Surrogate Endpoints for Cure in DLBCL: Are We There Yet?

Diffuse large B-cell lymphoma (DLBCL) is regarded as a potentially curable lymphoma with chemoimmunotherapy. Studies have demonstrated that patients who have not relapsed by month 24 following diagnosis (EFS24) have a five-year overall survival (OS) similar to that of age-matched controls; therefore, this has been considered a marker of likely-cured disease.¹ Most relapses occur in the first two years following diagnosis, and little is known about risks of relapse at later time points in the era of rituximab-based chemoimmunotherapy. Dr. Yucai Wang and colleagues performed a multicenter, prospective, observational trial of patients with DLBCL treated with rituximab-containing chemoimmunotherapy at the Mayo Clinic and the University of Iowa between 2002 and 2015. Double- and triple-hit lymphomas were not included in the study, but transformation from an indolent lymphoma was. Patients who were alive and disease-free at 24 months from diagnosis were analyzed for relapse rate.

Of 1,324 patients diagnosed and treated during this timeframe, 847 (64%) were alive and without evidence of disease relapse at EFS24, with a median follow-up of 83.2 months and 62.9 months from diagnosis and EFS24, respectively. Most of the initial cohort of patients had DLBCL alone (87%), whereas 13 percent had transformation from an indolent histology. More than half of the patients had advanced-stage disease (57.3%). Of the EFS24 patients, the cumulative risk of relapse at three, five, and eight years from EFS24 was 6.9 percent, 9.3 percent, and 10.3 percent, respectively. Among late relapses, a slight majority were men (56.4%), just under half had an elevated lactate dehydrogenase (LDH) at diagnosis (49.3%), and most had advanced-stage disease (75.6%), with 16.7 percent of patients having involvement of more than one extranodal site; the International Prognostic Index (IPI) was intermediate-high risk or high risk in 30.8 percent of patients. Approximately 30 percent of patients had a history of transformed lymphoma; the rest had DLBCL alone.

Among patients who had a late relapse following an initial diagnosis of DLBCL alone, most relapsed with DLBCL (73.5%), whereas patients with a history of transformed lymphoma were slightly more likely to relapse with an indolent lymphoma compared with DLBCL (55.0% vs. 45.0%). Overall, however, the cumulative risk of DLBCL relapse over time was greater than that of an indolent lymphoma relapse. While most patients who relapsed late had a germinal center B-cell (GCB) –like lymphoma, GCB lymphomas were associated with an increased risk of relapse of an indolent lymphoma, and not DLBCL, over the activated B-cell (ABC) –like subtype.

Salvage therapies and outcomes following salvage therapy were also analyzed among late-relapsing patients. Patients relapsing with DLBCL most commonly received a platinum or cytarabine-containing salvage regimen (44%), and 40 percent had a consolidation autologous stem cell transplantation (ASCT). In patients who relapsed with an indolent lymphoma, the most common second-line therapy was bendamustine-rituximab (37.5%), and approximately 20 percent of patients were consolidated with an ASCT. For all patients, the median postrelapse survival was 38.9 months; relapse with DLBCL was associated with a shorter survival than relapse with an indolent lymphoma (29.9 months vs. not reached). Following ASCT, median post-transplantation survival was 2.2 years.