Intra-pituitary follicle-stimulating hormone signaling regulates hepatic lipid metabolism in mice.
Sen QiaoSamer AlasmiAmanda WyattPhilipp WartenbergHongmei WangMichael CandlishDebajyoti DasMari AokiRamona GrünewaldZiyue ZhouQinghai TianQiang YuViktoria GötzAnouar BelkacemiAhsan RazaFabien EctorsKathrin KattlerGilles GasparoniJörn WalterPeter LippPatrice MollardDaniel J BernardErsin KaratayliSenem Ceren KaratayliFrank LammertUlrich BoehmPublished in: Nature communications (2023)
Inter-organ communication is a major hallmark of health and is often orchestrated by hormones released by the anterior pituitary gland. Pituitary gonadotropes secrete follicle-stimulating hormone (FSH) and luteinizing hormone (LH) to regulate gonadal function and control fertility. Whether FSH and LH also act on organs other than the gonads is debated. Here, we find that gonadotrope depletion in adult female mice triggers profound hypogonadism, obesity, glucose intolerance, fatty liver, and bone loss. The absence of sex steroids precipitates these phenotypes, with the notable exception of fatty liver, which results from ovary-independent actions of FSH. We uncover paracrine FSH action on pituitary corticotropes as a mechanism to restrain the production of corticosterone and prevent hepatic steatosis. Our data demonstrate that functional communication of two distinct hormone-secreting cell populations in the pituitary regulates hepatic lipid metabolism.
Keyphrases
- growth hormone
- high fat diet induced
- bone loss
- healthcare
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- fatty acid
- insulin resistance
- cell therapy
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- stem cells
- risk assessment
- artificial intelligence
- skeletal muscle
- mesenchymal stem cells
- adipose tissue
- autism spectrum disorder
- big data
- weight gain
- young adults
- physical activity
- smoking cessation
- human health
- childhood cancer