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Restenosis and Therapy

机译:再狭窄和治疗

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摘要

The vascular disease involves imbalanced function of the blood vessels. Risk factors playing a role in development of impaired vessel functions will be briefly discussed. In ischemia/reperfusion (I/R), ischemic hypoxia is one of the cardinal risk factors of restenosis. Various insults are shown to initiate the phenotype switch of VSMCs. The pathological process, leading to activated inflammatory process, complement activation, and release of growth factors, initiate the proliferation of VSMCs in the media and cause luminal narrowing and impaired vascular function. The review summarizes the alteration process and demonstrates some of the clinical genetic background showing the role of complement and the genotypes of mannose-binding lectin (MBL2). Those could be useful markers of carotid restenosis after stent implantation. Gene therapy and therapeutic angiogenesis is proposed for therapy in restenosis. We suggest a drug candidate (iroxanadine), which ensures a noninvasive treatment by reverse regulation of the highly proliferating VSMCs and the disturbed function of ECs.
机译:血管疾病涉及血管功能失衡。将简要讨论在血管功能受损的发展中起作用的风险因素。在缺血/再灌注(I / R)中,缺血性缺氧是再狭窄的主要危险因素之一。显示了各种侮辱来启动VSMC的表型转换。病理过程导致激活的炎症过程,补体激活和生长因子的释放,引发血管平滑肌细胞在培养基中的增殖,并引起管腔狭窄和血管功能受损。该综述总结了这一改变过程,并证明了一些临床遗传背景,显示了补体的作用和甘露糖结合凝集素(MBL2)的基因型。这些可能是支架植入后颈动脉再狭窄的有用标志。提出基因治疗和治疗性血管生成用于再狭窄的治疗。我们建议使用一种药物候选物(iroxanadine),通过反向调节高度增殖的VSMC和EC的功能来确保无创治疗。

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