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June 07, 2021
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Copanlisib regimen improves outcomes in pretreated follicular, marginal zone lymphoma

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The addition of copanlisib to rituximab extended PFS among patients with relapsed follicular lymphoma or marginal zone lymphoma, according to a subset analysis of the randomized phase 3 CHRONOS-3 trial.

Perspective from Lee Greenberger, PhD

The findings — presented during the virtual ASCO Annual Meeting — showed the combination appeared associated with a higher objective response rate and more durable responses than placebo and rituximab (Rituxan; Genentech, Biogen). The regimen also exhibited a manageable safety profile.

Infographic showing PFS and duration of response

Data derived from Matasar MJ, et al. Abstract 7510. Presented at: ASCO Annual Meeting (virtual meeting); June 4-8, 2021.

“Copanlisib is the first PI3 kinase inhibitor to be safely combined with rituximab in a randomized phase 3 setting, and the first to demonstrate broad and superior efficacy in combination with rituximab [for] patients with relapsed follicular lymphoma or marginal zone lymphoma,” Matthew J. Matasar, MD, medical oncologist and lymphoma specialist at Memorial Sloan Kettering Cancer Center, said during a presentation. “[This represents] a potential new treatment option [for] this population.”

Rituximab monotherapy is approved for patients with relapsed, indolent non-Hodgkin lymphoma who experience an extended progression-free and treatment-free interval after previous rituximab-based therapy and are either unfit or unwilling to receive chemotherapy.

Matthew J. Matasar, MD
Matthew J. Matasar

Copanlisib (Aliqopa, Bayer), a PI3 kinase inhibitor, received FDA approval in 2017 as monotherapy for adults with relapsed follicular lymphoma who received at least two prior systemic therapies.

The double-blind CHRONOS-3 study compared the copanlisib-rituximab combination with placebo-rituximab for patients with relapsed indolent NHL who relapsed after least one prior line of rituximab-containing therapy. Most patients had follicular lymphoma, marginal zone lymphoma, small lymphocytic lymphoma or lymphoplasmacytoid lymphoma/Waldenström macroglobulinemia.

All patients had been progression- and treatment-free for at least 12 months after prior rituximab-based therapy, or for at least 6 months if they were unwilling or unfit to receive chemotherapy.

Researchers randomly assigned patients 2:1 to copanlisib (60 mg via IV on days 1,8 and 15 of 28-day cycles) with rituximab (375 mg/m2 via IV on days 1, 8, 15 and 22 of cycle 1, then day 1 of cycles 3, 5, 7 and 9) or placebo-rituximab.

Centrally assessed PFS by Cheson 2014 criteria served as the primary endpoint. Secondary endpoints included ORR, duration of response, complete response rate, time to progression and treatment-emergent adverse events.

Investigators assessed all randomly assigned patients for efficacy; safety assessments included patients who received at least one copanlisib/placebo or rituximab dose.

Data cutoff was Aug. 31, 2020.

The study met its primary endpoint. As Healio previously reported, initial results showed the copanlisib-rituximab regimen reduced risk for disease progression or death by 48%.

During ASCO, Matasar reported results of a preplanned subset analysis of 370 patients (median age, 62 years; range, 28-91) with relapsed follicular lymphoma or marginal zone lymphoma. Researchers assigned 250 patients (follicular lymphoma, n = 184; marginal zone lymphoma, n = 66) to copanlisib-rituximab. The other 120 (follicular lymphoma, n = 91; marginal zone lymphoma, n = 29) received placebo-rituximab.

Treatment groups were balanced with regard to sex (male, 46% for copanlisib-rituximab vs. 51.7% for placebo-rituximab), ECOG performance status (0 or 1, 96.4% vs. 100%), medical history of diabetes (14.8% vs. 13.3%) or hypertension (38% vs. 34.2%), histology (follicular lymphoma, 73.6% vs. 75.8%), median time since last systemic therapy (25.2 months vs. 25.4 months), median time since initial diagnosis (68.1 months vs. 72.6 months), previous lines of therapy (one, 47.2% vs. 46.7%; two, 26% vs. 27.5%; three or more, 26.8% vs. 25.8%) and percentage of patients unwilling or unfit to receive chemotherapy (22.4% vs. 21.7%).

Median follow-up was 18.5 months.

Results showed a statistically significant improvement in PFS in the copanlisib-rituximab group (median, 22.2 months vs. 15.4 months; HR = 0.55; 95% CI, 0.4-0.76).

The combination also appeared superior with regard to median time to progression (27.5 months vs. 15.4 months; HR = 0.5; P = .00001), ORR (82.4% vs. 50.8%), complete response rate (37.6% vs. 18.3%), partial response rate (44.8% vs. 32.5%) and median duration of response (23.9 months vs. 17.9 months).

The safety analysis included 249 patients assigned copanlisib-rituximab and 116 patients assigned placebo-rituximab. The safety profile of the combination appeared consistent with known toxicities of each agent as monotherapy, Matasar said.

The most common treatment-emergent adverse events that occurred more frequently in the copanlisib-rituximab group included hyperglycemia (all grade, 72.7% vs. 23.3%; grade 3 or higher, 59% vs. 7.8%); hypertension (all grade, 53.8% vs. 19.8%; grade 3, 43% vs. 8.6%), diarrhea (all grade, 35.3% vs. 12.1%; grade 3, 5.6% vs. 0%), nausea (all grade, 22.5% vs. 13.8%; grade 3, 0.8% vs. 0.9%), pyrexia (all grade, 21.7% vs. 7.8%; grade 3, 2% vs. 0%), neutropenia (all grade, 19.3% vs. 18.1%; grade 3/grade 4, 15.2% vs. 13.8%) and anemia (all grade, 18.1% vs. 6.9%; grade 3/grade 4, 4.4% vs. 0.9%).

A higher percentage of patients assigned copanlisib-rituximab developed pneumonitis (all grade, 6.8% vs. 1.7%; grade 3 or higher, 2.8% vs. 0.9%).