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Mitochondrial RNA stimulates beige adipocyte development in young mice.


ABSTRACT: Childhood obesity is a serious public health crisis and a critical factor that determines future obesity prevalence. Signals affecting adipocyte development in early postnatal life have a strong potential to trigger childhood obesity; however, these signals are still poorly understood. We show here that mitochondrial (mt)RNA efflux stimulates transcription of nuclear-encoded genes for mitobiogenesis and thermogenesis in adipocytes of young mice and human infants. While cytosolic mtRNA is a potential trigger of the interferon (IFN) response, young adipocytes lack such a response to cytosolic mtRNA due to the suppression of IFN regulatory factor (IRF)7 expression by vitamin D receptor signalling. Adult and obese adipocytes, however, strongly express IRF7 and mount an IFN response to cytosolic mtRNA. In turn, suppressing IRF7 expression in adult adipocytes restores mtRNA-induced mitobiogenesis and thermogenesis and eventually mitigates obesity. Retrograde mitochondrion-to-nucleus signalling by mtRNA is thus a mechanism to evoke thermogenic potential during early adipocyte development and to protect against obesity.

SUBMITTER: Hoang AC 

PROVIDER: S-EPMC9771821 | biostudies-literature | 2022 Dec

REPOSITORIES: biostudies-literature

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Mitochondrial RNA stimulates beige adipocyte development in young mice.

Hoang Anh Cuong AC   Sasi-Szabó László L   Pál Tibor T   Szabó Tamás T   Diedrich Victoria V   Herwig Annika A   Landgraf Kathrin K   Körner Antje A   Röszer Tamás T  

Nature metabolism 20221128 12


Childhood obesity is a serious public health crisis and a critical factor that determines future obesity prevalence. Signals affecting adipocyte development in early postnatal life have a strong potential to trigger childhood obesity; however, these signals are still poorly understood. We show here that mitochondrial (mt)RNA efflux stimulates transcription of nuclear-encoded genes for mitobiogenesis and thermogenesis in adipocytes of young mice and human infants. While cytosolic mtRNA is a poten  ...[more]

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