Key bioactive reaction products of the NO/H<sub>2</sub>S interaction are S/N-hybrid species, polysulfides, and nitroxyl

Miriam M. Cortese‐Krott; Gunter Kuhnle; Alex Dyson; Bernadette Fernandez; Marian Grman; Jenna F. DuMond; Mark P. Barrow; George McLeod; Hidehiko Nakagawa; Karol Ondriaš; Péter Nagy; S. Bruce King; Joseph E. Saavedra; Larry K. Keefer; Mervyn Singer; Malte Kelm; Anthony R. Butler; Martin Feelisch

doi:10.1073/pnas.1509277112

Key bioactive reaction products of the NO/H<sub>2</sub>S interaction are S/N-hybrid species, polysulfides, and nitroxyl

Miriam M. Cortese‐Krott(Heinrich Heine University Düsseldorf), Gunter Kuhnle(University of Reading), Alex Dyson(Bury College), Bernadette Fernandez(Southampton General Hospital), Marian Grman(Slovak Academy of Sciences), Jenna F. DuMond(Wake Forest University), Mark P. Barrow(University of Warwick), George McLeod(Coventry (United Kingdom)), Hidehiko Nakagawa(Nagoya City University), Karol Ondriaš(Slovak Academy of Sciences), Péter Nagy(National Institute of Oncology), S. Bruce King(Wake Forest University), Joseph E. Saavedra(Leidos (United States)), Larry K. Keefer(Frederick National Laboratory for Cancer Research), Mervyn Singer(Bury College), Malte Kelm(Heinrich Heine University Düsseldorf), Anthony R. Butler(University of St Andrews), Martin Feelisch(Southampton General Hospital)

Proceedings of the National Academy of Sciences

July 29, 2015

10.1073/pnas.1509277112

Cited by 280Open Access

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Abstract

Experimental evidence suggests that nitric oxide (NO) and hydrogen sulfide (H2S) signaling pathways are intimately intertwined, with mutual attenuation or potentiation of biological responses in the cardiovascular system and elsewhere. The chemical basis of this interaction is elusive. Moreover, polysulfides recently emerged as potential mediators of H2S/sulfide signaling, but their biosynthesis and relationship to NO remain enigmatic. We sought to characterize the nature, chemical biology, and bioactivity of key reaction products formed in the NO/sulfide system. At physiological pH, we find that NO and sulfide form a network of cascading chemical reactions that generate radical intermediates as well as anionic and uncharged solutes, with accumulation of three major products: nitrosopersulfide (SSNO(-)), polysulfides, and dinitrososulfite [N-nitrosohydroxylamine-N-sulfonate (SULFI/NO)], each with a distinct chemical biology and in vitro and in vivo bioactivity. SSNO(-) is resistant to thiols and cyanolysis, efficiently donates both sulfane sulfur and NO, and potently lowers blood pressure. Polysulfides are both intermediates and products of SSNO(-) synthesis/decomposition, and they also decrease blood pressure and enhance arterial compliance. SULFI/NO is a weak combined NO/nitroxyl donor that releases mainly N2O on decomposition; although it affects blood pressure only mildly, it markedly increases cardiac contractility, and formation of its precursor sulfite likely contributes to NO scavenging. Our results unveil an unexpectedly rich network of coupled chemical reactions between NO and H2S/sulfide, suggesting that the bioactivity of either transmitter is governed by concomitant formation of polysulfides and anionic S/N-hybrid species. This conceptual framework would seem to offer ample opportunities for the modulation of fundamental biological processes governed by redox switching and sulfur trafficking.

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