeks of treatment with valsartan, celecoxib and metformin-HCl XR provides greater improvements in glycemic, inflammatory and atherogenic parameters compared to metformin monotherapy.
1000 mg metformin-HCL XR once-a-day or maintenance dose of metformin for 26 weeks
500 mg metformin-HCL XR plus 100 mg celecoxib once-a-day in the morning and 160 mg valsartan 6 hours later once-a-day in the afternoon for 26 weeks.
1000 mg metformin-HCL XR plus 200 mg celecoxib once-a-day in the morning and 320 mg valsartan once-a-day 6 hours later in the afternoon for 26 weeks.
Healthy adults with normal glucose tolerance (NGT) and beta cell function will be administered placebo.
Patients receive metformin once daily
Patients receive valsartan, celecoxib and metformin (low dose) once daily
Patients receive valsartan, celecoxib and metformin (high dose) once daily
Inclusion Criteria: Males and females, Age: >18 to 70 years at the time of screening visit. Women of childbearing potential (WOCBP) must have negative serum or urine pregnancy test (minimum sensitivity 25 IU/L or equivalent of HCG) within 24 hours prior to the start of the study. Women must not be breastfeeding. HbA1c≥8.0 Patients with inadequate blood glucose control with Metformin defined as a central laboratory glycosylated hemoglobin (HbA1c) >8.0 and <10.5 obtained at the screening visit. Metformin-HCl monotherapy was inadequate 3 months prior to the study as indicated by the lack of decrease and/or an increase in the A1c level. Newly diagnosed drug naïve patients as defined by HbA1c>7.0 at the screening visit. Drug naïve subjects diagnosed with type 2 diabetes within 6 months of diagnosis will be considered and selected. About half the patients are expected to be newly diagnosed in the study. Drug naive as well as osteoarthritis patients with Type 2 diabetes receiving a non-aspirin pain reliever (e.g. acetaminophen) or an NSAID (e.g. Naproxen). Max/maintenance dose Metformin. Subjects should have been taking the same daily dose of metformin for at least 8 weeks prior to the enrollment visit and subjects not receive these other antihyperglycemic medications within the 12 weeks prior to screening (except for short-term use of insulin [≤7 days] during concomitant illness or other stress). Patients with >25% AIRg at 2 minutes and 10 minutes. RAS blocker naïve patients 2-Hour OGTT ≥200 mg/dL FPG ≥140 mg/dL BMI ≥30 Impaired first phase and second phase of insulin secretion BP ≥140/90 mm Hg (These patients might be on an anti-hypertensive drug) Non-fasting laboratory glucose >200 mg/dL with symptoms of polydipsia, polyuria and/or Polyphagia eGFR ≥ 60 ml/min/1.73m2 Exclusion Criteria: Age >70 Patients with Type 1 diabetes, Screen for GAD (Glutamic acid decarboxylase) antibodies at the time of screening visit. To rule out latent autoimmune diabetes in adults (LADA), screening for other diabetes-related antibodies, such as insulinoma-associated protein (IA-2 and IA-2 beta), zinc transporter-8 (ZnT8), islet cell antibodies (ICA) or insulin autoantibody (IAA) will also be considered. Pregnant women Patients with a history of Ketoacidosis. Subjects at serious risk of gastrointestinal (GI) adverse events (e.g. current or recent history of GI bleeding ulceration, or perforation). Subjects with a planned radiologic study with intravenous contrast, surgery, or other planned procedures that may predispose them to metformin-associated lactic acidosis. Insulin dependent: <25% Beta-cell function: AIRg (Acute insulin response to glucose after 2 min and 10 min after glucose injection) INSULIN DEPENDENT STATE. Patients with a history of uncontrolled hyperglycemia >15.0 mmol/L (280 mg/dL) after an overnight fast that required rescue therapy. Patients with uncontrolled hyperglycemia >15.0 mmol/L (280 mg/dL) after an overnight fast that required rescue therapy during week 1-3 Metformin-HCl monotherapy or RK-01 therapy. eGFR, impaired kidney function < 60 ml/min/1.73m2. Poor metabolizers of Cyp450 2C9 to avoid very high concentration (Since Cytochrome 450 2C9 is responsible for the metabolism of both Valsartan and Celecoxib, patients who are known or suspected to be poor Cyp450 2C9 metabolizers based on previous history will be excluded from the study). Any of the following cardiovascular (CV)/Vascular diseases within 3 months of the enrollment visit: Myocardial infarction (MI) Cardiac surgery or revascularization (coronary artery bypass surgery, Coronary Artery Bypass Graft [(CABG]/Percutaneous transluminal coronary angioplasty (PTCA)]. Unstable angina Unstable congestive heart failure (CHF) Transient ischemic attack (TIA) or significant cerebrovascular disease Unstable or previously diagnosed arrhythmia Congestive heart failure, defined as New York Heart Association (NYHA) Class III and IV, unstable or acute heart failure and/or known left ventricular ejection fraction of ≤40%. Acute coronary syndrome, stroke or transient ischemic attack within 3 months prior to the informed consent. Previous bariatric surgery Treatment with anti-obesity drugs within 3 months prior to consent Patients with COPD Patients with liver disease Patients with renal disease Patients with autoimmune diseases e.g. Lupus, Psoriasis Patients with HIV/AIDS Patients with diabetes-related complications Patients with Hematological and Oncological Diseases/Conditions Hemoglobin <11.0 g/dL (110 g/L) for men; hemoglobin <10.0 g/dL (100 g/L) for women Patients with chronic disease e.g. Cancer, Epilepsy, Alzheimer, Parkinson, Asthma Abnormal free T4 Patients with serious infection
