| Literature DB >> 27466694 |
Yurong Xin1, Haruka Okamoto1, Jinrang Kim1, Min Ni1, Christina Adler1, Katie Cavino1, Erqian Na1, Andrew J Murphy1, George D Yancopoulos1, Calvin Lin1, Jesper Gromada1.
Abstract
Aging improves pancreatic β-cell function in mice. This is a surprising finding because aging is typically associated with functional decline. We performed single-cell RNA sequencing of β-cells from 3- and 26-month-old mice to explore how changes in gene expression contribute to improved function with age. The old mice were healthy and had reduced blood glucose levels and increased β-cell mass, which correlated to their body weight. β-Cells from young and old mice had similar transcriptome profiles. In fact, only 193 genes (0.89% of all detected genes) were significantly regulated (≥2-fold; false discovery rate < 0.01; normalized counts > 5). Of these, 183 were down-regulated and mainly associated with pathways regulating gene expression, cell cycle, cell death, and survival as well as cellular movement, function, and maintenance. Collectively our data show that β-cells from very old mice have transcriptome profiles similar to those of young mice. These data support previous findings that aging is not associated with reduced β-cell mass or functional β-cell decline in mice.Entities:
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Year: 2016 PMID: 27466694 DOI: 10.1210/en.2016-1235
Source DB: PubMed Journal: Endocrinology ISSN: 0013-7227 Impact factor: 4.736