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1991 Fiscal Year Final Research Report Summary

The effect of cytochrome P450 (metabolites) on pulmonary vascular tone

Research Project

Project/Area Number 02670339
Research Category

Grant-in-Aid for General Scientific Research (C)

Allocation TypeSingle-year Grants
Research Field Respiratory organ internal medicine
Research InstitutionFukui Medical School

Principal Investigator

ISHIZAKI Takeshi  Fukui Medical School Internal Medicine Assistant Professor, 医学部, 講師 (80151364)

Co-Investigator(Kenkyū-buntansha) SASAKI Fumihiko  Fukui Medical School Internal Medicine Assistant, 医学部, 助手 (70205863)
Project Period (FY) 1990 – 1991
KeywordsCytochrome P450 / Pulmonary vascular tone / Arachidonate epoxide / Leukotoxin / Endothelin / Cyclooxygenase / EDRF / Lung injury
Research Abstract

In isolated perfused lungs from rats treated with cytochrome P450 (CP450) inducer, pulmonary arterial pressor response to hypoxia or phenylephrine but not KC1 or U46619, a thromboxane mimic, was attenuated significantly and vasodilatory response to acetylcholine was augmented. Because such effects were never obvious in the case of isolated pulmonary arterial (PA) experiment, CP450 induced modification of pulmonary vascular tone seemed to occur selectively at the resistance vessel. A 5,6 epoxyeicosatrienoic acid (5,6 EET), an arachidonate derived CP450 epoxide, and leukotoxin (Lx), a linoleate derived CL450 epoxide dilated PA ring preconstricted with phenylephrine, though cyclooxygenase inhibitor offset the vasodilatory effect due to the former but not that of the latter. Further, Lx attenuated the pressor response to hypoxia, KC1 and endothelin 1. Vasodilatory effect of Lx was largely inhibited by the endothelium denudation or addition of LNMMA, an EDRF inhibitor, suggesting that major part of Lx-induced vasodilation depend on EDRF release. Lx also dilated denuded PA ring precontracted with phenylephrine or endothelin 1 and inhibited ^<45>Ca^<2+> up take in cultured rat aortic smooth muscle experiment stimulated with endothelin 1 or phorbol myristate acetate. Since Ca channel blocker (Diltiazem or nickel) did not interfere the vasodilatory effect of Lx, Lx may augment Ca^<2+> eflux from the cell. Finally, large dose of Lx caused lung injury which was suppressed by the pretreatment of LNMMA, suggesting that Lx-induced massive release of EDRF (NO) caused lung injury. Thus, CP450 (methabolites) have a potential of modulation of pulmonary vascular tone.

  • Research Products

    (6 results)

All Other

All Publications (6 results)

  • [Publications] 高橋 秀房: "Leukotoxin,9,10-Epoxy-12-Octa-decenoateはエンドセソン1で収縮したラット摘出肺動脈リングを拡張する" 日胸疾誌. 30. (1992)

    • Description
      「研究成果報告書概要(和文)」より
  • [Publications] H.Takahashi: "Leukotoxin,9,10-Epoxy-12-Octadecenoate inhibits pulmonary vasocontractive response to Endothelin 1" J.Appl.Physiol.

    • Description
      「研究成果報告書概要(和文)」より
  • [Publications] T.Ishizaki: "Leukotoxin,9,10-Epoxy-12-Octadecenoate causes pulmonary vasodilation in the rat" J.Appl.Physiol.

    • Description
      「研究成果報告書概要(和文)」より
  • [Publications] 石崎 武志: "Cytochrome P450と肺" 呼吸. 10. 1120-1130 (1991)

    • Description
      「研究成果報告書概要(和文)」より
  • [Publications] H.Takahashi: "High-Altitude Medical Science Effect of Leukotoxin,9,10-Epoxy-12-Octadecenoate,on Pulmonary Vessels" Press Committee of HAMS Symposium Department of Enviromental Physiology and 1st Internal Medicine,Shinshu University School of Medecine, 10 (1992)

    • Description
      「研究成果報告書概要(和文)」より
  • [Publications] T.Ishizaki: "High-Altitude Medical Science The Effect of Lung Cytochrome P450 Induction Vascular Reactivity of Rat Isolated Perfused Lung and Isolated Pulmonary artery" Press Committee of HAMS Symposium Department of Enviromental Physiology and 1st Internal Medicine Shinshu University School of Medicine,Matsumoto, 8 (1992)

    • Description
      「研究成果報告書概要(和文)」より

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Published: 1994-03-18  

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