| Literature DB >> 24485832 |
Laurent Boulanger1, Maëlle Pannetier1, Laurence Gall1, Aurélie Allais-Bonnet1, Maëva Elzaiat1, Daniel Le Bourhis2, Nathalie Daniel1, Christophe Richard1, Corinne Cotinot1, Norbert B Ghyselinck3, Eric Pailhoux4.
Abstract
The origin of sex reversal in XX goats homozygous for the polled intersex syndrome (PIS) mutation was unclear because of the complexity of the mutation that affects the transcription of both FOXL2 and several long noncoding RNAs (lncRNAs). Accumulating evidence suggested that FOXL2 could be the sole gene of the PIS locus responsible for XX sex reversal, the lncRNAs being involved in transcriptional regulation of FOXL2. In this study, using zinc-finger nuclease-directed mutagenesis, we generated several fetuses, of which one XX individual bears biallelic mutations of FOXL2. Our analysis demonstrates that FOXL2 loss of function dissociated from loss of lncRNA expression is sufficient to cause an XX female-to-male sex reversal in the goat model and, as in the mouse model, an agenesis of eyelids. Both developmental defects were reproduced in two newborn animals cloned from the XX FOXL2(-/-) fibroblasts. These results therefore identify FOXL2 as a bona fide female sex-determining gene in the goat. They also highlight a stage-dependent role of FOXL2 in the ovary, different between goats and mice, being important for fetal development in the former but for postnatal maintenance in the latter.Entities:
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Year: 2014 PMID: 24485832 DOI: 10.1016/j.cub.2013.12.039
Source DB: PubMed Journal: Curr Biol ISSN: 0960-9822 Impact factor: 10.834