Adipsin preserves beta cells in diabetic mice and associates with protection from type 2 diabetes in humans
Metadatos
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Gomez-Banoy, Nicolas; Guseh, J Sawalla; Li, Ge; Chen, Tong; Poirier, BreAnne; Putzel, Gregory; Rosselot, Carolina; Pabon, Maria A; Camporez, João Paulo; Vijeta, Bhambhani; Shih-Jen, Hwang; Chen, Yao; Perry, Rachel J; Sushmita, Mukherjee; Larson, Martin G; Levy, Daniel; Dow, Lukas E; Shulman, Gerald I; Dephoure, Noah; Garcia-Ocaña, Adolfo; Hao, Mingming; Spiegelman, Bruce M; Ho, Jennifer E; Lo, James C; Rubio-Navarro, AlfonsoEditorial
Springer Nature
Fecha
2019-11-25Referencia bibliográfica
Gómez-Banoy N, Guseh JS, Li G, Rubio-Navarro A, Chen T, Poirier B, Putzel G, Rosselot C, Pabón MA, Camporez JP, Bhambhani V, Hwang SJ, Yao C, Perry RJ, Mukherjee S, Larson MG, Levy D, Dow LE, Shulman GI, Dephoure N, Garcia-Ocana A, Hao M, Spiegelman BM, Ho JE, Lo JC. Adipsin preserves beta cells in diabetic mice and associates with protection from type 2 diabetes in humans. Nat Med. 2019 Nov;25(11):1739-1747. doi: 10.1038/s41591-019-0610-4. Epub 2019 Nov 7. PMID: 31700183; PMCID: PMC7256970.
Resumen
N.G.B. is supported by an American Diabetes Association postdoctoral fellowship (118PMF032). J.S.G. was supported by an MGH NIH T32 Training Grant (HL007208), the John S. LaDue Memorial Fellowship and the MGH Physician Scientist Development Program. This work was supported by a Weill Cornell Department of Medicine Seed Grant for Innovative Research to J.C.L., the JPB Foundation (to B.M.S.), Jill Roberts
IBD Institute (to G.P.) and NIH grants DK097303 (to J.C.L.), R03 DK111762 (to J.C.L.), R01 DK121844 (to J.C.L.), R01 HL140224 (to J.E.H.) and R01 HL134893 (to J.E.H.). This work was partially supported by the National Heart, Lung and Blood Institute’s Framingham Heart Study (contracts N01HC25195 and HHSN268201500001I) and by the Division of Intramural Research (to P.C., G.S., C.L., S.J.H. and D.L.) of the National Heart, Lung and Blood Institute. We acknowledge support from the Yale Mouse Metabolic Phenotyping Center via NIH grants nos. U24 DK059635, R01 DK116774, R01 DK114793 and P30 DK045735 (all to G.I.S.).