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   KATNAL1 regulation of sertoli cell microtubule dynamics is essential for spermiogenesis and male fertility  
   
نویسنده smith l.b. ,milne l. ,nelson n. ,eddie s. ,brown p. ,atanassova n. ,o'bryan m.k. ,o'donnell l. ,rhodes d. ,wells s. ,napper d. ,nolan p. ,lalanne z. ,cheeseman m. ,peters j.
منبع plos genetics - 2012 - دوره : 8 - شماره : 5
چکیده    Spermatogenesis is a complex process reliant upon interactions between germ cells (gc) and supporting somatic cells. testicular sertoli cells (sc) support gcs during maturation through physical attachment,the provision of nutrients,and protection from immunological attack. this role is facilitated by an active cytoskeleton of parallel microtubule arrays that permit transport of nutrients to gcs,as well as translocation of spermatids through the seminiferous epithelium during maturation. it is well established that chemical perturbation of sc microtubule remodelling leads to premature gc exfoliation demonstrating that microtubule remodelling is an essential component of male fertility,yet the genes responsible for this process remain unknown. using a random enu mutagenesis approach,we have identified a novel mouse line displaying male-specific infertility,due to a point mutation in the highly conserved atpase domain of the novel katanin p60-related microtubule severing protein katanin p60 subunit a-like1 (katnal1). we demonstrate that katnal1 is expressed in testicular sertoli cells (sc) from 15.5 days post-coitum (dpc) and that,consistent with chemical disruption models,loss of function of katnal1 leads to male-specific infertility through disruption of sc microtubule dynamics and premature exfoliation of spermatids from the seminiferous epithelium. the identification of katnal1 as an essential regulator of male fertility provides a significant novel entry point into advancing our understanding of how sc microtubule dynamics promotes male fertility. such information will have resonance both for future treatment of male fertility and the development of non-hormonal male contraceptives. © 2012 smith et al.
آدرس mrc centre for reproductive health,university of edinburgh,the queen's medical research institute,edinburgh, United Kingdom, mrc centre for reproductive health,university of edinburgh,the queen's medical research institute,edinburgh, United Kingdom, mrc centre for reproductive health,university of edinburgh,the queen's medical research institute,edinburgh, United Kingdom, mrc centre for reproductive health,university of edinburgh,the queen's medical research institute,edinburgh, United Kingdom, mrc centre for reproductive health,university of edinburgh,the queen's medical research institute,edinburgh, United Kingdom, institute of experimental morphology and anthropology with museum,bulgarian academy of sciences,sofia, Bulgaria, the department of anatomy and developmental biology,monash university,melbourne,vic, Australia, the department of anatomy and developmental biology,monash university,melbourne,vic,australia,prince henry's institute of medical research,clayton,vic, Australia, the department of anatomy and developmental biology,monash university,melbourne,vic, Australia, mary lyon centre,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom, mary lyon centre,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom, mammalian genetics unit,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom, mammalian genetics unit,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom, mary lyon centre,medical research council,harwell science and innovation campus,harwell,oxfordshire,united kingdom,mammalian genetics unit,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom, mammalian genetics unit,medical research council,harwell science and innovation campus,harwell,oxfordshire, United Kingdom
 
     
   
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