FSH blockade improves cognition in mice with Alzheimer's disease.
Jing XiongSeong Su KangZhihao WangXia LiuTan-Chun KuoFunda KorkmazAshley D PadillaSari MiyashitaPokman ChanZhaohui ZhangPavel KatselJocoll BurgessAnisa GumerovaKseniia IevlevaDamini SantShan Ping YuValeriia MuradovaTal FrolingerDaria LiznevaJameel IqbalKi Ann GoosensSakshi GeraClifford J RosenVahram HaroutunianVitaly RyuTony YuenMone ZaidiKeqiang YePublished in: Nature (2022)
Alzheimer's disease has a higher incidence in older women, with a spike in cognitive decline that tracks with visceral adiposity, dysregulated energy homeostasis and bone loss during the menopausal transition 1,2 . Inhibiting the action of follicle-stimulating hormone (FSH) reduces body fat, enhances thermogenesis, increases bone mass and lowers serum cholesterol in mice 3-7 . Here we show that FSH acts directly on hippocampal and cortical neurons to accelerate amyloid-β and Tau deposition and impair cognition in mice displaying features of Alzheimer's disease. Blocking FSH action in these mice abrogates the Alzheimer's disease-like phenotype by inhibiting the neuronal C/EBPβ-δ-secretase pathway. These data not only suggest a causal role for rising serum FSH levels in the exaggerated Alzheimer's disease pathophysiology during menopause, but also reveal an opportunity for treating Alzheimer's disease, obesity, osteoporosis and dyslipidaemia with a single FSH-blocking agent.
Keyphrases
- cognitive decline
- mild cognitive impairment
- high fat diet induced
- adipose tissue
- spinal cord
- signaling pathway
- bone mineral density
- dna methylation
- genome wide
- spinal cord injury
- gene expression
- body mass index
- weight gain
- weight loss
- machine learning
- deep learning
- artificial intelligence
- subarachnoid hemorrhage
- data analysis