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鱼类巨噬细胞激活后会表达一种环氧化酶-2同源物。

Fish macrophages express a cyclo-oxygenase-2 homologue after activation.

作者信息

Zou J, Neumann N F, Holland J W, Belosevic M, Cunningham C, Secombes C J, Rowley A F

机构信息

Department of Zoology, University of Aberdeen, Aberdeen, AB24 2TZ, UK.

出版信息

Biochem J. 1999 May 15;340 ( Pt 1)(Pt 1):153-9.

Abstract

In mammals, the increased generation of prostaglandins (PG) during the onset of inflammatory responses and activation of immune cell types has been attributed to the induction of a novel cyclo-oxygenase (COX) isoform, termed COX-2, which is distinct from the well-characterized constitutive activity (COX-1). Goldfish (Carassius auratus) macrophages exposed to bacterial lipopolysaccharide and leucocyte-derived macrophage-activating factor(s) showed a significant increase in the generation of the major COX product, PGE2, within the first 6 h of stimulation. The selective COX-2 inhibitor, NS398, inhibited this elevated generation of PGE, whereas the basal level of this product synthesized by unstimulated macrophages was unaffected by such exposure. PGE generation by goldfish macrophages was similarly inhibited by the glucocorticoid, dexamethasone, and an inhibitor of protein synthesis, cycloheximide, suggesting that this stimulation may be due to an inducible enzyme equivalent to mammalian COX-2. The complete coding sequence of rainbow trout (Oncorhynchus mykiss) COX-2 was obtained by PCR. The gene contains a 61 bp 5'-untranslated region (UTR), a 1821 bp open reading frame and a 771 bp 3'UTR containing multiple copies of an mRNA instability motif (ATTTA). The predicted translation product had high homology to known mammalian and chicken COX-2 (83-84%) and COX-1 (77%) sequences. Reverse-transcriptase PCR with cDNA from control and bacterially challenged fish revealed that trout COX-2 expression was not constitutive but could be induced. Overall, these studies show for the first time that the inducible isoform of COX has a long evolutionary history, probably dating back to the evolution of fish over 500 million years ago.

摘要

在哺乳动物中,炎症反应开始和免疫细胞类型激活期间前列腺素(PG)生成增加,这归因于一种新型环氧化酶(COX)同工型的诱导,该同工型称为COX-2,它与特征明确的组成型活性(COX-1)不同。暴露于细菌脂多糖和白细胞衍生的巨噬细胞激活因子的金鱼(Carassius auratus)巨噬细胞在刺激的最初6小时内,主要COX产物PGE2的生成显著增加。选择性COX-2抑制剂NS398抑制了PGE的这种升高生成,而未刺激的巨噬细胞合成的该产物的基础水平不受这种暴露的影响。金鱼巨噬细胞产生PGE同样受到糖皮质激素地塞米松和蛋白质合成抑制剂环己酰亚胺的抑制,这表明这种刺激可能是由于一种与哺乳动物COX-2等效的诱导酶。通过PCR获得了虹鳟(Oncorhynchus mykiss)COX-2的完整编码序列。该基因包含一个61 bp的5'非翻译区(UTR)、一个1821 bp的开放阅读框和一个771 bp的3'UTR,其中包含mRNA不稳定基序(ATTTA)的多个拷贝。预测的翻译产物与已知的哺乳动物和鸡的COX-2(83-84%)和COX-1(77%)序列具有高度同源性。用来自对照鱼和经细菌攻击的鱼的cDNA进行逆转录酶PCR显示,鳟鱼COX-2的表达不是组成型的,而是可以被诱导的。总体而言,这些研究首次表明,COX的诱导同工型具有悠久的进化历史,可能可追溯到5亿多年前鱼类的进化。

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