To the editor:
In chronic lymphocytic leukemia (CLL), the median age at diagnosis is 72 years, and most patients requiring therapy have coexisting medical conditions. Venetoclax is a potent BH3-mimetic compound that selectively antagonizes BCL-2 and has shown efficacy as monotherapy and with rituximab in patients with relapsed/refractory CLL.1-4 Obinutuzumab has also demonstrated impressive clinical activity in CLL as a single agent and in combination.5,6 First results from an ongoing phase 1b trial with both compounds suggest a venetoclax dose of 400 mg.7 In the phase 3 CLL14 trial, patients with previously untreated CLL and coexisting medical conditions as assessed by a cumulative illness rating scale (CIRS) total score >6 and/or an estimated creatinine clearance <70 mL/min were randomized to receive either 6 cycles of chlorambucil plus obinutuzumab plus 6 cycles of chlorambucil or 6 cycles of venetoclax plus obinutuzumab plus 6 cycles of venetoclax (NCT02242942). Here, we report the safety and efficacy results of the run-in phase of the CLL14 trial.
Between December 2014 and April 2015, 13 previously untreated patients with CLL from Australia, Canada, Germany, New Zealand, the United States, and Spain were enrolled to receive the combination of obinutuzumab and venetoclax. At baseline, the patients had a median age of 75 years (range, 59-88 years), a median creatinine clearance of 57.6 mL/min, and a median CIRS score of 8 (Table 1). Obinutuzumab was administered IV as follows: 100 mg on day 1 and 900 mg on day 2 (or 1000 mg on day 1), 1000 mg on day 8 and day 15 of cycle 1, and subsequently 1000 mg on day 1 for cycles 2 to 6. Daily oral doses of venetoclax were gradually ramped up each week, starting with 20 mg on day 22 of cycle 1 and then increased to 50 mg, 100 mg, 200 mg, and 400 mg daily, which was continued through to cycle 12.
At data cutoff, all patients had completed 12 months of therapy with the exception of 2 patients: 1 patient developed a grade 4 infusion-related reaction (IRR) during the first dose of obinutuzumab and was withdrawn from the study according to protocol requirements; the second patient discontinued at cycle 8 due to the patient’s wish. All patients experienced at least 1 adverse event (AE), and 10 patients (83.3%) had at least 1 grade 3/4 AE (Table 2). Seven patients (58.3%) had grade 3/4 neutropenia, and among these patients, 5 were treated successfully with granulocyte colony-stimulating factor and 3 events (25.0%) of grade 3/4 febrile neutropenia occurred. Reported infections (in 8 patients [66.7%]) were mostly mild, except for 2 grade 3/4 infections (16.7%) (1 case each of influenza and respiratory tract infection). No fatal AEs were reported. Two patients (16.7%) experienced laboratory tumor lysis syndrome (TLS); 1 event occurred during venetoclax ramp up to 200 mg at cycle 2 and the other event on the first day of cycle 1 after the 100-mg infusion of obinutuzumab. Both events were grade 3 with no evidence of clinical TLS in either patient; they were managed by IV fluids (1.5-2 L) and in 1 case by administration of sodium polystyrene sulfonate for treatment of hyperkalemia and resolved without sequelae. No clinical TLS events were reported. IRRs occurred in 9 patients (75.0%) during the first obinutuzumab administration.
Rapid reduction in the peripheral lymphocyte count was observed in all patients within the first cycle of obinutuzumab (supplemental Figure 1, available on the Blood Web site). Overall response rate 3 months after the end of treatment was 100%. Complete responses according to International Workshop on Chronic Lymphocytic Leukemia guidelines were achieved in 7 of 12 patients (58%), including 1 patient with incomplete bone marrow (BM) recovery due to a hemoglobin value of 10.2 g/dL. Five patients were reported with a partial response, 3 of whom had a normalization of blood count and resolved lymphadenopathy but did not consent to BM biopsy and were therefore graded as partial response. Two patients had residual lymph nodes of 18 mm and 16 mm. All patients showed reduction of lymphadenopathy (supplemental Figure 2). At cycle 7, 10 of 11 patients with available minimal residual disease (MRD) peripheral blood (PB) samples were MRD negative (<10−4), and 1 patient was assessed as intermediate (≥10−4 <10−2). At cycles 9 and 12, all patients with available MRD data were assessed as MRD negative in the PB, and at final staging (3 months after the end of treatment), 11 of 12 patients were MRD negative in the PB and 1 was assessed as intermediate (supplemental Table 1). At cycle 9, BM aspirates from 5 patients were available, and of those, 3 were MRD negative, 1 was intermediate, and 1 was positive (≥10−2) (supplemental Table 1). At final staging, BM aspirates of 7 patients were available, and of those, 5 were MRD negative and 2 were intermediate. One of 7 patients was assessed negative in PB and intermediate in BM at final staging. At a median follow-up of 15 months, there were no events of progressive disease or deaths.
Our results demonstrated that venetoclax could be safely combined with obinutuzumab, even in patients with comorbidities and at increased risk of TLS due to renal impairment. The occurrence of TLS in venetoclax-treated patients has been reported in previous studies, including 2 fatal events, and warrants careful monitoring.2 In our study, firstly, the individual risk for TLS was assessed prior to treatment administration based on lymphocyte count and lymph node mass. Secondly, patients received hydration with at least 1.5 to 2 L and allopurinol as prophylaxis, and patients at high risk of TLS and with high uric acid levels also received rasburicase prophylactically. Thirdly, the combination treatment was initiated with obinutuzumab followed by a gradual venetoclax dose ramp up over 5 weeks. Following this strategy, no clinical TLS event was observed in this study and 2 laboratory TLS events occurred; further treatment and observation is warranted in the main phase to assess TLS frequency in this patient population.
The frequency of neutropenia (66.7%) and febrile neutropenia (25%) was comparable to other venetoclax-based treatments,2,4 where neutropenia rates of 45% to 55% and neutropenic fever rates of 6% to 12% were observed. The rates of neutropenia with chlorambucil plus obinutuzumab were lower (eg, in CLL11),8 indicating that BCL-2 inhibition might induce clinically relevant cytopenias. This aspect needs to be carefully evaluated in the main phase of CLL14 and future trials utilizing BCL-2 inhibition.
Efficacy results for venetoclax and obinutuzumab demonstrate an increased response rate with an overall response rate of 100% and a 92% MRD negativity rate in PB 3 months after treatment completion. Given the limited number of available BM samples and a few discordances observed between MRD levels assessed in PB and BM, further follow-up is needed to evaluate the depth of response.9-11
A phase 1b study showed good safety and efficacy of venetoclax plus rituximab in 49 patients with relapsed/refractory CLL.4 Our data suggest that venetoclax and obinutuzumab can be safely administered in previously untreated CLL patients of advanced age with coexisting medical conditions. The regimen induces high rates of overall response, though the small patient population should be taken into account. Longer follow-up and a larger patient population will determine whether these responses remain durable. The randomized phase of the CLL14 (BO25323) study was opened in August 2015 and completed recruitment of 432 patients in August 2016.
Presented in abstract form at the 57th annual meeting of the American Society of Hematology, Orlando, FL, 7 December 2015 and at the 58th annual meeting of the American Society of Hematology, San Diego, CA, 3 December 2016.
The online version of this article contains a data supplement.
Authorship
Acknowledgments: This study is a collaborative effort between F. Hoffmann-La Roche Ltd, AbbVie, Inc., and the German CLL Study Group, and the authors thank all team members involved. In particular, the authors acknowledge Michele Porro Lurà, Johanna Wesselmann, and Greg Vosganian for their excellent contributions. The authors gratefully thank the patients who participated and their families.
This study was supported by F. Hoffmann-La Roche Ltd.
Contribution: K.F., O.A.-S., B.E., S.S., and M.H. designed the research, collected, analyzed and interpreted the data, and wrote the paper; A.-M.F. and S.B. collected, analyzed, and interpreted the data and wrote the paper; M.D. and S.W. analyzed data; J.B. and C.-M.W. analyzed and interpreted the data and wrote the paper; K.H. analyzed and interpreted the data; R.H. reviewed and approved the paper; E.T. collected the data and wrote the paper; L.F. and M.M. interpreted the data.; A.W.L., J.J.M.v.D., and M.R. collected and analyzed the data. V.G. designed the research and wrote the paper. T.J.K., R.W., S.R., T.S. S.O., C.O., and J.L. provided patients. All authors critically reviewed the paper and approved the final version.
Conflict-of-interest disclosure: K.F. received travel grants from Roche. O.A.-S. received a travel grant from Gilead; A.-M.F. received travel grants from Roche, Celgene, AbbVie and Mundipharma, and research funding from Celgene; M.D. is a Roche employee and equity owner. J.B. received honoraria and travel support from Roche. S.W. is a Roche employee. T.J.K. received consultancy fees from Gilead, Pharmacyclics, Celgene, Roche, and AbbVie; received honoraria from Gilead, Pharmacyclics, Celgene, Roche, and AbbVie; is on the speakers bureau of Pharmacyclics; and received research funding from Celgene and AbbVie. R.W. is employed by the Capital & Coast District Health Board, Malaghan Institute of Medical Research; received research funding from the Health Research Council of New Zealand; received honoraria from Avalia Immunotherapies and Janssen; is on the advisory committee of Avalia Immunotherapies and the Australasian Leukaemia & Lymphoma Group; and received funding from Roche for congress attendance. S.R. is on the advisory board of Roche, Celgene, AbbVie, Lundbeck, and Gilead; received research funding from Roche; is on the speakers bureau of Roche and Celgene; and received honorarium from Roche. S.O. received consultancy fees, research funding, honoraria, and provision of subsidized drugs from Roche. C.O. received clinical trial funding from Roche, Gilead, Pharmacyclics, Celgene, and Lundbeck and received honoraria from Roche, Janssen, Gilead, Celgene, AbbVie, Lundbeck, and Novartis. J.L. received consultancy fees from AbbVie, Roche, Gilead, Janssen, msd, and Novartis. K.H. is a Roche employee. R.H. is an AbbVie employee. E.T. is on the speakers bureau of Gilead and received travel support from Gilead, Celgene, and Amgen. L.F. received research funding from AbbVie and Roche. B.F.E. received consultancy fees from Roche, AbbVie, and Mundipharma; received research funding from AbbVie and Mundipharma; and is on the speaker’s bureau of Roche and Mundipharma. C.-M.W. received consultancy fees, research funding, and honoraria from Roche and AbbVie. S.S. received research support and honoraria from Roche and AbbVie. A.W.L. received research funding from Roche and patents and royalties from InVivoScribe Technologies. J.J.M.v.D. received consultancy fees from Roche; patents and royalties from BD Biosciences, Cytognos, DAKO, InVivoScribe, and Immunostep; and laboratory services from Roche, BD Biosciences. S.B. received research support from Roche, AbbVie, and Celgene and honoraria from Roche and AbbVie. M.R. received research funding from Roche and is a member of the Roche board of directors and advisory board. V.G. is on the advisory boards of Roche, Gilead, and Janssen; has an advisory role for Roche; received speaker honoraria from Roche and Glaxo; and received travel grants from Roche and Janssen. M.M. is a Roche employee. M.H. is a consultant or advisory board member for, and received honoraria and research support from, AbbVie, Amgen, Celgene, Roche, Gilead, Janssen, and Mundipharma. T.S. declares no competing financial interests.
The current affiliation for S.B. is Department of Internal Medicine, Hematology, Oncology, and Palliative Medicine, University of Rostock, Rostock, Germany.
Correspondence: Kirsten Fischer, Department I of Internal Medicine, Center of Integrated Oncology Köln Bonn, University Hospital of Cologne, Kerpener Str 62, 50937 Cologne, Germany; e-mail: kirsten.fischer@uk-koeln.de; and Michael Hallek, Department I of Internal Medicine, Center of Integrated Oncology Köln Bonn, University Hospital of Cologne, Kerpener Str 62, 50937 Cologne, Germany; e-mail: michael.hallek@uni-koeln.de.