Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.

Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.

Given limited resources for motility, sperm cell activation must be precisely timed to ensure the greatest likelihood of fertilization. Like those of most species, the sperm of C. elegans become active only after encountering an external signaling molecule. Activation coincides with spermiogenesis,...

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Main Authors: Wei-Siang Liau, Ubaydah Nasri, Daniel Elmatari, Jason Rothman, Craig W LaMunyon
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3590197?pdf=render
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spelling doaj-3a98701690a64b9c89c45e40f2efe5d82020-11-25T01:31:39ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0183e5726610.1371/journal.pone.0057266Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.Wei-Siang LiauUbaydah NasriDaniel ElmatariJason RothmanCraig W LaMunyonGiven limited resources for motility, sperm cell activation must be precisely timed to ensure the greatest likelihood of fertilization. Like those of most species, the sperm of C. elegans become active only after encountering an external signaling molecule. Activation coincides with spermiogenesis, the final step in spermatogenesis, when the spherical spermatid undergoes wholesale reorganization to produce a pseudopod. Here, we describe a gene involved in sperm activation, spe-46. This gene was identified in a suppressor screen of spe-27(it132ts), a sperm-expressed gene whose product functions in the transduction of the spermatid activation signal. While spe-27(it132ts) worms are sterile at 25°C, the spe-46(hc197)I; spe-27(it132ts)IV double mutants regain partial fertility. Single nucleotide polymorphism mapping, whole genome sequencing, and transformation rescue were employed to identify the spe-46 coding sequence. It encodes a protein with seven predicted transmembrane domains but with no other predicted functional domains or homology outside of nematodes. Expression is limited to spermatogenic tissue, and a transcriptional GFP fusion shows expression corresponds with the onset of the pachytene stage of meiosis. The spe-46(hc197) mutation bypasses the need for the activation signal; mutant sperm activate prematurely without an activation signal in males, and mutant males are sterile. In an otherwise wild-type genome, the spe-46(hc197) mutation induces a sperm defective phenotype. In addition to premature activation, spe-46(hc197) sperm exhibit numerous defects including aneuploidy, vacuolization, protruding spikes, and precocious fusion of membranous organelles. Hemizygous worms [spe-46(hc197)/mnDf111] are effectively sterile. Thus, spe-46 appears to be involved in the regulation of spermatid activation during spermiogenesis, with the null phenotype being an absence of functional sperm and hypomorphic phenotypes being premature spermatid activation and numerous sperm cell defects.http://europepmc.org/articles/PMC3590197?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Wei-Siang Liau
Ubaydah Nasri
Daniel Elmatari
Jason Rothman
Craig W LaMunyon
spellingShingle Wei-Siang Liau
Ubaydah Nasri
Daniel Elmatari
Jason Rothman
Craig W LaMunyon
Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
PLoS ONE
author_facet Wei-Siang Liau
Ubaydah Nasri
Daniel Elmatari
Jason Rothman
Craig W LaMunyon
author_sort Wei-Siang Liau
title Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
title_short Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
title_full Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
title_fullStr Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
title_full_unstemmed Premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in Caenorhabditis elegans.
title_sort premature sperm activation and defective spermatogenesis caused by loss of spe-46 function in caenorhabditis elegans.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Given limited resources for motility, sperm cell activation must be precisely timed to ensure the greatest likelihood of fertilization. Like those of most species, the sperm of C. elegans become active only after encountering an external signaling molecule. Activation coincides with spermiogenesis, the final step in spermatogenesis, when the spherical spermatid undergoes wholesale reorganization to produce a pseudopod. Here, we describe a gene involved in sperm activation, spe-46. This gene was identified in a suppressor screen of spe-27(it132ts), a sperm-expressed gene whose product functions in the transduction of the spermatid activation signal. While spe-27(it132ts) worms are sterile at 25°C, the spe-46(hc197)I; spe-27(it132ts)IV double mutants regain partial fertility. Single nucleotide polymorphism mapping, whole genome sequencing, and transformation rescue were employed to identify the spe-46 coding sequence. It encodes a protein with seven predicted transmembrane domains but with no other predicted functional domains or homology outside of nematodes. Expression is limited to spermatogenic tissue, and a transcriptional GFP fusion shows expression corresponds with the onset of the pachytene stage of meiosis. The spe-46(hc197) mutation bypasses the need for the activation signal; mutant sperm activate prematurely without an activation signal in males, and mutant males are sterile. In an otherwise wild-type genome, the spe-46(hc197) mutation induces a sperm defective phenotype. In addition to premature activation, spe-46(hc197) sperm exhibit numerous defects including aneuploidy, vacuolization, protruding spikes, and precocious fusion of membranous organelles. Hemizygous worms [spe-46(hc197)/mnDf111] are effectively sterile. Thus, spe-46 appears to be involved in the regulation of spermatid activation during spermiogenesis, with the null phenotype being an absence of functional sperm and hypomorphic phenotypes being premature spermatid activation and numerous sperm cell defects.
url http://europepmc.org/articles/PMC3590197?pdf=render
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