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αB-晶状体蛋白作为一种治疗剂的新作用:利弊

Emerging role for αB-crystallin as a therapeutic agent: pros and cons.

作者信息

Reddy V S, Reddy G B

机构信息

National Institute of Nutrition, Hyderabad-500 007, India.

出版信息

Curr Mol Med. 2015;15(1):47-61. doi: 10.2174/1566524015666150114112853.

Abstract

HSPB5 or αB-crystallin (αBC) is a major protein of the vertebrate eye lens belonging to the small heat-shock protein family of proteins that respond to various stressful conditions. αBC also is found outside the lens in various non-ocular tissues and acts as a molecular chaperone by preventing aggregation of proteins, inhibits apoptosis and inflammation, and maintains cytoskeletal architecture. The αBC protein is phosphorylated on three serine residues S59, S45, and S19, and several functions of αBC are modulated by phosphorylation. Numerous studies have revealed the upregulation of αBC in pathological conditions such as neurodegenerative diseases, cancers, diabetes, retinal diseases, cataracts, ischemia/repurfusion, aging, and others. However, it is unknown whether the up-regulation of αBC is causative or protective for these pathological conditions. Although αBC has been shown to provide a protective effect in neurodegenerative diseases, inflammation, diabetes, and retinal diseases, other studies have described a deleterious role of αBC in cancers and pulmonary fibrosis. The therapeutic potential of αBC alone or in combination with αA-crystallin has been reported. Acetylated αBC peptides have been shown to be more potent than native αBC for chaperone as well as therapeutic activities using both in vitro and in vivo models. Further, for efficient delivery of α BC into cells, carrier molecules such as polylacticcoglycolic acid, polycaprolactone and cell penetration peptides have been used. In this review, we have summarized current data from emerging and exciting studies of the therapeutic strategies of α BC and α BC peptides and the efficient delivery strategies of these proteins in various disease models, including neurodegenerative diseases, retinal diseases, platelet aggregation, inflammation, and ischemia.

摘要

HSPB5 或 αB 晶状体蛋白(αBC)是脊椎动物眼晶状体的一种主要蛋白质,属于对各种应激条件作出反应的小分子热休克蛋白家族。αBC 在晶状体之外的各种非眼部组织中也有发现,它通过防止蛋白质聚集发挥分子伴侣的作用,抑制细胞凋亡和炎症,并维持细胞骨架结构。αBC 蛋白在三个丝氨酸残基 S59、S45 和 S19 上发生磷酸化,αBC 的多种功能受磷酸化调节。大量研究表明,在神经退行性疾病、癌症、糖尿病、视网膜疾病、白内障、缺血/再灌注、衰老等病理状况下,αBC 会上调。然而,αBC 的上调对这些病理状况是致病的还是具有保护作用尚不清楚。尽管已证明 αBC 在神经退行性疾病、炎症、糖尿病和视网膜疾病中具有保护作用,但其他研究也描述了 αBC 在癌症和肺纤维化中的有害作用。已有报道称 αBC 单独或与 αA 晶状体蛋白联合使用具有治疗潜力。在体外和体内模型中,乙酰化的 αBC 肽已显示出比天然 αBC 更有效的伴侣活性和治疗活性。此外,为了将 αBC 有效递送至细胞内,已使用了聚乳酸 - 乙醇酸、聚己内酯和细胞穿透肽等载体分子。在这篇综述中,我们总结了来自新兴且令人兴奋的研究的当前数据,这些研究涉及 αBC 和 αBC 肽在各种疾病模型(包括神经退行性疾病、视网膜疾病、血小板聚集、炎症和缺血)中的治疗策略以及这些蛋白质的有效递送策略。

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