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VDAP-GUI:用于原始二代测序数据变异发现与注释的用户友好型流程

VDAP-GUI: a user-friendly pipeline for variant discovery and annotation of raw next-generation sequencing data.

作者信息

Menon Ramesh, Patel Namrata V, Mohapatra Amitbikram, Joshi Chaitanya G

机构信息

Department of Animal Biotechnology, College of Veterinary Sciences and Animal Husbandry, Anand Agricultural University, Anand, Gujarat, 388 001, India.

出版信息

3 Biotech. 2016 Jun;6(1):68. doi: 10.1007/s13205-016-0382-1. Epub 2016 Feb 15.

Abstract

Even though next-generation sequencing (NGS) has become an invaluable tool in molecular biology, several laboratories with NGS facilities lack trained Bioinformaticians for data analysis. Here, focusing on the variant detection application of NGS analysis, we have developed a fully automated pipeline, namely Variant Discovery and Annotation Tool-Graphical User Interface (VDAP-GUI), which detects and annotates single nucleotide polymorphisms and insertions/deletions from raw sequence reads. VDAP-GUI consolidates several proven methods in each step such as quality control, trimming, mapping, variant detection and annotation. It supports multiple NGS platforms and has four methodological choices for variant detection. Further, it can re-analyze existing data with alternate thresholds and generates easily interpretable reports in html and tab-delimited formats. Using VDAP-GUI, we have analyzed a publically available human whole-exome sequence dataset. VDAP-GUI is developed using Perl/Tk programming, and is available for free download and use at http://sourceforge.net/projects/vdapgui/ .

摘要

尽管下一代测序(NGS)已成为分子生物学中一项极具价值的工具,但一些拥有NGS设备的实验室却缺乏经过培训的生物信息学家来进行数据分析。在此,我们聚焦于NGS分析的变异检测应用,开发了一个全自动流程,即变异发现与注释工具-图形用户界面(VDAP-GUI),它可从原始序列读数中检测并注释单核苷酸多态性以及插入/缺失。VDAP-GUI在质量控制、修剪、比对、变异检测和注释等每个步骤中整合了多种经过验证的方法。它支持多个NGS平台,并且在变异检测方面有四种方法可供选择。此外,它可以使用替代阈值重新分析现有数据,并生成易于解释的html和制表符分隔格式的报告。我们使用VDAP-GUI分析了一个公开可用的人类全外显子序列数据集。VDAP-GUI是使用Perl/Tk编程开发的,可在http://sourceforge.net/projects/vdapgui/免费下载和使用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cebe/4754298/a8461c35db4e/13205_2016_382_Fig1_HTML.jpg

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