Effectiveness of Chemo-Immunotherapy (CIT) and Novel Therapies in Second or Later Line of Therapy (2L+) for Patients with Relapsed/Refractory (R/R) Aggressive Large B-Cell Lymphoma (LBCL)

Loretta J. Nastoupil; Clark R. Andersen; Amy Ayers; Yucai Wang; Thomas M. Habermann; Dai Chihara; Brad S. Kahl; Brian K. Link; Jonathon B. Cohen; Peter Martin; Izidore S. Lossos; Carla Casulo; Ruitao Lin; Ziyi Li; Melissa C. Larson; Matthew J. Maurer; Lynn Huynh; Chi Gao; Ramya Ramasubramanian; Mei Sheng Duh; Alex Mutebi; Tongsheng Wang; Monika Jun; Anthony Wang; Rajesh Kamalakar; Anupama Kalsekar; James R. Cerhan; Christopher R. Flowers

doi:10.1182/blood-2023-174497

$Effectiveness of Chemo-Immunotherapy (CIT) and Novel Therapies in Second or Later Line of Therapy (2L+) for Patients with Relapsed/Refractory (R/R) Aggressive Large B-Cell Lymphoma (LBCL)$

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Effectiveness of Chemo-Immunotherapy (CIT) and Novel Therapies in Second or Later Line of Therapy (2L+) for Patients with Relapsed/Refractory (R/R) Aggressive Large B-Cell Lymphoma (LBCL)

Loretta J. Nastoupil, Clark R. Andersen, Amy Ayers, Yucai Wang, Thomas M. Habermann, Dai Chihara, Brad S. Kahl, Brian K. Link, Jonathon B. Cohen, Peter Martin, …

Blood, Vol.142(Supplement 1), pp.309-309

11/28/2023

DOI: 10.1182/blood-2023-174497

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Abstract

Aim: Patients with R/R LBCL after first-line treatment have poor prognosis. Multiple novel therapies have been approved for R/R LBCL in recent years, but CIT regimens are still commonly used. This study evaluated the effectiveness of CIT and novel therapies in 2L+ in patients with R/R LBCL and the association between patient clinical characteristics and real-world outcomes. Methods: This was a multi-site retrospective observational study of patients aged ≥18 years with R/R LBCL in the Lymphoma Epidemiology of Outcomes (LEO) Consortium of Real-World Evidence (CReWE) cohort (patients followed from 1/1/2015 to 2/15/2023) who were treated with CIT or novel therapy in 2L+. CIT regimens included salvage/palliative chemotherapy, lenalidomide, rituximab, or obinutuzumab, used alone or in combination. Novel therapies included polatuzumab vedotin plus bendamustine and rituximab or variations thereof (i.e., pola-based regimen), tafasitamab plus lenalidomide or variations thereof (tafa-based regimen), and loncastuximab tesirine (lonca). Patients' demographic and clinical characteristics were assessed from the first confirmed R/R disease diagnosis and initiation of 2L+ therapy. When multiple lines of therapy (LOTs) were eligible for inclusion in the analysis, one was randomly selected as the index LOT. Real-world outcomes, determined by investigators at each clinical site, including overall response rate (ORR), complete response (CR) rate, duration of response (DOR), duration of complete response (DOCR), progression-free survival (PFS), and overall survival (OS) were described for all patients in each treatment group and for the subgroup of patients with prior chimeric antigen receptor (CAR) T-cell therapy. Multivariable Cox Proportional Hazards models were used to assess associations between select patient clinical characteristics and real-world outcomes. Results: The study population included patients treated with CIT (N=653), pola-based regimen (N=116), tafa-based regimen (N=55), and lonca (N=42) ( Figure 1A). The median (m) age at date of index treatment initiation across groups ranged from 63 to 74 years. Across groups, most patients had primary refractory disease-i.e., were refractory to the first LOT (69.5% CIT vs. 73.3% pola vs. 58.2% tafa vs. 71.4% lonca), whereas variable proportions had one prior LOT (65.5% vs. 17.2% vs. 43.6% vs. 7.1%) and prior CAR T-cell therapy (5.1% vs. 43.1% vs. 32.7% vs. 47.6%). In the CIT group, ORR was 33.8%, 15.5% of patients achieved CR, mPFS (95% CI) was 1.9 (1.7, 2.1) months, and mOS was 9.1 (8.1, 10.5) months. In the pola group, ORR was 42.2%, 24.1% of patients achieved CR, mPFS was 2.5 (2, 3.2) months and mOS was 7.8 (6.4, 11.8) months. In the tafa group, ORR was 25.5%, 14.5% of patients achieved CR, mPFS was 2.7 (2.1, 4.2) months, and mOS was 8 (5.3, 12.7) months. In the lonca group, ORR was 40.5%, 21.4% of patients achieved CR, mPFS was 3 (2.1, 5.1) months, and mOS was 4.7 (3.7, 10.8) months. Demographics and outcomes for all patients and those who received prior CAR T-cell therapy are summarized in Figure 1A. In the multivariable Cox regression analysis, International Prognostic Index (IPI) risk score ≥3, CIT as the index treatment type, and primary refractory status were significantly associated with time from response to progression/death (P<0.05; Figure 1B). IPI risk score ≥3, CIT as the index treatment type, and primary refractory status were significantly associated with worse PFS. IPI risk ≥3, ≥3 prior LOTs, and primary refractory status were significantly associated with OS. Conclusion: In this large clinical cohort of patients with R/R LBCL with high proportions having primary refractory disease, all common treatments were associated with modest ORR/CR and poor OS. Receiving CIT treatments, higher IPI score, primary refractory status, and higher number of prior LOTs were significantly associated with poor clinical outcomes. A study with larger sample size and longer follow-up may be warranted to further understand the clinical effectiveness of novel treatments. Thus, despite the availability of novel treatments during the study period, these findings highlight the need for more effective treatment alternatives beyond currently available options to improve outcomes.

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Title: Subtitle: Effectiveness of Chemo-Immunotherapy (CIT) and Novel Therapies in Second or Later Line of Therapy (2L+) for Patients with Relapsed/Refractory (R/R) Aggressive Large B-Cell Lymphoma (LBCL)
Creators: Loretta J. Nastoupil - The University of Texas MD Anderson Cancer Center
Clark R. Andersen - The University of Texas MD Anderson Cancer Center
Amy Ayers - The University of Texas MD Anderson Cancer Center
Yucai Wang - Mayo Clinic
Thomas M. Habermann - Mayo Clinic
Dai Chihara - The University of Texas MD Anderson Cancer Center
Brad S. Kahl - Washington University in St. Louis
Brian K. Link - University of Iowa
Jonathon B. Cohen - Emory University
Peter Martin - Cornell University
Izidore S. Lossos - University of Miami Health System
Carla Casulo - University of Rochester Medical Center
Ruitao Lin - The University of Texas MD Anderson Cancer Center
Ziyi Li - The University of Texas MD Anderson Cancer Center
Melissa C. Larson - Mayo Clinic
Matthew J. Maurer - Mayo Clinic
Lynn Huynh - Analysis Group (United States)
Chi Gao - Analysis Group (United States)
Ramya Ramasubramanian - Analysis Group (United States)
Mei Sheng Duh - Analysis Group (United States)
Alex Mutebi - Genmab (United States)
Tongsheng Wang - Genmab (United States)
Monika Jun - Genmab (United States)
Anthony Wang - AbbVie (United States)
Rajesh Kamalakar - AbbVie (United States)
Anupama Kalsekar - Genmab (United States)
James R. Cerhan - Mayo Clinic in Florida
Christopher R. Flowers - The University of Texas MD Anderson Cancer Center
Resource Type: Abstract
Publication Details: Blood, Vol.142(Supplement 1), pp.309-309
DOI: 10.1182/blood-2023-174497
ISSN: 0006-4971
eISSN: 1528-0020
Language: English
Date published: 11/28/2023
Academic Unit: Hematology, Oncology, and Blood & Marrow Transplantation; Epidemiology; Internal Medicine
Record Identifier: 9984539531202771

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