No safe renal warm ischemia time-The molecular network characteristics and pathological features of mild to severe ischemia reperfusion kidney injury

Ya-Lei Chen; Huai-Kang Li; Lei Wang; Jian-Wen Chen; Xin Ma

doi:10.3389/fmolb.2022.1006917

No safe renal warm ischemia time-The molecular network characteristics and pathological features of mild to severe ischemia reperfusion kidney injury

Front Mol Biosci. 2022 Nov 16:9:1006917. doi: 10.3389/fmolb.2022.1006917. eCollection 2022.

Authors

Ya-Lei Chen¹, Huai-Kang Li², Lei Wang², Jian-Wen Chen^{2

3}, Xin Ma²

Affiliations

¹ Department of Critical Care Medicine, Capital Medical University Electric Power Teaching Hospital/State Grid Beijing Electric Power Hospital, Beijing, China.
² Senior Department of Urology, The Third Medical Centre of PLA General Hospital, Beijing, China.
³ Department of Nephrology, State Key Laboratory of Kidney Diseases, Beijing Key Laboratory of Kidney Disease Research, First Medical Center of Chinese PLA General Hospital, Nephrology Institute of the Chinese People's Liberation Army, National Clinical Research Center for Kidney Diseases, Beijing, China.

Abstract

Ischemic acute kidney injury (AKI) has always been a hot and difficult research topic in the field of renal diseases. This study aims to illustrate the safe warm ischemia time of kidney and the molecular network characteristics and pathological features of mild to severe ischemia reperfusion kidney injury. We established varying degrees of renal injury due to different ischemia time (0 min, 16 min, 18 min, 20 min, 22 min, 24 min, 26 min, 28 min, and 30 min) on unilateral (left kidney) ischemia-reperfusion injury and contralateral (right kidney) resection (uIRIx) mouse model. Mice were sacrificed 24 h after uIRIx, blood samples were harvested to detect serum creatinine (Scr), and kidney tissue samples were harvested to perform Periodic Acid-Schiff (PAS) staining and RNA-Seq. Differentially expressed genes (DEGs) were identificated, time-dependent gene expression patterns and functional enrichment analysis were further performed. Finally, qPCR was performed to validated RNA-Seq results. Our results indicated that there was no absolute safe renal warm ischemia time, and every minute of ischemia increases kidney damage. Warm ischemia 26min or above in mice makes severe kidney injury, renal pathology and SCr were both significantly changed. Warm ischemia between 18 and 26 min makes mild kidney injury, with changes in pathology and renal molecular expression, while SCr did not change. No obvious pathological changes but significant differences in molecular expression were found less than 16min warm ischemia. There are two key time intervals in the process of renal ischemia injury, 0 min-16 min (short-term) and 26 min-28 min (long-term). Gene expression of immune-related pathways were most significantly down-regulated in short-term ischemia, while metabolism-related pathways were the mainly enriched pathway in long-term ischemia. Taken together, this study provides novel insights into safe renal artery occlusion time in partial nephrectomy, and is of great value for elucidating molecular network characteristics and pathological features of mild to severe ischemia reperfusion kidney injury, and key genes related to metabolism and immune found in this study also provide potential diagnostic and therapeutic biomarkers for AKI.

Keywords: acute kidney injury; ischemia reperfusion kidney injury; mild to severe ischemia reperfusion injury; molecular network characteristics; pathological features.

Grants and funding

This work was supported by grants from the National Natural Science Foundation of China (Grant No. 82100713, 82000631, 81970665, 81970594); China Postdoctoral Science Foundation (Grant No. 2021T140791); Fund of Chinese PLA 13th Five Year Plan for Medical Sciences (No. BLB19J009); National Sciences Foundation of Beijing (Grant No. 7222169); Military Medical Youth Special Project of PLA General Hospital (Grant No. QNF19035); and Young Elite Scientist Sponsorship Program by CAST (No. YESS20200400).