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一种新型肽类血小板生成素模拟物的设计与优化:计算方法的应用。

A Novel Peptide Thrombopoietin Mimetic Designing and Optimization Using Computational Approach.

机构信息

Founder and O/I Stem Cell Research Laboratory, Department of Biotechnology, INSPIRE Faculty, Delhi Technological University , Delhi , India.

Department of Chemistry, University of Delhi , Delhi , India.

出版信息

Front Bioeng Biotechnol. 2016 Aug 31;4:69. doi: 10.3389/fbioe.2016.00069. eCollection 2016.

Abstract

Thrombopoietin receptor (TPOR) is a cytokine receptor protein present on the cell surface. The activation of TPOR by thrombopoietin (TPO) (a glycoprotein hormone) triggers an intracellular cascade of megakaryocytopoiesis for the formation of platelets. Recent studies on ex vivo megakaryocytopoiesis have evolved the possibilities of therapeutics uses. These findings have paved the way for the development of various TPO alternatives (recombinant TPO, peptide, and non-peptide TPO mimetics), which are useful in regenerative medicine. However, these alternatives possess various limitations such as induction of autoimmune effects, high production cost, low specificity, and hence activity. In the present study, a novel peptidic TPO mimetic was designed through computational studies by studying the binding sites of TPO and TMP to TPOR and analogs of known mimetics. Screening of combinatorial library was done through molecular docking using ClusPro. These studies indicated mimetic-9 as a significant molecule since it was found to have better binding score of -938.8 kcal/mol with seven hydrogen bonds and a high number of hydrophobic interactions, than known mimetic TMP with docking score of -798.4 kcal/mol and TMP dimer with docking score of -811.9 kcal/mol for TPOR. Mimetic9-TPOR complex was further assessed by the molecular dynamics simulation, and their complex was found to be stable with an RMSD value of 0.091 Å. While studying the parameters, mimetic-9 was found to have overall good physiochemical properties with positive grand average hydropathy (GRAVY) score and high instability index score and was found to be localized in the extracellular region. The designed mimetic-9 might prove to be a useful lead molecule for mimicking the role of TPO for in vitro platelet production with higher efficiency.

摘要

血小板生成素受体 (TPOR) 是一种细胞表面的细胞因子受体蛋白。血小板生成素 (TPO)(一种糖蛋白激素)激活 TPOR 会触发巨核细胞生成的细胞内级联反应,从而形成血小板。最近对体外巨核细胞生成的研究已经发展出治疗用途的可能性。这些发现为各种 TPO 替代品(重组 TPO、肽和非肽 TPO 模拟物)的开发铺平了道路,这些替代品在再生医学中很有用。然而,这些替代品存在各种局限性,例如诱导自身免疫效应、生产成本高、特异性低以及因此的活性低。在本研究中,通过研究 TPO 和 TMP 与 TPOR 及其已知模拟物的结合位点,通过计算研究设计了一种新型肽 TPO 模拟物。通过使用 ClusPro 进行分子对接对组合文库进行了筛选。这些研究表明模拟物-9 是一种重要的分子,因为它被发现具有更好的结合评分-938.8 kcal/mol,有七个氢键和大量疏水相互作用,而已知的模拟物 TMP 的结合评分为-798.4 kcal/mol,TMP 二聚体的结合评分为-811.9 kcal/mol,用于 TPOR。进一步通过分子动力学模拟评估了模拟物-9-TPOR 复合物,发现其复合物稳定,RMSD 值为 0.091 Å。在研究参数时,模拟物-9 被发现具有整体良好的物理化学性质,具有正的平均水力亲合 (GRAVY) 评分和高不稳定性指数评分,并被发现定位于细胞外区域。设计的模拟物-9 可能被证明是一种有用的先导分子,可用于体外血小板生产模拟 TPO 的作用,效率更高。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/94c2/5006622/7fad02bc60ff/fbioe-04-00069-g001.jpg

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