Fas and Fas Ligand Expression in Inflamed Islets in Pancreas Sections of Patients with Recent-onset Type I Diabetes Mellitus

Overview

Journal Diabetologia

Specialty Endocrinology

Date 1999 Nov 7

PMID 10550417

Citations 38

Authors

M Moriwaki

N Itoh

J Miyagawa

K Yamamoto

A Imagawa

K Yamagata

H Iwahashi

H Nakajima

M Namba

S Nagata

T Hanafusa

Y Matsuzawa

Affiliations

Soon will be listed here.

Abstract

Aims/hypothesis: Type I (insulin-dependent) diabetes results mainly from T-cell-mediated autoimmune destruction of pancreatic beta cells. Cytotoxic T lymphocytes destroy target cells via a perforin-based or Fas-based mechanism. Our previous study indicated that the Fas-Fas ligand (FasL) pathway is required for the development of autoimmune diabetes in the NOD mouse. We now investigated whether or not the Fas-FasL system is involved in the beta-cell destruction in human Type I diabetes.

Methods: We immunohistochemically analysed pancreas biopsy specimens of 13 recent-onset patients.

Results: Pancreatic islets were identified but showed various degrees of reduction in beta-cell volume in all patients. Out of 13 patients 6 had insulitis. In these 6 patients Fas was expressed in both the islets and infiltrating cells but not in either cell type in the 7 other patients without insulitis. Double immunostaining showed that Fas was positive in 92.2 to 97.7 % of beta cells but only in 17.6 to 46.7 % of alpha cells in Fas-positive, insulin-remaining islets. We found FasL was expressed exclusively in islet-infiltrating cells in patients with insulitis. Double immunostaining revealed that the most prevalent phenotype of FasL-positive cells was CD8, which was followed by macrophages and CD4.

Conclusion/interpretation: The interaction between Fas on beta cells and FasL on infiltrating cells might trigger selective apoptotic beta-cell death in inflamed islets, leading to immune-mediated Type I diabetes. [Diabetologia (1999) 42: 1332-1340]

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