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Analysis of the co-evolutions of correlations as a tool for QSAR-modeling of carcinogenicity: an unexpected good prediction based on a model that seems untrustworthy

机译:相关性共同演化分析作为QSAR致癌性建模的工具:基于似乎不可信任的模型的意外良好预测

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To validate QSAR models an external test set is increasingly used. However the definition of the compounds for the test set is still debated. We studied, co-evolutions of correlations between optimal descriptors and carcinogenicity (pTD50) for the subtraining, calibration, and test set. Weak correlations for the sub-training set are sometimes accompanied by quite good correlations for the external test set. This can be explained in terms of the probability theory and can help define a suitable test set. The simplified molecular input line entry system (SMILES) was used to represent the molecular structure. Correlation weights for calculating the optimal descriptors are related to fragments of the SMILES. The statistical quality of the model is: n=170, r2=0.6638, q2=0.6554, s=0.828, F=331 (sub-training set); n=170, r2=0.6609, r2pred=0.6520, s=0.825, F=331 (calibration set); and n=61, r2=0.7796, r2pred=0.7658, Rm2=0.7448, s=0.563, F=221 (test set). The calculations were done with CORAL software (http://www.insilico.eu/coral/).
机译:为了验证QSAR模型,越来越多地使用外部测试集。但是,对于测试装置中化合物的定义仍存在争议。我们研究了最佳描述符与致癌性(pTD50)之间的相关性的协同进化,用于训练,校准和测试集。子训练集的弱相关性有时会伴随着外部测试集的良好相关性。这可以用概率论来解释,并且可以帮助定义合适的测试集。简化的分子输入线输入系统(SMILES)用于表示分子结构。用于计算最佳描述符的相关权重与SMILES的片段有关。模型的统计质量为:n = 170,r2 = 0.6638,q2 = 0.6554,s = 0.828,F = 331(子训练集); n = 170,r2 = 0.6609,r2pred = 0.6520,s = 0.825,F = 331(校准集);并且n = 61,r2 = 0.7796,r2pred = 0.7658,Rm2 = 0.7448,s = 0.563,F = 221(测试集)。使用CORAL软件(http://www.insilico.eu/coral/)进行计算。

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