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Distinguishing rational from irrational applications of pharmacogenetic synergies from the bench to clinical trials.

机译:从实验室到临床试验,从药物遗传协同的非理性应用中区分理性与非理性。

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摘要

Single therapeutic agents very often fail in unselected patients. It is therefore commonplace to combine an agent specifically with a selected patient subgroup or with another agent. To support such efforts, it is useful to clarify the distinctions between the terms and the mathematical models used in analyzing combinations. To incorporate molecular disease classifications, the familiar concept of the therapeutic window is modified to define a pharmacogenetic window, which is an unambiguous numerical measure of the magnitude of interaction produced by a combination, and to define a test of pharmacogenetic synergy. In contrast, certain common comparative methods, such as vertical windows (comparing effects at a given dose) and animal models of mutational targets may be dominated by undesirable features. Although this discussion is oriented towards cancer therapy, an extension of these concepts to other comparative biologic assays is feasible and advisable.
机译:在未选择的患者中,单一治疗剂经常失败。因此,通常将一种药剂与选定的患者亚组或另一种药剂专门结合。为支持此类工作,阐明术语和用于分析组合的数学模型之间的区别是很有用的。为了合并分子疾病分类,对治疗窗口的熟悉概念进行了修改,以定义一个药源窗口,这是对组合产生的相互作用程度的明确数值度量,并定义了药源协同作用的测试。相反,某些常见的比较方法,例如垂直窗口(给定剂量下的比较效果)和突变靶标的动物模型可能被不良特征所控制。尽管此讨论的重点是癌症治疗,但将这些概念扩展到其他比较性生物测定是可行且可取的。

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