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Limitations in Adjuvant Breast Cancer Therapy: The Predictive Potential of Pharmacogenetics and Pharmacogenomics

机译:辅助乳腺癌治疗的局限性:药物遗传学和药物基因组学的预测潜力

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Adjuvant therapy improves survival in breast cancer patients. However, both antihormonal agents and cytostatic chemotherapy meet with variable success. We have searched the literature for biological causes of variability in drug response. Evidence suggests that additional markers may be introduced because of their potentially predictive value in adjuvant therapy: i) overexpression of epidermal growth factor receptor is likely inversely correlated to the sensitivity to estrogen antagonists; ii) presence of the GAB2 adaptor protein and of the ABCC3 and mdr-1 efflux pumps modulates taxane sensitivity in HER2-positive breast cancer; and iii) CYP2D6 genotyping should be a routine measure to avoid failure of tamox-ifen treatment. In contrast, there is little in the way of genetic evidence for differences in the pharmacokinetics of other antihormonal or cytostatic drugs. Nevertheless, genotypes may affect efficacy and toxicity of cytostatic drugs (e.g. doxorubicin), but this evidence has to be confirmed by prospective trials.
机译:辅助治疗可提高乳腺癌患者的生存率。但是,抗激素药和细胞抑制化学疗法都取得了一定的成功。我们已经在文献中搜索了药物反应变异的生物学原因。有证据表明可能会引入其他标志物,因为它们在辅助治疗中具有潜在的预测价值:i)表皮生长因子受体的过表达可能与对雌激素拮抗剂的敏感性呈负相关; ii)GAB2衔接蛋白以及ABCC3和mdr-1外排泵的存在调节HER2阳性乳腺癌中紫杉烷的敏感性。 iii)CYP2D6基因分型应作为常规方法,以避免他莫昔芬治疗失败。相反,其他抗激素或抑制细胞生长药物的药代动力学差异的遗传学证据很少。尽管如此,基因型可能会影响细胞抑制药物(例如阿霉素)的功效和毒性,但这一证据必须通过前瞻性试验予以证实。

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