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Series GSE263655 Query DataSets for GSE263655
Status Public on Apr 15, 2024
Title Apobec-Mediated Retroviral Hypermutation In Vivo is Dependent on Mouse Strain [RNA-seq]
Organism Mus musculus
Experiment type Expression profiling by high throughput sequencing
Summary Retroviruses cause lifelong infections resulting from their ability to thwart innate immunity. The Apobec family of cytidine deaminases are part of the innate immune response that recognizes and mutates foreign nucleic acids, including those from multiple viruses. Multiple retroviral antagonists of Apobecs have been identified, including mouse mammary tumor virus (MMTV)-encoded Rem protein. Previous experiments have shown that Rem-null MMTV or closely related TBLV proviruses from BALB/c tumors accumulate G-to-A and C-to-T mutations typical of Apobecs compared to wild-type proviruses expressing Rem. The difference in mutations between Rem-expressing and non-expressing MMTV strains largely disappeared in mice lacking the Apobec family member, activation-induced cytidine deaminase (AID). These results suggested that Rem is an AID antagonist. In this study, we attempted to study AID-mediated mutations of TBLV proviruses lacking Rem expression obtained from tumors in C57BL/6 (B6) wild-type and AID-knockout backgrounds. Surprisingly, no differences in G-to-A mutations were observed in TBLV proviruses regardless of Rem expression, yet such mutations were significantly reduced in proviruses obtained from mA3/AID-double knockout mice relative to those from wild-type B6 or AID-knockout mice. Many cellular mRNAs involving the innate immune response, but not Apobecs, were elevated in the absence relative to the presence of Rem expression on the B6 AID-knockout background. These results revealed that Apobec-mediated mutagenesis is dependent on mouse strain and suggested a second means of Rem-dependent immune evasion.
 
Overall design Each of two mouse mammary tumor virus (MMTV) strains (TBLV-WT = Rem-expressing or TBLV-SD = lacks Rem expression) was used to generate tumors in C57BL/6 (B6) mice or AID-knockout B6 mice. For RNAseq, we extracted four or five tumors induced by infection with TBLV-WT (Rem+) or TBLV-SD (Rem-) either in wild-type B6 mice or AID-knockout mice. Total RNA was extracted separately from each tumor for analysis and used for library preparation prior to sequencing.
 
Contributor(s) Byun H, Singh GB, Xu WK, Das P, Reyes A, Battenhouse A, Wylie DC, Santiago ML, Lozano MM, Dudley JP
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Submission date Apr 10, 2024
Last update date Apr 15, 2024
Contact name Anna Battenhouse
Organization name The University of Texas at Austin
Department Center for Biomedical Research Support
Lab Bioinformatics Consulting Group
Street address 100 East 24th St., Stop A5000
City Austin
State/province TX
ZIP/Postal code 78712
Country USA
 
Platforms (1)
GPL24247 Illumina NovaSeq 6000 (Mus musculus)
Samples (19)
GSM8196052 AidWT_RemWT_b29_1
GSM8196053 AidWT_RemWT_b30_1
GSM8196054 AidWT_RemWT_b45a_1
Relations
BioProject PRJNA1098715

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Supplementary file Size Download File type/resource
GSE263655_RAW.tar 29.4 Mb (http)(custom) TAR (of TSV)
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Raw data are available in SRA

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