Background: Although many algorithms are now available that aim to characterize different classes of structural variation, discovery of balanced rearrangements such as inversions remains an open problem. This is mainly due to the fact that breakpoints of such events typically lie within segmental duplications or common repeats, which reduces the mappability of short reads. The algorithms developed within the 1000 Genomes Project to identify inversions are limited to relatively short inversions, and there are currently no available algorithms to discover large inversions using high throughput sequencing technologies. Results: Here we propose a novel algorithm, Valor, to discover large inversions using new sequencing methods that provide long...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
Comparison of human genomes shows that along with single nucleotide polymorphisms and small indels, ...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...
BackgroundAlthough many algorithms are now available that aim to characterize different classes of s...
Cataloged from PDF version of article.Thesis (M.S.): Bilkent University, Department of Computer Engi...
Here we propose novel algorithms to characterize large (>40 Kbp) interspersed segmental duplications...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
Motivation: Several algorithms have been developed that use high-throughput sequencing technology to...
International audienceGenomes evolve with both mutations and large scale events, such as inversions,...
Structural Variations (SVs) are genomic rearrangements that include both copy-number variants,such a...
MOTIVATION:Several algorithms have been developed that use high-throughput sequencing technology to ...
The incomplete identification of structural variants (SVs) from whole-genome sequencing data limits ...
Understanding genetic variation has emerged as a key research problem of the post-genomic era. Until...
The incomplete identification of structural variants (SVs) from whole-genome sequencing data limits ...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
Comparison of human genomes shows that along with single nucleotide polymorphisms and small indels, ...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...
BackgroundAlthough many algorithms are now available that aim to characterize different classes of s...
Cataloged from PDF version of article.Thesis (M.S.): Bilkent University, Department of Computer Engi...
Here we propose novel algorithms to characterize large (>40 Kbp) interspersed segmental duplications...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
Motivation: Several algorithms have been developed that use high-throughput sequencing technology to...
International audienceGenomes evolve with both mutations and large scale events, such as inversions,...
Structural Variations (SVs) are genomic rearrangements that include both copy-number variants,such a...
MOTIVATION:Several algorithms have been developed that use high-throughput sequencing technology to ...
The incomplete identification of structural variants (SVs) from whole-genome sequencing data limits ...
Understanding genetic variation has emerged as a key research problem of the post-genomic era. Until...
The incomplete identification of structural variants (SVs) from whole-genome sequencing data limits ...
One of the most used techniques to study structural variation at a genome level is paired-end mappin...
Comparison of human genomes shows that along with single nucleotide polymorphisms and small indels, ...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...