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血管内爬行的巡逻单核细胞:独特搜索功能的 Lévy 样运动?

Intravascular Crawling of Patrolling Monocytes: A Lèvy-Like Motility for Unique Search Functions?

机构信息

Molecular Biomedicine Department, Centro de Investigaciones Biológicas Margarita Salas (CIB-CSIC), Madrid, Spain.

出版信息

Front Immunol. 2021 Sep 17;12:730835. doi: 10.3389/fimmu.2021.730835. eCollection 2021.

Abstract

Patrolling monocytes (PMo) are the organism's preeminent intravascular guardians by their continuous search of damaged endothelial cells and harmful microparticles for their removal and to restore homeostasis. This surveillance is accomplished by PMo crawling on the apical side of the endothelium through regulated interactions of integrins and chemokine receptors with their endothelial ligands. We propose that the search mode governs the intravascular motility of PMo in a similar way to T cells looking for antigen in tissues. Signs of damage to the luminal side of the endothelium (local death, oxidized LDL, amyloid deposits, tumor cells, pathogens, abnormal red cells, etc.) will change the diffusive random towards a Lèvy-like crawling enhancing their recognition and clearance by PMo damage receptors as the integrin αMβ2 and CD36. This new perspective can help identify new actors to promote unique PMo intravascular actions aimed at maintaining endothelial fitness and combating harmful microparticles involved in diseases as lung metastasis, Alzheimer's angiopathy, vaso-occlusive disorders, and sepsis.

摘要

巡逻单核细胞(PMo)通过不断地寻找受损的内皮细胞和有害的微粒,以将其清除并恢复体内平衡,从而成为机体最重要的血管内卫士。这种监测是通过 PMo 在血管内皮的顶端侧爬行来完成的,这是通过整合素和趋化因子受体与内皮配体的调节相互作用实现的。我们提出,搜索模式以类似于 T 细胞在组织中寻找抗原的方式控制 PMo 的血管内运动。内皮管腔侧受损的迹象(局部死亡、氧化 LDL、淀粉样沉积物、肿瘤细胞、病原体、异常红细胞等)将使扩散随机运动转变为类 Lévy 爬行运动,增强 PMo 损伤受体的识别和清除能力,如整合素 αMβ2 和 CD36。这种新视角可以帮助识别新的因子,以促进独特的 PMo 血管内作用,旨在维持内皮细胞的适应性,并对抗与疾病相关的有害微粒,如肺转移、阿尔茨海默病血管病、血管阻塞性疾病和败血症。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c50e/8485030/249223f4a4e5/fimmu-12-730835-g001.jpg

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