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表征丙泊酚与不同物种血清白蛋白结合亲和力的新方法。

Novel Approach for Characterizing Propofol Binding Affinities to Serum Albumins from Different Species.

作者信息

Shityakov Sergey, Fischer Anneli, Su Kuan-Pin, Hussein Aqeel A, Dandekar Thomas, Broscheit Jens

机构信息

Department of Psychiatry and Mind-Body Interface Laboratory (MBI-Lab), China Medical University Hospital, Taichung 40402, Taiwan.

Department of Bioinformatics, Würzburg University, Würzburg 97074, Germany.

出版信息

ACS Omega. 2020 Sep 30;5(40):25543-25551. doi: 10.1021/acsomega.0c01295. eCollection 2020 Oct 13.

Abstract

The interaction between the main carrier (serum albumin, SA) of endogenous and exogenous compounds in the bloodstream of different species (human, bovine, canine, rat, rabbit, and sheep) and a general anesthetic agent (propofol, PR) was investigated using an experimental technique (high-performance liquid chromatography) and computational methods (molecular docking, molecular dynamics, sequence, and phylogenetic analyses). The obtained results revealed the differences in the PR binding affinity to various homologous forms of this protein with reliable statistics ( = 0.9 and -value < 0.005), correlating with the evolutionary relationships among SAs from different species. Additionally, the protein conformational changes (root-mean-square deviation ≈ 1.0 Å) and amino acid conservation of binding sites in protein domains were detected, contributing to the SA-PR binding modes. Overall, the outcomes from this study might provide a novel methodology to assess protein-ligand interactions and to gain some interesting insights into drug pharmacokinetics and pharmacodynamics to explain its variations among different species.

摘要

利用实验技术(高效液相色谱法)和计算方法(分子对接、分子动力学、序列分析和系统发育分析),研究了不同物种(人类、牛、犬、大鼠、兔子和绵羊)血液中内源性和外源性化合物的主要载体(血清白蛋白,SA)与一种全身麻醉剂(丙泊酚,PR)之间的相互作用。所得结果显示,PR与该蛋白各种同源形式的结合亲和力存在差异,且具有可靠的统计学意义( = 0.9,-值 < 0.005),这与不同物种SA之间的进化关系相关。此外,还检测到了蛋白质构象变化(均方根偏差≈1.0 Å)以及蛋白质结构域中结合位点的氨基酸保守性,这些都有助于SA-PR的结合模式。总体而言,本研究的结果可能为评估蛋白质-配体相互作用提供一种新方法,并为解释药物在不同物种间的差异提供一些有趣的药物动力学和药效学见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd1c/7557242/6556c7a688b3/ao0c01295_0001.jpg

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