{"database":"ENA","file_versions":[{"headers":{"Content-Type":["application/json"]},"body":{"files":{"Fastqsanger.gz":["ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/006/SRR1688636/SRR1688636.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/004/SRR1688634/SRR1688634.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/007/SRR1688637/SRR1688637.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/000/SRR1688640/SRR1688640.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/009/SRR1688639/SRR1688639.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/008/SRR1688638/SRR1688638.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/001/SRR1688641/SRR1688641.fastq.gz","ftp://ftp.sra.ebi.ac.uk/vol1/fastq/SRR168/005/SRR1688635/SRR1688635.fastq.gz"]},"type":"primary"},"statusCode":"OK","statusCodeValue":200}],"scores":null,"additional":{"omics_type":["Genomics"],"center_name":["Flavell Lab, Genetics/Immunobiology, Yale University"],"full_dataset_link":["https://www.ebi.ac.uk/ena/browser/view/PRJNA269079"],"scientific_name":["Mus musculus"],"tag":["xref:PubMed:25525875"],"long_description":["RNA sequencing of wild-type or Interferon Alpha receptor 1 Knockout MEF cells treated with DMSO or the Caspase Inhibitor Q-VD-OPh. The mechanism by which cells undergo death determines whether dying cells trigger inflammatory responses or remain immunologically silent. Mitochondria play a central role in the induction of cell death, as well as in immune signaling pathways. Here, we identify of a mechanism by which mitochondria and downstream pro-apoptotic caspases regulate the activation of antiviral immunity. In the absence of active caspases, mitochondrial outer membrane permeabilization by Bax and Bak results in the expression of type I interferons (IFNs). This induction is mediated by mitochondrial DNA-dependent activation of the cGAS/STING pathway and results in the establishment of a potent state of viral resistance. Our results show that mitochondria have the capacity to simultaneously expose a cell-intrinsic inducer of the IFN response, and to inactivate this response in a caspase-dependent manner. This mechanism provides a dual control, which determines whether mitochondria initiate an immunologically silent or a pro-inflammatory type of cell death. In order to determine whether the pharmacological inhibition of caspases could activate the type I interferon response, we treated WT MEFs with the caspase inhibitor Q-VD-OPH. The inhibitor induced an increased expression of ISGs, which was dependent on type I IFN receptor (IFNAR1) signaling. Overall design: RNA was extracted from duplicate samples and libraries generated for sequencing using the directional RNA-Seq library prep at the Yale Center for Genome Analysis. Libraries were sequenced using a Hiseq2500 sequencer to generate 76bp single-end reads. Duplicate samples were analyzed for each condition."],"repository":["ENA"],"description_synonyms":["DAGA4, mtDNA, DMDA, mitochondrial DNA, Caspase, DMDA1, mitochondrial genome, SCARMD2, Mitochondrial DNA., A4, MAM, SCG3, Interferon, TYPE, LGMD2C"],"name_synonyms":["Mus musculus, Laboratory Mice., House, Mus, Laboratory, Swiss, Mus domesticus, mouse, Mus musculus domesticus, Swiss Mouse, mouse , Mouse, House Mice, Swiss Mice, house mouse, Mice, Laboratory Mouse, House Mouse, mice C57BL/6xCBA/CaJ hybrid, domesticus, Mus muscaris"],"additional_accession":[]},"is_claimable":false,"name":"Mus musculus","description":"Apoptotic caspases prevent the induction of type I interferons by mitochondrial DNA","dates":{"last_updated":"2025-09-24","first_public":"2014-12-04"},"accession":"PRJNA269079","cross_references":{"GEO":["GSE63794"],"taxon":["10090"],"PubMed":["25525875"]}}