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Sujith Samarasinghe, BSc, MBBS, MRCPCH, FRCPath, PhD, discusses the use of blinatumomab in children with Down syndrome acute lymphoblastic leukemia.
Treatment with first-line blinatumomab (Blincyto) in lieu of consolidation chemotherapy could address a critical need for less toxic regimens among children with Down syndrome and intermediate- to high-risk acute lymphoblastic leukemia (ALL), who historically experience poor survival outcomes due to high treatment-related mortality and disease resistance, according to Sujith Samarasinghe, BSc, MBBS, MRCPCH, FRCPath, PhD.1
Initial data from the phase 2 ALLTogether1 DS study (NCT043067576) presented at the 2024 EHA Congress showed improved clearance rates of minimal residual disease (MRD) with first-line blinatumomab compared with chemotherapy blocks in this patient population, meeting the study’s primary end point. Undetectable MRD rates in evaluable patients at the end of cycle 1 were 91% (95% CI, 79.8%-99.3%) with blinatumomab (n = 33), and 61% among patients in a historical control arm treated with chemotherapy in the UKALL 2011 study (EudraCT/CTIS: 2010-020924-22; n = 22). Moreover, at a median follow-up of 15 months (interquartile range, 6.4-22.1) the event-free survival and overall survival rates were both 100% in the overall cohort.
Regarding safety, 77.3% of patients in the historical control arm experienced a grade 3/4 adverse effect (AE) vs 39.4% of those given blinatumomab (P = .0057). Notably, a trend for a higher rate of seizures with blinatumomab was observed in patients over 10 years of age, at 18.2% vs 4.5% in the blinatumomab and historical chemotherapy arms, respectively, (P = .14).
“The data in terms of MRD clearance were stunning,” Samarasinghe, who serves as a consultant in pediatric hematology and the Hematology Specialty Lead at Great Ormand Street Hospital in London, United Kingdom, stated during an interview with OncLive®. “For patients both with and without Down syndrome [who have] ALL, this [drug] is a game changer.”
In the interview, Samarasinghe explained how replacing chemotherapy with blinatumomab in the front line could address the unique challenges experienced by children with Down syndrome ALL; discussed key efficacy and safety results with this approach from the ALLTogether1 DS study; and outlined plans to introduce blinatumomab earlier in the treatment course to potentially reduce early mortality.
Samarasinghe:Children and young people with Down syndrome have a much higher risk of developing ALL. However, they are characterized by a much higher treatment-related mortality [rate] and high rates of disease resistance. Survival outcomes for children with Down syndrome and ALL are approximately 20% lower than [those for] children who don’t have [Down syndrome] ALL. Accordingly, there’s a real unmet need [in this patient population] for new, innovative treatments that are less toxic. One idea we came up with was to use blinatumomab in the front line as a replacement for toxic consolidation chemotherapy.
Patients had to have Down syndrome and CD19-positive [ALL], but they also had to be MRD-positive at the end of induction because the primary end point was an MRD-based end point. However, patients who had MRD of 25% or more were not eligible for the study.
We recruited 33 patients into the study, and in cycle 1, 2 patients had to come off [treatment] and couldn’t complete cycle 1 due to seizures. That left 31 patients who completed cycle 1. When we evaluated MRD clearance rates, all patients had a complete MRD response rate of 91%, which was significantly better than [the MRD response rate seen among patients in the] historical control arm treated with chemotherapy [in the UKALL 2011 study], which was 61%.
First, we looked at [the rates of] grade 3/4 AEs in the blinatumomab cycle and compared those with the [AEs observed at] equivalent time points in the historical control [patients who received] chemotherapy. We found that 77.3% of patients in the historical control arm experienced a grade 3/4 AE; in [our] study, [this rate] was 39.4%, so [the incidence was] significantly lower. However, there was a trend [for a] higher rate of seizures in the Down Syndrome blinatumomab arm, at 18.2% vs 4.5% in the historical control [arm].
We’ve brought in new measures to reduce the rate of seizures. We’re starting prophylactic levetiracetam 1 week before we administer blinatumomab. That means [patients experience] therapeutic levels [of this prophylaxis] before we start [treatment] with the agent. We also dose escalate the levetiracetam 2 weeks into treatment, so we’ll get optimal dosing.
In the next iteration [of this research, we aim to] bring blinatumomab earlier [in the treatment course]. We found that we were losing 1 in 10 children in the induction [phase] before they could benefit from blinatumomab. The idea is to give blinatumomab at day 15, once we’ve debulked the blast percentage to below 55%.
[Ultimately,] blinatumomab has generated stunning results in terms of efficacy for the whole population, including patients who don’t have Down syndrome, and has [been shown to] reduce AEs as well.
Hodder A, Kirkwood A, van der Sluis I, et al. Blinatumomab for first line treatment in intermediate and high risk Down syndrome B-cell acute lymphoblastic leukaemia: initial findings from the ALLTogether1 DS trial. HemaSphere. 2024;8(suppl 1):S111