靶向糖尿病伴侣蛋白以改善周围神经病变
Targeting the Diabetic Chaperome to Improve Peripheral Neuropathy.
作者信息
Dobrowsky Rick T
机构信息
Department of Pharmacology and Toxicology, The University of Kansas, 5064 Malott Hall 1251 Wescoe Hall Dr., Lawrence, KS, 66045, USA.
出版信息
Curr Diab Rep. 2016 Aug;16(8):71. doi: 10.1007/s11892-016-0769-8.
Abstract
The chaperome constitutes a broad family of molecular chaperones and co-chaperones that facilitate the folding, refolding, and degradation of the proteome. Heat shock protein 90 (Hsp90) promotes the folding of numerous oncoproteins to aid survival of malignant phenotypes, and small molecule inhibitors of the Hsp90 chaperone complex offer a viable approach to treat certain cancers. One therapeutic attribute of this approach is the selectivity of these molecules to target high affinity oncogenic Hsp90 complexes present in tumor cells, which are absent in nontransformed cells. This selectivity has given rise to the idea that disease may contribute to forming a stress chaperome that is functionally distinct in its ability to interact with small molecule Hsp90 modulators. Consistent with this premise, modulating Hsp90 improves clinically relevant endpoints of diabetic peripheral neuropathy but has little impact in nondiabetic nerve. The concept of targeting the "diabetic chaperome" to treat diabetes and its complications is discussed.
摘要
伴侣蛋白组构成了一个广泛的分子伴侣和共伴侣家族,它们促进蛋白质组的折叠、重新折叠和降解。热休克蛋白90(Hsp90)促进众多癌蛋白的折叠,以帮助恶性表型存活,Hsp90伴侣复合物的小分子抑制剂为治疗某些癌症提供了一种可行的方法。这种方法的一个治疗特性是这些分子对肿瘤细胞中存在的高亲和力致癌Hsp90复合物具有选择性,而在未转化细胞中不存在。这种选择性引发了一种观点,即疾病可能有助于形成一种应激伴侣蛋白组,其在与小分子Hsp90调节剂相互作用的能力方面功能独特。与这一前提一致,调节Hsp90可改善糖尿病周围神经病变的临床相关终点,但对非糖尿病神经几乎没有影响。本文讨论了靶向“糖尿病伴侣蛋白组”以治疗糖尿病及其并发症的概念。
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