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Mouse spermatogenic stem cells continually interconvert between equipotent singly isolated and syncytial states

机译:小鼠生精干细胞在单能等效状态和合胞体状态之间不断转换

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摘要

The identity and behavior of mouse spermatogenic stem cells have been a long-standing focus of interest. In the prevailing "As model," stem cell function is restricted to singly isolated (As) spermatogonia. By examining single-cell dynamics of GFRα1+ stem cells in vivo, we evaluate an alternative hypothesis that, through fragmentation, syncytial spermatogonia also contribute to stem cell function in homeostasis. We use live imaging and pulse labeling to quantitatively determine the fates of individual GFRα1+ cells and find that, during steady-state spermatogenesis, the entire GFRα1+ population comprises a single stem cell pool, in which cells continually interconvert between As and syncytial states. A minimal biophysical model, relying only on the rates of incomplete cell division and syncytial fragmentation, precisely predicts the stochastic fates of GFRα1+ cells during steady state and postinsult regeneration. Thus, our results define an alternative and dynamic model for spermatogenic stem cell function in the mouse testis.
机译:小鼠生精干细胞的身份和行为一直是人们长期关注的焦点。在流行的“ As模型”中,干细胞功能仅限于单独分离的(As)精原细胞。通过检查体内GFRα1+干细胞的单细胞动态,我们评估了另一种假设,即通过分裂,合胞性精原细胞也有助于体内稳态中的干细胞功能。我们使用实时成像和脉冲标记来定量确定单个GFRα1+细胞的命运,发现在稳态精子发生过程中,整个GFRα1+群体包括一个干细胞池,其中细胞不断地在As和合胞体状态之间相互转换。一个最小的生物物理模型,仅依赖于细胞分裂不完全和合胞体破碎的速率,可以精确预测GFRα1+细胞在稳态和损伤后再生过程中的随机命运。因此,我们的结果定义了小鼠睾丸中生精干细胞功能的替代动态模型。

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