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HLA-VBSeq: accurate HLA typing at full resolution from whole-genome sequencing data

机译:HLA-VBSEQ:精确的HLA以全基因组测序数据全分辨率打字

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Background: Human leucocyte antigen (HLA) genes play an important role in determining the outcome of organ transplantation and are linked to many human diseases. Because of the diversity and polymorphisms of HLA loci, HLA typing at high resolution ischallenging even with whole-genome sequencing data.Results: We have developed a computational tool, HLA-VBSeq, to estimate the most probable HLA alleles at full (8-digit) resolution from whole-genome sequence data. HLA-VBSeq simultaneously optimizes read alignments to HLA allele sequences and abundance of reads on HLA alleles by variational Bayesian inference. We show the effectiveness of the proposed method over other methods through the analysis of predicting HLA types for HLA class I (HLA-A, -B and -C) and class II (HLA-DQA1.-DQB1 and -DRB1) loci from the simulation data of various depth of coverage, and real sequencing data of human trio samples.Conclusions: HLA-VBSeq is an efficient and accurate HLA typing method using high-throughput sequencing data without the need of primer design for HLA loci. Moreover, it does not assume any prior knowledge about HLA allele frequencies, and hence HLA-VBSeqis broadly applicable to human samples obtained from a genetically diverse population.
机译:背景:人的白细胞抗原(HLA)基因在确定器官移植的结果并与许多人类疾病相关起作用重要作用。由于HLA LOCI的多样性和多态性,HLA在高分辨率isChallenging中键入即使是全基因组测序数据。结果:我们已经开发了一个计算工具HLA-VBSeq,以估计满满的最可能的HLA等位基因(8位数)来自全基因组序列数据的分辨率。 HLA-VBSEQ通过变分贝叶斯推理同时优化对HLA等位基因序列的读取对齐和HLA等位基因的读数。我们通过分析HLA类I(HLA-A,-B和-C)和II类(HLA-DQA1.-DQB1和-DRB1)基因座的预测HLA类型来展示所提出的方法对其他方法的有效性各种覆盖深度的仿真数据,以及人类三重奏样本的实际排序数据。结论:HLA-VBSEQ是一种使用高通量测序数据的高效准确的HLA键入方法,而无需为HLA基因座进行底漆设计。此外,它不假设关于HLA等位基因频率的任何先验知识,因此HLA-VBSeqis广泛适用于从遗传群体获得的人类样品。

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