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NIDDK Central Repository
Citation
Krischer, Jeffrey (2021). The Effects of Rituximab on the Progression of Type 1 Diabetes in New Onset Subjects (TN05) (Version 2) [Dataset] NIDDK Central Repository. https://doi.org/10.58020/1bv7-0y43
Data Availability Statement
Data from the The Effects of Rituximab on the Progression of Type 1 Diabetes in New Onset Subjects (TN05) [(Version 2) https://doi.org/10.58020/1bv7-0y43] reported here are available for request at the NIDDK Central Repository (NIDDK-CR) website, Resources for Research (R4R), https://repository.niddk.nih.gov/.
Acknowledgement Statement
This research was performed using resources generated by the Type 1 Diabetes TrialNet Study Group, a clinical trials network funded through a cooperative agreement by the National Institutes of Health (NIH) through the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), the National Institute of Allergy and Infectious Diseases (NIAID), the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD), and the Juvenile Diabetes Research Foundation (JDRF) and supplied by NIDDK Central Repository (NIDDK-CR). This manuscript was not prepared under the auspices of the TrialNet network and does not necessarily represent the opinions or views of TrialNet, NIDDK-CR, or NIH.
Data Package Version
Version 2 (Updated on: Feb 24, 2021)
Resource Availability
  • Data Available for Request
  • Specimens Require Collaboration with Parent Study
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General Description

Type 1 diabetes (T1D) is a chronic, slowly progressive autoimmune disease characterized by the destruction of β-cells in the pancreas. Although the presence of autoantibodies is a diagnostic criterion, the immunopathogenesis of β-cell destruction in T1D is typically associated with T-lymphocyte autoimmunity. B lymphocytes play a crucial role as antigen-presenting cells in the mechanism of T lymphocyte activation. The Effects of Rituximab on the Progression of Type 1 Diabetes in New Onset Subjects (TN05 antiCD20) is a randomized, placebo-controlled clinical trial that was established by TrialNet, a network of 18 clinical centers that conducts research on T1D, to test whether transient elimination of B lymphocytes with the anti-CD20 monoclonal antibody rituximab would decrease immune-mediated destruction of β-cells and thus preserve β-cell function in patients with T1D of recent onset.

Patients between the ages of 8 and 45 years who had T1D were screened for the presence of at least one type of detectable diabetes autoantibody (microinsulin autoantibody, glutamic acid decarboxylase 65, islet-cell antigen 512, or islet-cell autoantibody). Eligible patients were randomized to treatment with rituximab via intravenous infusion or placebo. The primary outcome measure was the mean area under the curve (AUC) for the stimulated C-peptide response during the first 2 hours of a 4-hour mixed-meal tolerance test conducted at 12 months, with the response expressed in picomoles per milliliter. Safety outcome measures included infusion reactions (occurring within 24 hours after an infusion), infections, and laboratory assessments of white-cell counts and immunoglobulin levels. Patients were followed for an additional year after evaluation of the primary outcome at 12 months.

Results showed that the mean AUC for the level of C peptide was significantly higher for the rituximab group than for the placebo group at 12 months. Additionally, the glycated hemoglobin level and the insulin dose were both significantly lower in the treatment group than in the placebo group. The group treated with rituximab showed higher rates of adverse events. Findings support the hypothesis that B lymphocytes play a role in the pathogenesis of T1D and that therapy targeting B cells may have a beneficial effect on β-cell function in early T1D. While initial improvements in C-peptide levels following rituximab administration resumed decline after 12 months, treatment with other anti-B-lymphocyte agents may open a new pathway for exploration in the treatment of patients with this condition.

Objectives

This study sought to determine to whether transient elimination of B lymphocytes with the anti-CD20 monoclonal antibody rituximab would decrease immune-mediated destruction of β-cells and thus preserve β-cell function in patients with T1D of recent onset.

Outcome Measure

The primary outcome measure was the mean area under the curve (AUC) for the stimulated C-peptide response during the first 2 hours of a 4-hour mixed-meal tolerance test conducted at 12 months, with the response expressed in picomoles per milliliter. Safety outcome measures included infusion reactions (occurring within 24 hours after an infusion), infections, and laboratory assessments of white-cell counts and immunoglobulin levels.

Eligibility Criteria

Patients between the ages of 8 and 45 years who met the following criteria were eligible for enrollment:

  • Diagnosis of type 1 diabetes within 3 months
  • Presence of at least one diabetes-related antibody (microinsulin autoantibody, glutamic acid decarboxylase 65, islet-cell antigen 512, or islet-cell autoantibody)
  • Stimulated C-peptide levels of at least 0.2 pmol/ml measure during a mixed meal tolerance test within one month of randomization
  • Had not received an immunization for at least 1 month

Exclusion criteria are documented in the study protocol.

Outcome

Results showed that the mean AUC for the level of C peptide was significantly higher for the rituximab group than for the placebo group at 12 months. Additionally, the glycated hemoglobin level and the insulin dose were both significantly lower in the treatment group than in the placebo group. These findings support the hypothesis that B lymphocytes play a role in the pathogenesis of T1D and that therapy targeting B cells may have a beneficial effect on β-cell function in early T1D. While initial improvements in C-peptide levels following rituximab administration resumed decline after 12 months, treatment with other anti-B-lymphocyte agents may open a new pathway for exploration in the treatment of patients with this condition.

Research Area

Diabetes

Study Type

Interventional

Study Sites

12

Study Start Date

2005-08

Study End Date

2009-11

Condition

Type 1 Diabetes Mellitus

Clinical Trials URL

http://www.clinicaltrials.gov/show/NCT00279305

Keywords

Diabetes Mellitus, Type 1, C Peptide, Rituximab

NIDDK Division

Division of Diabetes, Endocrinology, and Metabolic Diseases

126
Participants
Target Population
Children, Adults
Sex statistics is not available for this study
Location statistics is not available for this study

Public Documents Table
Document Name
Description
Document Type
File Format
Compliance
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Non-Public Documents (0)
There are currently no non-public documents available
Datasets (31)
Datasets Table
Dataset Name
Description
# of Records
# of Variables
File Format(s)
Diabetes Management Form (RIT09) Data
Diabetes Management form data indicating participant glucose, insulin, and hypoglycemia information863sas7bdat (1.38 MB); csv (113.17 KB)
Eligibility Form (RIT05) Data
Eligibility data indicating participant responses to inclusion/exclusion criteria117sas7bdat (321 KB); csv (12.26 KB)
Parent Survey
Participant parent survey data indicating information on participant health status and study experience 45sas7bdat (513 KB); csv (82.43 KB)
Physical Exam Form (RIT11) Data
Data collected on general physical exam performed on participant1164sas7bdat (4.88 MB); csv (207.99 KB)
Research Labs
Data collected on research labs indicating outcomes, results, and specimen names and collections31686sas7bdat (52.13 MB); csv (3.9 MB)
Participant Registration
Data collected on participant registration126sas7bdat (9 KB); csv (4.93 KB)
Participant Treatment Table
Data collected on participant treatments334sas7bdat (97 KB); csv (13.99 KB)
Pre-Randomization Exit Form (RIT01E)
Data collected on participant's ineligibility or withdrawal from the study39sas7bdat (33 KB); csv (2.94 KB)
Hepatitis A Administration Form (RIT18) Data
Data collected on participant Hepatitis A (H1N1) immunization status9sas7bdat (49 KB); csv (616 B)
Participant Survey
participant survey data indicating information on participant health status, study experience, and survey opinions72sas7bdat (641 KB); csv (79.23 KB)
Baseline Physical Exam Form (RIT03) Data
Baseline Physical Exam Form data indicating general examination information, tanner stage, and specimens to be drawn115sas7bdat (705 KB); csv (31.77 KB)
Study Drug Administration Form (RIT07)
Study drug administration data indicating participant medication experience information334sas7bdat (2.13 MB); csv (89 KB)
Neurologic Assessment Form (RIT22) Data
Neurologic assessment data indicating any abnormalities and completion of assessment404sas7bdat (201 KB); csv (43.65 KB)
CBC W/ Differential Results Transmittal Form (RIT99CB) Data
CDC w/ Differential test results indicating blood component composition1232sas7bdat (3.56 MB); csv (208.38 KB)
Adverse Event Review Data
Data collected on the review and outcome of reported adverse events18sas7bdat (257 KB); csv (1.39 KB)
Adverse Event Report Form (RIT13) Data
Adverse event report form data indicating report, general event, and severity information716sas7bdat (4.94 MB); csv (228.97 KB)
Concomitant Medications Form (RIT10) Data
Concomitant medications data indicating all information on study drugs taken by participants134sas7bdat (5.31 MB); csv (112.46 KB)
Baseline Medical History Form (RIT02) Data
Baseline Medical History Form data indicating Diabetes, autoimmune, vaccination, and other medical history and medications115sas7bdat (769 KB); csv (34.05 KB)
Diabetes Health Information
Diabetes Health Data indicating participant vital signs, and diabetes and vaccination history131sas7bdat (193 KB); csv (12.57 KB)
PHIX174 Administration Form (RIT19)
PhiX administration form data indicating vital signs and problems experienced during administration of PhiX174 immunization course322sas7bdat (385 KB); csv (18.57 KB)
Longterm Follow-Up Phase Authorization Data
Data collected on long-term follow-up phase authorization59sas7bdat (17 KB); csv (2.67 KB)
Follow-Up Visit Form (RIT12) Data
Follow-up visit data indicating new vaccinations, pregnancy monitoring, and specimens to be drawn943sas7bdat (4 MB); csv (128.67 KB)
Pregnancy Outcome Report Form (RIT14R) Data
Data collected on pregnancy outcome and infant information1sas7bdat (65 KB); csv (1.92 KB)
Protocol Deviation Form (RIT21) Data
Data collected on protocol deviation events188sas7bdat (4.41 MB); csv (52.25 KB)
Permanent Participant Site Transfer Form (RIT20) Data
Data collected on permanent participant site transfer form6sas7bdat (33 KB); csv (707 B)
Pregnancy Confirmation Form (RIT14) Data
Data collected on participant pregnancy confirmation indicating vital signs and health status of infant and participant3sas7bdat (65 KB); csv (696 B)
Change of Status Form (RIT15) Data
Data collected on change of participant's study status47sas7bdat (65 KB); csv (6.86 KB)
Missed Visit Form (RIT16) Data
Data collected on participant missed visit62sas7bdat (129 KB); csv (5.94 KB)
Dosing Vital Sign Monitoring Form (RIT08) Data
Data collected on vital sign monitoring during study drug dosing event325sas7bdat (705 KB); csv (81.11 KB)
Screening Form (RIT01)
Screening form data indicating participant informed consent, demographic information, medications, and specimens to be drawn213sas7bdat (904 KB); csv (36.58 KB)
Family History Form (RIT04) Data
Family history data indicating Type 1 Diabetes medical history for participant's first/second degree relatives115sas7bdat (577 KB); csv (14.44 KB)
Specimens (12,652)
Specimens Table
Specimen
Count
DNA221
PB-PBMC2584
Plasma5270
RNA1775
Serum2662
Supernatant134
Whole Blood6