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Protein kinase C isozymes as potential therapeutic targets in immune disorders

机译:蛋白激酶C同工酶作为免疫障碍中的潜在治疗靶标

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Background: Members of the protein kinase C (PKC) family are key signalling mediators in immune responses, and pharmacological inhibition of PKCs may be useful for treating immune-mediated diseases. Objective: To review and discuss the insights gained so far into various PKC isozymes and the therapeutic potential and challenges of developing PKC inhibitors for immune disorder therapy. Methods: A literature review of the role of PKCs in immune cell signalling and recent studies describing immune functions associated with PKC isozyme deficiency in relevant mouse disease models, followed by specific case studies of current and potential therapeutic strategies targeting PKCs. Results/conclusion: There is vast amount of data supporting PKC isozymes as attractive drug targets for certain immune disorders. Although the development of specific PKC isozyme inhibitors has been challenging, some progress has been made. It remains to be seen if broad-scale or isozyme-selective inhibition of PKC will have clinical efficacy.
机译:背景:蛋白激酶C(PKC)家族的成员是免疫应答中的关键信号传导介质,PKC的药理抑制可用于治疗免疫介导的疾病。目的:审查和讨论迄今为止进入各种PKC同工酶的见解及发育PKC抑制剂对免疫疾病治疗的治疗潜力和挑战。方法:对PKCS在免疫细胞信号传导中的作用和最近研究的文献综述,描述了与PKC同工酶缺乏相关的小鼠病程模型相关的免疫功能,其次是针对PKC的当前和潜在治疗策略的特定案例研究。结果/结论:将PKC Isozymes有大量数据,作为某些免疫疾病的吸引力药物靶标。虽然特异性PKC同工酶抑制剂的发展已经具有挑战性,但已经取得了一些进展。如果对PKC的宽度或同工酶选择性抑制具有临床疗效,则仍有待观察。

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