Yu Zhu, Yanyan Jin, Xue He, JunYi Chen, Yao Zhang, JingJing Wang
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Additionally, ALKBH5 knockout in transgenic animals was found to mitigate cisplatin-induced renal dysfunction, whereas its knock-in exacerbated the effects. Our study revealed that ALKBH5 controls the traditional ferroptosis metabolic pathway, leading to worsening of AKI in experiments conducted both in vivo and in vitro. The efficacy of pharmacological intervention targeting ALKBH5 in AKI animal models was demonstrated, and ALKBH5-based gene therapy confirmed these findings and displayed renoprotective effects against AKI. In conclusion, this study highlighted the crucial role of ALKBH5 as a key regulator of AKI. 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引用次数: 0
摘要
在临床环境中,顺铂诱导的肾毒性主要表现为急性肾损伤(AKI)。最近的研究表明,顺铂肾毒性与一种铁依赖性细胞死亡(ferroptosis)密切相关。AlkB 同源物 5(ALKBH5)是一种在包括肾脏在内的多种组织中表达的 N6-甲基腺苷(m6A)消除蛋白,已被认为与这一过程有关。然而,ALKBH5 在顺铂诱导的肾毒性中的具体作用仍然未知。我们的研究结果表明,ALKBH5 在顺铂诱导的 AKI 中上调,体内研究结果与体外研究结果一致。此外,在转基因动物中敲除 ALKBH5 可减轻顺铂诱导的肾功能障碍,而敲入 ALKBH5 则会加重肾功能障碍。我们的研究发现,ALKBH5 控制着传统的铁变态反应代谢途径,导致体内和体外实验中的 AKI 恶化。针对 ALKBH5 的药物干预在 AKI 动物模型中的疗效得到了证实,而基于 ALKBH5 的基因疗法也证实了这些发现,并显示出对 AKI 的肾保护作用。总之,这项研究强调了 ALKBH5 作为 AKI 关键调控因子的重要作用。总之,我们的研究证明了ALKBH5在顺铂诱导的AKI中控制铁变态反应的重要影响,这表明关注ALKBH5可能是治疗顺铂相关肾损伤的一种有前途的方法。
ALKBH5 insufficiency protects against ferroptosis-driven cisplatin-induced renal cytotoxicity.
In the clinical setting, cisplatin-induced nephrotoxicity primarily manifests as acute kidney injury (AKI). Recent studies have indicated that ferroptosis, a type of iron-dependent cell death, is closely involved in the cisplatin nephrotoxicity. AlkB homologue 5 (ALKBH5), an N6-methyladenosine (m6A) eraser protein expressed in various tissues, including the kidneys, has been implicated in this process. However, the specific role of ALKBH5 in cisplatin-induced nephrotoxicity remains unknown. Our findings indicated that ALKBH5 was upregulated in cisplatin-induced AKI, and the in vivo study results were consistent with the results of the in vitro study. Additionally, ALKBH5 knockout in transgenic animals was found to mitigate cisplatin-induced renal dysfunction, whereas its knock-in exacerbated the effects. Our study revealed that ALKBH5 controls the traditional ferroptosis metabolic pathway, leading to worsening of AKI in experiments conducted both in vivo and in vitro. The efficacy of pharmacological intervention targeting ALKBH5 in AKI animal models was demonstrated, and ALKBH5-based gene therapy confirmed these findings and displayed renoprotective effects against AKI. In conclusion, this study highlighted the crucial role of ALKBH5 as a key regulator of AKI. Overall, our research demonstrates the significant impact of ALKBH5 in controlling ferroptosis in cisplatin-induced AKI, suggesting that focusing on ALKBH5 could be a promising approach for treating cisplatin-related kidney damage.
期刊介绍:
Cell Biology and Toxicology (CBT) is an international journal focused on clinical and translational research with an emphasis on molecular and cell biology, genetic and epigenetic heterogeneity, drug discovery and development, and molecular pharmacology and toxicology. CBT has a disease-specific scope prioritizing publications on gene and protein-based regulation, intracellular signaling pathway dysfunction, cell type-specific function, and systems in biomedicine in drug discovery and development. CBT publishes original articles with outstanding, innovative and significant findings, important reviews on recent research advances and issues of high current interest, opinion articles of leading edge science, and rapid communication or reports, on molecular mechanisms and therapies in diseases.