%0 Journal Article
%T A novel soluble guanylate cyclase activator with reduced risk of hypotension by shortİ\acting vasodilation
%A Akihiro Kobayashi
%A Akiyuki Takaya
%A Kazuyuki Aihara
%A Kosuke Nagasaka
%A Toshihiro Sawabe
%A Toshiki Chiba
%J Archive of "Pharmacology Research & Perspectives".
%D 2019
%R 10.1002/prp2.463
%X Cinaciguat, a soluble guanylate cyclase (sGC) activator, was under clinical development for use in acute decompensated heart failure (ADHF), but was discontinued due to occurrence of hypotension. We hypothesized that shortİ\term activation of sGC in ADHF patients would exert a vasodilative effect without hypotension irrespective of disease state, using a novel shortİ\acting sGC activator, TYİ\55002. The objective of this study was to investigate the vasodilation and hemodynamic effects of TYİ\55002 in comparison with those of cinaciguat. TYİ\55002 and cinaciguat activated both normal and hemeİ\oxidized sGC in a doseİ\dependent manner and caused rapid relaxation of phenylephrineİ\contracted rat aorta. However, TYİ\55002 had a milder effect than cinaciguat in enhancing the doseİ\activity response between normal and oxidized sGC. Therefore, we suggest that the pharmacological effect of TYİ\55002 is less subject than cinaciguat to oxidative stress associated with complications such as cardiovascular disease or diabetes. In normal dogs, the effects of intravenous TYİ\55002 or cinaciguat on blood pressure were evaluated in conjunction with the plasma concentrations of the compounds, and pharmacokinetic (PK)İ\pharmacodynamic (PD) analyses were carried out. The plasmaİ\toİ\effectİ\site transfer rate constant (Ke0) for TYİ\55002 was three times greater than for cinaciguat. On the other hand, there was a small difference in blood halfİ\life (T1/2) between the compounds. It is possible that the rapid fall in blood pressure after the initial administration of TYİ\55002 and the quick recovery after cessation were due to the pharmacodynamic property of the compound. In heart failureİ\model dogs, TYİ\55002 and cinaciguat improved the condition to the same degree, and the shortİ\term action of TYİ\55002 was replicated. In conclusion, TYİ\55002 is a novel shortİ\acting sGC activator, which offers the possibility of easy dose management without excessive hypotension. It therefore holds potential to serve as an innovative drug in the pharmacotherapy of ADHF
%K acute decompensate heart failure
%K pharmacokineticİ\pharmacodynamic
%K soluble guanylate cyclase activator
%K TYİ\55002
%U https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6399102/