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人类1型糖尿病中CD4 + T细胞特异性基因表达降低。

Reduced CD4+ T-cell-specific gene expression in human type 1 diabetes mellitus.

作者信息

Orban Tihamer, Kis Janos, Szereday Laszlo, Engelmann Peter, Farkas Klara, Jalahej Heyam, Treszl Andras

机构信息

Section of Immunology and Immunogenetics, Joslin Diabetes Center, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Autoimmun. 2007 Jun;28(4):177-87. doi: 10.1016/j.jaut.2007.01.002. Epub 2007 Feb 22.

Abstract

Type 1 diabetes mellitus (T1DM) in humans is characterized by the T-cell-dependent destruction of the insulin producing pancreatic beta cells; however, the precise pathogenesis of the disease, especially the initiation of pathologic immune response, is still largely unknown. We hypothesized that the function of human CD4+ T cells is altered in T1DM and analyzed unstimulated human peripheral blood CD4+ T-cell gene expression. We used a novel three-way comparison of DNA microarray data of CD4+ T cells isolated from patients with new onset T1DM, patients with long-term Type 2 diabetes (T2DM), and from healthy control subjects in order to eliminate any possible influence of glucose homeostasis on our findings. We analyzed the T1DM specific gene-expression changes and their functional relevance to T1DM autoimmunity. Our genetic and functional data show that T1DM CD4+ T cells are down-regulated specifically affecting key immune functions and cell cycle. Histone deacetylase gene expression, a key regulator of epigenetic modification is also reduced. The CD4+ T cells showed impaired function, including an abnormal immune response, which may be a key element that leads to the breakdown of self-tolerance.

摘要

人类1型糖尿病(T1DM)的特征是胰岛β细胞在T细胞依赖作用下被破坏;然而,该疾病的确切发病机制,尤其是病理性免疫反应的起始,在很大程度上仍不清楚。我们推测人类CD4 + T细胞的功能在T1DM中发生改变,并分析了未经刺激的人外周血CD4 + T细胞的基因表达。我们对从新发T1DM患者、长期2型糖尿病(T2DM)患者和健康对照者中分离出的CD4 + T细胞的DNA微阵列数据进行了新颖的三向比较,以消除葡萄糖稳态对我们研究结果的任何可能影响。我们分析了T1DM特异性基因表达变化及其与T1DM自身免疫的功能相关性。我们的基因和功能数据表明,T1DM CD4 + T细胞被下调,具体影响关键免疫功能和细胞周期。组蛋白脱乙酰酶基因表达,一种表观遗传修饰的关键调节因子,也降低了。CD4 + T细胞显示功能受损,包括异常免疫反应,这可能是导致自身耐受性破坏的关键因素。

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