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单核细胞迁移至成人主动脉内皮细胞与平滑肌细胞共培养体系的内皮下间隙。

Monocyte migration into the subendothelial space of a coculture of adult human aortic endothelial and smooth muscle cells.

作者信息

Navab M, Hough G P, Stevenson L W, Drinkwater D C, Laks H, Fogelman A M

机构信息

Department of Medicine, University of California, Los Angeles School of Medicine 90024.

出版信息

J Clin Invest. 1988 Dec;82(6):1853-63. doi: 10.1172/JCI113802.

Abstract

Human aortic endothelial cells (EC) and smooth muscle cells (SMC) were isolated and used to form a multilayer of EC-SMC separated by a layer of collagen. SMC and/or collagen layers exerted minimal effects on Na+ transport but impeded the transport of LDL. The presence of an endothelial monolayer markedly reduced the transport of Na+ and LDL. When monocytes were presented to the complete coculture, in the absence of added chemoattractant, one monocyte entered the subendothelial space for every one to three EC present. In contrast, neither collagen nor SMC plus collagen nor EC plus collagen induced comparable monocyte migration. Despite massive migration of monocytes into the coculture, no significant alteration in Na+ transport was observed. LDL transport into the preparation during massive monocyte migration increased modestly, but this was far less than the amount of LDL transported in the absence of an endothelial monolayer. We conclude that (a) the endothelial monolayer was the principal permeability barrier, (b) a substantial migration of monocytes occurred in the absence of added chemoattractant when both EC and SMC were present in the coculture, (c) endothelial barrier function was largely maintained after monocyte migration; and (d) these experiments indicate the need to study all three cell types (monocytes, EC, and SMC) together to understand the complex interactions that occur between these cells.

摘要

人主动脉内皮细胞(EC)和平滑肌细胞(SMC)被分离出来,用于形成由一层胶原蛋白分隔的EC - SMC多层结构。SMC层和/或胶原蛋白层对Na⁺转运影响极小,但会阻碍低密度脂蛋白(LDL)的转运。内皮单层的存在显著降低了Na⁺和LDL的转运。当将单核细胞加入到完整的共培养体系中时,在未添加趋化因子的情况下,每存在一到三个EC,就有一个单核细胞进入内皮下间隙。相比之下,单独的胶原蛋白、SMC加胶原蛋白或EC加胶原蛋白均未诱导出类似的单核细胞迁移。尽管大量单核细胞迁移到共培养体系中,但未观察到Na⁺转运有明显改变。在大量单核细胞迁移过程中,LDL向该制剂中的转运略有增加,但这远低于在内皮单层不存在时LDL的转运量。我们得出以下结论:(a)内皮单层是主要的通透性屏障;(b)当共培养体系中同时存在EC和SMC时,在未添加趋化因子的情况下会发生大量单核细胞迁移;(c)单核细胞迁移后内皮屏障功能基本得以维持;(d)这些实验表明需要同时研究所有三种细胞类型(单核细胞、EC和SMC),以了解这些细胞之间发生的复杂相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/978a/442764/57020034e1d8/jcinvest00103-0062-a.jpg

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