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Publication : Circadian clock control of Nox4 and reactive oxygen species in the vasculature.

First Author  Anea CB Year  2013
Journal  PLoS One Volume  8
Issue  10 Pages  e78626
PubMed ID  24205282 Mgi Jnum  J:209225
Mgi Id  MGI:5566728 Doi  10.1371/journal.pone.0078626
Citation  Anea CB, et al. (2013) Circadian clock control of Nox4 and reactive oxygen species in the vasculature. PLoS One 8(10):e78626
abstractText  Recent studies have shown that circadian clock disruption is associated with pathological remodeling in the arterial structure and vascular stiffness. Moreover, chronic circadian disruption is associated with dysfunction in endothelial responses and signaling. Reactive oxygen species have emerged as key regulators in vascular pathology. Previously, we have demonstrated that circadian clock dysfunction exacerbates superoxide production through eNOS uncoupling. To date, the impact of circadian clock mutation on vascular NADPH oxidase expression and function is not known. The goal in the current study was to determine if the circadian clock controls vascular Nox4 expression and hydrogen peroxide formation in arteries, particularly in endothelial and vascular smooth muscle cells. In aorta, there was an increase in hydrogen peroxide and Nox4 expression in mice with a dysfunctional circadian rhythm (Bmal1-KO mice). In addition, the Nox4 gene promoter is activated by the core circadian transcription factors. Lastly, in synchronized cultured human endothelial cells, Nox4 gene expression exhibited rhythmic oscillations. These data reveal that the circadian clock plays an important role in the control of Nox4 and disruption of the clock leads to subsequent production of reaction oxygen species.
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