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Literature DB >> 26711335

Synergistic Actions of Ogg1 and Mutyh DNA Glycosylases Modulate Anxiety-like Behavior in Mice.

Monica D Bjørge¹, Gunn A Hildrestrand¹, Katja Scheffler², Rajikala Suganthan¹, Veslemøy Rolseth¹, Anna Kuśnierczyk³, Alexander D Rowe¹, Cathrine B Vågbø³, Susanne Vetlesen¹, Lars Eide⁴, Geir Slupphaug⁵, Yusaku Nakabeppu⁶, Timothy W Bredy⁷, Arne Klungland¹, Magnar Bjørås⁸.

Abstract

Ogg1 and Mutyh DNA glycosylases cooperate to prevent mutations caused by 8-oxoG, a major premutagenic DNA lesion associated with cognitive decline. We have examined behavior and cognitive function in mice deficient of these glycosylases. Ogg1(-/-)Mutyh(-/-) mice were more active and less anxious, with impaired learning ability. In contrast, Mutyh(-/-) mice showed moderately improved memory. We observed no apparent change in genomic 8-oxoG levels, suggesting that Ogg1 and Mutyh play minor roles in global repair in adult brain. Notably, transcriptome analysis of hippocampus revealed that differentially expressed genes in the mutants belong to pathways known to be involved in anxiety and cognition. Esr1 targets were upregulated, suggesting a role of Ogg1 and Mutyh in repression of Esr1 signaling. Thus, beyond their involvement in DNA repair, Ogg1 and Mutyh regulate hippocampal gene expression related to cognition and behavior, suggesting a role for the glycosylases in regulating adaptive behavior.

Entities: Disease Gene Species

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Year: 2015 PMID： 26711335 DOI： 10.1016/j.celrep.2015.12.001

Source DB: PubMed Journal: Cell Rep Impact factor: 9.423

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Cited

14 in total

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