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Application of scaling factors in simultaneous modeling of microarray data from diverse chips.

机译:比例因子在同时建模来自不同芯片的微阵列数据中的应用。

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PURPOSE: Microarrays have been utilized in many biological, physiological and pharmacological studies as a high-throughput genomic technique. Several generations of Affymetrix GeneChip microarrays are widely used in gene expression studies. However, differences in intensities of signals for different probe sets that represent the same gene on various types of Affymetrix chips make comparison of datasets complicated. MATERIALS AND METHODS: A power coefficient scaling factor was applied in the pharmacokinetic/pharmacodynamic (PK/PD) modeling to account for differences in probe set sensitivities (i.e., signal intensities). Microarray data from muscle and liver following methylprednisolone 50 mg/kg i.v. bolus and 0.3 mg/kg/h infusion regimens were taken as an exemplar. RESULTS: The scaling factor applied to the pharmacodynamic output function was used to solve the problem of intensity differences between probe sets. This approach yielded consistent pharmacodynamic parameters for the applied models. CONCLUSIONS: Modeling of pharmacodynamic/pharmacogenomic (PD/PG) data from diverse chips should be performed with caution due to differential probe set intensities. In such circumstances, a power scaling factor can be applied in the modeling.
机译:目的:微阵列已作为高通量基因组技术在许多生物学,生理学和药理学研究中得到利用。几代Affymetrix GeneChip芯片广泛用于基因表达研究。但是,代表各种基因型Affymetrix芯片上相同基因的不同探针组的信号强度差异使数据集的比较复杂。材料与方法:在药代动力学/药效学(PK / PD)模型中应用了功率系数比例因子,以说明探针组灵敏度(即信号强度)的差异。甲基强的松龙50 mg / kg腹腔注射后肌肉和肝脏的微阵列数据推注和0.3 mg / kg / h输注方案为例。结果:应用到药效输出函数的比例因子解决了探针组之间的强度差异问题。该方法为所应用的模型产生了一致的药效学参数。结论:由于探针集强度的差异,对来自不同芯片的药效学/药物基因组学(PD / PG)数据进行建模应谨慎。在这种情况下,可以在建模中应用功率缩放因子。

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