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Publication : Abnormal behavior, striatal dopamine turnover and opioid peptide gene expression in histamine-deficient mice.

First Author  Abdurakhmanova S Year  2019
Journal  Genes Brain Behav Volume  18
Issue  8 Pages  e12595
PubMed ID  31216095 Mgi Jnum  J:324746
Mgi Id  MGI:7281419 Doi  10.1111/gbb.12595
Citation  Abdurakhmanova S, et al. (2019) Abnormal behavior, striatal dopamine turnover and opioid peptide gene expression in histamine-deficient mice. Genes Brain Behav 18(8):e12595
abstractText  Hypothalamic histaminergic neurons regulate a variety of homeostatic, metabolic and cognitive functions. Recent data have suggested a modulatory role of histamine and histamine receptors in shaping striatal activity and connected the histaminergic system to neuropsychiatric disorders. We characterized exploratory behavior and striatal neurotransmission in mice lacking the histamine producing enzyme histidine decarboxylase (Hdc). The mutant mice showed a distinct behavioral pattern during exploration of novel environment, specifically, increased frequency of rearing seated against the wall, jumping and head/body shakes. This behavioral phenotype was associated with decreased levels of striatal dopamine and serotonin and increased level of dopamine metabolite DOPAC. Gene expression levels of dynorphin and enkephalin, opioids released by medium spiny neurons of striatal direct and indirect pathways respectively, were lower in Hdc mutant mice than in control animals. A low dose of amphetamine led to similar behavioral and biochemical outcomes in both genotypes. Increased striatal dopamine turnover was observed in Hdc KO mice after treatment with dopamine precursor l-Dopa. Overall, our study suggests a role for striatal dopamine and opioid peptides in formation of distinct behavioral phenotype of Hdc KO mice.
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