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人内皮细胞通过淋巴细胞功能相关抗原3(LFA-3)介导的mRNA稳定作用增强活化的CD4⁺T细胞中早期CD40配体的表达。

Human endothelial cells augment early CD40 ligand expression in activated CD4+ T cells through LFA-3-mediated stabilization of mRNA.

作者信息

Murakami K, Ma W, Fuleihan R, Pober J S

机构信息

Molecular Cardiobiology Program, Boyer Center for Molecular Medicine, Department of Pediatrics, Yale University School of Medicine, New Haven, CT 06510, USA.

出版信息

J Immunol. 1999 Sep 1;163(5):2667-73.

Abstract

Human endothelial cells (EC) augment CD40 ligand (CD40L) expression on PHA-activated CD4+ T cells at early times (e.g., 4-6 h). Fixed EC, devoid of mRNA, are comparable to living EC in their capacity to augment early CD40L expression on CD4+ T cells. Fixed EC increase T cell mRNA expression of both IL-2 and CD40L compared with PHA alone at 6 h. EC are unable to increase the rate of transcription of CD40L compared with PHA alone as measured with a promoter-reporter gene, although they do increase transcription of an IL-2 promoter-reporter gene. Fixed EC prolong the half-life of CD40L mRNA >2-fold. Inclusion of anti-human LFA-3 (CD58) mAb or pretreatment of EC with an LFA-3 antisense oligonucleotide blocks EC-induced increases in CD40L expression, whereas mAb to ICAM-1 or pretreatment with ICAM-1 antisense oligonucleotide does not. Moreover, mAb to LFA-3 reverses the capacity of EC to prolong the half-life of CD40L mRNA, whereas mAb to ICAM-1, even in combination with mAb to ICAM-2, does not. We conclude that EC use LFA-3 to increase early CD40L protein expression on newly activated CD4+ T cells by stabilizing CD40L mRNA.

摘要

人内皮细胞(EC)在早期(如4 - 6小时)可增强PHA激活的CD4⁺T细胞上CD40配体(CD40L)的表达。缺乏mRNA的固定化EC在增强CD4⁺T细胞早期CD40L表达的能力方面与活EC相当。与单独使用PHA相比,固定化EC在6小时时可增加T细胞中IL - 2和CD40L的mRNA表达。尽管固定化EC确实能增加IL - 2启动子 - 报告基因的转录,但与单独使用PHA相比,其无法增加CD40L启动子 - 报告基因所检测到的CD40L转录速率。固定化EC使CD40L mRNA的半衰期延长超过2倍。加入抗人LFA - 3(CD58)单克隆抗体或用LFA - 3反义寡核苷酸预处理EC可阻断EC诱导的CD40L表达增加,而抗ICAM - 1单克隆抗体或用ICAM - 1反义寡核苷酸预处理则无此作用。此外,抗LFA - 3单克隆抗体可逆转EC延长CD40L mRNA半衰期的能力,而抗ICAM - 1单克隆抗体,即使与抗ICAM - 2单克隆抗体联合使用,也不能。我们得出结论,EC通过稳定CD40L mRNA,利用LFA - 3增加新激活的CD4⁺T细胞上早期CD40L蛋白的表达。

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