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首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >PXR pharmacogenetics: association of haplotypes with hepatic CYP3A4 and ABCB1 messenger RNA expression and doxorubicin clearance in Asian breast cancer patients.
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PXR pharmacogenetics: association of haplotypes with hepatic CYP3A4 and ABCB1 messenger RNA expression and doxorubicin clearance in Asian breast cancer patients.

机译:PXR药物遗传学:亚洲乳腺癌患者单倍型与肝CYP3A4和ABCB1信使RNA表达及阿霉素清除率的关系。

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PURPOSE: To characterize pregnane X receptor (PXR) polymorphic variants in healthy Asian populations [Chinese, Malay and Indian (n=100 each)], and to investigate the association between PXR haplotypes and hepatic mRNA expression of PXR and its downstream target genes, CYP3A4 and ABCB1, as well as their influence on the clearance of doxorubicin in Asian breast cancer patients. EXPERIMENTAL DESIGN: PXR genotyping was done by direct DNA sequencing, and PXR haplotypes and haplotype clusters were derived by expectation-maximization algorithm. Genotype-phenotype correlations were done using Mann-Whitney U test and Kruskal-Wallis test. RESULTS: Significant interethnic variations were observed in PXR pharmacogenetics among the three Asian ethnic groups. The expression of PXR mRNA in liver tissues harboring the PXR*1B haplotype clusters was 4-fold lower compared with the non-PXR*1B (*1A + *1C) haplotype clusters [PXR*1B versus PXR*1A; P=0.015; PXR*1B versus PXR*1C; P=0.023]. PXR*1B-bearing liver tissues were associated with significantly lower expression of CYP3A4 (PXR*1B versus non-PXR*1B, P=0.030) and ABCB1 (PXR*1B versus non-PXR*1B, P=0.060) compared with non-PXR*1B-bearing liver tissues. Doxorubicin clearance in breast cancer patients harboring the PXR*1B haplotypes was significantly lower compared with patients carrying the non-PXR*1B haplotypes [PXR*1B versus non-PXR*1B, CL/BSA (L h(-1) m(-2)): 20.84 (range, 8.68-29.24) versus 24.85 (range, 13.80-55.66), P=0.022]. CONCLUSIONS: This study showed that PXR*1B was associated with reduced hepatic mRNA expression of PXR and its downstream targets, CYP3A4 and ABCB1. Genotype-phenotype correlates in breast cancer patients showed PXR*1B to be significantly associated with lower doxorubicin clearance, suggesting that PXR haplotype constitution could be important in influencing interindividual and interethnic variations in disposition of its putative drug substrates.
机译:目的:表征健康亚洲人群[中国人,马来人和印度人(每人n = 100)]孕烷X受体(PXR)多态性变异,并研究PXR单倍型与PXR及其下游靶基因肝mRNA表达之间的关系, CYP3A4和ABCB1以及它们对亚洲乳腺癌患者中阿霉素清除率的影响。实验设计:通过直接DNA测序进行PXR基因分型,并通过期望最大化算法推导PXR单倍型和单倍型簇。使用Mann-Whitney U检验和Kruskal-Wallis检验进行基因型与表型的相关性。结果:在三个亚洲族裔的PXR药物遗传学中观察到显着的种族间差异。与非PXR * 1B(* 1A + * 1C)单倍型簇相比,带有PXR * 1B单倍型簇的肝组织中PXR mRNA的表达低4倍[PXR * 1B与PXR * 1A; P = 0.015; PXR * 1B与PXR * 1C; P = 0.023]。与不含PXR * 1B的肝组织相比,与不含PXR * 1B的肝组织相比,CYP3A4(PXR * 1B与非PXR * 1B,P = 0.030)和ABCB1(PXR * 1B与非PXR * 1B,P = 0.060)的表达显着降低-PXR * 1B-肝组织。与携带非PXR * 1B单倍型的患者相比,具有PXR * 1B单倍型的乳腺癌患者中的阿霉素清除率显着降低[PXR * 1B与非PXR * 1B,CL / BSA(L h(-1)m(- 2)):20.84(范围8.68-29.24)与24.85(范围13.80-55.66),P = 0.022]。结论:本研究表明PXR * 1B与PXR及其下游靶标CYP3A4和ABCB1的肝mRNA表达降低有关。乳腺癌患者的基因型与表型相关性表明PXR * 1B与较低的阿霉素清除率显着相关,这表明PXR单倍体构成可能在影响个体和种族间的推定药物底物配置方面很重要。

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