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自噬在T细胞发育、激活和分化过程中的作用

Autophagy in T-cell development, activation and differentiation.

作者信息

Bronietzki Alisha W, Schuster Marc, Schmitz Ingo

机构信息

1] Systems-Oriented Immunology and Inflammation Research Group, Helmholtz Centre for Infection Research, Braunschweig, Germany [2] Institute for Molecular and Clinical Immunology, Otto-von-Guericke University, Magdeburg, Germany.

出版信息

Immunol Cell Biol. 2015 Jan;93(1):25-34. doi: 10.1038/icb.2014.81. Epub 2014 Oct 7.

Abstract

Autophagy is a vital catabolic process for degrading bulky cytosolic contents, which cannot be resorbed via the proteasome. First described as a survival mechanism during nutrient starvation conditions, recent reports have demonstrated that autophagy supports metabolic functions of T cells at various stages of maturation and effector function. Autophagy is crucial for T-cell development at the precursor stage as self-renewability and quiescence of hematopoietic stem cells depend on autophagy of the mitochondria and the endoplasmic reticulum. Later, during development in the thymus, autophagy regulates peptide presentation in stromal cells and professional antigen-presenting cells, which mediate thymocyte selection. Furthermore, the metabolic changes when mature T cells enter the periphery and when they are activated are both dependent on autophagy. Lastly, autophagy prevents early aging and, thus, ensures maintenance of memory T cells.

摘要

自噬是一种重要的分解代谢过程,用于降解无法通过蛋白酶体重新吸收的大量胞质内容物。自噬最初被描述为营养饥饿条件下的一种生存机制,最近的报道表明,自噬在T细胞成熟和效应功能的各个阶段都支持其代谢功能。自噬在前体阶段对T细胞发育至关重要,因为造血干细胞的自我更新能力和静止状态依赖于线粒体和内质网的自噬。随后,在胸腺发育过程中,自噬调节基质细胞和专职抗原呈递细胞中的肽呈递,介导胸腺细胞选择。此外,成熟T细胞进入外周以及被激活时的代谢变化均依赖于自噬。最后,自噬可防止过早衰老,从而确保记忆T细胞的维持。

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