Ovulated oocytes in adult mice derive from non-circulating germ cells

被引:0
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作者
Kevin Eggan
Sara Jurga
Roger Gosden
Irene M. Min
Amy J. Wagers
机构
[1] Harvard University,The Stowers Medical Institute, Harvard Stem Cell Institute and The Department of Molecular and Cellular Biology
[2] Harvard Medical School,Section on Developmental and Stem Cell Biology, Joslin Diabetes Center and Department of Pathology
[3] Harvard Stem Cell Institute,undefined
[4] Center for Reproductive Medicine and Infertility,undefined
[5] Weill Medical College,undefined
[6] Cornell University,undefined
来源
Nature | 2006年 / 441卷
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摘要
Decades of research in reproductive biology have led to the generally accepted belief that in female mammals, all surviving germ cells enter meiosis at the end of fetal development and as a result, the postnatal ovary harbours a limited supply of oocytes that cannot be replenished or regenerated if lost to injury or disease. However, recent reports have challenged this view, suggesting instead that oocyte production is maintained through continual seeding of the ovary by circulating, bone-marrow-derived germ cells. To test directly the physiological relevance of circulating cells for female fertility, we established transplantation and parabiotic mouse models to assess the capacity of circulating bone marrow cells to generate ovulated oocytes, both in the steady state and after induced damage. Our studies showed no evidence that bone marrow cells, or any other normally circulating cells, contribute to the formation of mature, ovulated oocytes. Instead, cells that travelled to the ovary through the bloodstream exhibited properties characteristic of committed blood leukocytes.
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页码:1109 / 1114
页数:5
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