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Combined sequence and sequence-structure based methods for analyzing FGF23 CYP24A1 and VDR genes

机译:基于序列和序列结构的组合方法分析FGF23CYP24A1和VDR基因

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摘要

FGF23, CYP24A1 and VDR altogether play a significant role in genetic susceptibility to chronic kidney disease (CKD). Identification of possible causative mutations may serve as therapeutic targets and diagnostic markers for CKD. Thus, we adopted both sequence and sequence-structure based SNP analysis algorithm in order to overcome the limitations of both methods. We explore the functional significance towards the prediction of risky SNPs associated with CKD. We assessed the performance of four widely used pathogenicity prediction methods. We compared the performances of the programs using Mathews correlation Coefficient ranged from poor (MCC = 0.39) to reasonably good (MCC = 0.42). However, we got the best results for the combined sequence and structure based analysis method (MCC = 0.45). 4 SNPs from FGF23 gene, 8 SNPs from VDR gene and 13 SNPs from CYP24A1 gene were predicted to be the causative agents for human diseases. This study will be helpful in selecting potential SNPs for experimental study from the SNP pool and also will reduce the cost for identification of potential SNPs as a genetic marker.
机译:FGF23,CYP24A1和VDR在慢性肾脏病(CKD)的遗传易感性中共起重要作用。可能的致病突变的鉴定可以作为CKD的治疗靶标和诊断标记。因此,为了克服两种方法的局限性,我们同时采用了基于序列和基于序列结构的SNP分析算法。我们探索功能性意义对与CKD相关的危险SNP的预测。我们评估了四种广泛使用的致病性预测方法的性能。我们使用Mathews相关系数比较了程序的性能,其范围从较差(MCC = 0.39)到相当不错(MCC = 0.42)。但是,对于基于序列和结构的组合分析方法(MCC = 0.45),我们获得了最佳结果。 FGF23基因的4个SNP,VDR基因的8个SNP和CYP24A1基因的13个SNP被预测为人类疾病的病原体。这项研究将有助于从SNP库中选择潜在的SNP用于实验研究,还将减少鉴定潜在SNP作为遗传标记的成本。

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