Health benefits attributed to 17α-estradiol, a lifespan-extending compound, are mediated through estrogen receptor α

Mann, Shivani N.; Hadad, Niran; Holte, Molly Nelson; Rothman, Alicia R.; Sathiaseelan, Roshini; Mondal, Samim Ali; Agbaga, Martin-Paul; Unnikrishnan, Archana; Subramaniam, Malayannan; Hawse, John R.; Huffman, Derek M.; Freeman, Willard M.; Stout, Michael B.

doi:10.7554/elife.59616

Cited by 30 publications

(27 citation statements)

References 157 publications

(282 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Interestingly, both SHAM and OVX mice receiving 17α-E2 displayed similar body mass and adiposity levels as the SHAM CON group, thereby suggesting that 17α-E2 treatment elicits similar effects as endogenous estrogens (likely 17β-E2), yet is not particularly synergistic. This suggests 17α-E2 and 17β-E2 are likely competing for the same receptors in vivo, which we provide evidence for in other reports ( Mann et al, 2020 ). We also evaluated intra- (periovarian [POV]) and extra-peritoneal (inguinal [ING]) white adipose tissue (WAT) masses because a redistribution of lipid to ectopic sites occurs and intra-peritoneal WAT depots increase with aging ( Stout et al, 2014 ; Stout et al, 2017b ).…”

Section: Resultssupporting

confidence: 87%

“…17α-E2 has recently been shown to induce considerable benefits on healthspan and lifespan in male mice ( Harrison et al, 2014 ; Strong et al, 2016 ; Stout et al, 2017a ; Garratt et al, 2017 ; Mann et al, 2020 ; Garratt et al, 2018 ), although little benefit has been observed in females receiving the compound ( Garratt et al, 2017 ; Garratt et al, 2018 ). We have postulated that the lack of beneficial effects of 17α-E2 in females may be due to the high levels of endogenous 17β-E2, which may outcompete the less-potent 17α-E2 at estrogen receptors ( Mann et al, 2020 ). In this report we sought to determine if 17α-E2 could elicit beneficial outcomes on age-related phenotypes associated with ovariectomy in female mice, with a specific emphasis on bone loss.…”

Section: Discussionmentioning

confidence: 99%

“…Given that it elicits such robust sexually dimorphic responses in mice, studies employing 17α-E2 can provide critical insight into the mechanisms underlying the differences in aging biology between the sexes. To our knowledge, the effects of 17α-E2 on bone dynamics has not been previously evaluated, although our recent work shows that 17α-E2 induces metabolic benefits through ERα ( Mann et al, 2020 ), a receptor known to be highly involved in bone homeostasis ( Khosla and Monroe, 2018 ). This led us to hypothesize that 17α-E2 would induce beneficial effects in OVX mice, which is a model for post-menopausal bone loss in humans.…”

Section: Discussionmentioning

confidence: 99%

“…Despite the collective evidence outlined above, it must be noted that most of the studies to date have evaluated health parameters that deteriorate to a greater degree in male mammals with advancing age ( Garratt and Stout, 2018 ), including nutrient-sensing pathway perturbations, systemic metabolic parameters, and pro-inflammatory stress ( Stout et al, 2017a ; Steyn et al, 2018 ; Garratt et al, 2017 ; Mann et al, 2020 ; Garratt et al, 2018 ). In fact, it is well-established that female mammals possess an inherent advantage as compared to their male counterparts with regard to metabolic plasticity, immunological responses, and DNA damage ( Austad and Fischer, 2016 ; Moran et al, 2013 ).…”

Section: Introductionmentioning

confidence: 99%

“…This is known to be at least partially mediated by endogenous 17β-E2 due to its ability to beneficially effect a myriad of pathways and processes including glucose homeostasis, insulin sensitivity, immune cell migration and activation, and the mTOR signaling pathway in an estrogen receptor α (ERα)-dependent manner ( Mauvais-Jarvis et al, 2013 ; Bian et al, 2019 ). Despite 17α-E2 having lesser binding affinity for ERα than 17β-E2 ( Edwards and McGuire, 1980 ; Anstead et al, 1997 ), we have recently determined that ERα likely plays an important role in mediating 17α-E2 effects on health parameters in male mice ( Mann et al, 2020 ). In light of these recent findings, coupled with the fact that no studies to date have explored the effects of 17α-E2 on female-dominant age-related conditions (e.g.…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

17α-Estradiol prevents ovariectomy-mediated obesity and bone loss

Mann

Pitel

Nelson-Holte

et al. 2020

Experimental Gerontology

Self Cite

View full text Add to dashboard Cite

Menopause is a natural physiological process in older women that is associated with reduced estrogen production and results in increased risk for obesity, diabetes, and osteoporosis. 17α-estradiol (17α-E2) treatment in males, but not females, reverses several metabolic conditions associated with advancing age, highlighting sexually dimorphic actions on age-related pathologies. In this study we sought to determine if 17α-E2 could prevent ovariectomy (OVX)-mediated detriments on adiposity and bone parameters in females. Eight-week-old female C57BL/6J mice were subjected to SHAM or OVX surgery and received dietary 17α-E2 during a six-week intervention period. We observed that 17α-E2 prevented OVX-induced increases in body weight and adiposity. Similarly, uterine weight and luminal cell thickness were decreased by OVX and prevented by 17α-E2 treatment. Interestingly, 17α-E2 prevented OVX-induced declines in tibial metaphysis cancellous bone. And similarly, 17α-E2 improved bone density parameters in both tibia and femur cancellous bone, primarily in OVX mice. In contrast, to the effects on cancellous bone, cortical bone parameters were largely unaffected by OVX or 17α-E2. In the non-weight bearing lumbar vertebrae, OVX reduced trabecular thickness but not spacing, while 17α-E2 increased trabecular thickness and reduced spacing. Despite this, 17α-E2 did improve bone volume/tissue volume in lumbar vertebrae. Overall, we found that 17α-E2 prevented OVX-induced increases in adiposity and changes in bone mass and architecture, with minimal effects in SHAM-operated mice. We also observed that 17α-E2 rescued uterine tissue mass and lining morphology to control levels without inducing hypertrophy, suggesting that 17α-E2 could be considered as an adjunct to traditional hormone replacement therapies.

show abstract

Section: Resultssupporting

confidence: 87%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

17α-Estradiol prevents ovariectomy-mediated obesity and bone loss

Mann

Pitel

Nelson-Holte

et al. 2020

Experimental Gerontology

Self Cite

View full text Add to dashboard Cite

show abstract

Einstein-Nathan Shock Center: translating the hallmarks of aging to extend human health span

et al. 2021

View full text Add to dashboard Cite

Circulating testosterone and dehydroepiandrosterone are associated with individual motor unit features in untrained and highly active older men

et al. 2021

View full text Add to dashboard Cite

Long-term exercise training has been considered as an effective strategy to counteract age-related hormonal declines and minimise muscle atrophy. However, human data relating circulating hormone levels with motor nerve function are scant. The aims of the study were to explore associations between circulating sex hormone levels and motor unit (MU) characteristics in older men, including masters athletes competing in endurance and power events. Forty-three older men (mean ± SD age: 69.9 ± 4.6 years) were studied based on competitive status. The serum concentrations of dehydroepiandrosterone (DHEA), total testosterone (T) and estradiol were quantified using liquid chromatography mass spectrometry. Intramuscular electromyographic signals were recorded from vastus lateralis (VL) during 25% of maximum voluntary isometric contractions and processed to extract MU firing rate (FR), and motor unit potential (MUP) features. After adjusting for athletic status, MU FR was positively associated with DHEA levels (p = 0.019). Higher testosterone and estradiol were associated with lower MUP complexity; these relationships remained significant after adjusting for athletic status (p = 0.006 and p = 0.019, respectively). Circulating DHEA was positively associated with MU firing rate in these older men. Higher testosterone levels were associated with reduced MUP complexity, indicating reduced electrophysiological temporal dispersion, which is related to decreased differences in conduction times along axonal branches and/or MU fibres. Although evident in males only, this work highlights the potential of hormone administration as a therapeutic interventional strategy specifically targeting human motor units in older age.

show abstract

Health benefits attributed to 17α-estradiol, a lifespan-extending compound, are mediated through estrogen receptor α

Cited by 30 publications

References 157 publications

17α-Estradiol prevents ovariectomy-mediated obesity and bone loss

17α-Estradiol prevents ovariectomy-mediated obesity and bone loss

Einstein-Nathan Shock Center: translating the hallmarks of aging to extend human health span

Circulating testosterone and dehydroepiandrosterone are associated with individual motor unit features in untrained and highly active older men

Contact Info

Product

Resources

About