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动脉损伤后细胞增殖的动力学。II. 肝素对平滑肌生长的抑制作用。

Kinetics of cellular proliferation after arterial injury. II. Inhibition of smooth muscle growth by heparin.

作者信息

Clowes A W, Clowes M M

出版信息

Lab Invest. 1985 Jun;52(6):611-6.

PMID:4040189
Abstract

Heparin inhibits intimal thickening after arterial injury. Whether this effect is due to inhibition of medial smooth muscle cell (SMC) migration, SMC proliferation in the intima, or synthesis and deposition of connective tissue has not been evident. In this study we have investigated these possibilities in a rat carotid balloon injury model. Heparin (0.3 mg/kg/hour) was administered intravenously by means of osmotic pumps to experimental animals, and controls received lactated Ringer's solution. Smooth muscle proliferation (thymidine index), intimal smooth muscle accumulation, and endothelial regeneration were measured at intervals between 0 and 28 days. Total smooth muscle growth as determined biochemically at 14 days was markedly inhibited by heparin if the pumps were placed 24 hours before or at the time of injury and less so if inserted 48 or 96 hours after injury. SMC thymidine indices were maximal in the media at 4 days and in the intima at 7 days for injured arteries of both heparin-treated and control rats; at each time point SMC proliferation and intimal thickening were less in heparin-treated rats. The volume of connective tissue in the intima was the same in both groups at 28 days. Medial SMC migration into the intima was diminished by heparin treatment, but endothelial regeneration was not affected. These results support the hypothesis that heparin is a specific inhibitor of SMC migration and proliferation and is most effective if started before SMC enter S-phase.

摘要

肝素可抑制动脉损伤后的内膜增厚。这种作用是否归因于对中膜平滑肌细胞(SMC)迁移、内膜中SMC增殖或结缔组织合成与沉积的抑制尚不明确。在本研究中,我们在大鼠颈动脉球囊损伤模型中探究了这些可能性。通过渗透泵向实验动物静脉注射肝素(0.3毫克/千克/小时),对照组接受乳酸林格氏液。在0至28天期间定期测量平滑肌增殖(胸腺嘧啶核苷指数)、内膜平滑肌积聚和内皮再生情况。如果在损伤前24小时或损伤时放置泵,肝素在14天时通过生化方法测定的总平滑肌生长受到显著抑制;如果在损伤后48或96小时插入泵,则抑制作用较小。对于肝素处理组和对照组大鼠的损伤动脉,SMC胸腺嘧啶核苷指数在第4天时在中膜最大,在第7天时在内膜最大;在每个时间点,肝素处理组大鼠的SMC增殖和内膜增厚程度均较小。两组在第28天时内膜中结缔组织的体积相同。肝素处理可减少中膜SMC向内膜的迁移,但不影响内皮再生。这些结果支持以下假说:肝素是SMC迁移和增殖的特异性抑制剂,且如果在SMC进入S期之前开始使用则最为有效。

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