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Deficient DNA base-excision repair in the forebrain leads to a sex-specific anxiety-like phenotype in mice.

Flavia S MuellerRené AmportTina NotterSina M SchalbetterHan-Yu LinZuzana GarajovaParisa AminiUlrike Weber-StadlbauerEnni Markkanen
Published in: BMC biology (2022)
Our results suggest that accumulation of unrepaired DNA damage in the forebrain alters the GABAergic neurotransmitter system and causes behavioural deficits in relation to innate and learned anxiety in a sex-dependent manner. Moreover, the data uncover a previously unappreciated connection between BER deficiency, unrepaired DNA damage in the hippocampus and a sex-specific anxiety-like phenotype with implications for the aetiology and therapy of neuropsychiatric disorders.
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