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Series GSE89381 Query DataSets for GSE89381
Status Public on May 18, 2017
Title ChIP-Seq with Kumgang (Kmg), dMi-2, and Aly from wild-type and kmg KD Drosophila melanogaster testes
Organism Drosophila melanogaster
Experiment type Genome binding/occupancy profiling by high throughput sequencing
Summary Genome wide localization of Kumgang, dMi-2, and Aly in Drosophila melanogaster testes were evaluated by ChIP-Seq in wild-type and kmg knock down testes. / Title: Blocking promiscuous activation at cryptic promoters directs cell type–specific gene expression / Abstract: To selectively express cell type–specific transcripts during development, it is critical to maintain genes required for other lineages in a silent state. Here, we show in the Drosophila male germline stem cell lineage that a spermatocyte-specific zinc finger protein, Kumgang (Kmg), working with the chromatin remodeler dMi-2 prevents transcription of genes normally expressed only in somatic lineages. By blocking transcription from normally cryptic promoters, Kmg restricts activation by Aly, a component of the testis-meiotic arrest complex, to transcripts for male germ cell differentiation. Our results suggest that as new regions of the genome become open for transcription during terminal differentiation, blocking the action of a promiscuous activator on cryptic promoters is a critical mechanism for specifying precise gene activation.
 
Overall design 1) Kmg: Two replicates of ChIP of endogenous Kmg with specific antibody from wild-type testes. Two replicates of ChIP of Kmg from kmg knock down testes serve as negative controls / 2) dMi-2: Two replicates of ChIP of endogenous dMi-2 from wild-type testes and from kmg knock down testes / 3) Aly: Two replicates of ChIP of epitope(HA) tagged Aly from transgenic line bearing alyP-Aly-HA from wild-type for kmg and also from kmg KD testes. One ChIP of HA epitope from wild-type testes without Aly-HA transgene serves as a negative control.
Web link http://science.sciencemag.org/content/356/6339/717
 
Contributor(s) Kim J, Fuller MT
Citation(s) 28522526
NIH grant(s)
Grant ID Grant title Affiliation Name
R01 GM061986 Regulation of Cell-Type Specific Transcription in Spermatocytes STANFORD UNIVERSITY MARGARET T FULLER
Submission date Nov 01, 2016
Last update date May 15, 2019
Contact name Jongmin J Kim
E-mail(s) [email protected]
Organization name Cornell University
Department Biomedical Sciences
Lab Kim lab
Street address 930 Campus Road
City Ithaca
State/province NY
ZIP/Postal code 14853
Country USA
 
Platforms (1)
GPL19132 Illumina NextSeq 500 (Drosophila melanogaster)
Samples (26)
GSM2367707 Input for ChIP Kmg from wild-type rep1
GSM2367708 Input for ChIP Kmg from kmg KD rep1
GSM2367709 ChIP Kmg from wild-type rep1
This SubSeries is part of SuperSeries:
GSE89506 Blocking promiscuous activation at cryptic promoters directs cell type–specific gene expression
Relations
BioProject PRJNA352406
SRA SRP092554

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Supplementary file Size Download File type/resource
GSE89381_RAW.tar 4.4 Gb (http)(custom) TAR (of BW)
SRA Run SelectorHelp
Raw data are available in SRA
Processed data provided as supplementary file

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