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母体微嵌合体:在1型糖尿病胰腺的胰岛素阳性区域增加,但在浸润性免疫细胞或增殖的胰岛细胞中未增加。

Maternal microchimerism: increased in the insulin positive compartment of type 1 diabetes pancreas but not in infiltrating immune cells or replicating islet cells.

作者信息

Ye Jody, Vives-Pi Marta, Gillespie Kathleen M

机构信息

Diabetes and Metabolism Unit, School of Clinical Sciences, University of Bristol, Bristol, United Kingdom.

Immunology Department, Institut de Recerca Germans Trias i Pujol, Carretera Canyet s/n, Badalona, Spain.

出版信息

PLoS One. 2014 Jan 31;9(1):e86985. doi: 10.1371/journal.pone.0086985. eCollection 2014.

Abstract

BACKGROUND

Maternal microchimeric cells (MMc) transfer across the placenta during pregnancy. Increased levels of MMc have been observed in several autoimmune diseases including type 1 diabetes but their role is unknown. It has been suggested that MMc are 1) effector cells of the immune response, 2) targets of the autoimmune response or 3) play a role in tissue repair. The aim of this study was to define the cellular phenotype of MMc in control (n = 14) and type 1 diabetes pancreas (n = 8).

METHODS

Using sex chromosome-based fluorescence in-situ hybridization, MMc were identified in male pancreas and their phenotype determined by concomitant immunofluorescence.

RESULTS

In normal pancreas, MMc positive for endocrine, exocrine, duct and acinar markers were identified suggesting that these cells are derived from maternal progenitors. Increased frequencies of MMc were observed in type 1 diabetes pancreas (p = 0.03) with particular enrichment in the insulin positive fraction (p = 0.01). MMc did not contribute to infiltrating immune cells or Ki67+ islet cell populations in type 1 diabetes.

CONCLUSION

These studies provide support for the hypothesis that MMc in human pancreas are derived from pancreatic precursors. Increased frequencies of MMc beta cells may contribute to the initiation of autoimmunity or to tissue repair but do not infiltrate islets in type 1 diabetes.

摘要

背景

孕期母源微嵌合细胞(MMc)会穿过胎盘。在包括1型糖尿病在内的几种自身免疫性疾病中,已观察到MMc水平升高,但其作用尚不清楚。有人提出,MMc可能是:1)免疫反应的效应细胞;2)自身免疫反应的靶标;3)在组织修复中发挥作用。本研究的目的是确定对照组(n = 14)和1型糖尿病胰腺组(n = 8)中MMc的细胞表型。

方法

利用基于性染色体的荧光原位杂交技术,在雄性胰腺中鉴定MMc,并通过同步免疫荧光确定其表型。

结果

在正常胰腺中,鉴定出了对内分泌、外分泌、导管和腺泡标记物呈阳性的MMc,这表明这些细胞源自母源祖细胞。在1型糖尿病胰腺中观察到MMc的频率增加(p = 0.03),在胰岛素阳性部分中尤其富集(p = 0.01)。在1型糖尿病中,MMc对浸润性免疫细胞或Ki67 +胰岛细胞群体没有贡献。

结论

这些研究为以下假设提供了支持,即人类胰腺中的MMc源自胰腺前体细胞。MMcβ细胞频率的增加可能有助于自身免疫的启动或组织修复,但在1型糖尿病中不会浸润胰岛。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2faf/3909047/0fe0520cdf4a/pone.0086985.g001.jpg

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