Phase II study of bendamustine, rituximab, and venetoclax (BR-VEN) for the front-line treatment of Mantle Cell Lymphoma (MCL) in patients ≥60 years old; Updated survival and minimal residual disease (MRD) analysis of precog PrE0405 Free

With a median age of 60-70 years at diagnosis, many patients with MCL are ineligible for aggressive treatment. Bendamustine and rituximab (BR) is a standard therapy for older patients with MCL. Venetoclax (VEN) has shown pre-clinical evidence of synergy with chemotherapy. Thus, PrE0405 was designed to evaluate the addition of VEN to BR in previously untreated older patients with MCL. We have previously reported on response rate and short-term survival (Portell et al. ASH 2023). Here, we update survival and include minimal residual disease (MRD) at end of treatment (EOT).

Methods Eligible patients included those that were previously untreated and diagnosed with MCL by presence of t(11;14) or cyclin D1 expression. Patients must have been ≥60 years of age at the start of therapy with a good performance status (ECOG 0-2). Adequate marrow and organ function was required, specifically a creatinine clearance ≥ 40 ml/min.

Eligible subjects were treated with bendamustine 90mg/m² D1-2 and rituximab 375mg/m² IV D1 every 28 days for a planned 6 cycles of therapy. For patients ≥75 years, 70mg/m² of bendamustine was allowed. VEN was given concurrently with BR. During Cycle 1, VEN was dose escalated weekly, as done in chronic lymphocytic leukemia, from 20mg to 200mg. For Cycle 2-6, VEN was administered as 400mg PO daily on days 1-10 only. Maintenance rituximab was encouraged but was per investigator discretion.

Primary end point was PET-negative complete remission (CR) at EOT by Lugano Criteria and was confirmed by a negative bone marrow biopsy if involved at screening. MRD was assessed at EOT by next-generation sequencing (Clonoseq).

Amended accrual goal was 33 patients with a planned 32 being eligible and treated. This provided an 81% statistical power to detect a 17% difference in CR rate (from 60% [E1411, Smith et al Blood 2024] to 77%) using an exact binomial test with a 1-sided alpha of 11.6%. Thus, BR-VEN would be considered promising if 23 or more subjects attained a CR.

Results

From 1/2020 to 3/2022, 33 subjects were enrolled, deemed eligible, and treated on study. Subjects were followed until 7/2024. Median age was 71 (range 61-80) and 76% (n=25) were male. All but 1 subject (97%, n=32) were White. MIPI was high in 67% (n=22), intermediate in 27% (n=9) and low in 6% (n=2). Ki67 was available in 25 (76%) subjects and was ≥30% in 14 (56%) and ≥50% in 7 (28%). Only one subject started bendamustine treatment at 70mg/m²; though 6 others had dose reductions during treatment. Thirty (90%) subjects completed all 6 cycles of therapy. Maintenance rituximab was administered in 19 (56%) of subjects and 9 completed all 12 recommended doses.

Treatment was generally well tolerated. During BR-VEN, Grade ≥3 treatment-related adverse events (TRAE) occurring in >10% (i.e., 4 or more) of subjects were neutropenia (n=8, 24%), and thrombocytopenia (n=5, 15%). Other common TRAE of all grades were nausea/vomiting (n=19, 58%), diarrhea (n=10, 30%), and fatigue (n=19, 58%).

At EOT with BR-VEN, overall response and CR rate was 97% (32 of 33) and 85% (28 of 33) respectively. The study met its primary endpoint of at least 23 subjects with a CR best response (p=0.002). EOT MRD sample (blood or marrow aspirate) was available for 28 subjects (85%). At EOT, MRD was undetectable for 100% (n=28) of evaluable subjects at a sensitivity of 10^-4 and 10^-5. At a sensitivity of 10^-6, 64% (n=18) were undetectable, 4% (n=1) were detectable and 32% (n=9) were indeterminate.

With a median follow up of 39.1 months, 3-year progression free survival (PFS) was 68.9 and 3-year overall survival (OS) was 70.0%. There were 11 total PFS events during follow up. Four subjects in remission died due to COVID-19, 1 died from influenza, one died from HSV encephalitis, and 2 others died from other causes. Two subjects died shortly after progression and 1 subject is alive following disease progression. As this study enrolled during the height of the COVID-19 pandemic, a sensitivity analysis was performed censoring the COVID-19 attributable deaths – PFS and OS at 3 years was 78.7% and 80.0%.

Conclusions

BR-VEN was generally well tolerated as induction therapy in older patients with MCL. It achieved a high CR rate of 85% with 100% MRD undetectable rate at 10^-5 sensitivity in those evaluable. However, there were competing risks for survival in this older population as, of the 11 PFS events, only 3 events were due to progression; 8 were due to death without progression.