Estrogen receptor polymorphisms and incident dementia: The prospective 3C study

Ryan, Joanne; Carrière, Isabelle; Carcaillon, Laure; Dartigues, Jean‐François; Auriacombe, Sophie; Rouaud, Olivier; Berr, Claudine; Ritchie, Karen; Scarabin, P.Y.; Ancelin, Marie-Laure

doi:10.1016/j.jalz.2012.12.008

Cited by 36 publications

(27 citation statements)

References 54 publications

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“…However, significant associations with the ERβ polymorphism, rs1256049, were identified including an increased risk of substantial decline in visual memory, psychomotor speed, and on the incidence of MCI (Ryan et al, 2013). Further analysis indicated that, in support of the initial finding of a significant interaction between ERα and ERβ polymorphisms and the risk for AD (Lambert et al, 2001), the association between ERβ polymorphism and AD appeared to be modified by ERα polymorphism (Ryan et al, 2014). Interestingly, the same study showed a slight association between the minor allele of the ERβ SNP, rs4986938, and a decreased risk of decline in psychomotor speed (Ryan et al, 2013).…”

Section: Erβ Polymorphisms In Admentioning

confidence: 75%

Estrogen receptor β in Alzheimer’s disease: From mechanisms to therapeutics

Zhao

Woody

Chhibber

2015

Ageing Research Reviews

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Alzheimer's disease (AD) disproportionally affects women and men. The female susceptibility for AD has been largely associated with the loss of ovarian sex hormones during menopause. This review examines current understanding of the role of estrogen receptor β (ERβ) in the regulation of neurological health and its implication in the development and intervention of AD. Since its discovery in 1996, research conducted over the last 15-20 years has documented a great deal of evidence indicating that ERβ plays a pivotal role in a broad spectrum of brain activities from development to aging. ERβ genetic polymorphisms have been associated with cognitive impairment and increased risk for AD predominantly in women. The role of ERβ in the intervention of AD has been demonstrated by the alteration of AD pathology in response to treatment with ERβ-selective modulators in transgenic models that display pronounced plaque and tangle histopathological presentations as well as learning and memory deficits. Future studies that explore the potential interactions between ERβ signaling and the genetic isoforms of human apolipoprotein E (APOE) in brain aging and development of AD-risk phenotype are critically needed. The current trend of lost-in-translation in AD drug development that has primarily been based on early-onset familial AD (FAD) models underscores the urgent need for novel models that recapitulate the etiology of late-onset sporadic AD (SAD), the most common form of AD representing more than 95% of the current human AD population. Combining the use of FAD-related models that generally have excellent face validity with SAD-related models that hold more reliable construct validity would together increase the predictive validity of preclinical findings for successful translation into humans.

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Section: Erβ Polymorphisms In Admentioning

confidence: 75%

Estrogen receptor β in Alzheimer’s disease: From mechanisms to therapeutics

Zhao

Woody

Chhibber

2015

Ageing Research Reviews

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“…Estrogen receptors play a key and contrasting role in regulation of ApoE gene and protein expression (33) and risk of AD(141). ERα up-regulated ApoE mRNA and protein expression whereas in contrast, ERβ down-regulated ApoE mRNA and protein expression(33).…”

Section: Sex Differences In Apoe Genotype and Risk Of Alzheimer’smentioning

confidence: 99%

“…These data suggest that use of ER-selective ligands could provide therapeutic benefit to reduce the risk of AD by increasing ApoE expression in ApoE 2 or 3 allele carriers and decreasing ApoE expression in ApoE4 allele carriers. Polymorphisms in both estrogen receptor alpha (rs4986938) and estrogen receptor β (rs2234693) have been associated with increased risk of dementia and AD (141). …”

Section: Sex Differences In Apoe Genotype and Risk Of Alzheimer’smentioning

confidence: 99%

Age, APOE and sex: Triad of risk of Alzheimer’s disease

Riedel

Thompson

Brinton

2016

The Journal of Steroid Biochemistry and Molecular Biology

467

400

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Age, apolipoprotein E ɛ4 (APOE) and chromosomal sex are well-established risk factors for late-onset Alzheimer’s disease (LOAD; AD). Over 60% of persons with AD harbor at least one APOE-ɛ4 allele. The sex-based prevalence of AD is well documented with over 60% of persons with AD being female. Evidence indicates that the APOE-ɛ4 risk for AD is greater in women than men, which is particularly evident in heterozygous women carrying one APOE-ɛ4 allele. Paradoxically, men homozygous for APOE-ɛ4 are reported to be at greater risk for mild cognitive impairment and AD. Herein, we discuss the complex interplay between the three greatest risk factors for Alzheimer’s disease, age, APOE-ɛ4 genotype and female sex. We propose that the convergence of these three risk factors, and specifically the bioenergetic aging perimenopause to menopause transition unique to the female, creates a risk profile for AD unique to the female. Further, we discuss the unique risk of the APOE4 positive male which appears to emerge early in the aging process. Evidence for impact of the triad of AD risk factors is most evident in the temporal trajectory of AD progression and burden of pathology in relation to APOE genotype, age and sex. Collectively, the data indicate complex interactions between age, APOE genotype and gender that belies a one size fits all approach and argues for a precision medicine approach that integrates across the three main risk factors for Alzheimer’s disease.

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“…A recent study proposed that one dominant negative splice variant, ERβ2, may mediate differential responses to E 2 treatment early and late after ovariectomy (OVX) in rats, such that only if estrogen treatment is initiated early after OVX is it able to prevent induction of the dominant negative ERβ2 variant (Wang et al, 2012). In addition to splice variants, there are several ERα polymorphisms that increase the risk of Alzheimer’s disease (AD) specifically in women, particularly when associated with the APOE ε4 allele (Ryan et al, 2013). …”

Section: Estrogen Estrogen Receptors and Intracellular Signalingmentioning

confidence: 99%

Estrogen: A master regulator of bioenergetic systems in the brain and body

Rettberg

Yao

Brinton

2014

Frontiers in Neuroendocrinology

388

299

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Estrogen is a fundamental regulator of the metabolic system of the female brain and body. Within the brain, estrogen regulates glucose transport, aerobic glycolysis, and mitochondrial function to generate ATP. In the body, estrogen protects against adiposity, insulin resistance, and type II diabetes, and regulates energy intake and expenditure. During menopause, decline in circulating estrogen is coincident with decline in brain bioenergetics and shift towards a metabolically compromised phenotype. Compensatory bioenergetic adaptations, or lack thereof, to estrogen loss could determine risk of late-onset Alzheimer’s disease. Estrogen coordinates brain and body metabolism, such that peripheral metabolic state can indicate bioenergetic status of the brain. By generating biomarker profiles that encompass peripheral metabolic changes occurring with menopause, individual risk profiles for decreased brain bioenergetics and cognitive decline can be created. Biomarker profiles could identify women at risk while also serving as indicators of efficacy of hormone therapy or other preventative interventions.

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Estrogen receptor polymorphisms and incident dementia: The prospective 3C study

Cited by 36 publications

References 54 publications

Estrogen receptor β in Alzheimer’s disease: From mechanisms to therapeutics

Estrogen receptor β in Alzheimer’s disease: From mechanisms to therapeutics

Age, APOE and sex: Triad of risk of Alzheimer’s disease

Estrogen: A master regulator of bioenergetic systems in the brain and body

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