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主动脉环模型中不同细胞类型对血管生成的旁分泌调节。

Paracrine regulation of angiogenesis by different cell types in the aorta ring model.

作者信息

Nicosia Roberto F, Zorzi Penelope, Ligresti Giovanni, Morishita Ann, Aplin Alfred C

机构信息

Veterans Administration Puget Sound Health Care System, Seattle, WA, USA.

出版信息

Int J Dev Biol. 2011;55(4-5):447-53. doi: 10.1387/ijdb.103222rn.

Abstract

The development of blood vessels during angiogenesis is the result of paracrine interactions between tube-forming endothelial cells and angiogenic factor-producing nonendothelial cells. This process can be reproduced and studied under chemically defined culture conditions by culturing vascular explants in three-dimensional gels of extracellular matrix. Rings of rat or mouse aorta cultured in collagen, fibrin or basement membrane gels produce angiogenic outgrowths composed of a mixed population of endothelial cells and nonendothelial cells. Aortic angiogenesis is regulated by endogenous angiogenic factors, inflammatory cytokines, chemokines, extracellular matrix molecules, and proteolytic enzymes produced by cells of the vessel wall in response to the injury of the dissection procedure. In this paper, we review how macrophages, mural cells and fibroblasts regulate different stages of the angiogenic process, from the formation of immature endothelial sprouts to the reabsorption of the neovessels. We also describe how aortic cultures can be used to study interactions between angiogenic outgrowths and nonvascular cell types such as bone marrow macrophages, platelets or cancer cells. Morphologic, genetic and functional studies of this model have provided invaluable information on how vessels form, mature, interact with nonvascular cell types, and are eventually reabsorbed. Further analysis of the paracrine cross-talk between aortic endothelial and nonendothelial cells is likely to provide new insights into the angiogenic process and its key mechanisms.

摘要

血管生成过程中血管的发育是形成管腔的内皮细胞与产生血管生成因子的非内皮细胞之间旁分泌相互作用的结果。通过在细胞外基质的三维凝胶中培养血管外植体,这个过程可以在化学定义的培养条件下重现并进行研究。在胶原蛋白、纤维蛋白或基底膜凝胶中培养的大鼠或小鼠主动脉环会产生由内皮细胞和非内皮细胞混合组成的血管生成性生长物。主动脉血管生成受内源性血管生成因子、炎性细胞因子、趋化因子、细胞外基质分子以及血管壁细胞因解剖操作损伤而产生的蛋白水解酶的调节。在本文中,我们综述了巨噬细胞、壁细胞和成纤维细胞如何调节血管生成过程的不同阶段,从未成熟内皮芽的形成到新生血管的重吸收。我们还描述了如何利用主动脉培养物来研究血管生成性生长物与非血管细胞类型(如骨髓巨噬细胞、血小板或癌细胞)之间的相互作用。对该模型的形态学、遗传学和功能研究为血管如何形成、成熟、与非血管细胞类型相互作用以及最终被重吸收提供了宝贵的信息。对主动脉内皮细胞和非内皮细胞之间旁分泌相互作用的进一步分析可能会为血管生成过程及其关键机制提供新的见解。

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