| Literature DB >> 31522191 |
Hongqiang Wu1,2,3, Huanwen Chen4, Zhilong Zheng5, Jiafeng Li1,2,3, Jian Ding1,2,3, Zihuai Huang1,2,3, Chang Jia6, Zitong Shen7, Guodong Bao1,2,3, Lingyun Wu8, Abdullah Al Mamun5, Huazi Xu1,2,3, Weiyang Gao9,10,11, Kailiang Zhou12,13,14.
Abstract
Random-pattern skin flaps are commonly used and valuable tools in reconstructive surgery, however, post-operative random skin flap necrosis remains a major and common complication. Previous studies have suggested that activating autophagy, a major pathway for degradation of intracellular waste, may improve flap survival. In this study, we investigated whether trehalose, a novel and potent autophagy activator, improves random skin flap viability. Our results demonstrated that trehalose significantly improves viability, augments blood flow, and decreases tissue edema. Furthermore, we found that trehalose leads to increased angiogenesis, decreased apoptosis, and reduced oxidative stress. Using immunohistochestry and western blot, we demonstrated that trehalose augments autophagy, and that inhibition of autophagy augmentation using 3MA significantly blunted the aforementioned benefits of trehalose therapy. Mechanistically, we showed that trehalose's autophagy augmentation is mediated by activation and nuclear translocation of TFEB, which may be due to inhibition of Akt and activation of the AMPK-SKP2-CARM1 signaling pathway. Altogether, our results established that trehalose is a potent agent capable for significantly increasing random-pattern skin flap survival by augmenting autophagy and subsequently promoting angiogenesis, reducing oxidative stress, and inhibiting cell death.Entities:
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Year: 2019 PMID: 31522191 PMCID: PMC6745036 DOI: 10.1038/s41419-019-1704-0
Source DB: PubMed Journal: Cell Death Dis Impact factor: 8.469