Levels of Estrogen Receptors &amp;#945; and &amp;#946; in Frontal Cortex of Patients with Alzheimers Disease: Relationship to Mini-Mental State Examination Scores

Kelly, Jeremiah F.; Bienias, Julia L.; Shah, Avni; Meeke, Kathleen; Schneider, Julie A.; Soriano, E; Bennett, David A.

doi:10.2174/156720508783884611

Cited by 40 publications

(26 citation statements)

References 47 publications

(46 reference statements)

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“…Specifically, an ER shift from the nucleus to the cytoplasm has been observed in both human cases [115] and AD transgenic mice [116]. Further, various clinical studies have reported that cortical ER levels correlate with mini-mental state examination scores in AD women [117] and that certain ER allele differences correlate with higher AD risk in women with Down syndrome [118]. Even hippocampal ER immunoreactivity in AD is reportedly increased compared to age-matched controls [119].…”

Section: Neuroactive Selective Estrogen Recep-tor Modulatorsmentioning

confidence: 99%

The Potential Use of Hormone-Based Therapeutics for the Treatment of Alzheimers Disease

Carroll¹,

Rosario²

2012

CAR

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In both men and women, age-related loss of sex steroid hormones has been linked to an increased risk for Alzheimer's disease (AD). The primary female hormone estrogen, and the primary male hormone testosterone have numerous protective effects in the brain relevant to the prevention of AD such as the promotion of neuron viability, reduction of β- amyloid accumulation and alleviation of tau hyperphosphorylation. Therefore it has been hypothesized that the precipitous loss of these hormones either through menopause or normal aging, can increase susceptibility to AD pathogenesis. This review will discuss the basic science research and epidemiological evidence largely supporting this hypothesis, as well as the estrogen-based hormone therapy clinical findings that have recently shed doubt on this theory. The complications associated with estrogen-based hormone therapy such as the inclusion of a progestogen, hormone responsiveness with age, and natural vs. synthetic hormones will be discussed. Further, we will outline the cancer risks facing both estrogen and testosterone-based hormone therapy. Most importantly, this review will discuss the present and future strategies to translate the neuroprotective properties of sex steroid hormones into safe and efficacious treatments for AD. One of the most promising translational tools thus far may be the development of selective estrogen and androgen receptor modulators. However, additional research is needed to optimize these and other translational tools towards the successful use of hormone therapies in both men and women to delay, prevent, and or treat AD.

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Section: Neuroactive Selective Estrogen Recep-tor Modulatorsmentioning

confidence: 99%

The Potential Use of Hormone-Based Therapeutics for the Treatment of Alzheimers Disease

Carroll¹,

Rosario²

2012

CAR

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“…ERα also becomes less sensitive to E 2 treatment as animals age; this is in contrast to ERβ, which shows decreased levels with age but remains responsive to E 2 treatment (Waters et al, 2011). Clinical studies have shown a linear relationship between Mini Mental State Exam (MMSE) score and ERα β, in the frontal cortex of Alzheimer’s patients (Kelly et al, 2008). The existence of variant isoforms of ERα that may influence cognitive impairment has been proposed (Kelly et al, 2008); this was later observed in a cohort of non-demented elderly (Yaffe et al, 2009).…”

Section: Estrogen Estrogen Receptors and Intracellular Signalingmentioning

confidence: 99%

“…Clinical studies have shown a linear relationship between Mini Mental State Exam (MMSE) score and ERα β, in the frontal cortex of Alzheimer’s patients (Kelly et al, 2008). The existence of variant isoforms of ERα that may influence cognitive impairment has been proposed (Kelly et al, 2008); this was later observed in a cohort of non-demented elderly (Yaffe et al, 2009). Thus the data show that decreased ERα responsiveness may mediate cognitive impairment and dementia; during aging, although ERβ remains responsive to E 2 , it is unable to compensate for the loss of ERα.…”

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

371

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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“…The detected levels of ERs in postmortem brain tissue of AD patients is related to the severity of cognitive impairment assessed proximate to death, and only the reduction of ER-α from frontal cortex is correlated to Mini-Mental State Examination score, not the ER-β [95]. The spectrometry, immunohistochemistry, and quantitative real-time PCR of the autopsied Japanese AD patients compared to controls [96] have revealed a glial nuclear ER-β expression significantly lower in white matter in the AD group vs. controls, without any significant differences in estrogen concentrations, and the conclusion was that estrogens have effects on glias and neurons in the etiology of AD, and the correlation between BMI and estrogen concentrations in the frontal lobe suggests the importance of non-brain sources of estrogens particularly in controls.…”

Section: Estrogen Receptors (Ers) Genetic Polymorphism and Epigenetimentioning

confidence: 99%

“…Regarding ERs, there are new details about the genes, and mRNA variants of ER-α expressed in different parts of the human brain, and there are specific ER-α mRNA splice variants or isoforms of ER-α in the medial mammillary nucleus (MMN) in AD [102] or in the frontal cortex in AD patients [95], and their relationship to cognitive impairment.…”

Section: Estrogen Receptors (Ers) Genetic Polymorphism and Epigenetimentioning

confidence: 99%

New Insights for Hormone Therapy in Perimenopausal Women Neuroprotection

Russu¹,

Antonescu²

2018

Sex Hormones in Neurodegenerative Processes and Diseases

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Perimenopause is a mandatory period in women's life, when the medical staff may initiate hormone therapy with sex steroids for the delay of brain aging and neurodegenerative diseases, during the so-called "window of opportunity." Animals' models are helpful to sustain the still controversial results of human clinical observational and/or randomized controlled studies. Estrogens, progesterone, and androgens, with their nuclear and membrane receptors, genes, and epigenetics, with their connections to cholinergic, GABAergic, serotoninergic, and glutamatergic systems are involved in women'sn o r m a lb r a i no ri n brain's pathology. The sex steroids are active through direct and/or indirect mechanisms to modulate and/or to protect brain plasticity, and vessels network, fuel metabolism-glucose, ketones, ATP, to reduce insulin resistance, and inflammation of the aging brain through blood-brain barrier disruption, microglial aberrant activation, and neural cell survival/loss.

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Levels of Estrogen Receptors α and β in Frontal Cortex of Patients with Alzheimers Disease: Relationship to Mini-Mental State Examination Scores

Cited by 40 publications

References 47 publications

The Potential Use of Hormone-Based Therapeutics for the Treatment of Alzheimers Disease

The Potential Use of Hormone-Based Therapeutics for the Treatment of Alzheimers Disease

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

New Insights for Hormone Therapy in Perimenopausal Women Neuroprotection

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