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      Sperm-borne miRNAs and endo-siRNAs are important for fertilization and preimplantation embryonic development

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          Abstract

          Although it is believed that mammalian sperm carry small noncoding RNAs (sncRNAs) into oocytes during fertilization, it remains unknown whether these sperm-borne sncRNAs truly have any function during fertilization and preimplantation embryonic development. Germline-specific Dicer and Drosha conditional knockout (cKO) mice produce gametes (i.e. sperm and oocytes) partially deficient in miRNAs and/or endo-siRNAs, thus providing a unique opportunity for testing whether normal sperm (paternal) or oocyte (maternal) miRNA and endo-siRNA contents are required for fertilization and preimplantation development. Using the outcome of intracytoplasmic sperm injection (ICSI) as a readout, we found that sperm with altered miRNA and endo-siRNA profiles could fertilize wild-type (WT) eggs, but embryos derived from these partially sncRNA-deficient sperm displayed a significant reduction in developmental potential, which could be rescued by injecting WT sperm-derived total or small RNAs into ICSI embryos. Disrupted maternal transcript turnover and failure in early zygotic gene activation appeared to associate with the aberrant miRNA profiles in Dicer and Drosha cKO spermatozoa. Overall, our data support a crucial function of paternal miRNAs and/or endo-siRNAs in the control of the transcriptomic homeostasis in fertilized eggs, zygotes and two-cell embryos. Given that supplementation of sperm RNAs enhances both the developmental potential of preimplantation embryos and the live birth rate, it might represent a novel means to improve the success rate of assisted reproductive technologies in fertility clinics.

          Abstract

          Summary: The developmental potential of embryos fertilized with sperm from germline-specific Dicer or Drosha conditional knockout mice is impaired, highlighting key roles for paternal miRNAs/endo-siRNAs.

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          Author and article information

          Journal
          Development
          Development
          DEV
          develop
          Development (Cambridge, England)
          The Company of Biologists Ltd
          0950-1991
          1477-9129
          15 February 2016
          15 February 2017
          : 143
          : 4
          : 635-647
          Affiliations
          Department of Physiology and Cell Biology, University of Nevada School of Medicine , 1664 North Virginia Street, MS 0575, Reno, NV 89557, USA
          Author notes
          [* ]Author for correspondence ( wyan@ 123456medicine.nevada.edu )
          Article
          PMC4760322 PMC4760322 4760322 DEV131755
          10.1242/dev.131755
          4760322
          26718009
          f8861953-5a64-4f27-862a-4f11794a18bb
          © 2016. Published by The Company of Biologists Ltd
          History
          : 12 October 2015
          : 22 December 2015
          Funding
          Funded by: National Institutes of Health, http://dx.doi.org/10.13039/100000002;
          Award ID: HD060858, HD071736 and HD074573
          Award ID: 1P30GM110767
          Award ID: HD071736
          Award ID: HD074573
          Categories
          Research Article

          Epigenetics,Sperm,Small noncoding RNAs,Male infertility,Embryonic development,Assisted reproductive technologies,Maternal transcripts, In vitro fertilization

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