A Caenorhabditis elegans protein with a PRDM9-like SET domain localizes to chromatin-associated foci and promotes spermatocyte gene expression, sperm production and fertility
Author(s)
Engert, Christoph; Droste, Rita; van Oudenaarden, Alexander; Horvitz, Howard Robert
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To better understand the tissue-specific regulation of chromatin state in cell-fate determination and animal development, we defined the tissue-specific expression of all 36 C. elegans presumptive lysine methyltransferase (KMT) genes using single-molecule fluorescence in situ hybridization (smFISH). Most KMTs were expressed in only one or two tissues. The germline was the tissue with the broadest KMT expression. We found that the germline-expressed C. elegans protein SET-17, which has a SET domain similar to that of the PRDM9 and PRDM7 SET-domain proteins, promotes fertility by regulating gene expression in primary spermatocytes. SET-17 drives the transcription of spermatocyte-specific genes from four genomic clusters to promote spermatid development. SET-17 is concentrated in stable chromatin-associated nuclear foci at actively transcribed msp (major sperm protein) gene clusters, which we term msp locus bodies. Our results reveal the function of a PRDM9/7-family SET-domain protein in spermatocyte transcription. We propose that the spatial intranuclear organization of chromatin factors might be a conserved mechanism in tissue-specific control of transcription.
Date issued
2018-04Department
Massachusetts Institute of Technology. Computational and Systems Biology Program; Massachusetts Institute of Technology. Department of Biology; Massachusetts Institute of Technology. Department of Physics; McGovern Institute for Brain Research at MITJournal
PLOS Genetics
Citation
Engert, Christoph G., Rita Droste, Alexander van Oudenaarden, and H. Robert Horvitz. “A Caenorhabditis Elegans Protein with a PRDM9-Like SET Domain Localizes to Chromatin-Associated Foci and Promotes Spermatocyte Gene Expression, Sperm Production and Fertility.” Edited by Julie Ahringer. PLOS Genetics 14, no. 4 (April 27, 2018): e1007295.
Version: Final published version
ISSN
1553-7404