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一种细胞内铵转运蛋白对于[具体对象]的复制、分化以及对饥饿和渗透胁迫的抗性是必需的。

An Intracellular Ammonium Transporter Is Necessary for Replication, Differentiation, and Resistance to Starvation and Osmotic Stress in .

作者信息

Cruz-Bustos Teresa, Potapenko Evgeniy, Storey Melissa, Docampo Roberto

机构信息

Center for Tropical and Emerging Global Diseases, University of Georgia, Athens, Georgia, USA.

Department of Cellular Biology, University of Georgia, Athens, Georgia, USA.

出版信息

mSphere. 2018 Jan 17;3(1). doi: 10.1128/mSphere.00377-17. eCollection 2018 Jan-Feb.

Abstract

, the etiologic agent of Chagas disease, undergoes drastic metabolic changes when it transits between a vector and mammalian hosts. Amino acid catabolism leads to the production of ammonium (NH), which needs to be detoxified. However, does not possess a urea cycle, and it is unknown how intracellular levels of ammonium are controlled. In this work, we identified an intracellular ammonium transporter of (TcAMT) that localizes to acidic compartments (reservosomes, lysosomes). TcAMT has 11 transmembrane domains and possesses all conserved and functionally important amino acid residues that form the pore in other ammonium transporters. Functional expression in oocytes followed by a two-electrode voltage clamp showed an inward current that is NH dependent at a resting membrane potential ( ) lower than -120 mV and is not pH dependent, suggesting that TcAMT is not an NH/H cotransporter but an NH or NH/H transporter. Ablation of by clustered regularly interspaced short palindromic repeat analysis with Cas9 (CRISPR-Cas9) resulted in significant defects in epimastigote and amastigote replication, differentiation, and resistance to starvation and osmotic stress. is an important human and animal pathogen and the etiologic agent of Chagas disease. The parasite undergoes drastic changes in its metabolism during its life cycle. Amino acid consumption becomes important in the infective stages and leads to the production of ammonia (NH), which needs to be detoxified. We report here the identification of an ammonium (NH) transporter that localizes to acidic compartments and is important for replication, differentiation, and resistance to starvation and osmotic stress.

摘要

恰加斯病的病原体在从媒介宿主传播到哺乳动物宿主的过程中会经历剧烈的代谢变化。氨基酸分解代谢会产生铵(NH),需要对其进行解毒。然而,该病原体不具备尿素循环,目前尚不清楚细胞内铵的水平是如何控制的。在这项研究中,我们鉴定出了一种该病原体的细胞内铵转运蛋白(TcAMT),它定位于酸性区室(液泡体、溶酶体)。TcAMT有11个跨膜结构域,并且拥有在其他铵转运蛋白中形成孔道的所有保守且功能重要的氨基酸残基。在非洲爪蟾卵母细胞中进行功能表达,随后采用双电极电压钳技术,结果显示在静息膜电位()低于 -120 mV时,存在一种依赖于NH的内向电流,且不依赖于pH,这表明TcAMT不是NH/H共转运蛋白,而是一种NH或NH/H转运蛋白。通过使用Cas9的成簇规律间隔短回文重复序列分析(CRISPR-Cas9)敲除该转运蛋白,导致前鞭毛体和无鞭毛体在复制、分化以及对饥饿和渗透应激的抗性方面出现显著缺陷。该病原体是一种重要的人类和动物病原体,也是恰加斯病的病原体。这种寄生虫在其生命周期中会经历剧烈的代谢变化。在感染阶段,氨基酸消耗变得很重要,并会导致氨(NH)的产生,而氨需要被解毒。我们在此报告鉴定出一种定位于酸性区室的铵(NH)转运蛋白,它对于复制、分化以及对饥饿和渗透应激的抗性很重要。

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