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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00975286
Other study ID # EFC10781
Secondary ID EudraCT : 2008-0
Status Completed
Phase Phase 3
First received September 10, 2009
Last updated April 9, 2014
Start date October 2009
Est. completion date August 2011

Study information

Verified date April 2014
Source Sanofi
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

The purpose of the study is to evaluate the benefits and risks of lixisenatide (AVE0010), in comparison to placebo, as an add-on treatment to insulin glargine and metformin with or without thiazolidinediones (TZDs), over a period of 24 weeks of treatment.

The primary objective is to assess the effects of lixisenatide in comparison to placebo, when added to insulin glargine and metformin, on glycemic control in terms of glycosylated hemoglobin (HbA1c) reduction (absolute change) at Week 24.

The secondary objectives are to assess the effects of lixisenatide on the percentage of patients reaching HbA1c less than (<) 7 percent (%) and less than or equal to (<=) 6.5%, plasma glucose (fasting, postprandial during a standardized meal challenge test, 7-point self monitored profiles), body weight, insulin glargine doses, to evaluate safety and tolerability (including anti-lixisenatide antibody assessment), and to assess the impact on treatment satisfaction using the Diabetes Treatment Satisfaction Questionnaire (state) (DTSQs) in the participating countries where it is validated.


Description:

The study comprises 3 periods:

- An up to 14-week screening period, which includes an up to 2-week screening phase and a 12-week run-in phase with introduction and titration of insulin glargine on top of metformin +/-TZDs.

- At the end of the run-in phase, patients whose HbA1c (centralized assay) is greater than or equal to (>=) 7% and less than or equal to (<=) 9% and whose mean fasting self-monitored plasma glucose (SMPG) calculated from the self measurements for the 7 days prior to Visit 12 (Week -1) is <=140 milligram per deciliter (mg/dL) (7.8 millimole per liter [mmol/L]), would enter a 24-week double-blind randomized treatment period comparing lixisenatide to placebo (on top of insulin glargine + metformin +/- TZDs).

- A 3-day safety follow up period.

Maximum duration is of 39 weeks +/- 7 days.


Recruitment information / eligibility

Status Completed
Enrollment 446
Est. completion date August 2011
Est. primary completion date August 2011
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion criteria:

- Type 2 diabetes mellitus, diagnosed for at least 1 year before screening visit, insufficiently controlled with insulin glargine and metformin

Exclusion criteria:

- HbA1c <7% or greater than (>)10% at screening

- At the time of screening age < legal age of majority

- Pregnant or breastfeeding women or women of childbearing potential with no effective contraceptive method

- Type 1 diabetes mellitus

- Metformin not at a stable dose of at least 1.5 gram per day for at least 3 months prior to the screening visit

- Use of oral or injectable antidiabetic or hypoglycemic agents other than metformin, sulfonylurea (SU) and TZDs (for example, alpha glucosidase inhibitor, other glucagon like peptide-1 [GLP-1] receptor agonists, dipeptidyl peptidase-IV [DPP-IV] inhibitors, insulin etc.) within 3 months prior to the time of screening, use of weight loss drugs if not at a stable dose for at least 3 months prior to the screening visit

- History of hypoglycemia unawareness

- Body Mass Index (BMI) less than or equal to (<=) 20 kilogram per square meter (kg/m^2)

- History of unexplained pancreatitis, chronic pancreatitis, pancreatectomy, stomach/gastric surgery, inflammatory bowel disease, personal or family history of medullary thyroid cancer (MTC) or genetic conditions that predispose to MTC (for example, multiple endocrine neoplasia syndromes)

- History of metabolic acidosis, including diabetic ketoacidosis within 1 year prior to screening

- Hemoglobinopathy or hemolytic anemia, blood or plasma products transfusion within 3 months prior to the time of screening

- Within the last 6 months prior to screening: history of myocardial infarction, stroke, or heart failure requiring hospitalization

- Known history of drug or alcohol abuse within 6 months prior to the time of screening

- Any clinically significant abnormality identified on physical examination, laboratory tests, electrocardiogram or vital signs at the time of screening that in the judgment of the Investigator or any sub investigator precludes safe completion of the study or constrains efficacy assessment such as active malignant tumor or other major systemic diseases, presence of clinically significant diabetic retinopathy or presence of macular edema likely to require laser treatment within the study period

- Uncontrolled or inadequately controlled hypertension at the time of screening with a resting systolic or diastolic blood pressure >180 millimeter of mercury (mmHg) or >110 mmHg, respectively

- Laboratory findings at the time of screening: amylase and/or lipase, alanine aminotransferase >3 times upper limit of the normal (ULN) laboratory range; total bilirubin: >1.5 times ULN (except in case of Gilbert's syndrome); hemoglobin <11 gram/deciliter and/or neutrophils <1500 per cubic millimeter (mm^3) and/or platelets <100 000/mm^3; positive test for Hepatitis B surface antigen and/or Hepatitis C antibody, positive serum pregnancy test in females of childbearing potential; and calcitonin >=20 picogram per milliliter (pg/mL) (5.9 picomole per milliliter [pmol/L])

- Patients who are considered by the Investigator or any sub investigator as inappropriate for this study for any reason (for example, impossibility to meet specific protocol requirements, such as scheduled visits, being able to do self-injections, likelihood of requiring treatment during the screening phase and treatment phase with drugs not permitted by the clinical study protocol, patient being investigator or any sub investigator, pharmacist, study coordinator, other study staff or relative thereof directly involved in the conduct of the protocol etc.)

- Use of systemic glucocorticoids (excluding topical application or inhaled forms) for one week or more within 3 months prior to the time of screening

- Use of any investigational drug within 3 months prior to screening

- Renal impairment defined with serum creatinine > 1.4 mg/dL in women and > 1.5 mg/dL in men

- History of hypersensitivity to insulin glargine or to any of the excipients

- Clinically relevant history of gastrointestinal disease associated with prolonged nausea and vomiting, including (but not limited to): gastroparesis, unstable (that is, worsening) and not controlled (that is, prolonged nausea and vomiting) gastroesophageal reflux disease requiring medical treatment, within 6 months prior to the time of screening

- Any previous treatment with lixisenatide (for example, participation in a previous study with lixisenatide)

- Allergic reaction to any GLP-1 receptor agonist in the past (for example, exenatide, liraglutide) or to metacresol

- Additional exclusion criteria during or at the end of the run-in phase before randomization: informed consent withdrawal (patient who was not willing to continue or failed to return), mean fasting SMPG calculated from the self-measurements for the 7 days prior to Visit 12 (Week -1) was >140 mg/dL (7.8 mmol/L) and HbA1c measured at Visit 12 (Week -1) is <7% or >9%, amylase and/or lipase > 3 times the ULN at Visit 12 (Week -1), patients with fasting plasma glucose (FPG) above the threshold value described for rescue (that is, FPG >240 mg/dL [13.3 mmol/L]), patients with any adverse event, which, by the judgment of the Investigator precludes the inclusion in the double-blind randomized treatment phase, and lack of compliance to protocol or to insulin glargine treatment during the run-in phase

Study Design

Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Lixisenatide (AVE0010)
Self administered by subcutaneous injections once daily within the hour preceding breakfast.
Placebo
Self administered by subcutaneous injections once daily within the hour preceding breakfast.
Insulin glargine
Dose to be adjusted to maintain a fasting SMPG between 100 and 80 mg/dL (5.6 and 4.4 mmol/L), inclusive.
Device:
Pen auto-injector
Lantus® SoloStar® OptiClik®
Drug:
Metformin
Metformin to be continued at stable dose (at least 1.5 gram per day) up to Week 24.
Thiazolidinedione (TZD)
TZD (either rosiglitazone or pioglitazone) if given, to be continued at stable dose up to Week 24.

Locations

Country Name City State
Argentina Sanofi-Aventis Investigational Site Number 032204 Buenos Aires
Argentina Sanofi-Aventis Investigational Site Number 032201 Capital Federal
Argentina Sanofi-Aventis Investigational Site Number 032205 Capital Federal
Argentina Sanofi-Aventis Investigational Site Number 032209 Capital Federal
Argentina Sanofi-Aventis Investigational Site Number 032211 Corrientes
Argentina Sanofi-Aventis Investigational Site Number 032202 Parana
Argentina Sanofi-Aventis Investigational Site Number 032203 Rosario
Brazil Sanofi-Aventis Investigational Site Number 076207 Belem
Brazil Sanofi-Aventis Investigational Site Number 076202 Brasilia
Brazil Sanofi-Aventis Investigational Site Number 076205 Porto Alegre
Brazil Sanofi-Aventis Investigational Site Number 076204 Sao Paulo
Canada Sanofi-Aventis Investigational Site Number 124219 Brampton
Canada Sanofi-Aventis Investigational Site Number 124213 Chatham
Canada Sanofi-Aventis Investigational Site Number 124208 Chilliwack
Canada Sanofi-Aventis Investigational Site Number 124215 Etobicoke
Canada Sanofi-Aventis Investigational Site Number 124205 Quebec
Canada Sanofi-Aventis Investigational Site Number 124202 Red Deer
Canada Sanofi-Aventis Investigational Site Number 124218 Thornhill
Canada Sanofi-Aventis Investigational Site Number 124201 Toronto
Canada Sanofi-Aventis Investigational Site Number 124207 Toronto
Canada Sanofi-Aventis Investigational Site Number 124209 Victoria
Canada Sanofi-Aventis Investigational Site Number 124217 Winnipeg
Chile Sanofi-Aventis Investigational Site Number 152201 Santiago
Chile Sanofi-Aventis Investigational Site Number 152202 Santiago
Chile Sanofi-Aventis Investigational Site Number 152203 Santiago
Chile Sanofi-Aventis Investigational Site Number 152204 Santiago
Chile Sanofi-Aventis Investigational Site Number 152205 Santiago
Chile Sanofi-Aventis Investigational Site Number 152206 Santiago
Colombia Sanofi-Aventis Investigational Site Number 170204 Barranquilla
Colombia Sanofi-Aventis Investigational Site Number 170201 Bogota
Colombia Sanofi-Aventis Investigational Site Number 170202 Bogota
Czech Republic Sanofi-Aventis Investigational Site Number 203202 Hradec Kralove
Czech Republic Sanofi-Aventis Investigational Site Number 203204 Praha 5
Denmark Sanofi-Aventis Investigational Site Number 208202 Frederiksberg
Denmark Sanofi-Aventis Investigational Site Number 208201 København Nv
Denmark Sanofi-Aventis Investigational Site Number 208205 Slagelse
Estonia Sanofi-Aventis Investigational Site Number 233201 Pärnu
Estonia Sanofi-Aventis Investigational Site Number 233203 Tallinn
Estonia Sanofi-Aventis Investigational Site Number 233204 Tartu
Estonia Sanofi-Aventis Investigational Site Number 233202 Viljandimaa
France Sanofi-Aventis Investigational Site Number 250204 Amiens Cedex 1
France Sanofi-Aventis Investigational Site Number 250206 La Rochelle Cedex
France Sanofi-Aventis Investigational Site Number 250203 Le Creusot
France Sanofi-Aventis Investigational Site Number 250201 Nantes
France Sanofi-Aventis Investigational Site Number 250202 Pierre Benite
Germany Sanofi-Aventis Investigational Site Number 276201 Dresden
Germany Sanofi-Aventis Investigational Site Number 276202 Mainz
Germany Sanofi-Aventis Investigational Site Number 276204 St. Ingbert-Oberwürzbach
Hungary Sanofi-Aventis Investigational Site Number 348205 Balatonfüred
Hungary Sanofi-Aventis Investigational Site Number 348202 Budapest
Hungary Sanofi-Aventis Investigational Site Number 348207 Budapest
Hungary Sanofi-Aventis Investigational Site Number 348204 Debrecen
Hungary Sanofi-Aventis Investigational Site Number 348206 Gyula
Hungary Sanofi-Aventis Investigational Site Number 348203 Szeged
Hungary Sanofi-Aventis Investigational Site Number 348201 Zalaegerszeg
India Sanofi-Aventis Investigational Site Number 356210 Ahmedabad
India Sanofi-Aventis Investigational Site Number 356202 Bangalore
India Sanofi-Aventis Investigational Site Number 356204 Bangalore
India Sanofi-Aventis Investigational Site Number 356206 Bangalore
India Sanofi-Aventis Investigational Site Number 356201 Belgaum
India Sanofi-Aventis Investigational Site Number 356205 Chennai
India Sanofi-Aventis Investigational Site Number 356208 Indore
India Sanofi-Aventis Investigational Site Number 356203 Karnal
India Sanofi-Aventis Investigational Site Number 356207 Kochi
India Sanofi-Aventis Investigational Site Number 356209 Nagpur
Israel Sanofi-Aventis Investigational Site Number 376202 Haifa
Israel Sanofi-Aventis Investigational Site Number 376201 Holon
Israel Sanofi-Aventis Investigational Site Number 376204 Kfar Saba
Israel Sanofi-Aventis Investigational Site Number 376203 Tel Hashomer
Italy Sanofi-Aventis Investigational Site Number 380201 Milano
Italy Sanofi-Aventis Investigational Site Number 380202 Perugia
Malaysia Sanofi-Aventis Investigational Site Number 458203 Kelantan
Malaysia Sanofi-Aventis Investigational Site Number 458202 Kuala Lumpur
Mexico Sanofi-Aventis Investigational Site Number 484201 Cuernavaca
Mexico Sanofi-Aventis Investigational Site Number 484204 Durango
Mexico Sanofi-Aventis Investigational Site Number 484203 Guadalajara
Mexico Sanofi-Aventis Investigational Site Number 484206 México City
Mexico Sanofi-Aventis Investigational Site Number 484205 Tlalnepantla
Netherlands Sanofi-Aventis Investigational Site Number 528203 Amsterdam
Netherlands Sanofi-Aventis Investigational Site Number 528202 Groningen
Netherlands Sanofi-Aventis Investigational Site Number 528204 Zwijndrecht
Poland Sanofi-Aventis Investigational Site Number 616202 Krakow
Poland Sanofi-Aventis Investigational Site Number 616208 Lubin
Poland Sanofi-Aventis Investigational Site Number 616206 Plock
Poland Sanofi-Aventis Investigational Site Number 616207 Pulawy
Poland Sanofi-Aventis Investigational Site Number 616205 Sopot
Poland Sanofi-Aventis Investigational Site Number 616201 Szczecin
Poland Sanofi-Aventis Investigational Site Number 616203 Zabrze
Puerto Rico Sanofi-Aventis Investigational Site Number 840226 Ponce
Puerto Rico Sanofi-Aventis Investigational Site Number 840216 San Juan
Romania Sanofi-Aventis Investigational Site Number 642204 Brasov
Romania Sanofi-Aventis Investigational Site Number 642208 Bucharest
Romania Sanofi-Aventis Investigational Site Number 642205 Deva
Romania Sanofi-Aventis Investigational Site Number 642203 Iasi
Romania Sanofi-Aventis Investigational Site Number 642202 Oradea
Romania Sanofi-Aventis Investigational Site Number 642206 Targu Mures
Romania Sanofi-Aventis Investigational Site Number 642201 Timisoara
Romania Sanofi-Aventis Investigational Site Number 642207 Timisoara
Russian Federation Sanofi-Aventis Investigational Site Number 643203 Saratov
Russian Federation Sanofi-Aventis Investigational Site Number 643202 St. Petersburg
South Africa Sanofi-Aventis Investigational Site Number 710202 Cape Town
South Africa Sanofi-Aventis Investigational Site Number 710201 Durban
South Africa Sanofi-Aventis Investigational Site Number 710203 Pretoria
Sweden Sanofi-Aventis Investigational Site Number 752204 Göteborg
Sweden Sanofi-Aventis Investigational Site Number 752203 Härnösand
Sweden Sanofi-Aventis Investigational Site Number 752205 Luleå
Sweden Sanofi-Aventis Investigational Site Number 752202 Malmö
Sweden Sanofi-Aventis Investigational Site Number 752201 Stockholm
Taiwan Sanofi-Aventis Investigational Site Number 158204 Changhua
Taiwan Sanofi-Aventis Investigational Site Number 158203 Taichung
Taiwan Sanofi-Aventis Investigational Site Number 158201 Taichung R.O.C.
Taiwan Sanofi-Aventis Investigational Site Number 158202 Tainan Hsien
Ukraine Sanofi-Aventis Investigational Site Number 804203 Chernivtsi
Ukraine Sanofi-Aventis Investigational Site Number 804201 Kiev
Ukraine Sanofi-Aventis Investigational Site Number 804202 Kyiv
Ukraine Sanofi-Aventis Investigational Site Number 804205 Kyiv
Ukraine Sanofi-Aventis Investigational Site Number 804204 Vinnytsya
United States Sanofi-Aventis Investigational Site Number 840211 Baton Rouge Louisiana
United States Sanofi-Aventis Investigational Site Number 840219 Brighton Michigan
United States Sanofi-Aventis Investigational Site Number 840229 Bristol Tennessee
United States Sanofi-Aventis Investigational Site Number 840215 Concord California
United States Sanofi-Aventis Investigational Site Number 840210 Dallas Texas
United States Sanofi-Aventis Investigational Site Number 840208 Fargo North Dakota
United States Sanofi-Aventis Investigational Site Number 840205 Germantown Tennessee
United States Sanofi-Aventis Investigational Site Number 840214 Greenbrae California
United States Sanofi-Aventis Investigational Site Number 840206 Hot Springs Arkansas
United States Sanofi-Aventis Investigational Site Number 840217 Houston Texas
United States Sanofi-Aventis Investigational Site Number 840228 Houston Texas
United States Sanofi-Aventis Investigational Site Number 840230 Hyattsville Maryland
United States Sanofi-Aventis Investigational Site Number 840201 Little Rock Arkansas
United States Sanofi-Aventis Investigational Site Number 840225 Mentor Ohio
United States Sanofi-Aventis Investigational Site Number 840223 Mesa Arizona
United States Sanofi-Aventis Investigational Site Number 840212 Mountain Home Arkansas
United States Sanofi-Aventis Investigational Site Number 840227 Norfolk Virginia
United States Sanofi-Aventis Investigational Site Number 840221 Orlando Florida
United States Sanofi-Aventis Investigational Site Number 840202 Philadelphia Pennsylvania
United States Sanofi-Aventis Investigational Site Number 840213 Plano Texas
United States Sanofi-Aventis Investigational Site Number 840222 Portland Oregon
United States Sanofi-Aventis Investigational Site Number 840209 Rockville Maryland
United States Sanofi-Aventis Investigational Site Number 840231 Sea Girt New Jersey

Sponsors (1)

Lead Sponsor Collaborator
Sanofi

Countries where clinical trial is conducted

United States,  Argentina,  Brazil,  Canada,  Chile,  Colombia,  Czech Republic,  Denmark,  Estonia,  France,  Germany,  Hungary,  India,  Israel,  Italy,  Malaysia,  Mexico,  Netherlands,  Poland,  Puerto Rico,  Romania,  Russian Federation,  South Africa,  Sweden,  Taiwan,  Ukraine, 

References & Publications (1)

Riddle MC, Forst T, Aronson R, Sauque-Reyna L, Souhami E, Silvestre L, Ping L, Rosenstock J. Adding once-daily lixisenatide for type 2 diabetes inadequately controlled with newly initiated and continuously titrated basal insulin glargine: a 24-week, rando — View Citation

Outcome

Type Measure Description Time frame Safety issue
Other Percentage of Patients With at Least 5% Weight Loss From Baseline at Week 24 The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 3 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Other Number of Patients With Symptomatic Hypoglycemia and Severe Symptomatic Hypoglycemia Symptomatic hypoglycemia was an event with clinical symptoms that were considered to result from a hypoglycemic episode with an accompanying plasma glucose less than 60 mg/dL (3.3 mmol/L) or associated with prompt recovery after oral carbohydrate, intravenous glucose, or glucagon administration if no plasma glucose measurement was available. Severe symptomatic hypoglycemia was symptomatic hypoglycemia event in which the patient required the assistance of another person and was associated with either a plasma glucose level below 36 mg/dL (2.0 mmol/L) or prompt recovery after oral carbohydrate, intravenous glucose, or glucagon administration, if no plasma glucose measurement was available. First dose of study drug up to 3 days after the last dose administration Yes
Primary Absolute Change From Baseline in Glycosylated Hemoglobin (HbA1c) at Week 24 Absolute change = HbA1c value at Week 24 minus HbA1c value at baseline. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 14 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in 2-Hour Postprandial Plasma Glucose (PPG) at Week 24 The 2-hour PPG test measured blood glucose 2 hours after eating a standardized meal. Change was calculated by subtracting baseline value from Week 24 value. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to the last dosing day of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in Glucose Excursion at Week 24 Glucose excursion = 2-hour PPG minus plasma glucose 30 minutes prior to the standardized meal test, before study drug administration. Change was calculated by subtracting baseline value from Week 24 value. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to the last dosing day of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in Average 7-Point Self Monitored Plasma Glucose (SMPG) Profile at Week 24 Patients recorded a 7-point plasma glucose profile measured before and 2 hours after each meal and at bedtime once in a week and the average value for the 7-time points was calculated. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to the last dosing day of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in Body Weight at Week 24 Change was calculated by subtracting baseline value from Week 24 value. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 3 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in Average Insulin Glargine Daily Dose at Week 24 Change was calculated by subtracting the baseline value from Week 24 value. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to the last dosing day of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Change From Baseline in Fasting Plasma Glucose (FPG) at Week 24 Change was calculated by subtracting baseline value from Wee 24 value. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 1 day after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
Secondary Percentage of Patients With Glycosylated Hemoglobin (HbA1c) Level Less Than 7% at Week 24 The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 14 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Week 24 No
Secondary Percentage of Patients With Glycosylated Hemoglobin (HbA1c) Level Less Than or Equal to 6.5% at Week 24 The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 14 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Week 24 No
Secondary Percentage of Patients Requiring Rescue Therapy During the Double-blind Period Routine fasting SMPG, central laboratory FPG and HbA1c values were used to determine the requirement of rescue medication. If fasting SMPG value exceeded the specified limit for 3 consecutive days, the central laboratory FPG and HbA1c were performed. Threshold values - from baseline to Week 8: fasting SMPG/FPG >200 milligram/deciliter (mg/dL) (11.1 mmol/L) or HbA1c >9%, from Week 8 to Week 24: fasting SMPG/FPG >180 mg/dL (10.0 mmol/L) or HbA1c >8.5%. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline up to Week 24 No
Secondary Change From Baseline in Treatment Satisfaction Score (Sum of Items 1, 4, 5, 6, 7 and 8 of DTSQ) at Week 24 Change was calculated by subtracting baseline value from Week 24 value. DTSQ: 8-item questionnaire to assess treatment satisfaction and patient perception of hyper and hypoglycemia. Each question (Q) scored on a Likert scale from 0 to 6. Six items (Q1 and 4-8; higher score = more satisfaction) measured treatment satisfaction and were summed to calculate treatment satisfaction score which ranged from 0 (very dissatisfied) to 36 (very satisfied). Two items (Q2 and 3), which were not included, measured perceived hyperglycemia and hypoglycemia, respectively and lower scores represented good perceived blood glucose control. The on-treatment period for this efficacy variable is the time from the first dose of study drug up to 3 days after the last dose of study drug or up to the introduction of rescue therapy, whichever is the earliest. For a patient to be included in mITT population, both baseline and at least 1 post baseline assessment for at least 1 efficacy variable, were required. Baseline, Week 24 No
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