2010
DOI: 10.1242/dev.050799
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The Puf RNA-binding proteins FBF-1 and FBF-2 inhibit the expression of synaptonemal complex proteins in germline stem cells

Abstract: SUMMARYFBF-1 and FBF-2 (collectively FBF) are two nearly identical Puf-domain RNA-binding proteins that regulate the switch from mitosis to meiosis in the C. elegans germline. In germline stem cells, FBF prevents premature meiotic entry by inhibiting the expression of meiotic regulators, such as the RNA-binding protein GLD-1. Here, we demonstrate that FBF also directly inhibits the expression of structural components of meiotic chromosomes. HIM-3, HTP-1, HTP-2, SYP-2 and SYP-3 are components of the synaptonema… Show more

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Cited by 54 publications
(74 citation statements)
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“…HTP-1 and HTP-2 are two highly homologous HORMA domain meiotic proteins that are silenced by the FBFs in the mitotic region (Merritt and Seydoux, 2010). We observed ectopic expression of endogenous HTP-1 and HTP-2 in 87% of dlc-1; fbf-1 hermaphrodites compared with 18% and 8% derepression in dlc-1 and dlc-1; fbf-2, respectively (Fig.…”
Section: Dlc-1 Is Required For Fbf-2-mediated Rna Regulationmentioning
confidence: 70%
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“…HTP-1 and HTP-2 are two highly homologous HORMA domain meiotic proteins that are silenced by the FBFs in the mitotic region (Merritt and Seydoux, 2010). We observed ectopic expression of endogenous HTP-1 and HTP-2 in 87% of dlc-1; fbf-1 hermaphrodites compared with 18% and 8% derepression in dlc-1 and dlc-1; fbf-2, respectively (Fig.…”
Section: Dlc-1 Is Required For Fbf-2-mediated Rna Regulationmentioning
confidence: 70%
“…elegans germline stem cell maintenance depends on the activity of two conserved PUF family proteins, FBF-1 and FBF-2 (Zhang et al, 1997). In the absence of both FBF-1 and FBF-2, all cells in the mitotic zone precociously enter meiosis after the L4 stage of development when maintained at 20°C (Crittenden et al, 2002), but are maintained in a mitotic state if grown at 25°C (Merritt and Seydoux, 2010). FBF-1 and FBF-2 recognize the same motif present in the 3′UTR of their target mRNAs in vitro and form complexes with largely the same mRNAs in vivo Merritt and Seydoux, 2010;Prasad et al, 2016).…”
Section: Introductionmentioning
confidence: 99%
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“…The in vitro FBF binding element (FBE) is UGUNNNAU, where N is any ribonucleotide Opperman et al 2005). Moreover, the in vivo relevance of the FBE has been confirmed (Zhang et al 1997;Merritt and Seydoux 2010). Second, 15 FBF target mRNAs are known to be regulated post-transcriptionally via FBEs (Supplemental Fig.…”
Section: Fbf-1 and Fbf-2 Iclip In The Germline Of An Intact Animalmentioning
confidence: 99%
“…Concomitantly, the two translational activators, GLD-2 and GLD-3, enforce spatially regulated meiotic entry by presumably activating yet unknown meiotic genes (Eckmann et al 2004 ) . The bimodality of this cell fate switch is further assisted by FBF, which translationally represses GLD-1 (Crittenden et al 2002 ) , cyclin-dependent kinase inhibitor (CKI-1) accumulation (Kalchhauser et al 2011 ) , and the ectopic expression of meiotic proteins, such as the synaptonemal complex components HIM-3, HTP-1, SYP-1, and SYP-2 (Merritt and Seydoux 2010 ) (Table 8.5 ). Once female germ cells have entered meiosis, abundant GLD-1 levels ensure meiotic progression.…”
Section: Systems Biology Of Rna Regulatory Networkmentioning
confidence: 99%