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删除编码胰岛特异性葡萄糖-6-磷酸酶催化亚基相关蛋白的 G6pc2 基因不会影响 NOD/ShiLtJ 小鼠 1 型糖尿病的进展或发生率。

Deletion of the G6pc2 gene encoding the islet-specific glucose-6-phosphatase catalytic subunit-related protein does not affect the progression or incidence of type 1 diabetes in NOD/ShiLtJ mice.

机构信息

Department of Molecular Physiology and Biophysics, Vanderbilt University School of Medicine, Nashville, Tennessee, USA.

出版信息

Diabetes. 2011 Nov;60(11):2922-7. doi: 10.2337/db11-0220. Epub 2011 Sep 6.

DOI:10.2337/db11-0220
PMID:21896930
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3198073/
Abstract

OBJECTIVE

Islet-specific glucose-6-phosphatase catalytic subunit-related protein (IGRP), now known as G6PC2, is a major target of autoreactive T cells implicated in the pathogenesis of type 1 diabetes in both mice and humans. This study aimed to determine whether suppression of G6p2 gene expression might therefore prevent or delay disease progression.

RESEARCH DESIGN AND METHODS

G6pc2(-/-) mice were generated on the NOD/ShiLtJ genetic background, and glycemia was monitored weekly up to 35 weeks of age to determine the onset and incidence of diabetes. The antigen specificity of CD8(+) T cells infiltrating islets from NOD/ShiLtJ G6pc2(+/+) and G6pc2(-/-) mice at 12 weeks was determined in parallel.

RESULTS

The absence of G6pc2 did not affect the time of onset, incidence, or sex bias of type 1 diabetes in NOD/ShiLtJ mice. Insulitis was prominent in both groups, but whereas NOD/ShiLtJ G6pc2(+/+) islets contained CD8(+) T cells reactive to the G6pc2 NRP peptide, G6pc2 NRP-reactive T cells were absent in NOD/ShiLtJ G6pc2(-/-) islets.

CONCLUSIONS

These results demonstrate that G6pc2 is an important driver for the selection and expansion of islet-reactive CD8(+) T cells infiltrating NOD/ShiLtJ islets. However, autoreactivity to G6pc2 is not essential for the emergence of autoimmune diabetes. The results remain consistent with previous studies indicating that insulin may be the primary autoimmune target, at least in NOD/ShiLtJ mice.

摘要

目的

胰岛特异性葡萄糖-6-磷酸酶催化亚基相关蛋白(IGRP),现称为 G6PC2,是一种主要的自身反应性 T 细胞靶标,与小鼠和人类的 1 型糖尿病发病机制有关。本研究旨在确定抑制 G6p2 基因表达是否可以预防或延迟疾病进展。

研究设计和方法

在 NOD/ShiLtJ 遗传背景下生成 G6pc2(-/-) 小鼠,并每周监测血糖,直至 35 周龄,以确定糖尿病的发病和发生率。同时平行确定 12 周时来自 NOD/ShiLtJ G6pc2(+/+)和 G6pc2(-/-)小鼠胰岛内浸润的 CD8(+)T 细胞的抗原特异性。

结果

G6pc2 的缺失并不影响 NOD/ShiLtJ 小鼠 1 型糖尿病的发病时间、发生率或性别偏倚。两组的胰岛炎均很明显,但 NOD/ShiLtJ G6pc2(+/+)胰岛中含有对 G6pc2NRP 肽反应的 CD8(+)T 细胞,而 NOD/ShiLtJ G6pc2(-/-)胰岛中则不存在 G6pc2NRP 反应性 T 细胞。

结论

这些结果表明 G6pc2 是选择和扩增浸润 NOD/ShiLtJ 胰岛的胰岛反应性 CD8(+)T 细胞的重要驱动因素。然而,对 G6pc2 的自身反应并非自身免疫性糖尿病出现所必需的。这些结果与之前的研究结果一致,表明胰岛素可能是主要的自身免疫靶标,至少在 NOD/ShiLtJ 小鼠中是这样。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f45/3198073/5052ae473c2b/2922fig1.jpg

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