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血管壁中平滑肌细胞的迁移与增殖

[Migration and proliferation of smooth muscle cells in the vessel wall].

作者信息

Betz E

机构信息

Physiologisches Institut (I) der Universität Tübingen.

出版信息

Arzneimittelforschung. 1990 Mar;40(3A):362-5.

PMID:2185765
Abstract
  1. Intimal migration and proliferation causing artery stenoses in the course of atherogenesis can be inhibited by various drugs. 2. Secondary stenoses after ballooning of arteries are caused mainly by proliferation of smooth muscle cells. 3. Ballooning of arteries or repeated transmural electrical stimulations of artery walls with weak electrical current is followed by an increased mitotic activity of smooth muscle cells in the ballooned resp. stimulated area which reaches a maximal value about one week following the onset of the experiment. The mitotic activity returns then slowly to initial levels. 4. Adaptations to proliferation-inducing stimuli are possible. The experiments demonstrate that the proliferative phases in atherogenesis can be explained as a sequence of adaptations and deadaptations (= change of disposition) to the proliferation-inducing stimuli. 5. To select qualified drugs for an inhibition of the development of intimal proliferates in the course of atherogenesis makes it necessary to combine in vivo tests in animal experiments with tests on cell cultures of human cells from artery walls.
摘要
  1. 在动脉粥样硬化形成过程中,导致动脉狭窄的内膜迁移和增殖可被多种药物抑制。2. 动脉球囊扩张后的继发性狭窄主要由平滑肌细胞增殖引起。3. 动脉球囊扩张或用弱电流对动脉壁进行反复透壁电刺激后,球囊扩张或刺激区域的平滑肌细胞有丝分裂活性增加,在实验开始后约一周达到最大值。然后有丝分裂活性缓慢恢复到初始水平。4. 对增殖诱导刺激的适应是可能的。实验表明,动脉粥样硬化形成过程中的增殖阶段可解释为对增殖诱导刺激的一系列适应和去适应(= 易感性改变)。5. 为了选择在动脉粥样硬化形成过程中抑制内膜增殖发展的合格药物,有必要将动物实验中的体内试验与来自动脉壁的人类细胞的细胞培养试验相结合。

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