小鼠肝脏中Cyp2a5表达和活性的品系间差异。
Interstrain differences in the expression and activity of Cyp2a5 in the mouse liver.
作者信息
Poça Katia S, Parente Thiago E M, Chagas Lucas F, Leal Bruna S, Leal Hellen S, Paumgartten Francisco J R, De-Oliveira Ana C A X
机构信息
Laboratory of Environmental Toxicology, Department of Biological Sciences, National School of Public Health, Oswaldo Cruz Foundation, FIOCRUZ, Av. Brasil 4036, Rio de Janeiro, RJ, 21040-361, Brazil.
出版信息
BMC Res Notes. 2017 Mar 15;10(1):125. doi: 10.1186/s13104-017-2435-x.
BACKGROUND
Cytochrome P450 2A5 (Cyp2a5), a mouse enzyme orthologous of human CYP2A6, catalyzes a number of toxicologically important reactions, including the metabolism of nicotine, aflatoxin B1, and several other xeno- and endobiotics. Cyp2a5 expression is complex and not yet fully understood. We investigated inter-strain differences in the activity and mRNA expression of hepatic Cyp2a5. Cyp1a1/2 and Cyp2b9/10 activities were evaluated for comparative purposes. Data on the interstrain differences in the expression and activity of Cyp2a5 are important to select a suitable mouse model for studying CYP2A6-mediated metabolism.
RESULTS
Activity of Cyp2a5 (coumarin 7-hydroxylase) was highest in DBA-2 and DBA-1, intermediate in B6D2F1 (hybrid) and low in the remaining strains (C57BL/6, C57BL/10, CBA, BALB/cAn, SW). Contrasting with the activity, background levels of Cyp2a4/5 mRNA did not differ between high- and low-activity murine strains. Phenobarbital (PB, 80 mg/kg body weight/day × 3 days, i.p.) increased Cyp2a5, Cyp1a1/2 (ethoxyresorufin-O-deethylase) and Cyp2b9/10 (bezyloxyresorufin-O-debenzylase) activities while only Cyp2a5 was enhanced by pyrazole (PYR, 100 mg/kg body weight/day × 3 days, i.p.). Inductions of Cyp2a5 activity by PYR and PB were accompanied by increases of Cyp2a4/5 mRNA. PYR and PB did not upregulate heme oxygenase-1 (hmox-1) mRNA expression in any strain, a finding that is apparently at odds with the notion that Cyp2a5 and hmox-1 inductions are coordinated events.
CONCLUSIONS
Since background levels of Cyp2a4/5 gene transcripts of high-activity strains did not differ from those of low-activity mice, distinct constitutive activities did not result from different transcription rates and/or mRNA half-lives. Results therefore suggested that interstrain differences in constitutive activity of Cyp2a5 possibly arise from distinct translation efficiencies, protein half-lives and/or enzyme kinetics toward the substrate. Data from this study indicated that all tested strains are suitable models for studying toxicants that are substrates for human CYP2A6; DBA-2, DBA-1 and the hybrid B62DF1, however, have the advantage of presenting high constitutive activities of Cyp2a5.
背景
细胞色素P450 2A5(Cyp2a5)是人类CYP2A6的小鼠同源酶,催化许多毒理学上重要的反应,包括尼古丁、黄曲霉毒素B1以及其他几种外源性和内源性生物活性物质的代谢。Cyp2a5的表达情况复杂,尚未完全明确。我们研究了肝脏Cyp2a5活性和mRNA表达的品系间差异。为作比较,还评估了Cyp1a1/2和Cyp2b9/10的活性。Cyp2a5表达和活性的品系间差异数据对于选择合适的小鼠模型来研究CYP2A6介导的代谢具有重要意义。
结果
Cyp2a5(香豆素7 - 羟化酶)的活性在DBA - 2和DBA - 1中最高,在B6D2F1(杂交种)中居中,在其余品系(C57BL/6、C57BL/10、CBA、BALB/cAn、SW)中较低。与活性情况相反,高活性和低活性小鼠品系中Cyp2a4/5 mRNA的背景水平并无差异。苯巴比妥(PB,80毫克/千克体重/天×3天,腹腔注射)可提高Cyp2a5、Cyp1a1/2(乙氧基异吩恶唑酮 - O - 脱乙基酶)和Cyp2b9/10(苄氧基异吩恶唑酮 - O - 脱苄基酶)的活性,而吡唑(PYR,100毫克/千克体重/天×3天,腹腔注射)仅增强Cyp2a5的活性。PYR和PB对Cyp2a5活性的诱导伴随着Cyp2a4/5 mRNA的增加。PYR和PB在任何品系中均未上调血红素加氧酶 - 1(hmox - 1)mRNA的表达,这一发现显然与Cyp2a5和hmox - 1诱导是协同事件的观点相悖。
结论
由于高活性品系的Cyp2a4/5基因转录本的背景水平与低活性小鼠并无差异,不同的组成型活性并非由不同的转录速率和/或mRNA半衰期导致。因此,结果表明Cyp2a5组成型活性的品系间差异可能源于不同的翻译效率、蛋白质半衰期和/或酶对底物的动力学特性。本研究数据表明,所有测试品系都是研究作为人类CYP2A6底物的毒物的合适模型;然而,DBA - 2、DBA - 1和杂交种B62DFl具有Cyp2a5组成型活性高的优势。
Zotero 插件