Open AccessAdiponectin gene therapy prevents islet loss after transplantation
Author(s) -
Wang Chengshi,
Du Xiaojiong,
Fu Fudong,
Li Xiaoyu,
Wang Zhenghao,
Zhou Ye,
Gou Liping,
Li Wei,
Li Juan,
Zhang Jiayi,
Liao Guangneng,
Li Lan,
Han YuanPing,
Tong Nanwei,
Liu Jingping,
Chen Younan,
Cheng Jingqiu,
Cao Qi,
Ilegems Erwin,
Lu Yanrong,
Zheng Xiaofeng,
Berggren PerOlof
Publication year - 2022
Publication title -
journal of cellular and molecular medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.44
H-Index - 130
eISSN - 1582-4934
pISSN - 1582-1838
DOI - 10.1111/jcmm.17515
Subject(s) - islet , adiponectin , transplantation , adipokine , inflammation , endocrinology , medicine , oxidative stress , diabetes mellitus , immunology , insulin resistance
Significant pancreatic islet dysfunction and loss shortly after transplantation to the liver limit the widespread implementation of this procedure in the clinic. Nonimmune factors such as reactive oxygen species and inflammation have been considered as the primary driving force for graft failure. The adipokine adiponectin plays potent roles against inflammation and oxidative stress. Previous studies have demonstrated that systemic administration of adiponectin significantly prevented islet loss and enhanced islet function at post‐transplantation period. In vitro studies indicate that adiponectin protects islets from hypoxia/reoxygenation injury, oxidative stress as well as TNF‐α‐induced injury. By applying adenovirus mediated transfection, we now engineered islet cells to express exogenous adiponectin gene prior to islet transplantation. Adenovirus‐mediated adiponectin transfer to a syngeneic suboptimal islet graft transplanted under kidney capsule markedly prevented inflammation, preserved islet graft mass and improved islet transplant outcomes. These results suggest that adenovirus‐mediated adiponectin gene therapy would be a beneficial clinical engineering approach for islet preservation in islet transplantation.