4.5 Article

A-Single Spermatogonia Heterogeneity and Cell Cycles Synchronize with Rat Seminiferous Epithelium Stages VIII-IX

期刊

BIOLOGY OF REPRODUCTION
卷 90, 期 2, 页码 -

出版社

SOC STUDY REPRODUCTION
DOI: 10.1095/biolreprod.113.113555

关键词

A-single spermatogonia; epithelial cycle; ERBB3; germline stem cell; HER3; seminiferous; SNAP91; spermatogenesis; spermatogonia; spermatogonial stem cells; stem cell niche; stem cells; testis

资金

  1. Eunice Kennedy Shriver National Institute of Child Health and Human Development NIH grants [R01HD053889, R01HD061575]
  2. Cecil H. & Ida Green Center for Reproductive Biology Sciences

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In mammalian testes, A-single'' spermatogonia function as stem cells that sustain sperm production for fertilizing eggs. Yet, it is not understood how cellular niches regulate the developmental fate of A-single spermatogonia. Here, immunolabeling studies in rat testes define a novel population of ERBB3(+) germ cells as approximately 5% of total SNAP91(+) A-single spermatogonia along a spermatogenic wave. As a function of time, ERBB3(+) A-single spermatogonia are detected during a 1- to 2-day period each 12.9-day sperm cycle, representing 35%-40% of SNAP91(+) A-single spermatogonia in stages VIII-IX of the seminiferous epithelium. Local concentrations of ERBB3(+) A-single spermatogonia are maintained under the mean density measured for neighboring SNAP91(+) A-single spermatogonia, potentially indicative of niche saturation. ERBB3(+) spermatogonia also synchronize their cell cycles with epithelium stages VIII-IX, where they form physical associations with preleptotene spermatocytes transiting the blood-testis barrier and Sertoli cells undergoing sperm release. Thus, A-single spermatogonia heterogeneity within this short-lived and reoccurring microenvironment invokes novel theories on how cellular niches integrate with testicular physiology to orchestrate sperm development in mammals.

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