APOE4 genotype exacerbates the impact of menopause on cognition and synaptic plasticity in APOE-TR mice

Matthew G. Pontifex; Anneloes Martinsen; Rasha Noureldin M. Saleh; Glenn Harden; Noemi Tejera; Michael Müller; Chris Fox; David Vauzour; Anne Marie Minihane

Journal ArticleOPEN ACCESS

APOE4 genotype exacerbates the impact of menopause on cognition and synaptic plasticity in APOE-TR mice

FASEB Journal (2021) 35(5)

DOI: 10.1096/fj.202002621RR

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Abstract

The impact of sex and menopausal status in Alzheimer’s disease remains understudied despite increasing evidence of greater female risk, particularly in APOE4 carriers. Utilizing female APOE-TR mice maintained on a high-fat diet background we induced ovarian failure through repeated VCD injections, to mimic human menopause. At 12 months of age, recognition memory and spatial memory were assessed using object recognition, Y-maze spontaneous alternation, and Barnes maze. A VCD*genotype interaction reduced the recognition memory (P

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Pontifex, M. G., Martinsen, A., Saleh, R. N. M., Harden, G., Tejera, N., Müller, M., … Minihane, A. M. (2021). APOE4 genotype exacerbates the impact of menopause on cognition and synaptic plasticity in APOE-TR mice. FASEB Journal, 35(5). https://doi.org/10.1096/fj.202002621RR

APOE4 genotype exacerbates the impact of menopause on cognition and synaptic plasticity in APOE-TR mice

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