Upregulation of Beta 1 and Arachidonic Acid Metabolizing Enzymes in the Mouse Hearts and Kidneys after Sub Chronic Administration of Rofecoxib.

IF 2.4 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Noor Askar, Yazun Jarrar, Munir Gharaibeh, Mohammad Alqudah
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引用次数: 0

Abstract

Background: An imbalance in the levels of arachidonic acid (ARA) metabolites in cardiovascular disorders and drug-induced cardiotoxicity have been previously described.

Aims: This study aimed to investigate the influence of cyclooxygenase-2 (COX-2) selective inhibitors on the gene expression of ARA-metabolizing genes and beta1 gene in the hearts and kidneys of experimental mice.

Methods: Thirty-five balb/c mice were divided into five groups with seven mice per group. The groups were then given two distinct types of COX-2 selective inhibitors, rofecoxib and celecoxib, in two different doses equivalent to those used in human treatment for 30 days. The mRNA expression of beta1, ace2, and ARA-metabolizing genes, coxs, lipoxygenases (aloxs), and cytochrome p450 (cyp450s) in mice heart and kidneys were assessed. Genes were analyzed using real-time polymerase chain reaction analysis. In addition, rofecoxib-induced histological alterations were examined.

Results: It was found that only the high dose of rofecoxib (5 mg/kg) caused toxicological alterations, a finding that was indicated by a significant increase (P < 0.05) in the relative weight of the mouse hearts and increase in the ventricle wall thickness as observed through pathohistological examination. This increase was associated with a significant increase in the mRNA expression level of the beta1 receptor in both the heart and kidneys of the mice (53- and 12-fold, respectively). The expression of both cox1 and 2 genes was increased 4-fold in the kidneys. In addition, the expression of the alox12 gene increased significantly (by 67-fold in the heart and by 21-fold in the kidney), while alox15 gene expression was upregulated in the heart by 8-fold and 5-fold in the kidney. The genes responsible for synthesizing 20- Hydroxyeicosatetraenoic acid (cyp4a12 and cyp1a1) were significantly upregulated (P < 0.05) in the hearts of high-dose rofecoxib-treated mice by 7- and 17 -fold, respectively. In addition, the expression of epoxyeicosatrienoic acid-synthesizing genes, cyp2c29 and cyp2j5, was increased significantly (P < 0.05) in the hearts of high-dose rofecoxib-treated mice by 4- and 16-fold, respectively.

Conclusion: Rofecoxib caused upregulation of the mRNA expression of the beta 1 gene in association with increased expression of ARA-metabolizing genes in mouse hearts and kidneys. These findings may help us understand the molecular cardiotoxic mechanism of rofecoxib.

亚慢性给药罗非昔布后小鼠心脏和肾脏β 1和花生四烯酸代谢酶的上调。
背景:花生四烯酸(ARA)代谢物水平失衡在心血管疾病和药物引起的心脏毒性中已有报道。目的:研究环氧合酶-2 (COX-2)选择性抑制剂对实验小鼠心脏和肾脏中ara代谢基因和β 1基因表达的影响。方法:35只balb/c小鼠随机分为5组,每组7只。然后给予两种不同类型的COX-2选择性抑制剂,罗非昔布和塞来昔布,两种不同的剂量相当于人类治疗中使用的剂量,为期30天。测定小鼠心脏和肾脏中β 1、ace2和ala代谢基因、cox、脂氧合酶(aloxs)和细胞色素p450 (cyp450)的mRNA表达。采用实时聚合酶链式反应分析基因。此外,还检查了罗非昔布诱导的组织学改变。结果:病理组织学检查发现,只有高剂量(5 mg/kg)的罗非昔布才会引起毒理学改变,小鼠心脏相对重量显著增加(P < 0.05),心室壁厚度显著增加。这种增加与小鼠心脏和肾脏中β 1受体mRNA表达水平的显著增加有关(分别为53倍和12倍)。在肾脏中,cox1和2基因的表达增加了4倍。此外,alox12基因的表达显著增加(心脏增加67倍,肾脏增加21倍),alox15基因在心脏和肾脏中的表达分别上调8倍和5倍。高剂量罗非昔布处理小鼠心脏中负责合成20-羟基二碳四烯酸(cyp4a12和cyp1a1)的基因分别显著上调7倍和17倍(P < 0.05)。此外,高剂量罗非昔布处理小鼠心脏中环氧二碳三烯酸合成基因cyp2c29和cyp2j5的表达分别显著增加了4倍和16倍(P < 0.05)。结论:罗非昔布引起小鼠心脏和肾脏β 1基因mRNA表达上调,与ara代谢基因表达增加有关。这些发现可能有助于我们了解罗非昔布的分子心脏毒性机制。
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来源期刊
Current molecular pharmacology
Current molecular pharmacology Pharmacology, Toxicology and Pharmaceutics-Drug Discovery
CiteScore
4.90
自引率
3.70%
发文量
112
期刊介绍: Current Molecular Pharmacology aims to publish the latest developments in cellular and molecular pharmacology with a major emphasis on the mechanism of action of novel drugs under development, innovative pharmacological technologies, cell signaling, transduction pathway analysis, genomics, proteomics, and metabonomics applications to drug action. An additional focus will be the way in which normal biological function is illuminated by knowledge of the action of drugs at the cellular and molecular level. The journal publishes full-length/mini reviews, original research articles and thematic issues on molecular pharmacology. Current Molecular Pharmacology is an essential journal for every scientist who is involved in drug design and discovery, target identification, target validation, preclinical and clinical development of drugs therapeutically useful in human disease.
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