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非酒精性脂肪性肝炎调节膜蛋白回收和插入过程。

Nonalcoholic Steatohepatitis Modulates Membrane Protein Retrieval and Insertion Processes.

作者信息

Dzierlenga A L, Clarke J D, Cherrington N J

机构信息

Department of Pharmacology & Toxicology, University of Arizona, Tucson, Arizona.

Department of Pharmacology & Toxicology, University of Arizona, Tucson, Arizona

出版信息

Drug Metab Dispos. 2016 Nov;44(11):1799-1807. doi: 10.1124/dmd.116.071415. Epub 2016 Sep 7.

DOI:10.1124/dmd.116.071415
PMID:27604106
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5074469/
Abstract

Interindividual variability in drug response in nonalcoholic steatohepatitis (NASH) can be mediated by altered regulation of drug metabolizing enzymes and transporters. Among these is the mislocalization of multidrug resistance-associated protein (MRP2)/Mrp2 away from the canalicular membrane, which results in decreased transport of MRP2/Mrp2 substrates. The exact mechanism of this mislocalization is unknown, although increased activation of membrane retrieval processes may be one possibility. The current study measures the activation status of various mediators implicated in the active membrane retrieval or insertion of membrane proteins to identify which processes may be important in rodent methionine and choline deficient diet-induced NASH. The mediators currently known to be associated with transporter mislocalization are stimulated by oxidative stressors and choleretic stimuli, which play a role in the pathogenesis of NASH. The activation of protein kinases PKA, PKCα, PKCδ, and PKCε and substrates radixin, myristoylated alanine-rich C-kinase substrate, and Rab11 were measured by comparing the expression, phosphorylation, and membrane translocation between control and NASH. Many of the mediators exhibited altered activation in NASH rats. Consistent with membrane retrieval of Mrp2, NASH rats exhibited a decreased phosphorylation of radixin and increased membrane localization of PKCδ and PKCε, thought to be mediators of radixin dephosphorylation. Altered activation of PKCδ, PKA, and PKCα may impair the Rab11-mediated active insertion of Mrp2. Overall, these data suggest alterations in membrane retrieval and insertion processes that may contribute to altered localization of membrane proteins in NASH.

摘要

非酒精性脂肪性肝炎(NASH)中药物反应的个体间差异可能由药物代谢酶和转运蛋白的调节改变介导。其中包括多药耐药相关蛋白(MRP2)/Mrp2从胆小管膜的错误定位,这导致MRP2/Mrp2底物的转运减少。尽管膜回收过程的激活增加可能是一种可能性,但这种错误定位的确切机制尚不清楚。当前的研究测量了与膜蛋白的主动膜回收或插入相关的各种介质的激活状态,以确定哪些过程在啮齿动物蛋氨酸和胆碱缺乏饮食诱导的NASH中可能很重要。目前已知与转运蛋白错误定位相关的介质受到氧化应激源和利胆刺激的刺激,这些刺激在NASH的发病机制中起作用。通过比较对照组和NASH组之间的表达、磷酸化和膜转位,测量蛋白激酶PKA、PKCα、PKCδ和PKCε以及底物根蛋白、富含肉豆蔻酰化丙氨酸的C激酶底物和Rab11的激活情况。许多介质在NASH大鼠中表现出激活改变。与Mrp2的膜回收一致,NASH大鼠表现出根蛋白磷酸化减少以及PKCδ和PKCε的膜定位增加,它们被认为是根蛋白去磷酸化的介质。PKCδ、PKA和PKCα的激活改变可能会损害Rab11介导的Mrp2的主动插入。总体而言,这些数据表明膜回收和插入过程的改变可能导致NASH中膜蛋白定位的改变。

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