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We began analyzing https://journals.lww.com/jhypertension/abstract/2010/09000/systemic_peripheral_artery_relaxation_by_kcnq.14.aspx, but it redirected us to https://journals.lww.com/jhypertension/abstract/2010/09000/systemic_peripheral_artery_relaxation_by_kcnq.14.aspx. The analysis below is for the second page.
Title[redir]:
Journal of Hypertension
Description:
performed isometric contraction studies on systemic arteries of rats and mice. Results In mesenteric arteries and aortas without perivascular adipose tissue, the KCNQ channel openers retigabine, VRX0530727, VRX0621238, and VRX0621688 produced concentration-dependent vasorelaxation; VRX0621688 was the most potent vasodilator. The KCNQ inhibitor XE991 (30 μmol/l) blocked the effects of both the drugs and ADRF. Inhibitors of cystathionine gamma lyase (CSE) β-cyano-L-alanine (BCA, 5 mmol/l) and 4-propargyl glycine (PPG, 10 mmol/l) also blocked the relaxations. CSE is expressed in perivascular adipose tissue and endogenously generates H2S. The H2S donor NaHS produced concentration-dependent vasorelaxation, which was also blocked by XE991. The vasodilatory capacities of retigabine, VRX0530727, VRX0621238, and VRX0621688 were preserved following inhibition of H2S generation in perivascular fat. Conclusion We suggest that KCNQ channel opening is a powerful mechanism to produce vasorelaxation of systemic arteries in rats and mice. Furthermore, KCNQ channels play a major role in the paracrine control of vascular tone by perivascular adipose tissue, which is at least in part mediated or modulated by H2S. In conditions of reduced H2S release from perivascular adipose tissue, these paracrine effects can be mimicked by synthetic KCNQ channel openers....
Title[redir]:
Journal of Hypertension
Description:
performed isometric contraction studies on systemic arteries of rats and mice. Results In mesenteric arteries and aortas without perivascular adipose tissue, the KCNQ channel openers retigabine, VRX0530727, VRX0621238, and VRX0621688 produced concentration-dependent vasorelaxation; VRX0621688 was the most potent vasodilator. The KCNQ inhibitor XE991 (30 μmol/l) blocked the effects of both the drugs and ADRF. Inhibitors of cystathionine gamma lyase (CSE) β-cyano-L-alanine (BCA, 5 mmol/l) and 4-propargyl glycine (PPG, 10 mmol/l) also blocked the relaxations. CSE is expressed in perivascular adipose tissue and endogenously generates H2S. The H2S donor NaHS produced concentration-dependent vasorelaxation, which was also blocked by XE991. The vasodilatory capacities of retigabine, VRX0530727, VRX0621238, and VRX0621688 were preserved following inhibition of H2S generation in perivascular fat. Conclusion We suggest that KCNQ channel opening is a powerful mechanism to produce vasorelaxation of systemic arteries in rats and mice. Furthermore, KCNQ channels play a major role in the paracrine control of vascular tone by perivascular adipose tissue, which is at least in part mediated or modulated by H2S. In conditions of reduced H2S release from perivascular adipose tissue, these paracrine effects can be mimicked by synthetic KCNQ channel openers....
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Keywords {🔍}
journal, vrx, kcnq, perivascular, adipose, tissue, issue, channel, arteries, access, subscribe, alerts, submit, articles, authors, abstract, systemic, openers, adrf, channels, vasorelaxation, blocked, log, register, issues, peripheral, hydrogen, sulfide, buy, role, rats, mice, retigabine, produced, concentrationdependent, effects, cse, mmoll, paracrine, text, subscribers, request, browse, content, service, privacy, policy, manuscript, logo, advanced,
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adipocyte-derived relaxing factor β-cyano-l-alanine kcnq-type kv channels journal authors submit perivascular adipose tissue opens voltage-dependent kcnq channel openers kcnq channel opening full text access kcnq channels play cystathionine gamma lyase artificial intelligence training endogenously generates h2s reduced h2s release kcnq inhibitor xe991 service request 800-638-3030 register subscribe individual subscribers log journal tables produce vasorelaxation peripheral arteries perivascular fat systemic arteries etoc alerts hydrogen sulfide website subscribe journal h2s generation center submit authors christopher sd friedrich ca mesenteric arteries potent vasodilator 4-propargyl glycine vasodilatory capacities powerful mechanism paracrine control vascular tone part mediated email inbox rights reserved data mining issue major role paracrine effects content h2s channels kv
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