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鉴定动力蛋白轻链路障-1作为人还原型叶酸载体的新型相互作用伴侣。

Identification of dynein light chain road block-1 as a novel interaction partner with the human reduced folate carrier.

作者信息

Ashokkumar Balasubramaniem, Nabokina Svetlana M, Ma Thomas Y, Said Hamid M

机构信息

Department of Medical Research, Veterans Affairs Medical Center, Long Beach, California 90822, USA.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2009 Sep;297(3):G480-7. doi: 10.1152/ajpgi.00154.2009. Epub 2009 Jul 1.

Abstract

The reduced folate carrier (RFC) is a major folate transport system in mammalian cells. RFC is highly expressed in the intestine and believed to play a role in folate absorption. Studies from our laboratory and others have characterized different aspects of the intestinal folate absorption process, but little is known about possible existence of accessory protein(s) that interacts with RFC and influences its physiology and/or cell biology. We investigated this issue by employing a bacterial two-hybrid system to screen a BacterioMatch II human intestinal cDNA library using the large intracellular loop between transmembrane domains 6 and 7 of the human RFC (hRFC) as bait. Our screening has resulted in the identification of dynein light chain road block-1 (DYNLRB1) as an interacting partner with hRFC. Existence of a direct protein-protein interaction between hRFC and DYNLRB1 was confirmed by in vitro pull-down assay and in vivo mammalian two-hybrid luciferase assay and coimmunoprecipitation analysis. Furthermore, confocal imaging of live human intestinal epithelial HuTu-80 cells demonstrated colocalization of DYNLRB1 with hRFC. Coexpression of DYNLRB1 with hRFC led to a significant (P < 0.05) increase in folate uptake. On the other hand, inhibiting the endogenous DYNLRB1 with gene-specific small interfering RNA or pharmacologically with a specific inhibitor (vanadate) led to a significant (P < 0.05) decrease in folate uptake. This study demonstrates for the first time the identification of DYNLRB1 as an interacting protein partner with hRFC. Furthermore, DYNLRB1 appears to influence the function and cell biology of hRFC.

摘要

还原型叶酸载体(RFC)是哺乳动物细胞中主要的叶酸转运系统。RFC在肠道中高度表达,被认为在叶酸吸收中发挥作用。我们实验室和其他机构的研究已经对肠道叶酸吸收过程的不同方面进行了表征,但对于可能存在的与RFC相互作用并影响其生理学和/或细胞生物学的辅助蛋白知之甚少。我们通过使用细菌双杂交系统,以人RFC(hRFC)跨膜结构域6和7之间的大细胞内环为诱饵,筛选BacterioMatch II人肠道cDNA文库来研究这个问题。我们的筛选结果鉴定出动力蛋白轻链路障-1(DYNLRB1)是与hRFC相互作用的伙伴。通过体外下拉试验、体内哺乳动物双杂交荧光素酶试验和共免疫沉淀分析,证实了hRFC与DYNLRB1之间存在直接的蛋白质-蛋白质相互作用。此外,对活的人肠道上皮HuTu-80细胞进行共聚焦成像显示DYNLRB1与hRFC共定位。DYNLRB1与hRFC共表达导致叶酸摄取显著(P < 0.05)增加。另一方面,用基因特异性小干扰RNA或用特定抑制剂(钒酸盐)进行药理抑制内源性DYNLRB1会导致叶酸摄取显著(P < 0.05)下降。这项研究首次证明鉴定出DYNLRB1是与hRFC相互作用的蛋白伙伴。此外,DYNLRB1似乎影响hRFC的功能和细胞生物学。

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