Literature DB >> 25448133

Circulating miR-21, miR-146a and Fas ligand respond to postmenopausal estrogen-based hormone replacement therapy--a study with monozygotic twin pairs.

Reeta Kangas1, Eija Pöllänen2, Maria Rita Rippo3, Catia Lanzarini4, Francesco Prattichizzo3, Paula Niskala5, Juulia Jylhävä6, Sarianna Sipilä2, Jaakko Kaprio7, Antonio Domenico Procopio8, Miriam Capri4, Claudio Franceschi4, Fabiola Olivieri8, Vuokko Kovanen2.   

Abstract

Biological aging is associated with physiological deteriorations, which are partly due to changes in the hormonal profile. MicroRNAs regulate various processes associated with cell senescence; differentiation, replication and apoptosis. Serum microRNAs have potential to serve as noninvasive markers for diagnostics/prognostics and therapeutic targets. We analysed the association of estrogen-based hormone replacement therapy (HRT) with selected microRNAs and inflammation markers from the serum, leukocytes and muscle biopsy samples from 54 to 62 year-old postmenopausal monozygotic twins (n=11 pairs) discordant for HRT usage. Premenopausal 30-35 year-old women (n=8) were used as young controls. We focused on the hormonal aging and on the interaction between HRT use and the modulation of miR-21, miR-146a and classical inflammation markers. Fas-ligand was analysed since it functions in both apoptosis and inflammation. The inflammatory profile was healthier among the premenopausal women compared to the postmenopausal twins. Serum miR-21 and miR-146a levels and FasL concentrations were lower in HRT users compared to their non-using co-twins, demonstrating their responsiveness to HRT. Based on the pairwise FasL analysis, FasL concentration is likely to be genetically controlled. Overall, we suggest that postmenopausal estrogen deficiency sustains the development of "inflamm-aging". Estrogen sensitive, specific circulating microRNAs could be potential, early biomarkers for age-associated physiological deteriorations.
Copyright © 2014 Elsevier Ireland Ltd. All rights reserved.

Entities:  

Keywords:  Apoptosis; Estrogen; Hormone replacement therapy; Micrornas; “Inflamm-aging”

Mesh:

Substances:

Year:  2014        PMID: 25448133     DOI: 10.1016/j.mad.2014.11.001

Source DB:  PubMed          Journal:  Mech Ageing Dev        ISSN: 0047-6374            Impact factor:   5.432


  16 in total

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8.  Declining Physical Performance Associates with Serum FasL, miR-21, and miR-146a in Aging Sprinters.

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9.  Aging and serum exomiR content in women-effects of estrogenic hormone replacement therapy.

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10.  Menopause and adipose tissue: miR-19a-3p is sensitive to hormonal replacement.

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