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L-精氨酸对T细胞受体CD3ζ链表达的调节

Regulation of T cell receptor CD3zeta chain expression by L-arginine.

作者信息

Rodriguez Paulo C, Zea Arnold H, Culotta Kirk S, Zabaleta Jovanny, Ochoa Juan B, Ochoa Augusto C

机构信息

Tumor Immunology Program, Stanley S. Scott Cancer Center and Department of Pediatrics, Louisiana State University, Health Sciences Center, New Orleans, Louisiana 70112, USA.

出版信息

J Biol Chem. 2002 Jun 14;277(24):21123-9. doi: 10.1074/jbc.M110675200. Epub 2002 Apr 11.

Abstract

L-Arg plays a central role in the normal function of several organ systems including the immune system. L-Arg can be depleted by arginase I produced by macrophages and hepatocytes in several disease states such as trauma and sepsis and following liver transplantation. The decrease in L-Arg levels induces a profound decrease in T cell function through mechanisms that have remained unclear. The data presented here demonstrate that Jurkat T cells cultured in medium without L-Arg (L-Arg-free RPMI) have a rapid decrease in the expression of the T cell antigen receptor zeta chain (CD3zeta), the principal signal transduction element in this receptor, and a decrease in T cell proliferation. This phenomenon is completely reversed by the replenishment of L-Arg but not other amino acids. These changes are not caused by cell apoptosis; instead, the diminished expression of CD3zeta protein is paralleled by a decrease in CD3zeta mRNA. This change in CD3zeta mRNA expression is not caused by a decrease in the transcription rate but rather by a significantly shorter CD3zeta mRNA half-life. This mechanism is sensitive to cycloheximide. Therefore, the regulation of L-Arg concentration in the microenvironment could represent an important mechanism to modulate the expression of CD3zeta and the T cell receptor and consequently of T cell function.

摘要

L-精氨酸在包括免疫系统在内的多个器官系统的正常功能中发挥着核心作用。在创伤、脓毒症等多种疾病状态以及肝移植后,巨噬细胞和肝细胞产生的精氨酸酶I可消耗L-精氨酸。L-精氨酸水平的降低通过尚不清楚的机制导致T细胞功能显著下降。此处呈现的数据表明,在无L-精氨酸的培养基(无L-精氨酸的RPMI培养基)中培养的Jurkat T细胞,其T细胞抗原受体ζ链(CD3ζ)的表达迅速下降,CD3ζ是该受体中的主要信号转导元件,同时T细胞增殖也减少。补充L-精氨酸可完全逆转这一现象,但补充其他氨基酸则不能。这些变化并非由细胞凋亡引起;相反,CD3ζ蛋白表达的减少与CD3ζ mRNA的减少平行。CD3ζ mRNA表达的这种变化不是由转录速率降低引起的,而是由CD3ζ mRNA半衰期显著缩短所致。这种机制对环己酰亚胺敏感。因此,调节微环境中L-精氨酸的浓度可能是调节CD3ζ和T细胞受体表达从而调节T细胞功能的重要机制。

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