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Hsp60 chaperonopathies and chaperonotherapy: Targets and agents

机译:Hsp60伴侣病和伴侣疗法:目标和代理商

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Introduction: Hsp60 (Cpn60) assembles into a tetradecamer that interacts with the co-chaperonin Hsp10 (Cpn10) to assist client polypeptides to fold, but it also has other roles, including participation in pathogenic mechanisms. Area covered: Hsp60 chaperonopathies are pathological conditions, inherited or acquired, in which the chaperone plays a determinant etiologic-pathogenic role. These diseases justify selection of Hsp60 as a target for developing agents that interfere with its pathogenic effects. We provide information on how to proceed. Expert opinion: The information available encourages the development of ways to improve Hsp60 activity (positive chaperonotherapy) when deficient or to block it (negative chaperonotherapy) when pathogenic. Many questions are still unanswered and obstacles are obvious. More information is needed to establish when and why autologous Hsp60 becomes a pathogenic autoantigen, or induces cytokine formation and inflammation, or favors carcinogenesis. Clarification of these points will take considerable time. However, analysis of the Hsp60 molecule and a search for active compounds aimed at structural sites that will affect its functioning should continue without interruption. No doubt that some of these compounds will offer therapeutic hopes and will also be instrumental for dissecting structure-function relationships at the biochemical and biological (using animal models and cultured cells) levels.
机译:简介:Hsp60(Cpn60)组装成四聚体,与伴侣蛋白Hsp10(Cpn10)相互作用以协助客户多肽折叠,但它还具有其他作用,包括参与致病机制。覆盖区域:Hsp60伴侣病是遗传性或获得性的病理条件,其中伴侣起决定性病因-致病作用。这些疾病证明选择Hsp60作为干扰其致病作用的显影剂的靶标是正确的。我们提供有关如何进行的信息。专家意见:可获得的信息鼓励开发出在缺乏时提高Hsp60活性(阳性伴侣疗法)或在致病性时阻断Hsp60活性(阴性伴侣疗法)的方法。许多问题仍未解决,障碍显而易见。需要更多信息来确定何时以及为什么自体Hsp60成为致病性自身抗原,或诱导细胞因子形成和炎症,或促进癌变。澄清这些问题将花费大量时间。但是,应继续进行Hsp60分子的分析并寻找针对会影响其功能的结构位点的活性化合物。毫无疑问,这些化合物中的某些将提供治疗希望,并且还将有助于在生化和生物学(使用动物模型和培养的细胞)水平上解析结构-功能关系。

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