METTL3 诱导的 mmu-lncRNA 121686/hsa-lncRNA 520657 通过靶向 miR-328-5p/HtrA3 信号轴促进 AKI 的进展。

mmu-lncRNA 121686/hsa-lncRNA 520657 induced by METTL3 drive the progression of AKI by targeting miR-328-5p/HtrA3 signaling axis.

机构信息

Department of Emergency Medicine, Second Xiangya Hospital, Central South University, Changsha, Hunan 410011, People's Republic of China; Emergency Medicine and Difficult Diseases Institute, Second Xiangya Hospital, Central South University, Changsha, Hunan 410011, People's Republic of China; Hunan Clinical Medical Research Center for Acute Organ Injury and Repair, Changsha, Hunan 410011, People's Republic of China.

Department of Ophthalmology, Second Xiangya Hospital, Changsha, Hunan 410011, People's Republic of China.

出版信息

Mol Ther. 2022 Dec 7;30(12):3694-3713. doi: 10.1016/j.ymthe.2022.07.014. Epub 2022 Jul 21.

DOI:10.1016/j.ymthe.2022.07.014

PMID:35869629

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9734029/

Abstract

The pathogenesis of acute kidney injury (AKI) is still not fully understood, and effective interventions are lacking. Here, we explored whether methyltransferase 3 (METTL3) was involved in the progression of AKI via regulation of cell death. We reported that PT（proximal tubule）-METTL3-knockout (KO) noticeably suppressed ischemic-induced AKI via inhibition of renal cell apoptosis. Furthermore, we also found that the expression of mmu-long non-coding RNA (lncRNA) 121686 was upregulated in antimycin-treated Boston University mouse proximal tubule (BUMPT) cells and a mouse ischemia-reperfusion (I/R)-induced AKI model. Functionally, mmu-lncRNA 121686 could promote I/R-induced mouse renal cell apoptosis. Mechanistically, mmu-lncRNA 121686 acted as a competing endogenous RNA (ceRNA) to prevent microRNA miR-328-5p-mediated downregulation of high-temperature requirement factor A 3 (Htra3). PT-mmu-lncRNA 121686-KO mice significantly ameliorated the ischemic-induced AKI via the miR-328-5p/HtrA3 axis. In addition, hsa-lncRNA 520657, homologous with lncRNA 121686, sponged miR-328-5p and upregulated Htra3 to promote I/R-induced human renal cell apoptosis. Interestingly, we found that mmu-lncRNA 121686/hsa-lncRNA 520657 upregulation were dependent on METTL3 via N-methyladenosine (mA) modification. The mmu-lncRNA 121686/miR-328-5p or hsa-lncRNA 520657/miR-328-5p /HtrA3 axis was induced in vitro by METTL3 overexpression; in contrast, this effect was attenuated by METTL3 small interfering RNA (siRNA). Furthermore, we found that PT-METTL3-KO or METTL3 siRNA significantly suppressed ischemic, septic, and vancomycin-induced AKI via downregulation of the mmu-lncRNA 121686/miR-328-5p/HtrA3 axis. Taken together, our data indicate that the METTL3/mmu-lncRNA 121686/hsa-lncRNA 520657/miR-328-5p/HtrA3 axis potentially acts as a therapeutic target for AKI.

摘要

急性肾损伤 (AKI) 的发病机制仍不完全清楚，缺乏有效的干预措施。在这里，我们探讨了甲基转移酶 3 (METTL3) 是否通过调节细胞死亡参与 AKI 的进展。我们报道，PT（近端肾小管）-METTL3 敲除 (KO) 通过抑制肾小管细胞凋亡明显抑制缺血诱导的 AKI。此外，我们还发现，mmu-long 非编码 RNA (lncRNA) 121686 在抗霉素处理的波士顿大学小鼠近端肾小管 (BUMPT) 细胞和小鼠缺血再灌注 (I/R) 诱导的 AKI 模型中表达上调。功能上，mmu-lncRNA 121686 可促进 I/R 诱导的小鼠肾细胞凋亡。在机制上，mmu-lncRNA 121686 作为竞争性内源性 RNA (ceRNA) ，可防止高温需求因子 A3 (Htra3) 被 microRNA miR-328-5p 下调。PT-mmu-lncRNA 121686-KO 小鼠通过 miR-328-5p/HtrA3 轴显著改善缺血诱导的 AKI。此外，hsa-lncRNA 520657，与 lncRNA 121686 同源，可海绵吸附 miR-328-5p 并上调 Htra3 以促进 I/R 诱导的人肾细胞凋亡。有趣的是，我们发现 mmu-lncRNA 121686/hsa-lncRNA 520657 的上调依赖于 METTL3 通过 N-甲基腺苷 (mA) 修饰。mmu-lncRNA 121686/miR-328-5p 或 hsa-lncRNA 520657/miR-328-5p/HtrA3 轴在 METTL3 过表达时在体外被诱导；相反，这种效应被 METTL3 小干扰 RNA (siRNA) 减弱。此外，我们发现 PT-METTL3-KO 或 METTL3 siRNA 通过下调 mmu-lncRNA 121686/miR-328-5p/HtrA3 轴，显著抑制缺血、脓毒症和万古霉素诱导的 AKI。总之，我们的数据表明，METTL3/mmu-lncRNA 121686/hsa-lncRNA 520657/miR-328-5p/HtrA3 轴可能作为 AKI 的治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c4f/9734029/775b92db57ca/fx1.jpg

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METTL3 诱导的 mmu-lncRNA 121686/hsa-lncRNA 520657 通过靶向 miR-328-5p/HtrA3 信号轴促进 AKI 的进展。

mmu-lncRNA 121686/hsa-lncRNA 520657 induced by METTL3 drive the progression of AKI by targeting miR-328-5p/HtrA3 signaling axis.

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