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Fine Time Course Expression Analysis Identifies Cascades of Activation and Repression and Maps a Putative Regulator of Mammalian Sex Determination
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نویسنده
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munger s.c. ,natarajan a. ,looger l.l. ,ohler u. ,capel b.
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منبع
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plos genetics - 2013 - دوره : 9 - شماره : 7
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چکیده
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In vertebrates,primary sex determination refers to the decision within a bipotential organ precursor to differentiate as a testis or ovary. bifurcation of organ fate begins between embryonic day (e) 11.0-e12.0 in mice and likely involves a dynamic transcription network that is poorly understood. to elucidate the first steps of sexual fate specification,we profiled the xx and xy gonad transcriptomes at fine granularity during this period and resolved cascades of gene activation and repression. c57bl/6j (b6) xy gonads showed a consistent ∼5-hour delay in the activation of most male pathway genes and repression of female pathway genes relative to 129s1/svimj,which likely explains the sensitivity of the b6 strain to male-to-female sex reversal. using this fine time course data,we predicted novel regulatory genes underlying expression qtls (eqtls) mapped in a previous study. to test predictions,we developed an in vitro gonad primary cell assay and optimized a lentivirus-based shrna delivery method to silence candidate genes and quantify effects on putative targets. we provide strong evidence that lmo4 (lim-domain only 4) is a novel regulator of sex determination upstream of sf1 (nr5a1),sox9,fgf9,and col9a3. this approach can be readily applied to identify regulatory interactions in other systems. © 2013 munger et al.
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آدرس
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department of cell biology,duke university,durham,nc,united states,center for genome dynamics,the jackson laboratory,bar harbor,me, United States, program in computational biology and bioinformatics,duke university,durham,nc, United States, howard hughes medical institute,janelia farm research campus,ashburn,va, United States, institute for genome sciences and policy,duke university,durham,nc,united states,department of biostatistics and bioinformatics,duke university,durham,nc,united states,berlin institute for medical systems biology,max delbrueck center,berlin, Germany, department of cell biology,duke university,durham,nc, United States
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Authors
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