β Cell death and dysfunction during type 1 diabetes development in at-risk individuals
Kevan C. Herold, … , Jerry P. Palmer, the Type 1 Diabetes TrialNet Study Group
Kevan C. Herold, … , Jerry P. Palmer, the Type 1 Diabetes TrialNet Study Group
Published February 2, 2015
Citation Information: J Clin Invest. 2015;125(3):1163-1173. https://doi.org/10.1172/JCI78142.
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Clinical Medicine Clinical trials

β Cell death and dysfunction during type 1 diabetes development in at-risk individuals

Abstract

Role of the funding source: Funding from the NIH was used for support of the participating clinical centers and the coordinating center. The funding source did not participate in the collection or the analysis of the data.

BACKGROUND. The β cell killing that characterizes type 1 diabetes (T1D) is thought to begin years before patients present clinically with metabolic decompensation; however, this primary pathologic process of the disease has not been measured.

METHODS. Here, we measured β cell death with an assay that detects β cell–derived unmethylated insulin (INS) DNA. Using this assay, we performed an observational study of 50 participants from 2 cohorts at risk for developing T1D from the TrialNet Pathway to Prevention study and of 4 subjects who received islet autotransplants.

RESULTS. In at-risk subjects, those who progressed to T1D had average levels of unmethylated INS DNA that were elevated modestly compared with those of healthy control subjects. In at-risk individuals that progressed to T1D, the observed increases in unmethylated INS DNA were associated with decreases in insulin secretion, indicating that the changes in unmethylated INS DNA are indicative of β cell killing. Subjects at high risk for T1D had levels of unmethylated INS DNA that were higher than those of healthy controls and higher than the levels of unmethylated INS DNA in the at-risk progressor and at-risk nonprogressor groups followed for 4 years. Evaluation of insulin secretory kinetics also distinguished high-risk subjects who progressed to overt disease from those who did not.

CONCLUSION. We conclude that a blood test that measures unmethylated INS DNA serves as a marker of active β cell killing as the result of T1D-associated autoimmunity. Together, the data support the concept that β cell killing occurs sporadically during the years prior to diagnosis of T1D and is more intense in the peridiagnosis period.

TRIAL REGISTRATION. Clinicaltrials.gov NCT00097292.

FUNDING. Funding was from the NIH, the Juvenile Diabetes Research Foundation, and the American Diabetes Association.

Authors

Kevan C. Herold, Sahar Usmani-Brown, Tara Ghazi, Jasmin Lebastchi, Craig A. Beam, Melena D. Bellin, Michel Ledizet, Jay M. Sosenko, Jeffrey P. Krischer, Jerry P. Palmer

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Figure 2

β Cell death in progressors and nonprogressors to T1D in the PTP study followed for long periods of time.

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β Cell death in progressors and nonprogressors to T1D in the PTP study f...
(A) Comparison of the average levels (mean ± SEM) of unmethylated INS DNA (i.e., ratio of unmethylated/methylated INS DNA) in the at-risk progressors, nonprogressors, and healthy control subjects (HC) (P = 0.048, ANOVA; *P < 0.05, Bonferroni multiple comparison test). (B) All of the individual ratio measurements are shown for the at-risk progressors (n = 10, 49 measurements) and nonprogressors (n = 10, 56 measurements) and were compared with the average levels (n = 32, 62 measurements). Six measurements (of a total of 105) were unobtainable for technical reasons. The dashed line represents the mean + 2 SD of the nondiabetic control subjects. (C) The ISR AUC for the progressors and nonprogressors at the study visits over the observation period prior to the diagnosis of T1D in the progressors or the last study visit in the nonprogressors. The least-square mean ± SEM from the repeated-measures ANOVA is shown. Neither the 2 curves nor the individual time points differ significantly. (D) The relationship between the change in the ratio and the change in the ISR AUC (from the first study visit) is shown for the progressors and nonprogressors (progressors: Pearson correlation coefficient, r = –0.475, P = 0.0026; nonprogressors: P = NS). All of the data points are shown.