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Ischaemic preconditioning: therapeutic implications for stroke?

机译:缺血预处理:对中风的治疗意义?

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摘要

Ischaemic preconditioning (IPC), also known as ischaemic tolerance (IT), is a phenomenon whereby tissue is exposed to a brief, sublethal period of ischaemia, which activates endogenous protective mechanisms, thereby reducing cellular injury that may be caused by subsequent lethal ischaemic events. The first description of this phenomenon was in the heart, which was reported by Murry and co-workers in 1986. Subsequent studies demonstrated IPC in lung, kidney and liver tissue, whereas more recent studies have concentrated on the brain. The cellular mechanisms underlying the beneficial effects of IPC remain largely unknown. This phenomenon, which has been demonstrated by using various injury paradigms in both cultured neurons and animal brain tissue, may be utilised to identify and characterise therapeutic targets for small-molecule, antibody, or protein intervention. This review will examine the experimental evidence demonstrating the phenomenon termed IPC in models of cerebral ischaemia, the cellular mechanisms that may be involved and the therapeutic implications of these findings.
机译:缺血预处理(IPC),也称为缺血耐受(IT),是组织暴露于短暂的亚致死短暂缺血期间的一种现象,它激活内源性保护机制,从而减少可能由随后的致死性缺血事件引起的细胞损伤。这种现象的最初描述是在心脏中,这是Murry及其同事在1986年报道的。随后的研究表明IPC在肺,肾和肝组织中起作用,而最近的研究则集中在大脑上。 IPC有益作用的细胞机制仍然未知。通过在培养的神经元和动物脑组织中使用各种损伤范例已证明了这种现象,该现象可用于识别和表征小分子,抗体或蛋白质干预的治疗靶标。这篇综述将研究实验证据,这些证据证明在脑缺血模型中称为IPC的现象,可能涉及的细胞机制以及这些发现的治疗意义。

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