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Promoters and Antagonists of Phagocytosis: A Plastic and Tunable Response
Annual Review of Cell and Developmental Biology ( IF 11.3 ) Pub Date : 2021-10-06 , DOI: 10.1146/annurev-cellbio-120219-055903
Spencer Freeman 1, 2 , Sergio Grinstein 1, 2
Affiliation  

Recent observations indicate that, rather than being an all-or-none response, phagocytosis is finely tuned by a host of developmental and environmental factors. The expression of key phagocytic determinants is regulated via transcriptional and epigenetic means that confer memory on the process. Membrane traffic, the cytoskeleton, and inside-out signaling control the activation of phagocytic receptors and their ability to access their targets. An exquisite extra layer of complexity is introduced by the coexistence of distinct “eat-me” and “don't-eat-me” signals on targets and of corresponding “eat” and “don't-eat” receptors on the phagocyte surface. Moreover, assorted physical barriers constitute “don't-come-close-to-me” hurdles that obstruct the engagement of ligands by receptors. The expression, mobility, and accessibility of all these determinants can be modulated, conferring extreme plasticity on phagocytosis and providing attractive targets for therapeutic intervention in cancer, atherosclerosis, and dementia.

中文翻译:


吞噬作用的启动子和拮抗剂:一种可塑性和可调的反应

最近的观察表明,吞噬作用不是一种全有或全无的反应,而是受到许多发育和环境因素的微调。关键吞噬决定簇的表达是通过转录和表观遗传手段调节的,这些手段赋予过程记忆。膜运输、细胞骨架和由内而外的信号传导控制吞噬受体的激活及其接近目标的能力。目标上不同的“吃我”和“不吃我”信号以及吞噬细胞表面上相应的“吃”和“不吃”受体共存,引入了一层精致的额外复杂性. 此外,各种物理障碍构成了“不要靠近我”的障碍,阻碍了受体与配体的结合。表情,流动性,

更新日期:2021-10-07
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