Integrative genomic analysis of childhood acute lymphoblastic leukaemia lacking a genetic biomarker in the UKALL2003 clinical trial.
Claire SchwabRuth E CranstonSarra L RyanEllie ButlerEmily WintermanZoe HawkingMatthew BashtonAmir EnshaeiLisa J RussellZoya KingsburyJohn F PedenEmilio BarrettaJames MurrayJude GibsonAndrew C HinchliffeRobert BainAjay VoraDavid R BentleyMark T RossAnthony V MoormanChristine J HarrisonPublished in: Leukemia (2022)
Incorporating genetics into risk-stratification for treatment of childhood B-progenitor acute lymphoblastic leukaemia (B-ALL) has contributed significantly to improved survival. In about 30% B-ALL (B-other-ALL) without well-established chromosomal changes, new genetic subtypes have recently emerged, yet their true prognostic relevance largely remains unclear. We integrated next generation sequencing (NGS): whole genome sequencing (WGS) (n = 157) and bespoke targeted NGS (t-NGS) (n = 175) (overlap n = 36), with existing genetic annotation in a representative cohort of 351 B-other-ALL patients from the childhood ALL trail, UKALL2003. PAX5alt was most frequently observed (n = 91), whereas PAX5 P80R mutations (n = 11) defined a distinct PAX5 subtype. DUX4-r subtype (n = 80) was defined by DUX4 rearrangements and/or ERG deletions. These patients had a low relapse rate and excellent survival. ETV6::RUNX1-like subtype (n = 21) was characterised by multiple abnormalities of ETV6 and IKZF1, with no reported relapses or deaths, indicating their excellent prognosis in this trial. An inferior outcome for patients with ABL-class fusions (n = 25) was confirmed. Integration of NGS into genomic profiling of B-other-ALL within a single childhood ALL trial, UKALL2003, has shown the added clinical value of NGS-based approaches, through improved accuracy in detection and classification into the range of risk stratifying genetic subtypes, while validating their prognostic significance.
Keyphrases
- clinical trial
- end stage renal disease
- copy number
- newly diagnosed
- acute lymphoblastic leukemia
- chronic kidney disease
- ejection fraction
- genome wide
- study protocol
- liver failure
- peritoneal dialysis
- phase iii
- early life
- prognostic factors
- phase ii
- transcription factor
- randomized controlled trial
- intensive care unit
- childhood cancer
- cancer therapy
- free survival
- acute respiratory distress syndrome
- sensitive detection