Unknown

Dataset Information

0

High-resolution detection of chromosomal rearrangements in leukemias through mate pair whole genome sequencing.

ABSTRACT: The detection of recurrent somatic chromosomal rearrangements is standard of care for most leukemia types. Even though karyotype analysis-a low-resolution genome-wide chromosome analysis-is still the gold standard, it often needs to be complemented with other methods to increase resolution. To evaluate the feasibility and applicability of mate pair whole genome sequencing (MP-WGS) to detect structural chromosomal rearrangements in the diagnostic setting, we sequenced ten bone marrow samples from leukemia patients with recurrent rearrangements. Samples were selected based on cytogenetic and FISH results at leukemia diagnosis to include common rearrangements of prognostic relevance. Using MP-WGS and in-house bioinformatic analysis all sought rearrangements were successfully detected. In addition, unexpected complexity or additional, previously undetected rearrangements was unraveled in three samples. Finally, the MP-WGS analysis pinpointed the location of chromosome junctions at high resolution and we were able to identify the exact exons involved in the resulting fusion genes in all samples and the specific junction at the nucleotide level in half of the samples. The results show that our approach combines the screening character from karyotype analysis with the specificity and resolution of cytogenetic and molecular methods. As a result of the straightforward analysis and high-resolution detection of clinically relevant rearrangements, we conclude that MP-WGS is a feasible method for routine leukemia diagnostics of structural chromosomal rearrangements.

SUBMITTER: Tran AN 

PROVIDER: S-EPMC5846771 | biostudies-literature | 2018

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

High-resolution detection of chromosomal rearrangements in leukemias through mate pair whole genome sequencing.

Tran Anh Nhi AN   Taylan Fulya F   Zachariadis Vasilios V   Ivanov Öfverholm Ingegerd I   Lindstrand Anna A   Vezzi Francesco F   Lötstedt Britta B   Nordenskjöld Magnus M   Nordgren Ann A   Nilsson Daniel D   Barbany Gisela G  

PloS one 20180312 3

The detection of recurrent somatic chromosomal rearrangements is standard of care for most leukemia types. Even though karyotype analysis-a low-resolution genome-wide chromosome analysis-is still the gold standard, it often needs to be complemented with other methods to increase resolution. To evaluate the feasibility and applicability of mate pair whole genome sequencing (MP-WGS) to detect structural chromosomal rearrangements in the diagnostic setting, we sequenced ten bone marrow samples from  ...[more]

Similar Datasets

Unknown Mate pair sequencing for the detection of chromosomal aberrations in patients with intellectual disability and congenital malformations.
| S-EPMC3992577 | biostudies-literature
Unknown Gene rearrangements in hormone receptor negative breast cancers revealed by mate pair sequencing.
| S-EPMC3600027 | biostudies-literature
Genomics Mate pair sequencing
| PRJEB4453 | ENA
Genomics Evaluation of copy number variation detection between high-resolution array CGH and low-coverage short-insert and mate-pair whole-genome sequencing
2018-06-26 | GSE105092 | GEO
Unknown Mate pair sequencing of whole-genome-amplified DNA following laser capture microdissection of prostate cancer.
| S-EPMC3473372 | biostudies-literature
Unknown A de novo 10q11.23q22.1 deletion detected by whole genome mate-pair sequencing: a case report.
| S-EPMC8167982 | biostudies-literature
Unknown Accurate Breakpoint Mapping in Apparently Balanced Translocation Families with Discordant Phenotypes Using Whole Genome Mate-Pair Sequencing.
| S-EPMC5225008 | biostudies-literature
Unknown Structural Chromosomal Rearrangements Require Nucleotide-Level Resolution: Lessons from Next-Generation Sequencing in Prenatal Diagnosis.
| S-EPMC5097935 | biostudies-literature
Unknown Balanced Chromosomal Rearrangement Detection by Low-Pass Whole-Genome Sequencing.
| S-EPMC5924704 | biostudies-literature
Unknown Copy number variant analysis using genome-wide mate-pair sequencing.
| S-EPMC6117203 | biostudies-literature