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优化抗病毒联合疗法的方法。

Methods for optimizing antiviral combination therapies.

作者信息

Beerenwinkel Niko, Lengauer Thomas, Däumer Martin, Kaiser Rolf, Walter Hauke, Korn Klaus, Hoffmann Daniel, Selbig Joachim

机构信息

Max Planck Institute for Informatics, Stuhlsatzenhausweg 85, 66123 Saarbrücken, Germany.

出版信息

Bioinformatics. 2003;19 Suppl 1:i16-25. doi: 10.1093/bioinformatics/btg1001.

Abstract

MOTIVATION

Despite some progress with antiretroviral combination therapies, therapeutic success in the management of HIV-infected patients is limited. The evolution of drug-resistant genetic variants in response to therapy plays a key role in treatment failure and finding a new potent drug combination after therapy failure is considered challenging.

RESULTS

To estimate the activity of a drug combination against a particular viral strain, we develop a scoring function whose independent variables describe a set of antiviral agents and viral DNA sequences coding for the molecular targets of the respective drugs. The construction of this activity score involves (1) predicting phenotypic drug resistance from genotypes for each drug individually, (2) probabilistic modeling of predicted resistance values and integration into a score for drug combinations, and (3) searching through the mutational neighborhood of the considered strain in order to estimate activity on nearby mutants. For a clinical data set, we determine the optimal search depth and show that the scoring scheme is predictive of therapeutic outcome. Properties of the activity score and applications are discussed.

摘要

动机

尽管抗逆转录病毒联合疗法取得了一些进展,但在管理HIV感染患者方面的治疗成功仍然有限。治疗过程中耐药基因变异的演变在治疗失败中起着关键作用,并且在治疗失败后找到新的有效药物组合被认为具有挑战性。

结果

为了估计药物组合对特定病毒株的活性,我们开发了一种评分函数,其自变量描述了一组抗病毒药物和编码各药物分子靶点的病毒DNA序列。该活性评分的构建涉及:(1)分别从每种药物的基因型预测表型耐药性;(2)对预测的耐药值进行概率建模并整合为药物组合的评分;(3)在考虑的病毒株的突变邻域中进行搜索,以估计对附近突变体的活性。对于一个临床数据集,我们确定了最佳搜索深度,并表明该评分方案可预测治疗结果。还讨论了活性评分的特性和应用。

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