International Union of Basic and Clinical Pharmacology. CII: Pharmacological Modulation of H₂S Levels: H₂S Donors and H₂S Biosynthesis Inhibitors

Abstract: Over the last decade, hydrogen sulfide (HS) has emerged as an important endogenous gasotransmitter in mammalian cells and tissues. Similar to the previously characterized gasotransmitters nitric oxide and carbon monoxide, HS is produced by various enzymatic reactions and regulates a host of physiologic and pathophysiological processes in various cells and tissues. HS levels are decreased in a number of conditions (e.g., diabetes mellitus, ischemia, and aging) and are increased in other states (e.g., inflammati… Show more

“…In no instance was H 2 S production completely inhibited. This could be attributed to poor absorption by cells or lack of inhibitor specificity . It is also possible that H 2 S may be produced by one or several other “unconventional” pathways that are unaffected by these inhibitors and are independent of Cys.…”

Extended hypoxia‐mediated H₂S production provides for long‐term oxygen sensing

“…In no instance was H 2 S production completely inhibited. This could be attributed to poor absorption by cells or lack of inhibitor specificity . It is also possible that H 2 S may be produced by one or several other “unconventional” pathways that are unaffected by these inhibitors and are independent of Cys.…”

Extended hypoxia‐mediated H₂S production provides for long‐term oxygen sensing

“…In addition, intravesically instilled NaHS at 1 mM increased the frequency of micturition and reduced voiding volume in Sprague‐Dawley rats, while GYY4137, a slow‐releasing H 2 S donor, at a submicromolar order prolonged ICI and tended to reduce MVP in Wistar rats in this study. In general, responses induced by gasotransmitters are highly dependent on the dose, the physiological response at lower doses and the toxic effect at higher doses, and fatal effects of H 2 S occur at approximately 0.1% (=29 mM) . Therefore, NaHS‐induced contraction in vitro and in vivo might indicate a toxic effect of H 2 S on the bladder.…”

“…A limitation of this study is that effects of H 2 S biosynthesis inhibition or H 2 S scavenging on bladder and prostate contractility were not investigated. Some compounds are reported to inhibit CBS, CSE, or MPST, and in human urothelium, carbachol‐induced enhancement of H 2 S production was attenuated by a “CBS inhibitor.” However, these compounds have limitations, low potency and non‐selectivity . In addition, to our knowledge, there is nor report demonstrating selective H 2 S scavengers.…”

“…After a 30 min‐washout period, prostate strips were pre‐treated with propranolol (1 × 10 −6 M) to prevent β‐adrenoceptor‐mediated relaxation. The relaxation response to NaHS (a rapid‐releasing H 2 S donor: 1 × 10 −9 to 3 × 10 −4 M) was measured cumulatively in bladder strips pre‐contracted by carbachol (1 × 10 −5 M) and prostate strips pre‐contracted by noradrenaline (1 × 10 −5 M). NaHS solutions were quickly prepared before use.…”

“…Cystometry was performed under urethane anesthesia (0.8 g/kg, ip) according to previous reports . Saline was intravesically instilled (2.4 mL/h) in all animals until 4‐5 voidings were detected, and then ether GYY4137 (a slow‐releasing H 2 S donor: 10 −8 , 10 −7 , and 10 −6 M in saline) or vehicle (3.3 × 10 −5 % N , N ‐dimethylformamide/saline) was instilled (2.4 mL/h). In the GYY4137‐treated group, after detecting 4‐5 voidings, the dose was increased in turn, and a total of 12‐15 voidings were recorded after starting GYY4137 instillation.…”

Possible role of hydrogen sulfide as an endogenous relaxation factor in the rat bladder and prostate

Persulfide Prodrugs