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大鼠肾毒性肾炎中肾小球12/15-脂氧合酶与白细胞介素-4信使核糖核酸的共同调节表达

Co-regulated expression of glomerular 12/15-lipoxygenase and interleukin-4 mRNAs in rat nephrotoxic nephritis.

作者信息

Katoh T, Lakkis F G, Makita N, Badr K F

机构信息

Department of Medicine, Emory University, Atlanta, Georgia.

出版信息

Kidney Int. 1994 Aug;46(2):341-9. doi: 10.1038/ki.1994.280.

DOI:10.1038/ki.1994.280
PMID:7967345
Abstract

Arachidonate 12- and 15-lipoxygenase (LO) products are generated in experimental glomerulonephritis. 15-S-HETE (a 15-LO product) and lipoxins (interaction products between 5-LO and either 12-LO or 15-LO) counteract the proinflammatory actions of leukotrienes. IL-4 has been shown to up-regulate 15-LO gene expression in human leukocytes. Based on homology with human 15-LO, we cloned a 0.76 kbp fragment of a rat LO cDNA from leukocytes stimulated by interleukin-4 (IL-4). The deduced amino acid sequence shows 71.0% and 60.1% homology to human 15-LO and 12-LO, respectively, and 100% homology to a recently cloned "leukocyte type" rat 12-lipoxygenase enzyme, which possesses significant 15-lipoxygenase activity (heretofore referred to as "12/15-LO"). A deletion mutant was utilized to generate internal standard cRNA in quantitative PCR assays. Glomerular 12/15-LO mRNA increased significantly over controls 24 and 48 hours after NTS injection, then decreased at 72 hours. RNA from NTS glomeruli contained higher levels of 12/15-LO mRNA than that from unstimulated peripheral leukocytes, suggesting that 12/15-LO transcription is up-regulated locally in native and/or infiltrating glomerular cells. Glomerular IL-4 mRNA increased markedly 16 hours post-NTS, and was then reduced, suggesting a potential role for T cell-derived IL-4 in directing the expression of 12/15-LO during glomerulonephritis. This represents the first demonstration of tandem regulated in vivo gene expression for a lymphokine (IL-4) and a lipoxygenase, both of which promote counter-inflammatory influences in immune complex-mediated injury.

摘要

花生四烯酸12-和15-脂氧合酶(LO)产物在实验性肾小球肾炎中生成。15-S-羟二十碳四烯酸(一种15-LO产物)和脂氧素(5-LO与12-LO或15-LO之间的相互作用产物)可抵消白三烯的促炎作用。白细胞介素-4(IL-4)已被证明可上调人白细胞中15-LO基因的表达。基于与人15-LO的同源性,我们从白细胞介素-4(IL-4)刺激的大鼠白细胞中克隆了一个0.76 kbp的大鼠LO cDNA片段。推导的氨基酸序列与人15-LO和12-LO的同源性分别为71.0%和60.1%,与最近克隆的具有显著15-脂氧合酶活性的“白细胞型”大鼠12-脂氧合酶(迄今称为“12/15-LO”)的同源性为100%。在定量PCR分析中,利用缺失突变体生成内标cRNA。在注射NTS后24小时和48小时,肾小球12/15-LO mRNA水平相对于对照组显著升高,然后在72小时下降。NTS肾小球的RNA中12/15-LO mRNA水平高于未刺激的外周白细胞,这表明12/15-LO转录在天然和/或浸润的肾小球细胞中局部上调。NTS注射后16小时,肾小球IL-4 mRNA显著增加,然后减少,这表明T细胞衍生的IL-4在肾小球肾炎期间指导12/15-LO表达中可能发挥作用。这首次证明了细胞因子(IL-4)和脂氧合酶在体内的串联调控基因表达,二者均在免疫复合物介导的损伤中促进抗炎作用。

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