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1-氨基苯并三唑对动脉导管向氧气收缩的抑制作用,1-氨基苯并三唑是一种基于机制的细胞色素P450失活剂。

Inhibition of the contraction of the ductus arteriosus to oxygen by 1-aminobenzotriazole, a mechanism-based inactivator of cytochrome P450.

作者信息

Coceani F, Kelsey L, Seidlitz E, Korzekwa K

机构信息

Research Institute, Hospital for Sick Children, Toronto, Ontario, Canada.

出版信息

Br J Pharmacol. 1996 Apr;117(7):1586-92. doi: 10.1111/j.1476-5381.1996.tb15325.x.

DOI:10.1111/j.1476-5381.1996.tb15325.x
PMID:8730758
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909445/
Abstract
  1. We have proposed that contractile tension of the ductus arteriosus is sustained by a cytochrome P450-linked mechanism acting as a limiting step in the synthesis of endothelin-1 (ET-1). In the present study, we have used the isolated ductus from near-term foetal lambs and guinea-pigs to investigate the effect on both muscle tone and ET-1 formation of 1-aminobenzotriazole (ABT), a suicide substrate for mono-oxygenase reactions. 2. ABT relaxed the lamb ductus at rest (2.5% O2) and during the oxygen contraction (15 to 95% O2). The effect was seen at 40 microM, and at 0.8 mM active tone was almost completely abolished. ABT (1 mM) also reversed the oxygen contraction in the guinea-pig ductus. 3. In the lamb ductus, the ABT response was not affected by removal of the endothelium or by treatment with 2.8 microM indomethacin (at 2.5% O2) and the ensuing contraction. 4. At both low and high concentration, ABT relaxed marginally, or not at all, the potassium-contracted (55 mM) ductus from either species. 5. ET-1 release from either the intact or endothelium-denuded lamb ductus tended to decrease in the presence of ABT (1 mM), whilst during the same treatment cyclic GMP content of the tissue remained unchanged. 6. We conclude that ABT relaxation is due to suppression of a contractile mechanism and not to activation of prostaglandin- and NO-mediated relaxing mechanisms. This contractile mechanism has a cytochrome P450-based mono-oxygenase reaction as a key component.
摘要
  1. 我们曾提出,动脉导管的收缩张力由一种细胞色素P450相关机制维持,该机制是内皮素-1(ET-1)合成中的一个限速步骤。在本研究中,我们使用了来自近足月胎羊和豚鼠的离体动脉导管,以研究单加氧酶反应的自杀底物1-氨基苯并三唑(ABT)对肌肉张力和ET-1形成的影响。2. ABT使静息状态(2.5%氧气)和氧收缩期间(15%至95%氧气)的羊动脉导管舒张。在40微摩尔时可见此效应,在0.8毫摩尔时主动张力几乎完全消失。ABT(1毫摩尔)也可逆转豚鼠动脉导管的氧收缩。3. 在羊动脉导管中,ABT反应不受去除内皮或用2.8微摩尔吲哚美辛处理(在2.5%氧气时)及随后的收缩影响。4. 在低浓度和高浓度下,ABT对两种动物钾收缩(55毫摩尔)的动脉导管舒张作用微弱或无舒张作用。5. 在存在ABT(1毫摩尔)的情况下,完整或去内皮的羊动脉导管释放的ET-1均有减少趋势,而在相同处理期间组织的环鸟苷酸含量保持不变。6. 我们得出结论,ABT舒张是由于抑制了收缩机制,而非激活了前列腺素和一氧化氮介导的舒张机制。这种收缩机制以基于细胞色素P450的单加氧酶反应为关键成分。

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Inhibition of the contraction of the ductus arteriosus to oxygen by 1-aminobenzotriazole, a mechanism-based inactivator of cytochrome P450.1-氨基苯并三唑对动脉导管向氧气收缩的抑制作用,1-氨基苯并三唑是一种基于机制的细胞色素P450失活剂。
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