4.5 Article

Reproductive age-associated fibrosis in the stroma of the mammalian ovary

期刊

REPRODUCTION
卷 152, 期 3, 页码 245-260

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BIOSCIENTIFICA LTD
DOI: 10.1530/REP-16-0129

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资金

  1. Center for Reproductive Health After Disease [P50 HD076188]
  2. National Centers for Translational Research in Reproduction and Infertility (NCTRI)
  3. Centers of Biomedical Research Excellence [P20 GM104936]
  4. National Institutes of Health
  5. National Center for Research Resources [P20 RR021940]
  6. National Institute of General Medical Sciences P20 GM103549
  7. National Institute of Environmental Health Sciences 'Training Program in Environmental Toxicology' [T32 ES007079]
  8. Kansas Institutional Development Award (IDeA) [P20 GM103418]
  9. NIH COBRE [9P20GM104936]
  10. NICHD (Kansas IDDRC). [P30 HD002528]
  11. [S10RR027564]

向作者/读者索取更多资源

Under normal physiological conditions, tissue remodeling in response to injury leads to tissue regeneration without permanent damage. However, if homeostasis between synthesis and degradation of extracellular matrix (ECM) components is altered, fibrosis or the excess accumulation of ECM - can disrupt tissue architecture and function. Several organs, including the heart, lung and kidney, exhibit age-associated fibrosis. Here we investigated whether fibrosis underlies aging in the ovary - an organ that ages chronologically before other organs. We used Picrosirius Red (PSR), a connective tissue stain specific for collagen I and III fibers, to evaluate ovarian fibrosis. Using bright-field, epifluorescence, confocal and polarized light microscopy, we validated the specific staining of highly ordered PSR-stained fibers in the ovary. We next examined ovarian PSR staining in two mouse strains (CD1 and CB6F1) across an aging continuum and found that PSR staining was minimal in ovaries from reproductively young adult animals, increased in distinct foci in animals of mid- to- advanced reproductive age, and was prominent throughout the stroma of the oldest animals. Consistent with fibrosis, there was a reproductive age- associated increase in ovarian hydroxyproline content. We also observed a unique population of multinucleated macrophage giant cells, which are associated with chronic inflammation, within the ovarian stroma exclusively in reproductively old mice. In fact, several genes central to inflammation had significantly higher levels of expression in ovaries from reproductively old mice relative to young mice. These results establish fibrosis as an early hallmark of the aging ovarian stroma, and this altered microenvironment may contribute to the age-associated decline in gamete quality.

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