Divergent antioxidant capacity of human islet cell subsets: A potential cause of beta-cell vulnerability in diabetes and islet transplantation.
Atsushi MikiCamillo RicordiYasunaru SakumaToshiyuki YamamotoRyosuke MisawaAtsuyoshi MitaRuth D MolanoNosratola D VaziriAntonello PileggiHirohito IchiiPublished in: PloS one (2018)
Catalase and GPX expression was much lower in β- than α-cells. The β/α-cell ratio fells significantly following islet isolation and transplantation. Exposure to oxidative stress caused a significantly lower survival and viability, with higher DNA damage in β- than α-cells. These findings identified the weakness of β-cell antioxidant capacity as a main cause of vulnerability to oxidative stress. Potential strategies to enhance β-cell antioxidant capacity might be effective in prevention/treatment of diabetes.