Effects of inhibitors of EDRF and EDHF on vasoreactivity of perfused rat lungs
| Autor: | Takashi Yamaguchi, David M. Rodman, Kiichi Hasunuma, Richard F. O'Brien, Ivan F. McMurtry |
|---|---|
| Rok vydání: | 1991 |
| Předmět: |
Pulmonary and Respiratory Medicine
Male medicine.medical_specialty Pulmonary Circulation Vascular smooth muscle Physiology Vasodilation Blood Pressure In Vitro Techniques Pulmonary Artery Nitric Oxide Glibenclamide chemistry.chemical_compound Biological Factors Hemoglobins Physiology (medical) Internal medicine Hypoxic pulmonary vasoconstriction Glyburide medicine Animals Channel blocker Hypoxia Analysis of Variance Tetraethylammonium business.industry Angiotensin II Rats Inbred Strains Cell Biology Hypoxia (medical) Tetraethylammonium Compounds Rats Perfusion Endocrinology chemistry cardiovascular system medicine.symptom business Histamine circulatory and respiratory physiology medicine.drug |
| Zdroj: | The American journal of physiology. 260(2 Pt 1) |
| ISSN: | 0002-9513 |
| Popis: | Recent studies indicate that the endothelium of isolated rat pulmonary arteries releases two different factors, endothelium-derived relaxing factor (EDRF) and hyperpolarizing factor (EDHF), which participate in histamine- and acetylcholine-induced relaxation. There is evidence for EDRF vasoreactivity in perfused lungs, but a role for EDHF, which hyperpolarizes vascular smooth muscle by activating membrane K+ channels, has not been reported. We used the inhibitors of EDRF, 20 microM hemoglobin, 200 microM NG-mono-methyl-L-arginine, and 2 mM L-canavanine, the nonselective blocker of K+ channels, 10 mM tetraethylammonium (TEA), and the inhibitor of ATP-sensitive K+ channels, 20 microM glibenclamide, to compare the roles of EDRF and EDHF in the vasoregulation of meclofenamate-treated, salt solution-perfused rat lungs. The three EDRF inhibitors had little or no effect on baseline perfusion pressure, but each potentiated the peak pressor response to airway hypoxia. Neither of them inhibited the pulmonary vasodilation to 5 microM histamine. TEA, but not glibenclamide, increased baseline pressure and potentiated the peak hypoxic response. Both K+ channel blockers, but not the EDRF inhibitors, also prolonged the hypoxic response by reducing the rate of spontaneous vasodilation. TEA, but not glibenclamide, inhibited histamine vasodilation. These results suggest roles for both EDRF and EDHF in the control of rat pulmonary vascular reactivity. EDRF is apparently not responsible for the low vascular tone of the normoxic lung and does not mediate the vasodilation to histamine, but it does modulate the hypoxic pressor response. The exact role of EDHF is uncertain, but it may also modulate hypoxic vasoconstriction and mediate at least part of the histamine vasodilation. |
| Databáze: | OpenAIRE |
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