The multidrug resistance pump ABCB1 is a substrate for the ubiquitin ligase NEDD4-1.

Q3 Biochemistry, Genetics and Molecular Biology Molecular Membrane Biology Pub Date : 2015-01-01 Epub Date: 2015-05-26 DOI:10.3109/09687688.2015.1023378
Begum G Akkaya, Joseph K Zolnerciks, Tasha K Ritchie, Bjoern Bauer, Anika M S Hartz, James A Sullivan, Kenneth J Linton
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引用次数: 25

Abstract

Abstract The ATP Binding Cassette transporter ABCB1 can export the neurotoxic peptide β-amyloid from endothelial cells that line the blood-brain barrier (BBB). This has the potential to lower cerebral levels of β-amyloid, but ABCB1 expression in the BBB appears to be progressively reduced in patients with Alzheimer’s disease. The surface density of many membrane proteins is regulated by ubiquitination catalyzed by ubiquitin E3 ligases. In brain capillaries of mice challenged with β-amyloid ex vivo, we show that the level of the ubiquitin ligase Nedd4 increases concomitant with reduction in Abcb1. In vitro we show that human ABCB1 is a substrate for human NEDD4-1 ligase. Recombinant ABCB1 was purified from Sf21 insect cells and incubated with recombinant NEDD4-1 purified from Escherichia coli. The treated ABCB1 had reduced mobility on SDS-PAGE, and mass spectrometry identified eight lysine residues, K271, K272, K575, K685, K877, K885, K887 and K1062 that were ubiquitinated by NEDD4-1. Molecular modelling showed that all of the residues are exposed on the surface of the intracellular domains of ABCB1. K877, K885 and K887 in particular, are located in the intracellular loop of transmembrane helix 10 (TMH10) in close proximity, in the tertiary fold, to a putative NEDD4-1 binding site in the intracellular helix extending from TMH12 (PxY motif, residues 996–998). Transient expression of NEDD4-1 in HEK293 Flp-In cells stably expressing ABCB1 was shown to reduce the surface density of the transporter. Together, the data identify this ubiquitin ligase as a potential target for intervention in the pathophysiology of Alzheimer’s disease.

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多药耐药泵ABCB1是泛素连接酶NEDD4-1的底物。
ATP结合盒转运蛋白ABCB1可以从血脑屏障(BBB)内皮细胞中输出神经毒性肽β-淀粉样蛋白。这有可能降低大脑中β-淀粉样蛋白的水平,但在阿尔茨海默病患者中,血脑屏障中ABCB1的表达似乎逐渐减少。许多膜蛋白的表面密度是由泛素E3连接酶催化的泛素化调控的。在体外β-淀粉样蛋白攻击小鼠的脑毛细血管中,我们发现泛素连接酶Nedd4的水平随着Abcb1的减少而增加。在体外,我们发现人ABCB1是人NEDD4-1连接酶的底物。重组ABCB1从Sf21昆虫细胞中纯化,并与大肠杆菌纯化的重组NEDD4-1孵育。处理后的ABCB1在SDS-PAGE上迁移率降低,质谱鉴定出8个赖氨酸残基K271、K272、K575、K685、K877、K885、K887和K1062被NEDD4-1泛素化。分子模拟表明,所有残基都暴露在ABCB1的胞内结构域表面。尤其是K877、K885和K887,它们位于跨膜螺旋10 (TMH10)的胞内环上,位于第三层,靠近从TMH12延伸出来的胞内螺旋上推测的NEDD4-1结合位点(PxY基序,残基996-998)。在稳定表达ABCB1的HEK293 flip - in细胞中短暂表达NEDD4-1可降低转运蛋白的表面密度。总之,这些数据确定了这种泛素连接酶是干预阿尔茨海默病病理生理的潜在靶标。
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来源期刊
Molecular Membrane Biology
Molecular Membrane Biology 生物-生化与分子生物学
CiteScore
4.80
自引率
0.00%
发文量
0
审稿时长
>12 weeks
期刊介绍: Cessation. Molecular Membrane Biology provides a forum for high quality research that serves to advance knowledge in molecular aspects of biological membrane structure and function. The journal welcomes submissions of original research papers and reviews in the following areas: • Membrane receptors and signalling • Membrane transporters, pores and channels • Synthesis and structure of membrane proteins • Membrane translocation and targeting • Lipid organisation and asymmetry • Model membranes • Membrane trafficking • Cytoskeletal and extracellular membrane interactions • Cell adhesion and intercellular interactions • Molecular dynamics and molecular modelling of membranes. • Antimicrobial peptides.
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