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内皮细胞合成的细胞外基质对血管平滑肌细胞生长的调节

Regulation of vascular smooth muscle cell growth by endothelial-synthesized extracellular matrices.

作者信息

Herman I M, Castellot J J

机构信息

Department of Anatomy and Cellular Biology, Tufts University School of Medicine, Boston, Massachusetts 02111.

出版信息

Arteriosclerosis. 1987 Sep-Oct;7(5):463-9. doi: 10.1161/01.atv.7.5.463.

DOI:10.1161/01.atv.7.5.463
PMID:3675305
Abstract

Previous work has demonstrated that aortic endothelial cells (EC) produce a heparin-like inhibitor of smooth muscle cell (SMC) growth when both cell types were cultured on plastic. We have now tested the influence of the extracellular matrix on this EC-SMC interaction. Specifically, we examined: 1) the role of different substrates (plastic, fibronectin, monomeric, and fibrillar collagens I and III, and EC-derived matrices) on the growth rate and population density of SMC; 2) the heparin-sensitivity of SMC on these diverse substrates; and 3) the effect of these same substrates on EC ability to secrete heparin-like and polypeptide inhibitors of SMC growth. SMC demonstrated a sixfold difference in sensitivity to heparin when grown on different substrates, with the following rank order: EGTA matrix greater than collagens = plastic = fibronectin greater than deoxycholic acid (DOC) matrix. Maximally, we found a 10-fold difference in the potency of the inhibitory activity secreted by EC grown on different substrates, with the following order: plastic = EGTA matrix greater than fibronectin greater than collagens = DOC matrix. Treatment of the conditioned mediums with heparinase and trypsin indicated that 58% to 76% of the inhibitory activity was due to heparin-like species, and 24% to 42% was due to protein(s). When EC cultured on EGTA matrix are compared to those pleated on DOC matrix, the potency of the heparin-like and peptide inhibitory activities increased 8- and 17-fold, respectively. Hypothetically, one would predict a 60-fold change in the potency of the antiproliferative effect if the contributions of substrate to EC production of inhibitors and SMC sensitivity were additive.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

先前的研究表明,当主动脉内皮细胞(EC)和平滑肌细胞(SMC)在塑料培养皿上共同培养时,主动脉内皮细胞会产生一种类肝素的平滑肌细胞生长抑制剂。我们现在测试了细胞外基质对这种内皮细胞与平滑肌细胞相互作用的影响。具体而言,我们研究了:1)不同底物(塑料、纤连蛋白、单体及纤维状I型和III型胶原以及内皮细胞衍生基质)对平滑肌细胞生长速率和群体密度的作用;2)平滑肌细胞在这些不同底物上对肝素的敏感性;3)这些相同底物对内皮细胞分泌类肝素和平滑肌细胞生长多肽抑制剂能力的影响。平滑肌细胞在不同底物上生长时对肝素的敏感性有6倍差异,顺序如下:乙二醇双四乙酸(EGTA)基质>胶原=塑料=纤连蛋白>脱氧胆酸(DOC)基质。最大程度上,我们发现不同底物上生长的内皮细胞分泌的抑制活性效力有10倍差异,顺序如下:塑料=EGTA基质>纤连蛋白>胶原=DOC基质。用肝素酶和胰蛋白酶处理条件培养基表明,58%至76%的抑制活性归因于类肝素物质,24%至42%归因于蛋白质。将在EGTA基质上培养的内皮细胞与在DOC基质上培养的内皮细胞相比,类肝素和肽抑制活性的效力分别增加了8倍和17倍。假设底物对内皮细胞产生抑制剂和平滑肌细胞敏感性的影响是累加的,那么抗增殖作用的效力预计会有60倍的变化。(摘要截选至250词)

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