Milk derived hexapeptide reduces alcohol －induced oxidative stress and alleviates liver injury through FoxO3a －MnSOD signaling pathway

Anqi Li; Xiaomei Zhu; Jiujiu Huang; Yide Qin; Nan Qi

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Milk derived hexapeptide reduces alcohol －induced oxidative stress and alleviates liver injury through FoxO3a －MnSOD signaling pathway

Author: Anqi Li ¹ ; Xiaomei Zhu ² ; Jiujiu Huang ¹ ; Yide Qin ¹ ; Nan Qi ¹
Author Information

1. Dept of Biochemistry and Molecular Biology，School of Basic Medical Science，Anhui Medical University，Hefei 230032
2. Dept of Histology and Embryology， School of Basic Medical Science，Anhui Medical University，Hefei 230032
Publication Type:Journal Article
Keywords: PGPIPN; alcoholic liver damage; oxidative stress; FoxO3a; MnSOD
From: Acta Universitatis Medicinalis Anhui 2022;57(12):1864-1869
CountryChina
Language:Chinese
Abstract: Objective :To investing ate the milk-derived hexapeptide PGPIPN and its truncated pentapeptide PGPIP to alleviate chronic alcoholic liver injury in mice and its associated molecular mechanisms．
Methods :Sixty Kun- ming mice were randomly divided into control group，model group，GSH group，PGPIPN group，and truncated pen- tapeptide PGPIP group．The model of chronic alcoholic liver injury in mice was established by gavage with gradient alcohol． Drug intervention was given at the same time for 12 weeks． Liver HE staining was used to analyze the pathological effects of each treatment group on alcoholic liver injury in mice．Primary mouse hepatocytes and human normal hepatocyte line L-02 were isolated and cultured in vitro．The appropriate PGPIPN induction concentrations of both cells were determined by WST-1 method． L-02 cells were induced at different times． The expression of FoxO3a and phosphorylated FoxO3a protein were detected by Western blot to determine the appropriate induction time．The subcellular localization of FoxO3a in L-02 cells was detected by cellular immunofluorescence．The mR- NA changes of FoxO3a and MnSOD genes in primary hepatocytes and L-02 cells of mice in different treatment groups were detected by qRT-PCR.
Results :The pathological examination of PGPIPN group and PGPIP group was similar to that of GSH group，and the liver injury of mice was significantly reduced．Medium and high concentra- tions of PGPIPN were respectively selected to induce mouse primary hepatocytes and L-02 cells．At 16 hours，the expression of FoxO3a protein in L-02 cells increased significantly．FoxO3a protein was mainly expressed in the nu- cleus．In addition，mRNA levels in both types of cells increased significantly after induction with the corresponding dose of PGPIPN．
Conclusion :PGPIPN and truncated pentapeptide PGPIP can reduce chronic alcoholic liver injury in mice．The mechanism may be to reduce alcohol-induced oxidative stress through FoxO3a-MnSOD signaling path- way.
Full text:2024072115094728110乳源六肽通过FoxO3a-...精诱导的氧化应激缓解肝损伤_李安琪.pdf