Inhibition of cysteine-serine-rich nuclear protein 1 ameliorates ischemia–reperfusion injury during liver transplantation in an MAPK-dependent manner

Zhoucheng Wang; Wenwen Ge; Xinyang Zhong; Shizheng Tong; Shusen Zheng; Xiao Xu; Kai Wang

doi:10.1186/s43556-024-00185-z

Molecular Biomedicine (Jun 2024)

Inhibition of cysteine-serine-rich nuclear protein 1 ameliorates ischemia–reperfusion injury during liver transplantation in an MAPK-dependent manner

Zhoucheng Wang,
Wenwen Ge,
Xinyang Zhong,
Shizheng Tong,
Shusen Zheng,
Xiao Xu,
Kai Wang

Affiliations

Zhoucheng Wang: NHC Key Laboratory of Combined Multi-organ Transplantation
Wenwen Ge: NHC Key Laboratory of Combined Multi-organ Transplantation
Xinyang Zhong: NHC Key Laboratory of Combined Multi-organ Transplantation
Shizheng Tong: The Fourth School of Clinical Medicine, Zhejiang Chinese Medical University
Shusen Zheng: NHC Key Laboratory of Combined Multi-organ Transplantation
Xiao Xu: NHC Key Laboratory of Combined Multi-organ Transplantation
Kai Wang: Department of Hepatobiliary & Pancreatic Surgery and Minimally Invasive Surgery, Zhejiang Provincial People’s Hospital (Affiliated People’s Hospital), Hangzhou Medical College

DOI: https://doi.org/10.1186/s43556-024-00185-z
Journal volume & issue: Vol. 5, no. 1
pp. 1 – 17

Abstract

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Abstract Hepatic ischemia–reperfusion injury (HIRI) is a critical pathophysiological process during liver transplantation (LT). Multiple genes and signal pathways are dysregulated during HIRI. This study aims to identify genes as potential therapeutic targets for ameliorating HIRI. Datasets containing samples from the human donor liver (GSE151648) and mouse HIRI model (GSE117066) were analyzed to determine differentially expressed genes (DEGs). The selected DEGs were confirmed by real-time PCR and western blot in the hepatocyte hypoxia-reoxygenation (HR) model, mouse HIRI model, and human liver samples after transplantation. Genetic inhibition was used to further clarify the underlying mechanism of the gene in vitro and in vivo. Among the DEGs, CSRNP1 was significantly upregulated (|log FC|= 2.08, P < 0.001), and was positively correlated with the MAPK signal pathway (R = 0.67, P < 0.001). CSRNP1 inhibition by siRNA significantly suppressed apoptosis in the AML-12 cell line after HR (mean Annexin+ ratio = 60.62% vs 42.47%, P = 0.0019), but the protective effect was eliminated with an additional MAPK activator. Knocking down CSRNP1 gene expression by intravenous injection of AAV-shRNA markedly reduced liver injury in mouse HIRI model (ALT: AAV-NC vs AAV-shCsrnp1 = 26,673.5 ± 2761.2 vs 3839.7 ± 1432.8, P < 0.001; AST: AAV-NC vs AAV-shCsrnp1 = 8640.5 ± 1450.3 vs 1786.8 ± 518.3, P < 0.001). Liver-targeted delivery of siRNA by nanoparticles effectively inhibited intra-hepatic genetic expression of Csrnp1 and alleviated IRI by reducing tissue inflammation and hepatocyte apoptosis. Furthermore, CSRNP1 inhibition was associated with reduced activation of the MAPK pathway both in vitro and in vivo. In conclusion, our results demonstrated that CSRNP1 could be a potential therapeutic target to ameliorate HIRI in an MAPK-dependent manner.

Published in Molecular Biomedicine

ISSN: 2662-8651 (Online)
Publisher: Springer
Country of publisher: Switzerland
LCC subjects: Medicine
Website: https://www.springer.com/journal/43556

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