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Estrogen-Mediated Gaseous Signaling Molecules in Cardiovascular Disease

Journal

TRENDS IN ENDOCRINOLOGY AND METABOLISM
Volume 31, Issue 10, Pages 773-784

Publisher

CELL PRESS
DOI: 10.1016/j.tem.2020.06.001

Keywords

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Funding

  1. National Natural Science Foundation [81871137, 81471426]
  2. Project of Principal Scientists Guangzhou Municipal Universities 'Yangcheng Scholars' [1201541587]
  3. Project of Department of Education of Guangdong Province [2015KTSCX109]
  4. National Funds of Developing Local Colleges and Universities [B16056001]
  5. Science and Technology Program of Guangzhou [201904010289, 201804010376]
  6. Guangzhou 121 Talent Program
  7. Outstanding Young Medical Talent Program in Guangdong Province
  8. Innovation Team Project of the Educational Commission of Guangdong Province of China
  9. National Natural Science Foundation for Young Scientists of China [81800428]
  10. Innovation Project of Department of Education of Guangdong Province [2017KTSCX158]
  11. Guangdong Natural Science Foundation [2018A030310178]

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Gender difference is well recognized as a key risk factor for cardiovascular disease (CVD). Estrogen, the primary female sex hormone, improves cardiovascular functions through receptor (ER alpha, ER beta, or G protein-coupled estrogen receptor)-initiated genomic or non-genomic mechanisms. Gaseous signaling molecules, including nitric oxide (NO), hydrogen sulfide (H2S), and carbon monoxide (CO), are important regulators of cardiovascular function. Recent studies have demonstrated that estrogen regulates the production of these signaling molecules in cardiovascular cells to exert its cardiovascular protective effects. We discuss current understanding of gaseous signaling molecules in cardiovascular disease (CVD), the underlying mechanisms through which estrogen exerts cardiovascular protective effects by regulating these molecules, and how these findings can be translated to improve the health of postmenopausal women.

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