4.7 Article

Nitrosopersulfide (SSNO-) accounts for sustained NO bioactivity of S-nitrosothiols following reaction with sulfide

期刊

REDOX BIOLOGY
卷 2, 期 -, 页码 234-244

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.redox.2013.12.031

关键词

Hydrogen sulfide; Nitric oxide; Polysulfides; cGMP; HSNO; Nitroxyl

资金

  1. Susanne-Bunnenberg-Stiftung of the Dusseldorf Heart Center
  2. COST action (European Network on Gasotransmitters) [BM1005]
  3. FP7 Marie Curie International Reintegration program [PIRG08-GA-2010-277006]
  4. Faculty of Medicine, University of Southampton

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Sulfide salts are known to promote the release of nitric oxide (NO) from S-nitrosothiols and potentiate their vasorelaxant activity, but much of the cross talk between hydrogen sulfide and NO is believed to occur via functional interactions of cell regulatory elements such as phosphodiesterases. Using RFL-6 cells as an NO reporter system we sought to investigate whether sulfide can also modulate nitrosothiol-mediated soluble guanylyl cyclase (sGC) activation following direct chemical interaction. We find a U-shaped dose response relationship where low sulfide concentrations attenuate sGC stimulation by S-nitrosopenicillamine (SNAP) and cyclic GMP levels are restored at equimolar ratios. Similar results are observed when intracellular sulfide levels are raised by pre-incubation with the sulfide donor, GYY4137. The outcome of direct sulfide/nitrosothiol interactions also critically depends on molar reactant ratios and is accompanied by oxygen consumption. With sulfide in excess, a 'yellow compound' accumulates that is indistinguishable horn the product of solid-phase transnitrosation of either hydrosulfide or hydrodisulfide and assigned to be nitrosopersulfide (perthionitrite, SSNO----; lambda(max) 412 nm in aqueous buffers, pH 7.4; 448 nm in DMF). Time-resolved chemiluminescence and UV-visible spectroscopy analyses suggest that its generation is preceded by formation of the short-lived NO-donor, thionitrite (SNO----). In contrast to the latter, SSNO---- is rather stable at physiological pH and generates both NO and polysulfides on decomposition, resulting in sustained potentiation of SNAP-induced sGC stimulation. Thus, sulfide reacts with nitrosothiols to form multiple bioactive products; SSNO---- rather than SNO---- may account for some of the longer-lived effects of nitrosothiols and contribute to sulfide and NO signaling. (C) 2014 The Authors. Published by Elsevier B.V. All rights reserved

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