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Deep Sequencing of Target Linkage Assay-Identified Regions in Familial Breast Cancer: Methods,Analysis Pipeline and Troubleshooting
Authors:Juan Manuel Rosa-Rosa  Francisco Javier Gracia-Aznárez  Emily Hodges  Guillermo Pita  Michelle Rooks  Zhenyu Xuan  Arindam Bhattacharjee  Leonardo Brizuela  José M Silva  Gregory J Hannon  Javier Benitez
Abstract:

Background

The classical candidate-gene approach has failed to identify novel breast cancer susceptibility genes. Nowadays, massive parallel sequencing technology allows the development of studies unaffordable a few years ago. However, analysis protocols are not yet sufficiently developed to extract all information from the huge amount of data obtained.

Methodology/Principal Findings

In this study, we performed high throughput sequencing in two regions located on chromosomes 3 and 6, recently identified by linkage studies by our group as candidate regions for harbouring breast cancer susceptibility genes. In order to enrich for the coding regions of all described genes located in both candidate regions, a hybrid-selection method on tiling microarrays was performed.

Conclusions/Significance

We developed an analysis pipeline based on SOAP aligner to identify candidate variants with a high real positive confirmation rate (0.89), with which we identified eight variants considered candidates for functional studies. The results suggest that the present strategy might be a valid second step for identifying high penetrance genes.
Keywords:
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