首页> 外文会议>IEEE International Workshop on Genomic Signal Processing and Statistics >BAYESIAN DETECTION OF RECURRENT COPY NUMBER ALTERATIONS ACROSS MULTIPLE ARRAY SAMPLES
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BAYESIAN DETECTION OF RECURRENT COPY NUMBER ALTERATIONS ACROSS MULTIPLE ARRAY SAMPLES

机译:贝叶斯检测多阵列样本的复制副本次数改变

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Copy number alterations (CNA) affecting small portions of chromosomes are difficult to identify. Advances in microarray technology now allow very high resolution scans of large cohorts of samples but at the price of severe degradation. Our proposed genome alteration detection algorithm (GADA) has been shown to be a highly accurate and efficient approach to analyze a single array sample. In this paper, the sparse Bayesian learning (SBL) used in GADA is extended to find CNA on multiple samples that share breakpoint positions but may have different magnitude of alteration. Our model is especially well suited to analyze sample replicates, i.e., multiple arrays from the same specimen. Our results show mat replicates greatly improve the accuracy and robustness in detection. In some cases, a single replicate sample offers an accuracy equivalent to a 2-fold increase in the signal to noise ratio, while reducing by up to a 50% the detection of false CNA caused by outliers. The computational cost of the algorithm is essentially linear O(NM) in the number of the microarray probes M and samples N. In conclusion, the multiple sample GADA (N-GADA) presented here appears to be a promising tool for finely locating small CNAs that are shared across multiple samples.
机译:影响影响小部分染色体的拷贝数改变(CNA)很难识别。微阵列技术的进步现在允许大量的样品群体的高分辨率扫描,但在严重降解的价格下。我们所提出的基因组改变检测算法(GADA)被证明是一种高度准确和有效的方法来分析单个阵列样本。在本文中,GADA中使用的稀疏贝叶斯学习(SBL)扩展到在共享断点位置的多个样本上找到CNA,但可能具有不同的改变程度。我们的模型特别适用于分析样品复制,即来自同一标本的多个阵列。我们的结果表明,垫子重复地提高了检测中的准确性和鲁棒性。在某些情况下,单个复制样品提供了相当于信号与信噪比的2倍增加的精度,同时通过异常值引起的假CNA的检测减少了50%。算法的计算成本基本上是线性O(nm)在微阵列探针M和样品N的数量中。总之,这里呈现的多个样品GADA(N-GADA)似乎是精细定位小CNA的有希望的工具在多个样本中共享。

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