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A novel mouse model overexpressing Nocturnin results in decreased fat mass in male mice.


ABSTRACT: Nocturnin (NOCT) belongs to the Mg2+ dependent Exonucleases, Endonucleases, Phosphatase (EEP) family of enzymes that exhibit various functions in vitro and in vivo. NOCT is known to function as a deadenylase, cleaving poly-A tails from mRNA (messenger RNA) transcripts. Previously, we reported a role for NOCT in regulating bone marrow stromal cell differentiation through its interactions with PPAR?. In this study, we characterized the skeletal and adipose tissue phenotype when we globally overexpressed Noct in vivo. After 12 weeks of Noct overexpression, transgenic male mice had lower fat mass compared to controls, with no significant differences in the skeleton. Based on the presence of a mitochondrial target sequence in NOCT, we determined that mouse NOCT protein localizes to the mitochondria; subsequently, we found that NOCT overexpression led to a significant increase in the preadipocytes ability to utilize oxidative phosphorylation for ATP (adenosine triphosphate) generation. In summary, the effects of NOCT on adipocytes are likely through its novel role as a mediator of mitochondrial function.

SUBMITTER: Le PT 

PROVIDER: S-EPMC6660355 | biostudies-literature | 2019 Nov

REPOSITORIES: biostudies-literature

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A novel mouse model overexpressing Nocturnin results in decreased fat mass in male mice.

Le Phuong T PT   Bornstein Sheila A SA   Motyl Katherine J KJ   Tian Li L   Stubblefield Jeremy J JJ   Hong Hee-Kyung HK   Takahashi Joseph S JS   Green Carla B CB   Rosen Clifford J CJ   Guntur Anyonya R AR  

Journal of cellular physiology 20190405 11


Nocturnin (NOCT) belongs to the Mg<sup>2+</sup> dependent Exonucleases, Endonucleases, Phosphatase (EEP) family of enzymes that exhibit various functions in vitro and in vivo. NOCT is known to function as a deadenylase, cleaving poly-A tails from mRNA (messenger RNA) transcripts. Previously, we reported a role for NOCT in regulating bone marrow stromal cell differentiation through its interactions with PPARγ. In this study, we characterized the skeletal and adipose tissue phenotype when we globa  ...[more]

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