This trial is active, not recruiting.

Conditions diabetes mellitus, type i, diabetes mellitus, insulin-dependent, 1, type 1 diabetes mellitus, insulin-dependent diabetes mellitus 1, iddm
Treatments imatinib mesylate, placebo (for imatinib mesylate)
Phase phase 2
Sponsor University of California, San Francisco
Collaborator Juvenile Diabetes Research Foundation
Start date January 2014
End date September 2017
Trial size 67 participants
Trial identifier NCT01781975, 17-2013-6


Type 1 diabetes mellitus (T1DM) results from the autoimmune destruction of insulin-producing ß cells. Although exogenous insulin is widely available, it is not possible for affected individuals to consistently achieve euglycemia with current technology, and thus they are at risk for devastating long-term complications. This phase II study is designed to evaluate the safety and efficacy of imatinib mesylate as a novel therapy for new-onset T1DM. Imatinib is a first-in-class tyrosine kinase inhibitor.

This study will explore the potential role of short-term therapy with imatinib to induce tolerance and possibly lead to a durable long-term remission of T1DM.

United States No locations recruiting
Other Countries No locations recruiting

Study Design

Allocation randomized
Endpoint classification safety/efficacy study
Intervention model parallel assignment
Masking double blind (subject, caregiver, investigator)
Primary purpose treatment
400 mg imatinib given once daily basis.
imatinib mesylate GLEEVEC
(Placebo Comparator)
Placebo given once daily basis.
placebo (for imatinib mesylate)

Primary Outcomes

Effect of treatment with imatinib versus placebo in individuals
time frame: Visit 9 (Week 52)

Secondary Outcomes

Mean area under the stimulated C-peptide curve (AUC) curve at 12 months
time frame: Visit 9 (Week 52)
Mean area under the stimulated C-peptide curve (AUC) over 4 hours at 24 months
time frame: Visit 13 (Week 104)
Change in HbA1c levels over time
time frame: Visit 9 (Week 52) and Visit 13 (Week 104)
Change in Insulin dose (units/kg) over time
time frame: Visit 9 (Week 52) and Visit 13 (Week 104)
Number of severe hypoglycemic events
time frame: Visit 0 (Week 0), Visit 9 (Week 52), and Visit 13 (Week 52)
Number and severity of adverse events
time frame: Adverse Events will be assessed at Visit 0 (week 0), Visit 1 (Week 2), Visit 2 (Week 4), and every month thereafter.

Eligibility Criteria

Male or female participants from 18 years up to 45 years old.

Inclusion Criteria: - Males and females age 12-45 years of age who meet the ADA standard T1DM criteria1. Positive for at least one islet cell autoantibody. Initial enrollment will be for subjects ages 18-45, with the goal to lower the age down to 12 upon acceptable safety review and prospect of benefit for this initial older cohort. - Diagnosis of T1DM within 100 days of Visit 0. - Peak stimulated C-peptide level >0.2 pmol/mL following an MMTT. - Participants of childbearing age who are sexually active must agree to use an effective form of birth control (e.g., barrier method, oral contraception, or surgery). For females, these contraceptive measures must be maintained throughout the study; for males these measures must be followed for a minimum of 3 months after discontinuation of imatinib therapy. Exclusion Criteria: - Prior history of any significant cardiac disease such as congestive heart failure, myocardial infarction, arrhythmia, or structural defects or suspicion thereof. - Leukopenia (<3,000 leukocytes/μL), neutropenia (<1,500 neutrophils/μL), or thrombocytopenia (<125,000 platelets/μL). - Low Hemoglobin (baseline hemoglobin below lower limit of normal) - Prior history of anaphylaxis, angioedema or serious cutaneous drug reactions - Any sign of significant chronic active infection (e.g., hepatitis, tuberculosis, EBV, CMV, or toxoplasmosis), or screening laboratory evidence consistent with a significant chronic active infection (such as positive for HIV, PPD, or HBSAg). Significant acute infections must be resolved before treatment may commence, e.g., acute respiratory tract, urinary tract, or gastrointestinal tract infections. - Anticipated ongoing use of diabetes medications other than insulin that affect glucose homeostasis, such as metformin, sulfonylureas, thiazolidinediones, glucagon-like peptide 1 (GLP-1) mimetics, dipeptidyl peptidase IV (DPP-IV) inhibitors, or amylin. - Prior or current treatment that is known to cause a significant, ongoing change in the course of T1DM or immunologic status, including high-dose inhaled, extensive topical or systemic glucocorticoids. - Evidence of liver dysfunction, with alanine aminotransferase (ALT) or aspartate aminotransferase (AST) >2.0 times the upper limit of normal persistent for 1 week or greater. - Evidence of renal insufficiency as indicated by serum creatinine > 1.2 times the upper limit of normal and confirmed in a repeat test at least one week apart. Evidence of clinically significant metabolic bone disease (except adequately treated rickets). - Females who are pregnant at the time of screening or unwilling to defer pregnancy during the 24-month study period. - Prior treatment with imatinib or related tyrosine kinase inhibitor. - Unable to avoid medications that affect CYP3A4: either inducers that may decrease imatinib levels, or inhibitors that may increase drug concentrations. (Refer to section for a complete list of inducers and inhibitors.) - Height standard deviation score ≥2 standard deviations below mean - Any sign of QT prolongation on Visit -1 noted on ECG (> 450 ms in males and > 470 ms in females) - Known coagulation disorders or use of anticoagulants - Current and anticipated on-going treatment with drugs that may increase or decrease imatinib plasma concentrations (CYP3A4 family inhibitors or inducers) or drugs that may have their plasma concentration altered by imatinib (drugs metabolized by CYP3A4/5 and CYP2D6). - Any condition that, in the investigator's opinion, may compromise study participation or may confound the interpretation of the study results.

Additional Information

Official title Safety and Efficacy of Imatinib for Preserving Beta-Cell Function in New-Onset Type 1 Diabetes Mellitus
Principal investigator Stephen E Gitelman, MD
Description Eligible participants will be randomized to receive either imatinib mesylate or placebo daily. All participants randomized into this study will be seen at a study site for a follow-up evaluation, 2 weeks and 4 weeks after randomization, and every month month thereafter for the first year. Participants will come in for a visit ever 6 months for the second year. At the study visits, participants will undergo assessments of their insulin production, immunologic status, and overall health. Subjects will be followed until the conclusion of the study. The trial is expected to last approximately 2-4 years or until the required amount of information is gathered.
Trial information was received from ClinicalTrials.gov and was last updated in July 2016.
Information provided to ClinicalTrials.gov by University of California, San Francisco.