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Identification of ABCG2 as an Exporter of Uremic Toxin Indoxyl Sulfate in Mice and as a Crucial Factor Influencing CKD Progression

机译:ABCG2作为小鼠尿毒症吲哚硫酸盐的出口者和作为影响CKD进程的关键因素的鉴定。

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摘要

Chronic kidney disease (CKD) patients accumulate uremic toxins in the body, potentially require dialysis, and can eventually develop cardiovascular disease. CKD incidence has increased worldwide, and preventing CKD progression is one of the most important goals in clinical treatment. In this study, we conducted a series of in vitro and in vivo experiments and employed a metabolomics approach to investigate CKD. Our results demonstrated that ATP-binding cassette transporter subfamily G member 2 (ABCG2) is a major transporter of the uremic toxin indoxyl sulfate. ABCG2 regulates the pathophysiological excretion of indoxyl sulfate and strongly affects CKD survival rates. Our study is the first to report ABCG2 as a physiological exporter of indoxyl sulfate and identify ABCG2 as a crucial factor influencing CKD progression, consistent with the observed association between ABCG2 function and age of dialysis onset in humans. The above findings provided valuable knowledge on the complex regulatory mechanisms that regulate the transport of uremic toxins in our body and serve as a basis for preventive and individualized treatment of CKD.
机译:慢性肾脏病(CKD)患者在体内积累尿毒症毒素,可能需要透析,最终可能发展为心血管疾病。 CKD的发病率在全世界范围内都有所增加,而预防CKD的进展是临床治疗中最重要的目标之一。在这项研究中,我们进行了一系列的体外和体内实验,并采用代谢组学方法研究了CKD。我们的结果表明,ATP结合盒转运蛋白亚家族G成员2(ABCG2)是尿毒症毒素吲哚酚硫酸盐的主要转运蛋白。 ABCG2调节硫酸吲哚酚的病理生理排泄,并强烈影响CKD的存活率。我们的研究首次报道ABCG2作为硫酸吲哚酚的生理输出,并确定ABCG2是影响CKD进展的关键因素,这与观察到的ABCG2功能与人类透析年龄之间的关联一致。上述发现为调节尿毒症毒素在我们体内的运输的复杂调节机制提供了有价值的知识,并为CKD的预防和个体化治疗奠定了基础。

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