| Literature DB >> 35981426 |
Jessica Klusek1, Roger Newman-Norlund2, Amanda J Fairchild3, Sarah Newman-Norlund4, Sara Sayers4, Jill C Stewart5, Elizabeth Berry-Kravis6, Julius Fridriksson4.
Abstract
The FMR1 gene plays a key role in adult neurogenesis and neuroplasticity, and thus may contribute to age-related health in the population. The current study focused on the "low normal" FMR1 genotype, defined by lower-than-typical numbers of FMR1 CGG repeats (<26), as a potential genetic determinant of age-related health. We characterized the effect of the low normal FMR1 genotype on psychological well-being and motor function in a racially diverse non-clinical sample of older adult women. Women with low CGG repeats were distinguished from those with CGGs falling within the mid-high end of the normal range by reduced performance on multimodal assessments of motor function and psychological well-being, with large effect sizes. Robust continuous associations were also detected between lower CGG repeat length and reduced psychological well-being, balance, and dexterity. Findings suggest that FMR1 may represent an important mediator of individual differences in age-related health; larger epidemiological studies are needed. Given that approximately 23-35% of females carry the low normal genotype, efforts to understand its clinical effects have relevance a broad swath of the aging population.Entities:
Keywords: Age-related health; Balance; CGG repeat length; Dexterity; Fragile X-associated conditions; Healthy aging; Low zone CGGs
Year: 2022 PMID: 35981426 PMCID: PMC9464716 DOI: 10.1016/j.archger.2022.104789
Source DB: PubMed Journal: Arch Gerontol Geriatr ISSN: 0167-4943 Impact factor: 4.163