缺乏DNA拓扑异构酶3β的小鼠自身免疫性的发展

Development of autoimmunity in mice lacking DNA topoisomerase 3beta.

作者信息

Kwan Kelvin Y, Greenwald Rebecca J, Mohanty Subhasis, Sharpe Arlene H, Shaw Albert C, Wang James C

机构信息

Department of Molecular and Cellular Biology, Harvard University, 7 Divinity Avenue, Cambridge, MA 02138, USA.

出版信息

Proc Natl Acad Sci U S A. 2007 May 29;104(22):9242-7. doi: 10.1073/pnas.0703587104. Epub 2007 May 21.

DOI:10.1073/pnas.0703587104

PMID:17517607

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1890479/

Abstract

Mice lacking DNA topoisomerase 3beta are predisposed to a shortened lifespan, infertility, and lesions in multiple organs resulting from inflammatory responses. Examination of the immune system of 6- and 52-week-old top3beta(-/-) mice revealed no significant aberrations in their central and peripheral tolerance or in T lymphocyte activation. However, the older but not the younger cohort shows a high incidence of serum autoantibodies relative to their TOP3beta(+/+) age-mates. The mutant mice also show an increase in numerical aberrations of chromosomes in splenocytes and bone marrow cells, as well as an increase in apoptotic cells in the thymus. Thus, it appears plausible that the inflammatory lesions in top3beta(-/-) mice are caused by the development of autoimmunity as they age: Chromosomal abnormalities in top3beta(-/-) mice might lead to a persistent increase in apoptotic cells, which might in turn lead to the progression of autoimmunity.

摘要

缺乏DNA拓扑异构酶3β的小鼠易出现寿命缩短、不育以及由炎症反应导致的多器官损伤。对6周龄和52周龄的top3beta(-/-)小鼠的免疫系统检查发现，它们的中枢和外周耐受性以及T淋巴细胞激活均无明显异常。然而，与同龄的TOP3beta(+/+)小鼠相比，年龄较大而非较年轻的top3beta(-/-)小鼠血清自身抗体的发生率较高。突变小鼠的脾细胞和骨髓细胞中染色体数目畸变也有所增加，胸腺中的凋亡细胞也增多。因此，随着年龄增长，top3beta(-/-)小鼠的炎症损伤似乎是由自身免疫的发展引起的，这似乎是合理的：top3beta(-/-)小鼠的染色体异常可能导致凋亡细胞持续增加，进而可能导致自身免疫的进展。

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