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A new concept of development of neointimal hyperplasia

机译:新生增生的新概念

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The intima hyperplasia is a major morphological feature of various arterial pathologies such as atherosclerosis, postangioplasty restenosis and transplantation arteriopathy. It is commonly assumed that smooth muscle cells (SMC) comprising loci of the intima hyperplasia originate from arterial media. However, recent studies suggest that the bone marrow could also supply circulating vascular progenitor of SMCs and endothelial cells (EC). Such bone marrow progenitors participate in the formation of a cellular mass of neointima after experimental allotransplantation, mechanical vessel injury or hyperlipidemia induced experimental atherosclerosis. Circulating SMC and EC progenitors are also likely to be involved in the transplantation arteriopathy development in humans but their roles in the atherosclerosis and restenosis remain to be determined. Stages of the mobilization, defferentiation and proliferation of SMC progenitors could provide point of attack for new therapeutic strategies for the treatment of proliferative vascular diseases. The precise understanding of the neointima cells origin could provide a key for development of the optimal therapeutic strategy of treatnent of such disorders. This review is focused on the pathological significance of circulating progenitors of the bone marrow origin, particularly on the SMC progenitors, for development of vascular wall disorders.
机译:Intima增生是各种动脉病理学的主要形态学特征,如动脉粥样硬化,破旧的后成形术再狭窄和移植动脉病变。通常假设含有Intima增生的表位的平滑肌细胞(SMC)源自动脉介质。然而,最近的研究表明,骨髓也可以提供SMC和内皮细胞(EC)的循环血管祖。这种骨髓祖细胞参与在实验同种异体持续,机械损伤或高脂血症诱导的实验动脉粥样硬化后形成细胞瘤的细胞质量。循环的SMC和EC祖细胞也可能参与人类的移植动脉病变,但它们在动脉粥样硬化和再狭窄中的作用仍有待确定。 SMC祖细胞的动员,脱模和增殖的阶段可以为治疗增殖血管疾病的新治疗策略提供攻击点。确切理解新内膜细胞来源可以为这种疾病治疗的最佳治疗策略的发展提供键。本综述专注于骨髓原产地循环祖细胞的病理意义,特别是在SMC祖细胞上,用于血管壁障碍的发展。

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