Diffuse large B-cell lymphoma: 10 years' real-world clinical experience with rituximab plus cyclophosphamide, doxorubicin, vincristine and prednisolone
- Authors:
- Published online on: January 11, 2018 https://doi.org/10.3892/ol.2018.7774
- Pages: 3602-3609
-
Copyright: © Horvat et al. This is an open access article distributed under the terms of Creative Commons Attribution License.
Abstract
Introduction
Diffuse large B-cell lymphoma (DLBCL) is the most common subtype of non-Hodgkin lymphomas, constituting up to 40% of cases globally (1). Global epidemiological data on DLBCL are limited, but the estimated incidence is 7 per 100,000 in the USA (2). In Slovenia, the annual incidence of non-Hodgkin lymphomas was 374 in 2013 (3); 36% of these cases are believed to be DLBCL (3) Although most commonly observed in older patients, DLBCL can affect any age group, including children (4).
DLBCL is an aggressive condition and many patients have advanced disease at diagnosis (5). The prognosis of a patient with DLBCL can be predicted using their International Prognostic Index (IPI) score. The IPI score is calculated based on age, serum lactate dehydrogenase level, Eastern Cooperative Oncology Group performance score, disease stage, and the number of extranodal disease sites (6).
Treatment for patients with DLBCL generally consists of a combination of chemotherapy [cyclophosphamide, doxorubicin, vincristine and prednisolone (CHOP)] and rituximab (R-CHOP). Although many clinical trials have demonstrated the efficacy and tolerability of R-CHOP in patients with DLBCL, (7–9) less is known about the use of this regimen in the real-world setting.
Real-world studies can complement the results of clinical trials and provide additional information that can help guide physicians making treatment decisions. Clinical trial data may not be generalizable to the broad range of patients commonly encountered in the clinical setting, as they may be limited to younger patients with good baseline characteristics. Patients encountered in real-world clinical practice may be older and have comorbidities that would have excluded their participation in rigorously designed clinical trials. Consequently, real-world studies can provide a valuable insight into these less widely studied patients.
We previously described the real-world use of R-CHOP in patients with DLBCL in Slovenia (10). We now present the results of extended follow-up in an expanded patient group.
Materials and methods
This was a single-center retrospective database analysis
Records were searched for all patients with DLBCL who were treated at the Institute of Oncology Ljubljana between 2004 and 2013 for inclusion in this analysis.
All procedures followed in this study were in accordance with the ethical standards of the responsible committee on human experimentation (institutional and national) and the Helsinki Declaration of 1975, as revised in 2000. Individual patient consent was not collected for this study as this was a retrospective database analysis and the institutional informed consent form for treatment included consent to use the patient's data, materials and/or test results for research purposes. The study was approved as such by the institutional review board of the Institute of Oncology Ljubljana.
Patient characteristics, pathohistological diagnosis, disease stage, and response to treatment were taken from patient records. Survival data were retrieved from the Cancer Registry of the Republic of Slovenia [www.slora.si]. Treatment response was evaluated according to Cheson criteria, with the exception of criteria regarding positron-emission tomography (PET) evaluation, which was not routinely used in Slovenia before January 2016 (11). Progression-free survival (PFS) and Overall survival (OS) were calculated using Kaplan-Meier survival curves. PFS, which was determined for patients receiving first-line treatment only, was defined as the time from the beginning of treatment to disease progression for patients achieving complete or partial remission; OS was defined as the time from the beginning of treatment to the time of death or the end of observation for all patients.
Patients were categorized according to IPI (6) and revised IPI (R-IPI) (12) scores. We also compared younger patients (aged <60 years) with good (IPI 0 or 1) vs. poor (IPI ≥2) prognosis and we compared older (aged ≥60 years) vs. younger (aged <60 years) patients. Statistically significant differences were calculated using log-rank and χ2 tests.
Results
Patients
Between 2004 and 2013, 624 patients with DLBCL were treated at the Institute of Oncology Ljubljana, Slovenia. The diagnosis of DLBCL was established histologically in 523 patients (84%) and cytologically in 101 patients (16%). Patient characteristics are summarized in Table I.
All patients received first-line chemotherapy; 607 patients (97%) whose tumors were CD20 positive received rituximab with their chemotherapy. Chemotherapy consisted of CHOP or a CHOP-like regimen in 575 patients (92%); a further 32 patients (5%) received another non-anthracycline chemotherapy regimen in combination with rituximab and the remaining 17 patients (3%) received chemotherapy alone. A total of 136 patients (22%) received second-line therapy and 56 patients (9%) received third-line therapy. The average number of treatment cycles was 6.7 in the first line, 3.7 in the second line, and 2.4 in the third line. Overall, 26 patients (4%) were receiving maintenance or consolidation treatment with rituximab because of an associated follicular lymphoma component to their disease.
IPI risk category and R-IPI prognosis category were assessed in 573 patients. When categorized according to the IPI system, 170 patients (30%) were considered ‘low’ risk, 134 (23%) were ‘low-intermediate’ risk, 129 (23%) were ‘high-intermediate’ risk, and 140 (24%) were ‘high’ risk. According to the R-IPI prognostic system, 59 patients (10%) fell into the ‘very good’ prognosis group, 245 patients (43%) into the ‘good’ prognosis group, and 269 patients (47%) into the ‘poor’ prognosis group.
Response to treatment
The median follow-up time was 45.3 months (range, 0.1–143.0 months). The overall response rate in all patients was 90%. In the IPI ‘low-risk’ group, 168 patients (99%) had a complete or partial response. The overall response rates in the ‘low-intermediate’, ‘high-intermediate’, and ‘high-risk’ groups were 94, 87, and 79%, respectively (χ2 test; P<0.0001) (Table II). In the R-IPI ‘very good’ prognosis group, 59 patients (100%) had a complete or partial response (Table II). The overall response rates in the R-IPI ‘good’ and ‘poor’ prognosis groups were 96 and 83%, respectively; the difference between R-IPI groups was statistically significant (P<0.0001).
Progression-free survival
PFS was only determined in patients undergoing first-line treatment. The median PFS was not reached in the overall population, as shown in Table III, nor in any of the subgroups analyzed. PFS according to IPI and R-IPI category is shown in Fig. 1; PFS rates are shown in Table III. Among patients classified as IPI ‘low risk’, 75% were progression-free 10 years after treatment; 10-year PFS rates in the ‘low-intermediate’, ‘high-intermediate’, and ‘high-risk’ groups were 75, 64, and 71%, respectively. Among those classified as having an R-IPI ‘very good’ prognosis, 84% were progression-free at 10 years after treatment; 10-year PFS rates in the good and poor prognosis groups were 73 and 66%, respectively. The PFS difference between groups was statistically significant for the IPI (log-rank P=0.01) and R-IPI groups (P=0.001).
When analyzed according to age alone, no statistically significant difference was seen in PFS rates between older and younger patients. Survival outcomes were also evaluated in younger patients (aged <60 years) with good vs. poor prognosis (IPI 0 or 1 and IPI ≥2, respectively) (Table IV and Fig. 2). PFS rates were similar in both groups of patients.
Overall survival
OS was determined in all patients undergoing treatment. The median OS was 124 months in the overall population. OS according to IPI and R-IPI category is shown in Fig. 1; OS rates are shown in Table V. Among patients classified as having an IPI ‘low risk’, 80% were alive at 10 years; the 10-year OS rates in the ‘low-intermediate’, ‘high-intermediate’, and ‘high-risk’ groups were 60, 43, and 30%, respectively. Ten-year OS for the R-IPI ‘very good prognosis’ group was 87%; 10-year rates in the good and poor prognosis groups were 67 and 37%, respectively. Between-group differences were statistically significant for OS for the IPI (log-rank test P<0.0001) and R-IPI groups (log-rank test P<0.0001).
Median OS was not reached in younger patients and was 81 months in older patients. The difference in OS rates between the younger and older groups was statistically significant (P<0.0001). Regarding OS in younger patients (aged <60 years), outcomes were statistically significantly better in those with a good vs. poor prognosis (IPI 0 or 1 vs. IPI ≥2, respectively) (P=0.001; Table IV and Fig. 2).
Discussion
Long-term follow-up data for patients with DLBCL are scarce, particularly among patients treated in the real-world setting. We have described the use of rituximab-based regimens in over 600 patients of varying ages and disease stages over a prolonged follow-up period. To the best of our knowledge, no other studies have assessed outcomes in patients with DLBCL in the real-world setting.
In our patient population, an overall 10-year PFS rate of 72% was observed, ranging from 64% in patients classed according to IPI as ‘high-intermediate’ risk (IPI 3) to 75% in patients with low risk (IPI 0 or 1) and from 66% in patients with R-IPI poor prognosis (R-IPI 3–5) to 84% in those with very good prognosis (R-IPI 0). Median PFS was not reached in any of the IPI risk categories. PFS rates were numerically but not statistically significantly higher in patients aged <60 years compared with those aged ≥60 years, with 79% of younger patients and 70% of older patients free from progression after 10 years. Coiffier et al reported a 10-year PFS rate of 37% in their group of patients aged 60–80 years in the LNH-98.5 trial (13) lower than the 10-year rates seen in our older patients. The median PFS was 4.8 years in the LNH-98.5 trial; median PFS has not yet been reached in our group of patients after a median follow-up of 45 months. However, differences between the two patient populations and study designs call for caution when comparing the results of the two studies.
With regard to OS, we observed a 10-year OS rate of 51% in the overall population and 41% in older patients, the latter being comparable with the 43.5% reported for patients aged ≥60 years in the LNH-98.5 study (13). Purroy et al reported a 10-year OS rate of 64% in their group of patients with DLBCL, with little difference between older and younger patients (64% for those aged <60 years and 63% for those aged ≥60 years) in contrast to the present study (14). They also reported a 10-year OS rate of 59% in patients with high-risk disease (IPI score ≥3), somewhat higher than the rates we observed in our patients. Once again, however, cross-study comparisons are complicated by many factors, including differences in the treatment settings and patient populations.
We observed a statistically significant difference in OS between younger patients with good vs. poor prognosis, with 10-year OS rates of 87 and 67%, respectively. This was in line with our observations at the 5-year timepoint (10). Younger, high-risk patients clearly represent a population for whom better treatment options are needed. Intensive regimens such as R-CHOEP-14 (rituximab, cyclophosphamide, doxorubicin, vincristine, etoposide, and prednisolone) and megaCHOEP (high-dose cyclophosphamide, doxorubicin, vincristine, etoposide, and prednisolone) (15,16) and R-ACVBP (rituximab, doxorubicin, vindesine, cyclophosphamide, bleomycin, and prednisolone) (17) are frequently used (18) but have not been shown to be superior to R-CHOP in this patient population (19). Consequently, European treatment guidelines currently recommend recruitment into clinical trials for young ‘high-risk’ and ‘high-intermediate’ risk patients (18). In the activated B-cell subtype of DLBCL that is more commonly seen in older patients, the addition of bortezomib, lenalidomide, or ibrutinib to standard therapy has provided encouraging indications of activity in early (20,21). Results from ongoing studies such as ROBUST (NCT02285062) and PHOENIX (NCT01855750) will provide an indication as to whether this is a valid approach for this poor-prognosis group of patients.
A plateau was observed in our PFS curves according to IPI category, with few relapses after 6 years in patients with ‘low-intermediate’ and ‘high-risk’ disease. This mirrors observations in the LNH-98.5 study (13). In contrast, an analysis of the SWOG S8736 and S0014 studies, which only included patients with limited-stage disease, revealed a pattern of late relapse in those patients (22). Patients with limited-stage disease comprised 40% of our patient population; in our group of ‘low-risk’ patients, some evidence of late disease progression was evident at 5–7 years post therapy, highlighting the need for continued observation of these patients.
Five-year OS rates ranged from 86% in IPI ‘low-risk’ patients to 45% in IPI ‘high-risk’ patients. Our OS rates were higher than the 5-year OS rates reported for patients in a large validation study by Olszewski et al those authors reported 5-year OS of 74, 58, 49, and 33% for ‘low-risk’, ‘low-intermediate’, ‘high-intermediate’ and ‘high-risk’ patients, compared with 86, 67, 58, and 45%, respectively, in the present study (23). Five-year OS rates in our study were higher in all three R-IPI categories compared with the validation study (‘very good’ prognosis: 96% vs. 87%; ‘good’ prognosis: 73% vs. 64%; ‘poor’ prognosis: 51% vs. 41%, respectively), differences that may have been due to the characteristics of the two patient populations.
Some limitations of the present study should be considered in addition to those inherent in retrospective observational studies. PET was not used for disease staging until 2016; consequently, some patients may have been understaged at diagnosis. Since the introduction of diagnostic PET, we have observed discrete paraspinal lymphomatous masses in some patients that might have been overlooked with computed tomography. This has the potential to affect our survival data.
Although many studies have examined the efficacy of R-CHOP and similar regimens in patients with DLBCL, real-world data are scarce for these patients. We have shown that many patients treated with R-CHOP and R-CHOP-like regimens in the real-world setting can have excellent outcomes; however, accurate disease staging is essential to confidently assign prognostic scores and assess likely outcomes for patients.
Acknowledgements
The present study was supported by the Slovenian Ministry of Higher Education, Science and Technology (grant no. P3-0321). Support for third-party editorial assistance for this manuscript was provided by F. Hoffmann-La Roche, Ltd.
References
|
World Health Organization, . Diffuse large B-cell lymphoma. http://www.who.int/selection_medicines/committees/expert/20/applications/DiffuseLargeBCellLymphoma.pdf16–December. 2016 | |
|
Li Y, Wang Y, Wang Z, Yi D and Ma S: Racial differences in three major NHL subtypes: Descriptive epidemiology. Cancer Epidemiol. 39:8–13. 2015. View Article : Google Scholar : PubMed/NCBI | |
|
Cancer in Slovenia 2013, . Ljubljana: Institute of Oncology Ljubljana, Epidemiology and Cancer Registry. http://www.onko-i.si/fileadmin/onko/datoteke/dokumenti/RRS/LP_2013.pdf8–March. 2017 | |
|
Cairo MS and Perkins SL: Hematological Malignancies in Children, Adolescents and Young Adults. First edition. World Scientific Publishing Co.; Singapore: 2012, View Article : Google Scholar | |
|
Sehn LH and Gascoyne RD: Diffuse large B-cell lymphoma: Optimizing outcome in the context of clinical and biologic heterogeneity. Blood. 125:22–32. 2015. View Article : Google Scholar : PubMed/NCBI | |
|
International Non-Hodgkin's Lymphoma Prognostic Factors Project: A predictive model for aggressive non-Hodgkin's lymphoma. N Engl J Med. 329:987–994. 1993. View Article : Google Scholar : PubMed/NCBI | |
|
Coiffier B, Lepage E, Brier J, Herbrecht R, Tilly H, Bouabdallah R, Morel P, Van Den Neste E, Salles G, Gaulard P, et al: CHOP chemotherapy plus rituximab compared with CHOP alone in elderly patients with diffuse large-B-cell lymphoma. N Engl J Med. 346:235–242. 2002. View Article : Google Scholar : PubMed/NCBI | |
|
Habermann TM, Weller EA, Morrison VA, Gascoyne RD, Cassileth PA, Cohn JB, Dakhil SR, Woda B, Fisher RI, Peterson BA and Horning SJ: Rituximab-CHOP versus CHOP alone or with maintenance rituximab in older patients with diffuse large B-cell lymphoma. J Clin Oncol. 24:3121–3127. 2006. View Article : Google Scholar : PubMed/NCBI | |
|
Pfreundschuh M, Trümper L, Österborg A, Pettengell R, Trneny M, Imrie K, Ma D, Gill D, Walewski J, Zinzani PL, et al: CHOP-like chemotherapy plus rituximab versus CHOP-like chemotherapy alone in young patients with good-prognosis diffuse large-B-cell lymphoma: A randomised controlled trial by the MabThera International Trial (MInT) Group. Lancet Oncol. 7:379–391. 2006. View Article : Google Scholar : PubMed/NCBI | |
|
Gregoric B, Zadnik V and Novakovic Jezersek B: The diffuse large B-cell lymphoma-where do we stand now in everyday clinical practice. Radiol Oncol. 46:153–159. 2012. View Article : Google Scholar : PubMed/NCBI | |
|
Cheson BD, Fisher RI, Barrington SF, Cavalli F, Schwartz LH, Zucca E and Lister TA: Alliance, Australasian Leukaemia and Lymphoma Group; Eastern Cooperative Oncology Group; European Mantle Cell Lymphoma Consortium: Recommendations for initial evaluation, staging, and response assessment of Hodgkin and non-Hodgkin lymphoma: The Lugano classification. J Clin Oncol. 32:3059–3068. 2014. View Article : Google Scholar : PubMed/NCBI | |
|
Sehn LH, Berry B, Chhanabhai M, Fitzgerald C, Gill K, Hoskins P, Klasa R, Savage KJ, Shenkier T, Sutherland J, et al: The revised international prognostic index (R-IPI) is a better predictor of outcome than the standard IPI for patients with diffuse large B-cell lymphoma treated with R-CHOP. Blood. 109:1857–1861. 2007. View Article : Google Scholar : PubMed/NCBI | |
|
Coiffier B, Thieblemont C, Van Den Neste E, Lepeu G, Plantier I, Castaigne S, Lefort S, Marit G, Macro M, Sebban C, et al: Long-term outcome of patients in the LNH-98.5 trial, the first randomized study comparing rituximab-CHOP to standard CHOP chemotherapy in DLBCL patients: A study by the Groupe d'Etudes des Lymphomes de l'Adulte. Blood. 116:2040–2045. 2010. View Article : Google Scholar : PubMed/NCBI | |
|
Purroy N, Bergua J, Gallur L, Prieto J, Lopez LA, Sancho JM, García-Marco JA, Castellví J, Montes-Moreno S, Batlle A, et al: Long-term follow-up of dose-adjusted EPOCH plus rituximab (DA-EPOCH-R) in untreated patients with poor prognosis large B-cell lymphoma. A phase II study conducted by the Spanish PETHEMA Group. Br J Haematol. 169:188–198. 2015. View Article : Google Scholar : PubMed/NCBI | |
|
Holte H, Leppä S, Björkholm M, Fluge O, Jyrkkiö S, Delabie J, Sundström C, Karjalainen-Lindsberg ML, Erlanson M, Kolstad A, et al: Dose-densified chemoimmunotherapy followed by systemic central nervous system prophylaxis for younger high-risk diffuse large B-cell/follicular grade 3 lymphoma patients: Results of a phase II Nordic Lymphoma Group study. Ann Oncol. 24:1385–1392. 2013. View Article : Google Scholar : PubMed/NCBI | |
|
Schmitz N, Nickelsen M, Ziepert M, Haenel M, Borchmann P, Schmidt C, Viardot A, Bentz M, Peter N, Ehninger G, et al: Conventional chemotherapy (CHOEP-14) with rituximab or high-dose chemotherapy (MegaCHOEP) with rituximab for young, high-risk patients with aggressive B-cell lymphoma: An open-label, randomised, phase 3 trial (DSHNHL 2002–1). Lancet Oncol. 13:1250–1259. 2012. View Article : Google Scholar : PubMed/NCBI | |
|
Fitoussi O, Belhadj K, Mounier N, Parrens M, Tilly H, Salles G, Feugier P, Ferme C, Ysebaert L, Gabarre J, et al: Survival impact of rituximab combined with ACVBP and upfront consolidation autotransplantation in high-risk diffuse large B-cell lymphoma for GELA. Haematologica. 96:1136–1143. 2011. View Article : Google Scholar : PubMed/NCBI | |
|
Tilly H, da Silva Gomes M, Vitolo U, Jack A, Meignan M, Lopez-Guillermo A, Walewski J, André M, Johnson PW, Pfreundschuh M, et al: Diffuse large B-cell lymphoma (DLBCL): ESMO clinical practice guidelines for diagnosis, treatment and follow-up. Ann Oncol. 5 Suppl 26:v116–v125. 2015. View Article : Google Scholar | |
|
Le Gouill S, Milpied JN, Lamy T, Delwail V, Gressin R, Guyotat D, Damaj GL, Foussard C, Cartron G, Maisonneuve H, et al: First-line rituximab (R) high-dose therapy (R-HDT) versus R-CHOP14 for young adults with diffuse large B-cell lymphoma: Preliminary results of the GOELAMS 075 prospective multicenter randomized trial. J Clin Oncol. 29 Suppl 15:S80032011. View Article : Google Scholar | |
|
Wilson WH, Young RM, Schmitz R, Yang Y, Pittaluga S, Wright G, Lih CJ, Williams PM, Shaffer AL, Gerecitano J, et al: Targeting B cell receptor signalling with ibrutinib in diffuse large B cell lymphoma. Nat Med. 21:922–926. 2015. View Article : Google Scholar : PubMed/NCBI | |
|
Hong JY, Suh C and Kim WS: Evolution of frontline treatment of diffuse large B-cell lymphoma: A brief review and recent update. F1000Res. 5:pii: F1000 Faculty Rev-1933. 2016. View Article : Google Scholar : PubMed/NCBI | |
|
Stephens DM, Li H, LeBlanc ML, Puvvada SD, Persky D, Friedberg JW and Smith SM: Continued risk of relapse independent of treatment modality in limited-stage diffuse large B-cell lymphoma: Final and long-term analysis of Southwest Oncology Group Study S8736. J Clin Oncol. 34:2997–3004. 2016. View Article : Google Scholar : PubMed/NCBI | |
|
Olszewski AJ, Winer ES and Castillo JJ: Validation of clinical prognostic indices for diffuse large B-cell lymphoma in the national cancer data base. Cancer Causes Control. 26:1163–1172. 2015. View Article : Google Scholar : PubMed/NCBI |
