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β7整合素和其他细胞黏附分子在不同淋巴细胞群体中受到肿瘤坏死因子β的差异性表达和调控。

Beta 7 integrins and other cell adhesion molecules are differentially expressed and modulated by TNF beta in different lymphocyte populations.

作者信息

Ni J, Porter A G, Hollander D

机构信息

Department of Medicine, University of California, Irvine 92717.

出版信息

Cell Immunol. 1995 Apr 1;161(2):166-72. doi: 10.1006/cimm.1995.1023.

Abstract

To explore the role of beta 7 integrins subfamily and TNF beta in intestinal mucosal immunity and disease, we have examined the expression and modulation by TNF beta of beta 7 integrins and other cell adhesion molecules on mouse intestinal lymphocytes. Most of the small intestine intraepithelial lymphocytes (SIEL) and lamina propria lymphocytes (LPL) were M293 (beta 7) and M290 (alpha M290 beta 7) positive, whereas only 10-20% of SIEL and approximately 50% of LPL were R1-2 (alpha 4 beta 1/alpha 4 beta 7) positive. Only the expression of the R1-2 integrin was downregulated by TNF beta on SIEL. In contrast, expression of R1-2 was unaffected and expression of M290 was partially down-regulated by TNF beta on LPL. About 2-3% of spleen lymphocytes (SL) were M293, M290, and R1-2 positive, and on these cells expression of M290 (and M293) was strongly induced by TNF beta. CD45 expression was partially downregulated by TNF beta on SIEL, LPL, and SL, whereas the expression of ICAM-1 and CD45RB was upregulated by TNF beta only on SIEL. TNF beta strongly downregulated CD44 expression on SIEL, upregulated CD44 expression on LPL, and had no effect on CD44 on SL. These phenotypic differences and different responses to TNF beta modulation between SIEL, LPL, and SL may reflect differences in the microenvironments in which these cells reside and imply that SIEL and LPL may play different roles in intestinal immunity. Further, TNF beta may play an important role in regulating the function of beta 7 integrins and other cell adhesion molecules.

摘要

为探讨β7整合素亚家族和肿瘤坏死因子β(TNFβ)在肠道黏膜免疫及疾病中的作用,我们检测了TNFβ对小鼠肠道淋巴细胞上β7整合素及其他细胞黏附分子的表达及调节作用。大多数小肠上皮内淋巴细胞(SIEL)和固有层淋巴细胞(LPL)呈M293(β7)和M290(αM290β7)阳性,而只有10 - 20%的SIEL和大约50%的LPL呈R1 - 2(α4β1/α4β7)阳性。仅SIEL上的R1 - 2整合素表达受TNFβ下调。相反,LPL上R1 - 2的表达未受影响,而M290的表达受TNFβ部分下调。约2 - 3%的脾淋巴细胞(SL)呈M293、M290和R1 - 2阳性,TNFβ可强烈诱导这些细胞上M290(及M293)的表达。TNFβ可使SIEL、LPL和SL上的CD45表达部分下调,而ICAM - 1和CD45RB的表达仅在SIEL上受TNFβ上调。TNFβ可使SIEL上的CD44表达强烈下调,使LPL上的CD44表达上调,对SL上的CD44无影响。SIEL、LPL和SL之间的这些表型差异以及对TNFβ调节的不同反应可能反映了这些细胞所处微环境的差异,提示SIEL和LPL在肠道免疫中可能发挥不同作用。此外,TNFβ可能在调节β7整合素及其他细胞黏附分子的功能中起重要作用。

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