Publication date: Available online 2 December 2017
Source:Cancer Genetics
Author(s): Sarah H. Johnson, James B. Smadbeck, Stephanie A. Smoley, Athanasios Gaitatzes, Stephen J. Murphy, Faye R. Harris, Travis M. Drucker, Roman M. Zenka, Beth A. Pitel, Ross A. Rowsey, Nicole L. Hoppman, Umut Aypar, William R. Sukov, Robert B. Jenkins, Andrew L. Feldman, Hutton M. Kearney, George Vasmatzis
Mate-pair sequencing (MPseq), using long-insert, paired-end genomic libraries, is a powerful next-generation sequencing-based approach for the detection of genomic structural variants. SVAtools is a set of algorithms to detect both chromosomal rearrangements and large (>10kb) copy number variants (CNVs) in genome-wide MPseq data. SVAtools can also predict gene disruptions, gene fusions, and characterize the genomic structure of complex rearrangements.To illustrate the power of SVAtools' junction detection methods to provide comprehensive molecular karyotypes, MPseq data was compared against a set of samples previously characterized by traditional cytogenetic methods. Karyotype, FISH and chromosomal microarray (CMA), performed for 29 patients in a clinical laboratory setting, collectively revealed 285 breakpoints in 87 rearrangements. The junction detection methods of SVAtools detected 87% of these breakpoints compared to 48%, 42% and 57% for karyotype, FISH and CMA respectively. Breakpoint resolution was also reported to 1 kb or less and additional genomic rearrangement complexities not appreciable by standard cytogenetic techniques were revealed. For example, 63% of CNVs detected by CMA were shown by SVAtools' junction detection to occur secondary to a rearrangement other than a simple deletion or tandem duplication. SVAtools with MPseq provides comprehensive and accurate whole-genome junction detection with improved breakpoint resolution, compared to karyotype, FISH, and CMA combined. This approach to molecular karyotyping offers considerable diagnostic potential for the simultaneous detection of both novel and recurrent genomic rearrangements in hereditary and neoplastic disorders.
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Σφακιανάκης Αλέξανδρος
ΩτοΡινοΛαρυγγολόγος
Αναπαύσεως 5 Άγιος Νικόλαος
Κρήτη 72100
00302841026182
00306932607174
alsfakia@gmail.com
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- Design, synthesis, and evaluation of polyamine-mem...
- Supported carbon dots serve as high-performance ad...
- Preliminary survey of matrix effects in the Microw...
- Turn-on fluorescent sensor for the detection of gl...
- Theta-burst modulation of mid-ventrolateral prefro...
- The effect of gender, age and product type on the ...
- Toward new forms of meal sharing? Collective habit...
- Editorial Board
- Do the right thing: neural network mechanisms of m...
- The significant prognostic value of circulating tu...
- Breast cancer and synchronous multiple myeloma as ...
- Hepatocellular carcinoma in the era of immunotherapy
- Locally advanced pancreatic cancer: An emerging en...
- Is the limit of 60mg of oral morphine equivalent d...
- Meta-analysis of safety and efficacy of rolapitant...
- Title Page
- Information for Readers
- Table of Contents
- Familial Colorectal Cancer Type X (FCCTX) and the ...
- Anti-PD1/PDL1 induced psoriasis
- Complications in the treatment of mandibular condy...
- Effect of different resistance-training protocols ...
- Editorial Board
- OBC
- Ultrasound assessment of soft tissue augmentation ...
- Distribution and neurochemistry of porcine urinary...
- Polymer nanostructures for bioapplications induced...
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- Role of the orexin receptors within the nucleus ac...
- Evaluation of patients' compliance in different ag...
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