AI Article Synopsis

  • There is new evidence suggesting that nitric oxide (NO) influences biological signaling through more mechanisms than previously understood, including interactions with thiols and metals to form various compounds.
  • Research shows that products of N-nitrosation and heme-nitrosylation are just as prevalent as the more studied S-nitrosation in living organisms, and these compounds have short lifetimes linked to tissue oxygen levels and redox status.
  • The study proposes that nitroso compounds form mainly through oxidative nitrosylation rather than simply from NO breakdown, indicating that tissue nitrite could be an important source of NO during low oxygen conditions and may reflect the balance of oxidative stress in tissues.

Article Abstract

There is mounting evidence that the established paradigm of nitric oxide (NO) biochemistry, from formation through NO synthases, over interaction with soluble guanylyl cyclase, to eventual disposal as nitrite/nitrate, represents only part of a richer chemistry through which NO elicits biological signaling. Additional pathways have been suggested that include interaction of NO-derived metabolites with thiols and metals to form S-nitrosothiols (RSNOs) and metal nitrosyls. Despite the overwhelming attention paid in this regard to RSNOs, little is known about the stability of these species, their significance outside the circulation, and whether other nitros(yl)ation products are of equal importance. We here show that N-nitrosation and heme-nitrosylation are indeed as ubiquitous as S-nitrosation in vivo and that the products of these reactions are constitutively present throughout the organ system. Our study further reveals that all NO-derived products are highly dynamic, have fairly short lifetimes, and are linked to tissue oxygenation and redox state. Experimental evidence further suggests that nitroso formation occurs substantially by means of oxidative nitrosylation rather than NO autoxidation, explaining why S-nitrosation can compete effectively with nitrosylation. Moreover, tissue nitrite can serve as a significant extravascular pool of NO during brief periods of hypoxia, and tissue nitrate/nitrite ratios can serve as indicators of the balance between local oxidative and nitrosative stress. These findings vastly expand our understanding of the fate of NO in vivo and provide a framework for further exploration of the significance of nitrosative events in redox sensing and signaling. The findings also raise the intriguing possibility that N-nitrosation is directly involved in the modulation of protein function.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC384737PMC
http://dx.doi.org/10.1073/pnas.0306706101DOI Listing

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