Optical Genome Mapping in Routine Cytogenetic Diagnosis of Acute Leukemia

Soler, Gwendoline; Ouédraogo, Zangbéwendé Guy; Goumy, Carole; Lebecque, Benjamin; Requena, Gaspar Aspas; Ravinet, Aurélie; Kanold, Justyna; Véronèse, Lauren; Tchirkov, Andréï

doi:10.3390/cancers15072131

Cited by 7 publications

(8 citation statements)

References 40 publications

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“…Around 20% of leukemic blasts are required for SNP‐array in a diagnostic setting for large CN alterations 34 , 35 . Our study and others 14 , 36 , 37 showed that OGM performance on samples with blast amounts of about 20%–30% could also detect alterations observed by conventional diagnostic methods. Hence, OGM could be an attractive option for routine diagnostic workup of hematological malignancies, as it has a fast turnaround time of ≈5 days from sample acquisition to data analysis.…”

Section: Discussionsupporting

confidence: 61%

Optical Genome Mapping Identifies Novel Recurrent Structural Alterations in Childhood ETV6::RUNX1+ and High Hyperdiploid Acute Lymphoblastic Leukemia

et al. 2023

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The mutational landscape of B-cell precursor acute lymphoblastic leukemia (BCP-ALL), the most common pediatric cancer, is not fully described partially because commonly applied short-read next generation sequencing has a limited ability to identify structural variations. By combining comprehensive analysis of structural variants (SVs), single-nucleotide variants (SNVs), and small insertions-deletions, new subtype-defining and therapeutic targets may be detected. We analyzed the landscape of somatic alterations in 60 pediatric patients diagnosed with the most common BCP-ALL subtypes, ETV6::RUNX1+ and classical hyperdiploid (HD), using conventional cytogenetics, single nucleotide polymorphism (SNP) array, whole exome sequencing (WES), and the novel optical genome mapping (OGM) technique. Ninety-five percent of SVs detected by cytogenetics and SNP-array were verified by OGM. OGM detected an additional 677 SVs not identified using the conventional methods, including (subclonal) IKZF1 deletions. Based on OGM, ETV6::RUNX1+ BCP-ALL harbored 2.7 times more SVs than HD BCP-ALL, mainly focal deletions. Besides SVs in known leukemia development genes (ETV6, PAX5, BTG1, CDKN2A), we identified 19 novel recurrently altered regions (in n ≥ 3) including 9p21.3 (FOCAD/HACD4), 8p11.21 (IKBKB), 1p34.3 (ZMYM1), 4q24 (MANBA), 8p23.1 (MSRA), and 10p14 (SFMBT2), as well as ETV6::RUNX1+ subtype-specific SVs (12p13.1 (GPRC5A), 12q24.21 (MED13L), 18q11.2 (MIB1), 20q11.22 (NCOA6)). We detected 3 novel fusion genes (SFMBT2::DGKD, PDS5B::STAG2, and TDRD5::LPCAT2), for which the sequence and expression were validated by long-read and whole transcriptome sequencing, respectively. OGM and WES identified double hits of SVs and SNVs (ETV6, BTG1, STAG2, MANBA, TBL1XR1, NSD2) in the same patient demonstrating the power of the combined approach to define the landscape of genomic alterations in BCP-ALL.

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Section: Discussionsupporting

confidence: 61%

Optical Genome Mapping Identifies Novel Recurrent Structural Alterations in Childhood ETV6::RUNX1+ and High Hyperdiploid Acute Lymphoblastic Leukemia

et al. 2023

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“…Highly repetitive regions, such as centromeric regions, short arms of acrocentric chromosomes, pseudo-autosomal regions (PARs), and telomeric regions, are often poorly covered by OGM because of missing labels and unreliable reference map data. Consequently, OGM may fail to detect SVs involving these regions, a well-known limitation [ 14 - 17 ]. However, as these regions may contain clinically relevant SVs, efforts should be undertaken to identify recurrent SVs in these areas.…”

Section: Discussionmentioning

confidence: 99%

“…We analyzed OGM results of diagnostic samples from patients with hematologic malignancies and evaluated their concordance with the results of conventional methods in detecting SVs. Several recent studies have assessed the clinical usefulness of SV detection using OGM in patients with blood cancer [13][14][15][16][17][18][19][20][21]. These studies mainly used CBA, FISH, RT-PCR, CMA, or MLPA as conventional methods for comparison.…”

Section: Introductionmentioning

confidence: 99%

Comparison of Optical Genome Mapping With Conventional Diagnostic Methods for Structural Variant Detection in Hematologic Malignancies

Shim,

Koo,

Shin

et al. 2024

Ann Lab Med

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Background Structural variants (SVs) are currently analyzed using a combination of conventional methods; however, this approach has limitations. Optical genome mapping (OGM), an emerging technology for detecting SVs using a single-molecule strategy, has the potential to replace conventional methods. We compared OGM with conventional diagnostic methods for detecting SVs in various hematologic malignancies. Methods Residual bone marrow aspirates from 27 patients with hematologic malignancies in whom SVs were observed using conventional methods (chromosomal banding analysis, FISH, an RNA fusion panel, and reverse transcription PCR) were analyzed using OGM. The concordance between the OGM and conventional method results was evaluated. Results OGM showed concordance in 63% (17/27) and partial concordance in 37% (10/27) of samples. OGM detected 76% (52/68) of the total SVs correctly (concordance rate for each type of SVs aneuploidies, 83% [15/18]; balanced translocation, 80% [12/15] unbalanced translocation, 54% [7/13] deletions, 81% [13/16]; duplications, 100% [2/2] inversion 100% [1/1]; insertion, 100% [1/1]; marker chromosome, 0% [0/1]; isochromosome, 100% [1/1]). Sixteen discordant results were attributed to the involvement of centromeric/telomeric regions, detection sensitivity, and a low mapping rate and coverage. OGM identified additional SVs, including submicroscopic SVs and novel fusions, in five cases. Conclusions OGM shows a high level of concordance with conventional diagnostic methods for the detection of SVs and can identify novel variants, suggesting its potential utility in enabling more comprehensive SV analysis in routine diagnostics of hematologic malignancies, although further studies and improvements are required.

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“…This is becoming increasingly important in newer technologies that depend on high molecular weight DNA for analysis, such as long-read sequencing and optical genome mapping [8,18]. Protocols for these applications can generate even longer DNA fragments ranging from 30 kb to 2000 kb [19][20][21]. High molecular weight DNA allows for more precise detection of large structural variants that are often associated with tumors that are genomically unstable [9,22].…”

Section: Discussionmentioning

confidence: 99%

DNA Quantity and Quality Comparisons between Cryopreserved and FFPE Tumors from Matched Pan-Cancer Samples

Okojie,

O’Neal,

Burr

et al. 2024

Current Oncology

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Personalized cancer care requires molecular characterization of neoplasms. While the research community accepts frozen tissues as the gold standard analyte for molecular assays, the source of tissue for testing in clinical cancer care comes almost universally from formalin-fixed, paraffin-embedded tissue (FFPE). As newer technologies emerge for DNA characterization that requires higher molecular weight DNA, it was necessary to compare the quality of DNA in terms of DNA length between FFPE and cryopreserved samples. We hypothesized that cryopreserved samples would yield higher quantity and superior quality DNA compared to FFPE samples. We analyzed DNA metrics by performing a head-to-head comparison between FFPE and cryopreserved samples from 38 human tumors representing various cancer types. DNA quantity and purity were measured by UV spectrophotometry, and DNA from cryopreserved tissue demonstrated a 4.2-fold increase in DNA yield per mg of tissue (p-value < 0.001). DNA quality was measured on a fragment microelectrophoresis analyzer, and again, DNA from cryopreserved tissue demonstrated a 223% increase in the DNA quality number and a 9-fold increase in DNA fragments > 40,000 bp (p-value < 0.0001). DNA from the cryopreserved tissues was superior to the DNA from FFPE samples in terms of DNA yield and quality.

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Optical Genome Mapping in Routine Cytogenetic Diagnosis of Acute Leukemia

Cited by 7 publications

References 40 publications

Optical Genome Mapping Identifies Novel Recurrent Structural Alterations in Childhood ETV6::RUNX1+ and High Hyperdiploid Acute Lymphoblastic Leukemia

Optical Genome Mapping Identifies Novel Recurrent Structural Alterations in Childhood ETV6::RUNX1+ and High Hyperdiploid Acute Lymphoblastic Leukemia

Comparison of Optical Genome Mapping With Conventional Diagnostic Methods for Structural Variant Detection in Hematologic Malignancies

DNA Quantity and Quality Comparisons between Cryopreserved and FFPE Tumors from Matched Pan-Cancer Samples

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