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氨基磷脂不对称性:生死攸关的问题。

Aminophospholipid asymmetry: A matter of life and death.

作者信息

Balasubramanian Krishnakumar, Schroit Alan J

机构信息

Department of Cancer Biology, The University of Texas M. D. Anderson Cancer Center, Houston, Texas 77030, USA.

出版信息

Annu Rev Physiol. 2003;65:701-34. doi: 10.1146/annurev.physiol.65.092101.142459. Epub 2002 May 1.

Abstract

Maintenance of membrane lipid asymmetry is a dynamic process that influences many events over the lifespan of the cell. With few exceptions, most cells restrict the bulk of the aminophospholipids to the inner membrane leaflet by means of specific transporters. Working in concert with each other, these proteins correct for sporadic incursions of the aminophospholipids to the outer membrane leaflet as a result of bilayer imbalances created by various cellular events. A shift in the relative contribution in each of these activities can result in sustained exposure of the aminophospholipids at the cell surface, which allows capture of the cells by phagocytes before the integrity of the plasma membrane is compromised. The absence of an efficient recognition and elimination mechanism can result in uncontrolled and persistent presentation of self-antigens to the immune system, with development of autoimmune syndromes. To prevent this, phagocytes have developed a diverse array of distinct and redundant receptor systems that drive the postphagocytic events along pathways that facilitate cross-talk between the homeostatic and the immune systems. In this work, we review the basis for the proposed mechanism(s) by which apoptotic ligands appear on the target cell surface and the phagocyte receptors that recognize these moieties.

摘要

维持膜脂不对称性是一个动态过程,在细胞的整个生命周期中影响着许多事件。除了少数例外,大多数细胞通过特定的转运蛋白将大部分氨基磷脂限制在内膜小叶上。这些蛋白质相互协同工作,纠正由于各种细胞事件导致的双层膜失衡而使氨基磷脂偶尔侵入外膜小叶的情况。这些活动中每一项相对贡献的变化都可能导致氨基磷脂在细胞表面持续暴露,这使得吞噬细胞在质膜完整性受损之前就能捕获细胞。缺乏有效的识别和清除机制可能导致自身抗原不受控制地持续呈递给免疫系统,从而引发自身免疫综合征。为了防止这种情况发生,吞噬细胞已经发展出了各种各样独特且冗余的受体系统,这些系统沿着促进稳态系统和免疫系统之间相互作用的途径驱动吞噬后事件。在这项工作中,我们综述了凋亡配体出现在靶细胞表面的假定机制以及识别这些部分的吞噬细胞受体的基础。

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