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- Leptin Receptor Signaling Regulates Protein Synthesis Pathways and Neuronal Differentiation in Pluripotent Stem Cells.
Leptin Receptor Signaling Regulates Protein Synthesis Pathways and Neuronal Differentiation in Pluripotent Stem Cells.
Citation | “Leptin Receptor Signaling Regulates Protein Synthesis Pathways And Neuronal Differentiation In Pluripotent Stem Cells.”. Stem Cell Reports, pp. 1067-1079. . |
Center | Joslin Diabetes Center |
Author | Manoj K Gupta, Heidrun Vethe, Samir Softic, Tata Nageswara Rao, Vilas Wagh, Jun Shirakawa, Harald Barsnes, Marc Vaudel, Tomozumi Takatani, Sevim Kahraman, Masaji Sakaguchi, Rachael Martinez, Jiang Hu, Yngvild Bjørlykke, Helge Raeder, Rohit N Kulkarni |
Keywords | EIF4E, STAT3, cancer, diabetes, Embryonic development, Leptin receptor, neuronal lineage, Pluripotency |
Abstract |
The role of leptin receptor (OB-R) signaling in linking pluripotency with growth and development and the consequences of dysfunctional leptin signaling on progression of metabolic disease is poorly understood. Using a global unbiased proteomics approach we report that embryonic fibroblasts (MEFs) carrying the db/db mutation exhibit metabolic abnormalities, while their reprogrammed induced pluripotent stem cells (iPSCs) show altered expression of proteins involved in embryonic development. An upregulation in expression of eukaryotic translation initiation factor 4e (Eif4e) and Stat3 binding to the Eif4e promoter was supported by enhanced protein synthesis in mutant iPSCs. Directed differentiation of db/db iPSCs toward the neuronal lineage showed defects. Gene editing to correct the point mutation in db/db iPSCs using CRISPR-Cas9, restored expression of neuronal markers and protein synthesis while reversing the metabolic defects. These data imply a direct role for OB-R in regulating metabolism in embryonic fibroblasts and key developmental pathways in iPSCs. |
Year of Publication |
2020
|
Journal |
Stem cell reports
|
Volume |
15
|
Issue |
5
|
Number of Pages |
1067-1079
|
Date Published |
11/2020
|
ISSN Number |
2213-6711
|
DOI |
10.1016/j.stemcr.2020.10.001
|
Alternate Journal |
Stem Cell Reports
|
PMID |
33125875
|
PMCID |
PMC7664055
|
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