人类 ABCC11 变异的功能特征,ABCC11 是一种腋窝湿疹风险因子。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-07-01 Epub Date: 2024-05-15 DOI:10.1007/s13577-024-01074-x
Yu Toyoda, Hirotaka Matsuo, Tappei Takada
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摘要

人类 ATP 结合盒转运体 C11(ABCC11)是一种膜蛋白,具有 ATP 依赖性转运活性,可转运多种亲脂阴离子,包括内源性物质和抗癌剂等异种生物。越来越多的证据表明,ABCC11 野生型是造成人类分泌腺高分泌表型的原因,包括耳屎潮湿型和腋窝渗透症风险。此外,据报道,ABCC11 的低功能变体与人类的药物毒性风险有关。因此,ABCC11的功能变化可能会影响个人体质和药物毒性,这使我们认为对ABCC11基因变异进行功能验证具有重要意义。因此,除了p.G180R(ABCC11的一个特征明确的非功能变异体)之外,我们还研究了ABCC11的10个变异体的细胞表达和功能。在这项研究中,利用表达 ABCC11 的质膜囊泡对 ABCC11 的功能进行了评估,即 ATP 依赖性转运放射性标记的硫酸脱氢表雄酮。除 p.G180R 外,其他 10 个变异体均成熟为 N-连接的糖蛋白,并在质膜上表达。我们发现,6个变体损害了ABCC11的细胞净功能。其中,p.R630W 的影响最大。包括这次发现的一个明显功能障碍变体在内,我们的发现将扩展我们对 ABCC11 蛋白遗传变异和生化特征的理解。
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Functional characterization of variants in human ABCC11, an axillary osmidrosis risk factor.

Human ATP-binding cassette transporter C11 (ABCC11) is a membrane protein exhibiting ATP-dependent transport activity for a variety of lipophilic anions including endogenous substances and xenobiotics such as anti-cancer agents. Accumulating evidence indicates that ABCC11 wild type is responsible for the high-secretion phenotypes in human apocrine glands including wet type of earwax and the risk of axillary osmidrosis. Also, a less-functional variant of ABCC11 was reportedly associated with a risk for drug-induced toxicity in humans. Thus, functional change in ABCC11 may affect individual's constitution and drug toxicity, which led us to reason that functional validation of genetic variations in ABCC11 should be of importance. Therefore, in addition to p.G180R (a well-characterized non-functional variant of ABCC11), we studied cellular expression and function of 10 variants of ABCC11. In this study, ABCC11 function was evaluated as an ATP-dependent transport of radio labeled-dehydroepiandrosterone sulfate using ABCC11-expressing plasma membrane vesicles. Except for p.G180R, other 10 variants were maturated as an N-linked glycoprotein and expressed on the plasma membrane. We found that six variants impaired the net cellular function of ABCC11. Among them, p.R630W was most influential. Including this identification of a significantly-dysfunctional variant, our findings will extend our understanding of genetic variations and biochemical features of ABCC11 protein.

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