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普列克底物蛋白同源结构域与磷脂分解介导的信号转导之间的神秘关系。

Enigmatic relationship of Pleckstrin homology domain with phospholipid breakdown mediated signal transduction.

作者信息

Tyagi M G, Bapna J S

机构信息

Department of Neuropsycho-Pharmacology & Neurochemistry, Institute of Human Behaviour and Allied Sciences, Jhilmil, Delhi, India.

出版信息

Indian J Exp Biol. 1999 Jan;37(1):1-5.

Abstract

Research into phospholipid signaling continues to flourish, as more and more bioactive lipids and proteins are being identified and their actions characterised. The Pleckstrin homology (PH) domain is one such newly recognized protein module thought to play an important role in intracellular signal transduction. The tertiary structures of several PH domains have been determined, some of them complexed with ligands and on the basis of structural similarities between PH domains and lipid binding proteins it has been suggested that PH domains may be binding to lipophilic molecules. In fact many of the proteins that contain this domain can interfere with the membrane association. This review examines the specificity of this binding and illustrates the importance of charge-charge interactions in PIP2-PH domain complex formation. The precise physiological functions of PH domain in vivo remains to be explored therefore this review examines the biochemical aspects of the interaction of PH domains with phospholipid breakdown mediated products and proto-oncogenic serine-threonine kinase (Akt), protein tyrosine kinases, which have been found to be a target of phospholipid second messengers. Thus, number of cellular processes mediated by this way, ranging from insulin signaling and protein synthesis to differentiation and cell survival are regulated by this intracellular signaling protein module.

摘要

随着越来越多的生物活性脂质和蛋白质被鉴定出来并对其作用进行了表征,磷脂信号传导的研究持续蓬勃发展。普列克底物蛋白同源(PH)结构域就是这样一种新发现的蛋白质模块,被认为在细胞内信号转导中发挥重要作用。已经确定了几个PH结构域的三级结构,其中一些与配体复合,并且基于PH结构域与脂质结合蛋白之间的结构相似性,有人提出PH结构域可能与亲脂性分子结合。事实上,许多含有该结构域的蛋白质会干扰膜结合。本综述研究了这种结合的特异性,并阐述了电荷相互作用在PIP2-PH结构域复合物形成中的重要性。PH结构域在体内的确切生理功能仍有待探索,因此本综述研究了PH结构域与磷脂分解介导产物和原癌基因丝氨酸-苏氨酸激酶(Akt)、蛋白质酪氨酸激酶相互作用的生化方面,这些激酶已被发现是磷脂第二信使的作用靶点。因此,通过这种方式介导的许多细胞过程,从胰岛素信号传导和蛋白质合成到分化和细胞存活,都受这种细胞内信号蛋白模块的调节。

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