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砷暴露导致……金属蛋白质组的全局变化 。(原文中“of”后面缺少具体内容)

Arsenic Exposure Causes Global Changes in the Metalloproteome of .

作者信息

Larson James, Tokmina-Lukaszewska Monika, Fausset Hunter, Spurzem Scott, Cox Savannah, Cooper Gwendolyn, Copié Valérie, Bothner Brian

机构信息

Department of Chemistry and Biochemistry, Montana State University, Bozeman, MT 59715, USA.

出版信息

Microorganisms. 2023 Feb 2;11(2):382. doi: 10.3390/microorganisms11020382.

Abstract

Arsenic is a toxic metalloid with differential biological effects, depending on speciation and concentration. Trivalent arsenic (arsenite, As) is more toxic at lower concentrations than the pentavalent form (arsenate, As). In , the proteins encoded by the operon are the major arsenic detoxification mechanism. Our previous transcriptional analyses indicate broad changes in metal uptake and regulation upon arsenic exposure. Currently, it is not known how arsenic exposure impacts the cellular distribution of other metals. This study examines the metalloproteome of strains with and without the operon in response to sublethal doses of As and As. Size exclusion chromatography coupled with inductively coupled plasma mass spectrometry (SEC-ICPMS) was used to investigate the distribution of five metals (Fe, Mg, Zn, As, and Cu) in proteins and protein complexes under native conditions. Parallel analysis by SEC-UV-Vis spectroscopy monitored the presence of protein cofactors. Together, these data reveal global changes in the metalloproteome, proteome, protein cofactors, and soluble intracellular metal pools in response to arsenic stress in This work brings to light one outcome of metal exposure and suggests that metal toxicity on the cellular level arises from direct and indirect effects.

摘要

砷是一种具有不同生物学效应的有毒类金属,其生物学效应取决于化学形态和浓度。三价砷(亚砷酸盐,As(III))在较低浓度下比五价形式(砷酸盐,As(V))毒性更强。在[具体细菌名称]中,由[操纵子名称]操纵子编码的蛋白质是主要的砷解毒机制。我们之前的转录分析表明,砷暴露后金属摄取和调控发生了广泛变化。目前,尚不清楚砷暴露如何影响其他金属的细胞分布。本研究检测了有和没有[操纵子名称]操纵子的[细菌名称]菌株的金属蛋白质组,以响应亚致死剂量的As(III)和As(V)。尺寸排阻色谱与电感耦合等离子体质谱联用(SEC-ICPMS)用于研究在天然条件下五种金属(铁、镁、锌、砷和铜)在蛋白质和蛋白质复合物中的分布。通过SEC-UV-Vis光谱进行的平行分析监测了蛋白质辅因子的存在。这些数据共同揭示了[细菌名称]在砷胁迫下金属蛋白质组、蛋白质组、蛋白质辅因子和可溶性细胞内金属池的全局变化。这项工作揭示了金属暴露的一个结果,并表明细胞水平上的金属毒性源于直接和间接效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1f6/9965246/d243a6654073/microorganisms-11-00382-g001.jpg

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