Literature DB >> 36206387

Contributions of sex and genotype to exploratory behavior differences in an aged humanized APOE mouse model of late-onset Alzheimer's disease.

John W McLean1,2, Avnish Bhattrai1,3, Francesca Vitali1, Adam C Raikes1, Jean-Paul L Wiegand1, Roberta Diaz Brinton1,3.   

Abstract

Age, genetics, and chromosomal sex have been identified as critical risk factors for late-onset Alzheimer's disease (LOAD). The predominant genetic risk factor for LOAD is the apolipoprotein E ε4 allele (APOE4), and the prevalence of LOAD is higher in females. However, the translational validity of APOE4 mouse models for AD-related cognitive impairment remains to be fully determined. The present study investigated the role of both sex and genotype on learning and memory in aged, humanized APOE knock-in mice. Aged (23.27 mo ± 1.21 mo; 39 male/37 female) APOE3/3, APOE3/4, and APOE4/4 mice performed a novel object recognition (NOR) assay. Task-related metrics were analyzed using two-way sex by genotype ANOVAs. Sex differences were more prominent relative to APOE genotype. Prior to NOR, female mice exhibited thigmotaxic center zone avoidance during the open field task relative to males, regardless of genotype. Within object familiarization and NOR tasks, females had greater object interaction and locomotion. Interestingly, only APOE4/4 females on average recognized the novel object. These results suggest that APOE4, although strongly related to LOAD pathogenesis, does not drive cognitive decline in the absence of other risk factors even in very aged mice. Chromosomal sex is a key driver of behavioral phenotypes and thus is a critical variable for translatability of interventions designed to preserve learning and memory in animal models of LOAD. Last, there was a very high degree of variability in behavioral performance across APOE genotypes. A cluster analysis of the behavioral data revealed a low-activity and a high-activity cluster. APOE4 carriers were overrepresented in the low-activity cluster, while male:female distributions did not differ. Collectively, the behavioral data indicate that chromosomal sex has the greatest impact on behavioral phenotype, and APOE4 carrier status may confer greater risk for cognitive decline in some animals.
© 2022 McLean et al.; Published by Cold Spring Harbor Laboratory Press.

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Year:  2022        PMID: 36206387      PMCID: PMC9488030          DOI: 10.1101/lm.053588.122

Source DB:  PubMed          Journal:  Learn Mem        ISSN: 1072-0502            Impact factor:   2.699


  75 in total

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Review 2.  Estrogen: a master regulator of bioenergetic systems in the brain and body.

Authors:  Jamaica R Rettberg; Jia Yao; Roberta Diaz Brinton
Journal:  Front Neuroendocrinol       Date:  2013-08-29       Impact factor: 8.606

Review 3.  Animal models of anxiety and depression: how are females different?

Authors:  P Palanza
Journal:  Neurosci Biobehav Rev       Date:  2001-05       Impact factor: 8.989

4.  mclust 5: Clustering, Classification and Density Estimation Using Gaussian Finite Mixture Models.

Authors:  Luca Scrucca; Michael Fop; T Brendan Murphy; Adrian E Raftery
Journal:  R J       Date:  2016-08       Impact factor: 3.984

5.  APOE ε4 differentially influences change in memory performance depending on age. The SMART-MR study.

Authors:  Hadassa M Jochemsen; Majon Muller; Yolanda van der Graaf; Mirjam I Geerlings
Journal:  Neurobiol Aging       Date:  2011-09-09       Impact factor: 4.673

6.  Isoform-specific effects of human apolipoprotein E on brain function revealed in ApoE knockout mice: increased susceptibility of females.

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7.  Accumulation of intraneuronal Abeta correlates with ApoE4 genotype.

Authors:  Ditte Z Christensen; Thomas Schneider-Axmann; Paul J Lucassen; Thomas A Bayer; Oliver Wirths
Journal:  Acta Neuropathol       Date:  2010-03-10       Impact factor: 17.088

8.  Gait analysis in demented subjects: Interests and perspectives.

Authors:  Olivier Beauchet; Gilles Allali; Gilles Berrut; Caroline Hommet; Véronique Dubost; Frédéric Assal
Journal:  Neuropsychiatr Dis Treat       Date:  2008-02       Impact factor: 2.570

Review 9.  Triad of Risk for Late Onset Alzheimer's: Mitochondrial Haplotype, APOE Genotype and Chromosomal Sex.

Authors:  Yiwei Wang; Roberta D Brinton
Journal:  Front Aging Neurosci       Date:  2016-10-04       Impact factor: 5.750

Review 10.  Inflammation: Bridging Age, Menopause and APOEε4 Genotype to Alzheimer's Disease.

Authors:  Aarti Mishra; Roberta D Brinton
Journal:  Front Aging Neurosci       Date:  2018-10-09       Impact factor: 5.750

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