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Pathologies Associated with the p53 Response

机译:与p53反应相关的病理

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摘要

Although p53 is a major cancer preventive factor, under certain extreme stress conditions it may induce severe pathologies. Analyses of animal models indicate that p53 is largely responsible for the toxicity of ionizing radiation or DNA damaging drugs contributing to hematopoietic component of acute radiation syndrome and largely determining severe adverse effects of cancer treatment. p53-mediated damage is strictly tissue specific and occurs in tissues prone to p53-dependent apoptosis (e.g., hematopoietic system and hair follicles); on the contrary, p53 can serve as a survival factor in tissues that respond to p53 activation by cell cycle arrest (e.g., endothelium of small intestine). There are multiple experimental indications that p53 contributes to pathogenicity of acute ischemic diseases. Temporary reversible suppression of p53 by small molecules can be an effective and safe approach to reduce severity of p53-associated pathologies.
机译:尽管p53是主要的癌症预防因子,但在某些极端压力条件下,它可能会导致严重的病理。对动物模型的分析表明,p53对造成急性放射综合症的造血成分的电离辐射或DNA损伤药物的毒性负主要责任,并在很大程度上决定了癌症治疗的严重不利影响。 p53介导的损伤严格是组织特异性的,并发生在倾向于p53依赖的细胞凋亡的组织中(例如造血系统和毛囊);相反,p53可以作为通过细胞周期停滞对p53激活作出反应的组织(例如小肠内皮)中的存活因子。有多种实验迹象表明,p53有助于急性缺血性疾病的致病性。小分子对p53的暂时可逆性抑制可能是一种有效和安全的方法,可以降低p53相关病理的严重程度。

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