| Literature DB >> 26518356 |
James E Tooley1,2, Nalini Vudattu1,2, Jinmyung Choi3, Chris Cotsapas3, Lesley Devine4, Khadir Raddassi3, Mario R Ehlers5, James G McNamara6, Kristina M Harris5, Sai Kanaparthi5, Deborah Phippard5, Kevan C Herold1,2.
Abstract
The mechanisms whereby immune therapies affect progression of type 1 diabetes (T1D) are not well understood. Teplizumab, an FcR nonbinding anti-CD3 mAb, has shown efficacy in multiple randomized clinical trials. We previously reported an increase in the frequency of circulating CD8(+) central memory (CD8CM) T cells in clinical responders, but the generalizability of this finding and the molecular effects of teplizumab on these T cells have not been evaluated. We analyzed data from two randomized clinical studies of teplizumab in patients with new- and recent-onset T1D. At the conclusion of therapy, clinical responders showed a significant reduction in circulating CD4(+) effector memory T cells. Afterward, there was an increase in the frequency and absolute number of CD8CM T cells. In vitro, teplizumab expanded CD8CM T cells by proliferation and conversion of non-CM T cells. Nanostring analysis of gene expression of CD8CM T cells from responders and nonresponders versus placebo-treated control subjects identified decreases in expression of genes associated with immune activation and increases in expression of genes associated with T-cell differentiation and regulation. We conclude that CD8CM T cells with decreased activation and regulatory gene expression are associated with clinical responses to teplizumab in patients with T1D.Entities:
Keywords: Anti-CD3 mAb ⋅ CD8+ T cells ⋅ Immune therapy ⋅ Tolerance ⋅ Type 1 diabetes
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Year: 2015 PMID: 26518356 PMCID: PMC4882099 DOI: 10.1002/eji.201545708
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532