| Literature DB >> 33420039 |
Jinyoung Kim1,2, Kihyoun Park1,3, Min Jung Kim4, Hyejin Lim1,2, Kook Hwan Kim1,2, Sun-Woo Kim1,2, Eun-Seo Lee5, Hyongbum Henry Kim5, Sung Joo Kim3,6,7, Kyu Yeon Hur3,8, Jae Hyeon Kim3,8, Jin Hee Ahn9, Kun-Ho Yoon4, Ji-Won Kim4, Myung-Shik Lee10,11.
Abstract
We have reported that autophagy is crucial for clearance of amyloidogenic human IAPP (hIAPP) oligomer, suggesting that an autophagy enhancer could be a therapeutic modality against human diabetes with amyloid accumulation. Here, we show that a recently identified autophagy enhancer (MSL-7) reduces hIAPP oligomer accumulation in human induced pluripotent stem cell-derived β-cells (hiPSC-β-cells) and diminishes oligomer-mediated apoptosis of β-cells. Protective effects of MSL-7 against hIAPP oligomer accumulation and hIAPP oligomer-mediated β-cell death are significantly reduced in cells with knockout of MiTF/TFE family members such as Tfeb or Tfe3. MSL-7 improves glucose tolerance and β-cell function of hIAPP+ mice on high-fat diet, accompanied by reduced hIAPP oligomer/amyloid accumulation and β-cell apoptosis. Protective effects of MSL-7 against hIAPP oligomer-mediated β-cell death and the development of diabetes are also significantly reduced by β-cell-specific knockout of Tfeb. These results suggest that an autophagy enhancer could have therapeutic potential against human diabetes characterized by islet amyloid accumulation.Entities:
Year: 2021 PMID: 33420039 DOI: 10.1038/s41467-020-20454-z
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919