猪眼组织合成12(R)-和12(S)-羟基二碳四烯酸。

T Asakura, M Matsuda, S Matsuda, H Shichi
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引用次数: 17

摘要

猪眼组织微粒体通过膜结合脂加氧酶从花生四烯酸合成12(S)-5,8,10,14-羟基二十碳四烯酸[12(S)-HETE],通过细胞色素p450依赖的单加氧酶系统合成12(R)-HETE。这两种活性在角膜微粒体中最高。角膜微粒体的12(R)-HETE合成活性依赖于NADPH,并被0.1 mM SKF-525A(一种P450酶抑制剂)抑制。3-甲基胆蒽或氯贝酸钠处理角膜上皮后,形成12(R)-对映体的活性显著增强。诱导活性被环己亚胺抑制,表明酶活性的诱导涉及一个翻译过程。这些诱导剂对12(R)-HETE合成活性的影响表现为加性作用。3 mM CaCl2明显促进了12(S)-对映体的形成。角膜微粒体的12-脂氧合酶除了能氧合花生四烯酸外,还能氧合亚油酸,这是白细胞型12-脂氧合酶的特征。12(R)-HETE在10(-6)M时几乎完全抑制角膜上皮的Na, k - atp酶,但对睫状上皮酶活性几乎没有影响。10(-6) M的12(S)-HETE也能抑制角膜酶活性,但抑制程度较轻,对睫状上皮Na、k - atp酶活性无显著影响。
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Synthesis of 12(R)- and 12(S)-hydroxyeicosatetraenoic acid by porcine ocular tissues.

Microsomal fractions from porcine ocular tissues synthesized 12(S)-5,8,10,14-hydroxyeicosatetraenoic acid [12(S)-HETE] from arachidonic acid by a membrane-bound lipoxygenase and 12(R)-HETE by the cytochrome P450-dependent monooxygenase system. Both activities were the highest in corneal microsomes. The 12(R)-HETE synthesizing activity of corneal microsomes was dependent on NADPH and inhibited by 0.1 mM SKF-525A, an inhibitor of P450 enzymes. The activity to form 12(R)-enantiomer was significantly enhanced by treatment of corneal epithelium with 3-methylcholanthrene or clofibrate. The induced activity was suppressed by cycloheximide, indicating that the induction of enzyme activities involved a translational process. The effect of these inducers on 12(R)-HETE synthesizing activity appeared to be additive. The activity to form 12(S)-enantiomer was markedly stimulated by 3 mM CaCl2. The 12-lipoxygenase of corneal microsomes was capable of oxygenating linoleic acid in addition to arachidonic acid, a characteristic of 12-lipoxygenases of the leukocyte type. 12(R)-HETE at 10(-6) M inhibited almost completely the Na,K-ATPase of corneal epithelium but had little or no effect on ciliary epithelial enzymic activity. 12(S)-HETE at 10(-6) M also inhibited corneal enzymic activity but to a lesser extent, and had no significant effect on ciliary epithelial Na,K-ATPase activity.

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