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Beta cell-targeted PD-1 agonist inhibits cell-mediated autoimmunity in pancreas tissue slices.

Science advances 2026 Vol.12(14) p. eaec9029

Becker MW, Brown ME, Wiseman K, Chiodetti AL, Huber MK, Cuaycal AE, Sintara P, Ferreira SM, Smurlick D, Barra JM, Ladd AM, Drotar DM, Atkinson MA, Weber P, Al-Mossawi H, Russ HA, Mahon TM, Brusko TM, Bossi G, Phelps EA

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This research evaluates a therapeutic approach based on tissue-targeted immunomodulation with a potential broad application to treat autoimmune diseases including type 1 diabetes (T1D).

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BibTeX ↓ RIS ↓
APA Becker MW, Brown ME, et al. (2026). Beta cell-targeted PD-1 agonist inhibits cell-mediated autoimmunity in pancreas tissue slices.. Science advances, 12(14), eaec9029. https://doi.org/10.1126/sciadv.aec9029
MLA Becker MW, et al.. "Beta cell-targeted PD-1 agonist inhibits cell-mediated autoimmunity in pancreas tissue slices.." Science advances, vol. 12, no. 14, 2026, pp. eaec9029.
PMID 41920992

Abstract

This research evaluates a therapeutic approach based on tissue-targeted immunomodulation with a potential broad application to treat autoimmune diseases including type 1 diabetes (T1D). We generated a bispecific immune agonist that binds beta cells and suppresses autoreactive T cells. These bispecific molecules called immune modulating monoclonal-T cell receptor (TCR) against autoimmune disease (ImmTAAI), consist of a human-specific TCR-targeting domain fused with a programmed death-1 agonist. We used live pancreas slices to demonstrate targeting of ImmTAAI molecules to preproinsulin peptide-HLA-A2 complexes on human beta cells. ImmTAAI molecules protected beta cells from T cell killing by increasing T cell motility and inhibiting effector molecule and cytokine secretion. ImmTAAI treatment also increased the motility of islet-infiltrating T cells in slices from a donor with recent-onset T1D and preserved insulin secretion in slices cocultured with T cell avatars transduced with diabetogenic TCRs. These data demonstrate that ImmTAAI molecules have the potential to limit T cell activity locally, making this an attractive platform to elicit targeted immunoregulation in T1D.

MeSH Terms

Humans; Insulin-Secreting Cells; Autoimmunity; Programmed Cell Death 1 Receptor; Diabetes Mellitus, Type 1; Receptors, Antigen, T-Cell; T-Lymphocytes; HLA-A2 Antigen; Animals; Pancreas; Insulin

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