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Oxidative Medicine and Cellular Longevity - Volume 2016 2016, Article ID 6549625, 2 pages -

Editorial

Department of Pharmacology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore 117597

Department of Physiology, University of Notre Dame, 1234 Notre Dame Avenue, South Bend, IN 46617, USA

Department of Physiology and Pathophysiology, Fudan University Shanghai Medical College, 138 Yi Xue Yuan Road, Shanghai 200032, China

Received 28 March 2016; Accepted 29 March 2016

Copyright © 2016 Jin-Song Bian et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

The seminal studies by Kimura’s group in the late 1990s 1, 2 ushered in a new era of biological signaling mediated by hydrogen sulfide H2S. H2S has been described as the third -gasotransmitter- along with nitric oxide NO and carbon monoxide CO; 3. While none of these molecules actually signal as a gas, their hydrophilicity and lipophilicity enable them to readily traverse intracellular compartments where they serve in a variety of autocrine and paracrine signals capacities.

Of the three, however, H2S is arguably the most chemically reactive and biologically diverse. As a weak acid, H2S exists as the dissolved gas and hydrosulfide anion HS

in nearly equal proportions in the circumneutral intracellular milieu. H2S is readily oxidized to per- and polysulfides forming a highly reactive group of molecules reactive sulfide species, RSS that readily form reversible covalent bonds, coordinate with metal ligands, and participate in a variety of redox reactions 4, 5. H2S was key in the origin of life 6 and it remains as the only inorganic substrate used by eukaryotic cells to generate ATP 7. H2S mediates many physiological functions in various biological systems including cytoprotection, neuromodulation, ischemic responses, and oxygen sensing. Exogenous application of H2S may protect cell function against ischemic and oxidant injuries. Despite the fact that the multiple roles of H2S in biology have been intensely discussed over the last twenty years, many questions remain to be resolved. The eclectic nature of H2S is featured in this special issue as a collection of original articles and reviews that examine a variety of the physiological functions of H2S as well as its therapeutic attributes.

The role of H2S in oxidative stress has been one of the main focuses over the last two decades. The review by Xie et al. focuses on the new understanding and mechanisms of the antioxidant effects of H2S based on recent reports. As a poor reducing agent, H2S may react directly with and quench superoxide, peroxynitrite, and other ROS. However, the direct antioxidant effect may not be its main function. H2S can scavenge free radicals via activation of both nonenzymatic e.g., glutathione and thioredoxin and enzymatic e.g., superoxide dismutase, catalase, and glutathione peroxidase antioxidants. Apart from stimulation of cellular antioxidant defenses, H2S may also inhibit the overproduction of ROS via modification of the structure of p66Shc at cysteine-59. This subsequently inhibits mitochondrial ROS generation in the mitochondria. Thus, this review provides new insights to better understand the important role of the H2S in oxidative stress and the related diseases.

Being gaseous molecules and mediators, both H2S and NO play important roles in various biological systems. While the individual signaling mechanisms mediated by H2S and NO in mammals are extensively studied, our understanding about the potential relationship between these two gasotransmitters is woefully incomplete. Nagpure and Bian reviewed recent research progress in the interactions between these two gaseous mediators. H2S may reduce oxidized NO leading to the formation of HSNO as an intermediate. Further reduction and direct displacement of HSNO by H2S result in the formation of another intermediate product, nitroxyl HNO. Interestingly, HNO produces chemical and physiological functions different from NO and H2S. The role of this interaction in heart and vascular physiology and pathology is also summarized in this review.

In the original article by D. Wu et al., the authors studied the interaction between H2S and NO in vasculature using a novel H2S and NO conjugated donor, ZYZ-803. The authors found that, by releasing H2S and NO, ZYZ-803 time- and dose-dependently relaxed rat aortic rings. Mechanistic studies revealed that the effect of ZYZ-803 was mediated by cGMP. Interestingly, suppression of either H2S or NO generation with their respective inhibitors abolished the vasorelaxant effect of ZYZ-803. These interesting data suggest that H2S and NO generated from ZYZ-803 can cooperatively regulate vascular tone.

In the original article by P. Huang et al., the authors investigated whether H2S can prevent high-salt diet-induced renal injury. Dahl rats on a high-salt diet for 8 weeks developed hypertension and kidney injury with excessive oxidative stress and an obvious reduction of endogenous H2S. Exogenous application of H2S, however, decreased blood pressure and improved renal function. The authors believe that the beneficial effects of H2S resulted from Keap1-Nrf2 disassociation.

Sulfur dioxide SO2 has also long been thought to be a toxic gas. A group of scientists in China recently reported that this gas can be produced endogenously. In the review article by Y. Huang et al., the authors summarized the physiological and pathological functions of SO2 in the cardiovascular system. These include regulation of vascular tone and heart contractility and its effects on disease status like systemic and pulmonary hypertension, atherosclerosis, and ischemic diseases. Based on these effects, they propose that endogenous SO2 may be a potential therapeutic target for cardiovascular diseases.

In the original article by N. Li et al., the authors examined the effect of H2S on protein expression of various H2S generating enzymes in both ischemic heart tissue and cultured cardiomyocytes during hypoxia. They found that NaHS treatment upregulated protein expression of various enzymes with different patterns in the two pathological situations. The authors believe that CSE may serve as the most important enzyme to regulate H2S production in myocardium. This is because when CSE was deleted, the compensatory expressions of CBS and 3-MST were not enough to rescue H2S levels and protect the heart. These interesting data suggest that exogenous H2S may alter the production of endogenous H2S and therefore protect the heart with a new mechanism.

Respiratory and gastrointestinal epithelia are directly exposed to environmental- or bacterial-derived H2S which can raise the H2S concentration in these tissues. E. Pouokam and M. Althaus discussed in their review article how epithelial cells quickly process and maintain H2S level to prevent excessive increases. They proposed a new concept that electrolyte and liquid transport machinery inside epithelia may serve as a fortress against potentially harmful higher level H2S. In this interesting review article, reactions to exposed H2S and potential physiological and pathophysiological implications were also discussed.

Vascular calcification VC is a refractory component of many cardiovascular diseases and is associated with hypertension HT and endoplasmic reticulum stress ERS. In this original research article, R. Yang et al. induced VC and HT in rats with vitamin D3 and observed that daily i.p. injection of H2S as NaSH over 28 days prevented VC, HT, and conversion of vascular smooth muscle cells from a contractile to an osteoblast-like phenotype common in VC. H2S also prevented VC-induced downregulation of cystathionine γ-lyase and the authors presented evidence that suggested H2S also ameliorated ERS. This article adds yet another piece to the ever growing body of evidence that H2S is a general cardiovascular protectant.

Unfortunately, this issue can only touch on a few select aspects of H2S biology. However, we hope this broad-spectrum, albeit limited, approach serves to illustrate the myriad of physiological processes potentially influenced by H2S and entice new investigators into this exciting field.

Jin-Song BianKenneth R. OlsonYi-Chun Zhu

References

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Autor: Jin-Song Bian, Kenneth R. Olson, and Yi-Chun Zhu

Fuente: https://www.hindawi.com/



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