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首页> 外文期刊>Drug Metabolism and Disposition: The Biological Fate of Chemicals >The Role of Protein-Protein and Protein-Membrane Interactions on P450 Function
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The Role of Protein-Protein and Protein-Membrane Interactions on P450 Function

机译:蛋白质和蛋白质膜相互作用对P450功能的作用

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摘要

This symposium summary, sponsored by the ASPET, was held at Experimental Biology 2015 on March 29, 2015, in Boston, Massachusetts. The symposium focused on: 1) the interactions of cytochrome P450s (P450s) with their redox partners; and 2) the role of the lipid membrane in their orientation and stabilization. Two presentations discussed the interactions of P450s with NADPH-P450 reductase (CPR) and cytochrome b(5). First, solution nuclear magnetic resonance was used to compare the protein interactions that facilitated either the hydroxylase or lyase activities of CYP17A1. The lyase interaction was stimulated by the presence of b(5) and 17 alpha-hydroxypregnenolone, whereas the hydroxylase reaction was predominant in the absence of b(5). The role of b(5) was also shown in vivo by selective hepatic knockout of b(5) from mice expressing CYP3A4 and CYP2D6; the lack of b(5) caused a decrease in the clearance of several substrates. The role of the membrane on P450 orientation was examined using computational methods, showing that the proximal region of the P450 molecule faced the aqueous phase. The distal region, containing the substrate-access channel, was associated with the membrane. The interaction of NADPH-P450 reductase (CPR) with the membrane was also described, showing the ability of CPR to "helicopter" above the membrane. Finally, the endoplasmic reticulum (ER) was shown to be heterogeneous, having ordered membrane regions containing cholesterol and more disordered regions. Interestingly, two closely related P450s, CYP1A1 and CYP1A2, resided in different regions of the ER. The structural characteristics of their localization were examined. These studies emphasize the importance of P450 protein organization to their function.
机译:该研讨会摘要由ASPET赞助,于2015年3月29日在美国马萨诸塞州波士顿举行的2015年实验生物学大会上举行。研讨会的重点是:1)细胞色素P450(P450)与氧化还原伙伴的相互作用; 2)脂质膜在其定向和稳定中的作用。两个演示文稿讨论了P450与NADPH-P450还原酶(CPR)和细胞色素b(5)的相互作用。首先,溶液核磁共振被用来比较促进CYP17A1羟化酶或裂解酶活性的蛋白质相互作用。 b(5)和17α-羟基孕烯醇酮的存在刺激了裂解酶的相互作用,而在不存在b(5)的情况下,羟化酶反应占主导。 b(5)的作用还通过选择性地从表达CYP3A4和CYP2D6的小鼠肝中剔除b(5)来显示。 b(5)的缺乏导致几种基材的间隙减小。使用计算方法检查了膜在P450取向上的作用,表明P450分子的近端区域面对水相。包含底物进入通道的远端区域与膜相连。还描述了NADPH-P450还原酶(CPR)与膜的相互作用,显示了CPR在膜上方“直升机”的能力。最后,内质网(ER)被证明是异质的,有序的膜区域包含胆固醇和更多的无序区域。有趣的是,两个紧密相关的P450,CYP1A1和CYP1A2,位于ER的不同区域。他们的本地化的结构特征进行了检查。这些研究强调了P450蛋白组织对其功能的重要性。

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