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1541 Lenalidomide in Combination with Bendamustine for Patients with Chemorefractory Hodgkin Lymphoma: Final Results of the Leben Multicenter Phase 1/2 Study

Lymphoma: Therapy with Biologic Agents, excluding Pre-Clinical Models
Program: Oral and Poster Abstracts
Session: 624. Lymphoma: Therapy with Biologic Agents, excluding Pre-Clinical Models: Poster I
Saturday, December 5, 2015, 5:30 PM-7:30 PM
Hall A, Level 2 (Orange County Convention Center)

Antonello Pinto, MD1*, Vincenzo Pavone, MD2, Francesco Angrilli, MD3*, Mariangela Saggese, PharmD1*, Stefania Crisci, ScD1*, Caterina Patti, MD4*, Pier Luigi Zinzani, MD, PhD5, Alfonso Maria D'Arco, MD6*, Elena Cavalieri, MD7*, Attilio Guarini, MD8*, Michele Spina, MD9, Daniela Carlino, MD2*, Simona Falorio, MD3*, Emanuela Morelli, MD1*, Manuela Arcamone, MD1*, Ferdinando Frigeri, MD, PhD1*, Annarosaria De Chiara, MD10*, Rosaria De Filippi, MD, PhD11* and Gaetano Corazzelli, MD1*

1Hematology-Oncology and Stem Cell Transplantation Unit, Istituto Nazionale Tumori, Fondazione 'G. Pascale', IRCCS, Naples, Italy
2Division of Hematology, Ospedale G. Panico, Tricase, Lecce, Italy
3Hematology and BMT Center, Spirito Santo Hospital, Pescara, Italy
4Dept. of Hematology, Ospedale V. Cervello, Palermo, Italy
5Institute of Hematology “L. & A. Serŕgnoli”, University of Bologna, Bologna, Italy
6Hematology-Oncology, Ospedale A. Tortora, Pagani, Italy
7Hematology, Azienda Ospedaliera Sant'Andrea, Rome, Italy
8Hematology, Ospedale oncologico 'Giovanni Paolo II', I.R.C.C.S., Bari, Italy
9Division of Medical Oncology, National Cancer Institute, Aviano, Italy
10Pathology Unit, Istituto Nazionale Tumori Fondazione 'G. Pascale', Naples, Italy
11Department of Clinical Medicine and Surgery, Federico II University, Naples, Italy

Background

Improving strategies for patients (pts) with relapsed/refractory (R/R) Hodgkin lymphoma (HL) who fail stem cell transplantation (SCT) or are unsuitable for the procedure remains an essential need. Lenalidomide and bendamustine are active and well tolerated as single agents in recurrent HL, with overall response rates (ORR) of 30% to 53% [Fenhinger, 2012; Corazzelli, 2012; Moskowitz, 2012].These agents independently frame different targets on tumor and microenvironment cells and may cooperate to override disturbed immunologic pathways and circumvent drug resistance in HL. In a Bayesian, multi-center, open label phase 1/2  study, we investigated for safety and efficacy the combination of continuous lenalidomide with weekly bendamustine (ClinicalTrials.gov # NTC01412307).

Methods

The study aimed at defining the optimal daily dose of continuous lenalidomide (10, 15, 20 or 25 mg) as combined, in a 28-day cycle, to weekly fixed-dose bendamustine (60 mg/m2; d 1, 8, 15). The dose-finding algorithm proceeded in cohorts of 3 pts, based on anticipated efficacy and toxicity pairs of probability (Thall & Cook, Biometrics 2004). Trade-offs between response [Cheson 2007 criteria] and dose-limiting toxicity [CTCv3.0 grade (G) >3 lasting >2 weeks] were assessed after 2 cycles (day +56) and pts were planned to receive up to 6 total courses, unless progression or unacceptable toxicity occurred. ORR and progression-free survival (PFS) were additional endpoints.

Results

Thirty-six pts (69% male) with a median age of 31 yrs (r 19-75) were enrolled. The median number of prior therapies was 4 (r 1-9) and the median time from upfront treatment was 24 mo.s (r 7-118). Twenty-six pts (72%) had primary refractory disease after ABVD, 16 pts (44%) failed prior SCT [single (n=7) or tandem (n=3) ASCT, tandem ASCT/alloSCT (n=6)]. Fifteen pts (42%) had previously received a median of 5 cycles (r 2-8) of brentuximab vedotin (BV) and 3 pts were already given bendamustine (>3 courses).  Overall, 23 pts (64%) were refractory to most recent therapy. Eff/Tox trade-offs at cycle 2 showed that 73% of pts had response w/o toxicity, 19% had no response w/o toxicity, 6% had response with toxicity and 2% had no response with toxicity. With such Eff/Tox profiles, the study algorithm did not prompt any dose escalation for lenalidomide after the first 18 pts and the initial dose level (10 mg) was adopted for the expansion phase. A total of 156 LeBen cycles were administered, and pts received a median of 4 courses (r 1-6). Overall, 16 cycles were delayed due to G3/G4 thrombocytopenia (n=6), G4 neutropenia (n=3), G3 pneumonia (n=3), G3 respiratory infection (n=2), G2 phlebitis (n=1), G2 supraventricular arrhythmia (n=1). Two patients discontinued treatment, while in PR and CR after 4 courses, due to protracted (>2 weeks) thrombocytopenia. No G4 extra-hematological toxicity was observed. The complete response (CR) rate was 44% (16/36) with an ORR of 75% (27/36; 95% CI, 59-86). Notably, substantial CR and PR rates were achieved after LeBen regardless of primary refractoriness, SCT and BV failure (Table). Most CRs (14/16) were obtained within the first 4 cycles; 6 responders (4 CRs and 2 PRs) underwent SCT. Median PFS was 3.2 mo.s (r 1.5-5.4) for pts with progressive (PD) or stable disease (SD) and 11.4 mo.s (r 4-31) for those achieving CR/PR. Median overall survival for the entire cohort was 24 mo.s. Overall, complete responders (including 6 pts consolidated with SCT) had a 2-year disease-free survival of 41% (median, 14.3 mo.s). 

Conclusions

The innovative schedule of the Leben combination is safe, yields high response rates in heavily pretreated and primary refractory HL pts, including SCT and BV failures, and steps over the 'single agent' activity of its components. Due to its immunomodulatory potential the Leben platform is amenable to further upgrading through lenalidomide maintenance, combination with immune checkpoint inhibitors and BV.

 

Table: Efficacy results

 

 

 

 


Responses

no. (%)

All pts

Refractory to upfront therapy

Refractory to most recent therapy

Failure after SCT

Failure after ASCT

Failure after AlloSCT

Failure after BV

Failure after SCT and BV

Failure after bendamustine

No BV

(n=36)

(n=26)

(n=23)

(n=16)

(n=10)

(n= 6)

(n=15)

(n=8)

(n=3)

(n=21)

CR

16 (44)

11 (42)

  8 (35)

  8 (50)

6 (60)

2 (33)

5 (33)

3 (37)

0

11

PR

11

  8

  9

  4

2

2

4

2

0

  7

SD

  2

  2

  2

  1

0

1

1

1

1

  1

PD

  7

  5

  4

  3

2

1

5

2

2

  2

CR+PR

27 (75)

19 (73)

17 (74)

12 (75)

8 (80)

4 (66)

9 (60)

5 (62)

0

18 (86)

Disclosures: Pinto: Takeda, Celgene, Roche, TEVA: Honoraria ; Takeda: Research Funding . Zinzani: Takeda: Membership on an entity’s Board of Directors or advisory committees ; J&J: Membership on an entity’s Board of Directors or advisory committees ; Gilead: Membership on an entity’s Board of Directors or advisory committees ; Celgene: Membership on an entity’s Board of Directors or advisory committees ; Pfizer: Membership on an entity’s Board of Directors or advisory committees .

*signifies non-member of ASH