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A preclinical overview of emerging therapeutic targets for glomerular diseases

机译:肾小球疾病的新兴治疗靶标的临床前概述

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ABSTRACT Introduction: Animal models have provided significant insights into the mechanisms responsible for the development of glomerular lesions and proteinuria; they have also helped to identify molecules that control the podocyte function as suitable target-specific therapeutics. Areas covered: We discuss putative therapeutic targets for proteinuric glomerular diseases. An exhaustive search for eligible studies was performed in PubMed/MEDUNE. Most of the selected reports were published in the last decade, but we did not exclude older relevant milestone publications. We consider the molecules that regulate podocyte cytoskeletal dynamics and the transcription factors that regulate the expression of slit-diaphragm proteins. There is a focus on SGLT2 and sirtuins which have recently emerged as mediators of podocyte injury and repair. We also examine paracrine signallings involved in the cross-talk of injured podocytes with the neighbouring glomerular endothelial cells and parietal epithelial cells. Expert opinion: There is a need to discover novel therapeutic moleecules with renoprotective effects for those patients with glomerular diseases who do not respond completely to standard therapy. Emerging strategies targeting components of the podocyte cytoskeleton or signallings that regulate cellular communication within the glomerulus are promising avenues for treating glomerular diseases.
机译:摘要介绍:动物模型为负责肾小球病变和蛋白尿的发育的机制提供了重要的见解;它们还有助于识别控制泛细胞功能作为合适的目标特异性治疗剂的分子。所涵盖的区域:我们讨论了蛋白质肾小球疾病的推定治疗靶标。在PubMed / Medune进行了详尽的符合条件的研究。大多数选定的报告在过去十年中发布,但我们并没有排除较旧的相关里程碑出版物。我们考虑调节细胞细胞细胞骨骼动力学和调节裂隙隔膜蛋白表达的转录因子的分子。 SGLT2和SIRTUINS焦点最近被出现为致统粒细胞损伤和修复的介质。我们还研究了与相邻的肾小球内皮细胞和椎廓管上皮细胞的受伤诱饵泛细胞串扰的帕拉克曲线标志。专家意见:需要探索新的治疗性MoleSecules,对那些没有完全响应标准治疗的肾小球疾病的患者进行重新调试影响。新出现的策略靶向龟细胞细胞骨架或标志物中调节肾小球内细胞通信的标志的组分是用于治疗肾小球疾病的途径。

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