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内分泌干扰:邻苯二甲酸酯类增塑剂与皮质类固醇结合球蛋白的计算相互作用。

Endocrine disruption: In silico interactions between phthalate plasticizers and corticosteroid binding globulin.

机构信息

King Fahd Medical Research Center, King Abdulaziz University, Jeddah, Kingdom of Saudi Arabia.

出版信息

J Appl Toxicol. 2017 Dec;37(12):1471-1480. doi: 10.1002/jat.3497. Epub 2017 Jul 4.

DOI:10.1002/jat.3497
PMID:28677244
Abstract

Endocrine disruption is a phenomenon when a man-made or natural compound interferes with normal hormone function in human or animal body systems. Endocrine-disrupting compounds (EDCs) have assumed considerable importance as a result of industrial activity, mass production of synthetic chemicals and environmental pollution. Phthalate plasticizers are a group of chemicals used widely and diversely in industry especially in the plastic industry, and many of the phthalate compounds have endocrine-disrupting properties. Increasing evidence indicates that steroid nuclear receptors and steroid binding proteins are the main targets of endocrine disruption. Corticosteroid-binding globulin (CBG) is a steroid binding protein that binds and transports cortisol in the blood circulation and is a potential target for endocrine disruption. An imbalance of cortisol in the body leads to many health problems. Induced fit docking of nine important and environmentally relevant phthalate plasticizers (DMP, BBP, DBP, DIBP, DnHP, DEHP, DINP, DnOP, DIDP) showed interactions with 10-19 amino acid residues of CBG. Comparison of the interacting residues of CBG with phthalate ligands and cortisol showed an overlapping of the majority (53-82%) of residues for each phthalate. Five of nine phthalate compounds and cortisol shared a hydrogen bonding interaction with the Arg-252 residue of CBG. Long-chain phthalates, such as DEHP, DINP, DnOP and DIDP displayed a higher binding affinity and formed a number of interactions with CBG in comparison to short-chain phthalates. The similarity in structural binding characteristics of phthalate compounds and native ligand cortisol suggested potential competitive conflicts in CBG-cortisol binding function and possible disruption of cortisol and progesterone homeostasis.

摘要

内分泌干扰是一种人为或天然化合物干扰人体或动物体系统中正常激素功能的现象。由于工业活动、合成化学品的大规模生产和环境污染,内分泌干扰化合物 (EDC) 变得非常重要。邻苯二甲酸酯类增塑剂是一类广泛应用于工业,尤其是塑料工业的化学物质,其中许多邻苯二甲酸酯类化合物具有内分泌干扰特性。越来越多的证据表明,甾体核受体和甾体结合蛋白是内分泌干扰的主要靶标。皮质甾醇结合球蛋白 (CBG) 是一种在血液循环中结合和转运皮质醇的甾体结合蛋白,是内分泌干扰的潜在靶标。体内皮质醇失衡会导致许多健康问题。对 9 种重要的环境相关邻苯二甲酸酯类增塑剂(DMP、BBP、DBP、DIBP、DnHP、DEHP、DINP、DnOP、DIDP)进行的诱导契合对接表明,它们与 CBG 的 10-19 个氨基酸残基相互作用。将 CBG 与邻苯二甲酸配体和皮质醇相互作用的残基进行比较,发现大多数(53-82%)邻苯二甲酸残基与 CBG 重叠。在 9 种邻苯二甲酸化合物中,有 5 种与 CBG 的 Arg-252 残基发生氢键相互作用,与皮质醇共享。与短链邻苯二甲酸相比,长链邻苯二甲酸如 DEHP、DINP、DnOP 和 DIDP 与 CBG 具有更高的结合亲和力,并形成了许多相互作用。邻苯二甲酸化合物与天然配体皮质醇在结构结合特征上的相似性表明,在 CBG-皮质醇结合功能中存在潜在的竞争冲突,以及皮质醇和孕酮平衡可能受到干扰。

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