According to results presented at the 2018 ASCO Annual Meeting, moxetumomab pasudotox, a first-in-class recombinant immunotoxin targeting CD22, demonstrated deep and durable responses in a substantial proportion of pretreated patients with relapsed/refractory hairy cell leukemia.
Robert J. Kreitman, MD
According to results presented at the 2018 ASCO Annual Meeting, moxetumomab pasudotox, a first-in-class recombinant immunotoxin targeting CD22, demonstrated deep and durable responses in a substantial proportion of pretreated patients with relapsed/refractory hairy cell leukemia (HCL).1
The best overall response in this pivotal multicenter, single-arm study was complete remission (CR) in 41% of patients, and 34% of patients had a CR with no minimal residual disease (MRD). A durable CR was achieved in 30% of patients.
“We believe that moxetumomab is a nonchemotherapeutic agent that has the potential to become a standard of care option for patients with relapsed/refractory HCL,” said Robert J. Kreitman, MD, chief, Clinical Immunotherapy Section, Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, Bethesda, Maryland.
HCL is a rare B-cell malignancy characterized by high CD22 expression. “Although first-line treatment offers durable response, relapsed/refractory HCL is not known to be curable and there remains an unmet need for new treatments,” he said. When moxetumomab binds to CD22 on the hairy cell and internalizes, it inhibits protein synthesis leading to an apoptotic cell death.
The primary objective of the study was to establish the rate of durable CR followed by hematologic remission (HR) for at least 6 months. HR was defined by resolution of cytopenias without the use of transfusions or growth factors for at least 4 weeks. CR was defined as HR for at least 4 weeks, clearing of hairy cells in the bone marrow by hematoxylin and eosin (H&E) stain, and resolution of hepatomegaly and lymphadenopathy by imaging.
Eligible patients had confirmed HCL and at least 1 cytopenia or symptomatic splenomegaly, at least 2 prior systemic therapies including at least 2 courses of purine nucleoside analog (PNA) or 1 prior course of PNA followed by either rituximab or a BRAF inhibitor. The study was conducted at 34 centers in 14 countries (NCT01829711).
Patients received moxetumomab pasudotox, 40 µg/kg, intravenously on days 1, 3, and 5 of 28-day treatment cycles, up to 6 cycles, unless stopped early due to disease progression, the start of alternate therapy, unacceptable toxicity, or if MRD-negative CR was documented by flow cytometry before 6 cycles. Disease response and immunohistochemistry (IHC) MRD status were assessed by blinded independent central review.
A total of 80 patients were treated. Fifty (62.5%) patients completed 6 cycles, 12 (15%) discontinued early because they were MRD-negative CR in fewer than 6 cycles, and 12 discontinued because of an adverse event, 8 (10%) of which were treatment related. One patient died, 2 discontinued because of disease progression, and 3 because of lack of benefit. The median duration of follow-up was 16.7 months as of data cut-off of May 24, 2017. Median age of patients was 60 years, 79% were male, 4% had variant HCL, and 6% had prior splenectomy. “The median baseline hematologic parameters were all in the cytopenic ranges and the median hairy cell involvement in the bone marrow was high at 85%,” said Kreitman.
The median number of prior systemic therapies was 3, 88% had at least 2 prior courses of PNA, 75% had prior rituximab, and 18% had prior BRAF inhibitor.
The objective response (OR) rate was 75% (60 out of 80) and 80% (64 out of 80) achieved HR, with a median onset of 1.1 months. Twenty-four patients (30%) achieved a durable CR and 33 (41%) had a CR. Of the 9 patients who achieved a CR without a durable CR, 2 patients relapsed from HR during the 6-month follow-up period. In 5 patients, CR onset was later than end of treatment “so it wasn’t captured by the reviewer,” he said. In 2 patients, consent was withdrawn due to logistical reasons. Twenty-seven of the 33 CRs were MRD-negative. The investigator-assessed response rates were somewhat higher due to the timing of the CR and interpretation of the bone marrow biopsy results. The OR rate by investigator assessment was 79% (63 out of 80).
The median immunoglobulin levels remained unchanged after treatment and median CD4 T-cell counts were stable or increased following a transient decrease on day 8, “confirming the nonimmunosuppressive effect of this treatment,” said Kreitman. Leukemic cell infiltration in the bone marrow by H&E decreased in all responders and in patients with stable disease.
The median duration of CR, HR from CR, and progression-free survival was not reached. The duration of CR was a median of 5.9 months in the 6 patients who were MRD-positive versus not reached in the 27 patients who were MRD-negative.
B-cell depletion, including malignant hairy cells, was sustained during treatment, with recovery by 6 months after the end of treatment. The disease response occurred despite significant immunogenicity, said Kreitman. The rate of antidrug antibodies was 59% at baseline and increased to 88% at any 1 time point during treatment, with increasing titer following treatment and a trend toward slower immunogenicity in patients who achieved a CR.
Treatment-related adverse events that occurred with a prevalence ≥20% were nausea (27.5%), peripheral edema (26.3%), headache (21.3%), and pyrexia (20.0%). The prevalence of any treatment-related grade-3/4 adverse event was 30.0%, and included capillary leak syndrome in 2.5%, hemolytic uremic syndrome in 5.0%, and lymphopenia in 7.5%. All events of capillary leak syndrome and hemolytic uremic syndrome resolved with supportive care and/or treatment discontinuation. Management of these adverse events included prophylactic oral hydration during the first week of each cycle and intravenous fluid supplementation on the day of infusion.
Kreitman RJ, Dearden C, Zinzani PL, et al. Moxetumomab pasudotox in heavily pretreated patients with relapsed/refractory hairy cell leukemia: Results of a pivotal international study.J Clin Oncol. 2018;36(suppl; abstr 7004).