Integrative genomic analysis of childhood acute lymphoblastic leukaemia lacking a genetic biomarker in the UKALL2003 clinical trial.

Schwab, Claire; Cranston, Ruth E.; Ryan, Sarra; Butler, Ellie; Winterman, Emily; Hawking, Zoe; Bashton, Matthew; Enshaei, Amir; Russell, Lisa J.; Kingsbury, Zoya; Peden, John F.; Barretta, Emilio; Murray, J. C.; Gibson, Jude; Hinchliffe, Andrew C; Bain, Robert; Vora, Ajay; Ross, Mark T.; Moorman, Anthony V.; Harrison, Christine J.

doi:10.21203/rs.3.rs-2159503/v1

Cited by 2 publications

(2 citation statements)

References 37 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Most studies have used target sequencing depths ranging from 60× to 90× to assess the diagnostic yield of WGS in hematological malignancies ( 15 , 19 , 20 , 60 ). In a study with an effective mean coverage of 50×, Duncavage and coworkers found that the sensitivity was 100% for the detection of CNVs and SVs but decreased to 84.6% for SNVs ( 19 ).…”

Section: Discussionmentioning

confidence: 99%

“…Of note, restricted analysis of leukemic samples (L-only) could call primary genetic abnormalities in 37 out of 38 patients ( 20 ). A further study based on WGS investigated a subset of pediatric B-other ALL patients from the UKALL2003 trial and identified a subtype-defining lesion in 94% of the patients ( 15 ), whereas a similar study of 47 adult B-other ALL patients detected a class-defining aberration in 87% of patients ( 21 ).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Feasibility to use whole-genome sequencing as a sole diagnostic method to detect genomic aberrations in pediatric B-cell acute lymphoblastic leukemia

Rezayee,

Eisfeldt,

Skaftason

et al. 2023

Front. Oncol.

View full text Add to dashboard Cite

IntroductionThe suitability of whole-genome sequencing (WGS) as the sole method to detect clinically relevant genomic aberrations in B-cell acute lymphoblastic leukemia (ALL) was investigated with the aim of replacing current diagnostic methods.MethodsFor this purpose, we assessed the analytical performance of 150 bp paired-end WGS (90x leukemia/30x germline). A set of 88 retrospective B-cell ALL samples were selected to represent established ALL subgroups as well as ALL lacking stratifying markers by standard-of-care (SoC), so-called B-other ALL.ResultsBoth the analysis of paired leukemia/germline (L/N)(n=64) as well as leukemia-only (L-only)(n=88) detected all types of aberrations mandatory in the current ALLTogether trial protocol, i.e., aneuploidies, structural variants, and focal copy-number aberrations. Moreover, comparison to SoC revealed 100% concordance and that all patients had been assigned to the correct genetic subgroup using both approaches. Notably, WGS could allocate 35 out of 39 B-other ALL samples to one of the emerging genetic subgroups considered in the most recent classifications of ALL. We further investigated the impact of high (90x; n=58) vs low (30x; n=30) coverage on the diagnostic yield and observed an equally perfect concordance with SoC; low coverage detected all relevant lesions.DiscussionThe filtration of the WGS findings with a short list of genes recurrently rearranged in ALL was instrumental to extract the clinically relevant information efficiently. Nonetheless, the detection of DUX4 rearrangements required an additional customized analysis, due to multiple copies of this gene embedded in the highly repetitive D4Z4 region. We conclude that the diagnostic performance of WGS as the standalone method was remarkable and allowed detection of all clinically relevant genomic events in the diagnostic setting of B-cell ALL.

show abstract