Schroth Werner, Winter Stefan, Mürdter Thomas, Schaeffeler Elke, Eccles Diana, Eccles Bryony, Chowbay Balram, Khor Chiea C, Tfayli Arafat, Zgheib Nathalie K, Eichelbaum Michel, Schwab Matthias, Brauch Hiltrud
Dr. Margarete Fischer-Bosch-Institute of Clinical PharmacologyStuttgart, Germany.
Department of Clinical Pharmacology, University of TübingenTübingen, Germany.
Front Pharmacol. 2017 Aug 24;8:582. doi: 10.3389/fphar.2017.00582. eCollection 2017.
Prediction of impaired tamoxifen (TAM) to endoxifen metabolism may be relevant to improve breast cancer treatment, e.g., via TAM dose increase. The polymorphic cytochrome P450 2D6 (CYP2D6) strongly determines an individual's capacity for endoxifen formation, however, CYP2D6 phenotype assignments inferred from genotype widely differ between studies. Thus, we modeled plasma endoxifen predictability depending on variable CYP2D6 genotype groupings. CYP2D6 diplotype and metabolite plasma concentrations were assessed in 908 pre- and post-menopausal estrogen receptor (ER)-positive, TAM treated early breast cancer patients of Caucasian ( = 678), Middle-Eastern Arab ( = 77), and Asian ( = 153) origin. Robust coefficients of determination () were estimated for endoxifen (E) or metabolic ratio endoxifen/desmethyl-TAM (E/DMT) as dependent and different CYP2D6 phenotype assignments as independent variables. Allele activity scores (ASs) were modified with respect to a reduced 10 allele activity. Predictability of endoxifen plasma concentrations above the clinical threshold of 5.9 ng/mL was investigated by receiver operating characteristic (ROC) analysis. CYP2D6 diplotypes ( = 898) were strongly associated with E and E/DMT independent of age ( < 10). Across all ethnicities, 68-82% inter-patient variability of E/DMT was explained by CYP2D6 diplotype, while plasma endoxifen was predictable by 39-58%. The previously used codeine specific phenotype classification showed worse prediction for both endpoints particularly in Asians (median < 20%; < 10). Downgrading of 10 activity slightly improved the explanatory value of metabolizer phenotype ( < 0.002). Endoxifen plasma concentrations above the clinical threshold of 5.9 ng/mL were achieved in 82.3% of patients and were predictable (96% sensitivity, 57% specificity) by CYP2D6 diplotypes with AS > 0.5, i.e., omitting PM/PM and PM/IM patients. The CYP2D6 explanatory power for active drug level assessment is maximized by TAM-specific phenotype assignments while a genotype cutoff that separates PM/PM and PM/IM from the remaining patients may improve clinical benefit via increased endoxifen concentrations.
预测他莫昔芬(TAM)向4-羟基他莫昔芬代谢受损可能与改善乳腺癌治疗相关,例如通过增加TAM剂量。多态性细胞色素P450 2D6(CYP2D6)强烈决定个体生成4-羟基他莫昔芬的能力,然而,不同研究中根据基因型推断的CYP2D6表型分类差异很大。因此,我们根据可变的CYP2D6基因型分组对血浆4-羟基他莫昔芬的可预测性进行建模。在908名绝经前和绝经后雌激素受体(ER)阳性、接受TAM治疗的早期乳腺癌患者中评估了CYP2D6双倍型和代谢物血浆浓度,这些患者来自白种人(n = 678)、中东阿拉伯人(n = 77)和亚洲人(n = 153)。以4-羟基他莫昔芬(E)或代谢比4-羟基他莫昔芬/去甲基-TAM(E/DMT)为因变量,不同的CYP2D6表型分类为自变量,估计了稳健的决定系数(R²)。根据降低的10个等位基因活性对等位基因活性评分(ASs)进行了修正。通过受试者工作特征(ROC)分析研究了血浆4-羟基他莫昔芬浓度高于临床阈值5.9 ng/mL的可预测性。CYP2D6双倍型(n = 898)与E和E/DMT密切相关,与年龄无关(P < 0.001)。在所有种族中,CYP2D6双倍型解释了E/DMT患者间68 - 82%的变异性,而血浆4-羟基他莫昔芬的可预测性为39 - 58%。先前使用的可待因特异性表型分类对两个终点的预测较差,尤其是在亚洲人中(中位数< 20%;P < 0.001)。将10个活性等级下调略微提高了代谢型表型的解释价值(P < 0.002)。82.3%的患者血浆4-羟基他莫昔芬浓度高于临床阈值5.9 ng/mL,并且通过AS > 0.5的CYP2D6双倍型可预测(敏感性96%,特异性57%),即排除PM/PM和PM/IM患者。对于活性药物水平评估,CYP2D6的解释力通过TAM特异性表型分类最大化,而将PM/PM和PM/IM与其余患者区分开的基因型临界值可能通过增加4-羟基他莫昔芬浓度来改善临床获益。
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