NPAS3

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Neuronal PAS domain protein 3
Identifiers
Symbols NPAS3 ; MOP6; PASD6; bHLHe12
External IDs OMIM609430 HomoloGene8461 GeneCards: NPAS3 Gene
Orthologs
Species Human Mouse
Entrez 64067 27386
Ensembl ENSG00000151322 ENSMUSG00000021010
UniProt Q8IXF0 n/a
RefSeq (mRNA) NM_001164749 NM_013780
RefSeq (protein) NP_001158221 NP_038808
Location (UCSC) Chr 14:
32.93 – 33.8 Mb
Chr 12:
53.25 – 54.07 Mb
PubMed search [1] [2]

NPAS3 or Neuronal PAS domain protein 3 is a brain-enriched transcription factor belonging to the bHLH-PAS superfamily of transcription factors, the members of which carry out diverse functions, including circadian oscillations, neurogenesis, toxin metabolism, hypoxia, and tracheal development. NPAS3 contains basic helix-loop-helix structural motif and PAS domain, like the other proteins in the superfamily.

Function

NPAS3 is also known as human accelerated region 21. It may, therefore, have played a key role in differentiating humans from apes.[1]

NPAS1 and NPAS3-deficient mice display behavioral abnormalities typical to the animal models of schizophrenia.[2]

According to the same study, NPAS1 and NPAS3 disruption leads to reduced expression of reelin, which is also consistently found to be reduced in the brains of human patients with schizophrenia and psychotic bipolar disorder. Among the 49 genomic regions that undergone rapid changes in humans compared with their evolutionary ancestors, NPAS3 was found to be located in the region 21.[1]

Clinical significance

Disruption of NPAS3 was found in one family affected by schizophrenia[3] and NPAS3 gene is thought to be associated with psychiatric illness and learning disability.[4][5] In a genetic study of several hundred subjects conducted in 2008, interacting haplotypes at the NPAS3 locus were found to affect the risk of schizophrenia and bipolar disorder.[6]

In a pharmacogenetical study, polymorphisms in NPAS3 gene were highly associated with response to iloperidone, a proposed atypical antipsychotic.[7]

References

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  7. Lavedan C, Volpi S, Mack K, et al. Whole-genome association study identifies polymorphisms in the NPAS3 gene associated with super-response to iloperidone treatment in patients with schizophrenia. Program and abstracts of the 57th Annual Meeting of the American Society of Human Genetics; October 23–27, 2007; San Diego, California. Abstract 1035/T

Further reading

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