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pHome, sodium/hydrogen exchange and vesicle trafficking.

机译:pHome,钠/氢交换和囊泡运输。

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Interwoven into the fabric of life, pH is sensed and cautiously regulated during all aspects of cellular physiology. In an ongoing project entitled "pHome", I developed in situ probes of cytoplasmic and vacuolar pH to analyze the response of 4,800 yeast deletion mutants to changes in environmental pH. Among the many sensors, regulators and direct contributors to cellular pH identified, herein. I focus on the endosomal Na +(K+)/H+ exchanger, Nhx1. I began to define its role in ion homeostasis by identifying novel salt and acid-sensitive phenotypes in the nhx1 null mutant. Specifically, I showed that Nhx1 serves as a "proton leak" pathway to alkalinize the endosomal lumen and regulate vesicular trafficking. By screening a panel of amiloride derivatives from Aventis Pharmaceuticals, I identified a specific inhibitor of Nhx1. Using this inhibitor and a large-scale phenomics approach, I further defined the role of Nhx1 as mediator of vesicle formation in cellular pathways of endosomal exit, including the multivesicular body pathway responsible for vacuolar mediated protein degradation and retrovirus particle formation (e.g. HIV-1). Detailed phylogenetic analysis established Nhx1 as a founding member of a newly-defined branch of the NHE gene family localized to endomembranes, including human orthologs NHE6, NHE7 and NHE9. Like yeast Nhx1, I showed that human NHE6 localizes to the recycling endosome of mammalian cells. Thus, yeast Nhx1 is a good model for the study of pH-mediated vesicle formation and use of inhibitors specific to human Nhx1 orthologs may be clinically relevant for treatment of retroviral infections, such as HIV.
机译:在细胞生理学的各个方面,pH值都被交织到生命的织物中,并被谨慎地调节。在正在进行的名为“ pHome”的项目中,我开发了细胞质和液泡pH值的原位探针,以分析4800个酵母缺失突变体对环境pH值变化的响应。在本文中,在许多传感器,调节剂和直接影响细胞pH的直接因素中。我专注于内体Na +(K +)/ H +交换子Nhx1。我开始通过鉴定nhx1 null突变体中新的盐和酸敏感性表型来定义其在离子稳态中的作用。具体来说,我表明Nhx1充当“质子泄漏”途径,以碱化内体腔并调节囊泡运输。通过筛选一组来自Aventis Pharmaceuticals的阿米洛利衍生物,我确定了Nhx1的特异性抑制剂。使用这种抑制剂和大规模的表型学方法,我进一步确定了Nhx1在内体出口的细胞途径中,包括在液泡介导的蛋白质降解和逆转录病毒颗粒形成(例如HIV-1)的多囊体途径中,作为囊泡形成的介质的作用。 )。详细的系统发育分析将Nhx1确立为NHE基因家族新定义分支的创始成员,该分支定位于子宫内膜,包括人类直系同源基因NHE6,NHE7和NHE9。像酵母Nhx1一样,我证明了人类NHE6定位于哺乳动物细胞的回收内体。因此,酵母Nhx1是研究pH介导的囊泡形成的良好模型,使用对人Nhx1直系同源物特异的抑制剂可能在临床上与逆转录病毒感染(如HIV)的治疗有关。

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