Abstract
Mantle cell lymphoma is included in the World Health Organization classification as distinct lymphoma subtype characterized by the t(11;14)(q13;q32) translocation, which results in overexpression of Cyclin D1. The clinical presentation often includes extranodal involvement, particularly of the bone marrow and gut. The prognosis of patients with mantle cell lymphoma (median overall survival, 3-5 years) is poorest among B-cell lymphoma patients, even though a prospectively difficult to identify subgroup can survive for years with little or no treatment. Conventional chemotherapy is not curative but obtains frequent remissions (60%-90%) which are usually shorter (1-2 years) compared with other lymphoma entities. Very intensive regimens, including autologous and allogeneic stem cell transplantation, seem required to improve the outcome, but with the median age of diagnosis being 60 years or more, such approaches are feasible only in a limited proportion of patients. The possibility of treating patients based on prognostic factors needs to be investigated prospectively.
Introduction
The lymphoma nowadays included in the WHO classification with the name “mantle cell lymphoma” (MCL)1 was first described by K. Lennert more than 30 years ago, and subsequently defined “centrocytic lymphoma” in the Kiel classification,2 but MCL was finally accepted as a separate entity only in the early 1990s, when it became evident that the t(11,14)(q13;q32) translocation was consistently present.3,4
Histologic diagnosis
The term MCL derives from the growth pattern of this lymphoma in its early stages, with neoplastic cells surrounding residual reactive germinal centers and replacing the normal follicle mantle (mantle zone pattern).5 At more advanced stages of tumor infiltration, MCL cells in the lymph nodes may show a vaguely nodular, or a diffuse, growth pattern.1,6
The classic cytologic appearance of MCL is a monomorphic proliferation of small- to medium-sized lymphoid cells with irregular nuclear contours and inconspicuous nucleoli.1 Four cytologic variants of MCL can be recognized, including the small cell variant, the marginal zone–like variant, the blastoid variant, and the pleomorphic variant.1,6 The blastoid and pleomorphic variants are considered to be associated with a poorer prognosis.1
The histologic diagnosis can be difficult, and immunophenotyping is usually required (Table 1). MCL cells express mature B-cell markers and IgM and/or IgD surface immunoglobulins (Igs). They are usually expressing CD5 but are negative for CD10 and BCL6. BCL2 protein is usually expressed, and Cyclin D1 expression, which is ectopically expressed because of the presence of the t(11;14)(q13;q32) translocation, can be shown in nearly all cases (including the very infrequent cases with aberrant CD5-negative phenotype). However, the immunohistochemistry efficiency in determining Cyclin D1 overexpression could be hampered by the quality of available material. Thus, fluorescence in situ hybridization (Figure 1) is the technique of choice to demonstrate the presence of the translocation t(11;14). Polymerase chain reaction (PCR) with primers directed to the breakpoint regions on 11q13 and 14q32 has a high false-negative rate (40%-60%); when positive, however, it is an excellent tool for molecular follow-up studies.6 These can be useful for the evaluation of the activity of new drugs or treatment strategies, whereas in clinical practice we abandoned this analysis, being expensive, time-consuming, and not useful for clinical decisions.
Main immunohistochemical markers enabling the distinction of MCL from other lymphomas
| Histologic subtype | CD5 | CD23 | CD43 | CD10 | BCL6 | Cyclin D1 | sIg | sIg type | cIg |
|---|---|---|---|---|---|---|---|---|---|
| MCL | + | − | + | − | − | + | + | M ± D | − |
| Follicular lymphoma | − | −/+ | − | +/− | + | − | + | G ± M | − |
| Small lymphocytic lymphoma/CLL | + | + | + | − | − | − | + | M ± D | −/+ |
| Lymphoplasmacytic lymphoma | − | − | −/+ | − | − | − | +/− | M | + |
| Splenic marginal zone lymphoma | − | − | − | − | − | − | + | M+ D | −/+ |
| Extranodal marginal zone lymphoma (MALT type) | − | −/+ | −/+ | − | − | − | + | M | +/− |
| Histologic subtype | CD5 | CD23 | CD43 | CD10 | BCL6 | Cyclin D1 | sIg | sIg type | cIg |
|---|---|---|---|---|---|---|---|---|---|
| MCL | + | − | + | − | − | + | + | M ± D | − |
| Follicular lymphoma | − | −/+ | − | +/− | + | − | + | G ± M | − |
| Small lymphocytic lymphoma/CLL | + | + | + | − | − | − | + | M ± D | −/+ |
| Lymphoplasmacytic lymphoma | − | − | −/+ | − | − | − | +/− | M | + |
| Splenic marginal zone lymphoma | − | − | − | − | − | − | + | M+ D | −/+ |
| Extranodal marginal zone lymphoma (MALT type) | − | −/+ | −/+ | − | − | − | + | M | +/− |
MCL differential diagnosis is not always straightforward, and immunohistochemical studies are usually needed: the most typical immunophenotypic features of indolent mature B-cell neoplasms are summarized.
sIg indicates surface immunoglobulin; cIg, cytoplasmic immunoglobulin; +, > 90% positive; +/−, > 50% positive; −/+, < 50% positive; and −, < 10% positive.
Fluorescence in situ hybridization analysis on interphase and metaphase nuclei (using the LSI IGH/CCND1 XT dual-color, dual-fusion translocation DNA probe) identifying the presence of the t(11;14)(q13;q32) chromosomal translocation. Interphase nuclei are shown in the left panel. One orange (CCND1 on chromosome 11q13), one green (IGH on chromosome 14q32), and 2 fusion signal patterns (der(11) and der(14), indicating the chromosomal rearrangements produced by the translocation) can be observed.
Fluorescence in situ hybridization analysis on interphase and metaphase nuclei (using the LSI IGH/CCND1 XT dual-color, dual-fusion translocation DNA probe) identifying the presence of the t(11;14)(q13;q32) chromosomal translocation. Interphase nuclei are shown in the left panel. One orange (CCND1 on chromosome 11q13), one green (IGH on chromosome 14q32), and 2 fusion signal patterns (der(11) and der(14), indicating the chromosomal rearrangements produced by the translocation) can be observed.
Molecular pathogenesis
The genetic hallmark of MCL is the t(11;14)(q13;q32) that fuses the Ig heavy chain enhancer-promoter to the transcription unit of the proto-oncogene CCND1, encoding Cyclin D1.7 The translocation determines the ectopic and deregulated expression of Cyclin D1, which is considered the primary molecular event in the pathogenesis of MCL, but additional oncogenic events are involved in MCL tumor progression. Comparative genomic hybridization and array-based genomic studies have shown a variety of altered chromosomal regions in MCL, with genomic losses containing the loci of tumor suppressor genes (including ATM, CDKN2A, TP53) and gains involving oncogenes (eg, MYC, SYK, BCL2). The presence of ataxia-telangiectasia mutated or cell-cycle checkpoint kinase 2 inactivating mutations in the germline of some MCL patients suggests that they can be implicated in development of the tumor and a model of multistep clinicopathologic and molecular pathogenesis, and progression has been proposed (Figure 2).8
Model of molecular pathogenesis and progression of MCL proposed by Jares et al.8 Ataxia-telangiectasia mutated or cell-cycle checkpoint kinase 2 inactivating mutations have been found in the germline of some MCL patients, and it has been suggested that these mutations may facilitate the lymphoma development. The t(11;14)(q13;q32) translocation occurs in an immature B cell and results in the ectopic and deregulated expression of Cyclin D1, and early expansion of tumor B cells in the mantle zone areas of lymphoid follicles. This translocation is considered a primary pathogenetic event that deregulates the cell-cycle control, probably by overcoming the suppressor effect of retinoblastoma 1 (RB1) and the cell-cycle inhibitor p27. Acquired inactivation of DNA damage response pathways may then facilitate additional oncogenic events and the development of classic MCL. Further genetic alterations may target genes of the cell-cycle and survival regulatory pathways, leading to more proliferative and aggressive variants. Adapted from Jares et al8 with permission.
Model of molecular pathogenesis and progression of MCL proposed by Jares et al.8 Ataxia-telangiectasia mutated or cell-cycle checkpoint kinase 2 inactivating mutations have been found in the germline of some MCL patients, and it has been suggested that these mutations may facilitate the lymphoma development. The t(11;14)(q13;q32) translocation occurs in an immature B cell and results in the ectopic and deregulated expression of Cyclin D1, and early expansion of tumor B cells in the mantle zone areas of lymphoid follicles. This translocation is considered a primary pathogenetic event that deregulates the cell-cycle control, probably by overcoming the suppressor effect of retinoblastoma 1 (RB1) and the cell-cycle inhibitor p27. Acquired inactivation of DNA damage response pathways may then facilitate additional oncogenic events and the development of classic MCL. Further genetic alterations may target genes of the cell-cycle and survival regulatory pathways, leading to more proliferative and aggressive variants. Adapted from Jares et al8 with permission.
Clinical features
In Western countries, MCL accounts for approximately 3% to 10% of all cases of non-Hodgkin lymphoma,11,12 with a striking predominance of the male sex (∼ 2:1 or greater in all series). The patients have a median age of 60 to 65 years and typically present with generalized nonbulky lymphadenopathy. Most cases are diagnosed at advanced Ann Arbor stage, and extranodal involvement is very frequent. Most common extranodal sites include bone marrow, liver, spleen, the Waldeyer ring, and the gastrointestinal tract, this latter often with the appearance of a multiple lymphomatous polyposis of the intestine. A clearly leukemic blood picture is not uncommon, and some degree of peripheral blood involvement can be detected in nearly all cases by flow cytometry.13 Skin involvement is usually a manifestation of disseminated disease and is often associated with blastoid cytologic features.14 Symptomatic involvement of the central nervous system is exceedingly rare at presentation, but relapses in the central nervous system have been reported in 4% to 22% in retrospective series,15 more frequently in patients with blastoid histology16 and in the very rare subset of Cyclin D1–negative MCL.17
The clinical course is often indolent or moderately aggressive at diagnosis, with few or no symptoms and a good performance status, but with time the disease invariably become clinically aggressive and chemotherapy refractory, showing the worst long-term survival among all B-cell lymphoma subtypes18 (Figure 3). The median survival in most published series was in the range of 3 years in the past decades and has been reported to have risen to 5 years in most recent times.19 However, a subset of patients may show prolonged indolent behavior and a longer survival. Unfortunately, there are no reliable tools to prospectively identify these cases.
Cause-specific survival of the main B-cell lymphoma subtypes in the series of the Oncology Institute of Southern Switzerland, 1980-2006. MZL indicates marginal zone lymphoma; and DLCL, diffuse large cell lymphoma.
Cause-specific survival of the main B-cell lymphoma subtypes in the series of the Oncology Institute of Southern Switzerland, 1980-2006. MZL indicates marginal zone lymphoma; and DLCL, diffuse large cell lymphoma.
Prognostic factors
The choice of the best treatment for each individual patient and the proper evaluation of the novel therapeutic options requires the possibility of stratifying the patients according to their individual risk of relapse and death. Gene expression analysis profiles identified a cohort of 20 “proliferation signature” genes that predict patient survival,20 but this approach cannot be applied in daily practice. A PCR-based surrogate method based on a 5-gene model and which can as well be applied on paraffin-embedded tissue has been recently proposed,21 but it still needs proper validation. In addition to the common lymphoma indicators of prognosis (extranodal involvement, stage, age, performance status, lactic dehydrogenase), the Ki-67 proliferation index seems the most powerful predictor of survival in MCL also in the rituximab era.5,22 A blastoid morphology has often been associated with poorer outcome,23 whereas the influence of the growth pattern on survival is less clear.24-26 The utility of the International Prognostic Index is controversial, but recently a specific MCL prognostic score (Mantle Cell International Prognostic Index) has been proposed.27 This score, based on the study of 455 patients only (the International Prognostic Index and the Follicular Lymphoma International Prognostic Index as a comparison are based on series of thousands of cases), identified 4 independent prognostic factors (age, performance status, lactic dehydrogenase, and leukocyte count) that can be used to stratify patients into 3 risk groups with an overall survival (OS) of approximately 2 (high risk), 4 (intermediate) and 6 years (low risk).
Leukemic presentation and splenomegaly have been considered adverse prognostic indicators28 ; however, recent data suggest that, if associated with the lack of nodal disease (especially if showing small cell variant morphology), they may indicate a subset of patients with particularly indolent behavior.29,30
All the aforementioned prognostic factors correlate with survival, but none of them was validated as a tool for the selection of therapy.
Staging procedures
Standard staging procedures include routine laboratory analysis, bone marrow examination as well as immunophenotyping by flow cytometry of bone marrow and peripheral blood, computed tomography scan of the chest, the abdomen and the pelvis. There is very limited information on the use of [18F]fluorodeoxyglucose positron emission tomography in MCL31-33 hence, at present, the use of [18F]fluorodeoxyglucose positron emission tomography in MCL should still be considered investigational.
Cerebrospinal fluid evaluation is not usually required at presentation for MCL patients with classic morphology, unless neurologic symptoms are present. However, careful cerebrospinal fluid examination by cytology and flow cytometry should be considered in the initial staging of patients with the blastoid variant.16
Gastrointestinal involvement is a common feature, which however may not necessarily be symptomatic at presentation and can therefore be easily missed if endoscopy studies are not performed. Gastrointestinal symptoms are present in approximately one-fourth of patients but, when baseline endoscopy studies are performed, gastrointestinal tract involvement can be found in up to 80% of cases, often in biopsies from macroscopically normal mucosa.34,35 Although not an essential examination, because of the modest impact on therapeutic decisions,34 we usually perform upper and lower endoscopy in all patients who are fit enough to tolerate it, with the purpose of better defining the indication to localized treatment in the rare patients with early stage disease and for the purpose of better documenting complete response (CR) in patients included into clinical trials.
Therapy
There are few solid data on how to treat MCL. This surprising fact is the result of the recent definition of the disease, its relatively low incidence and the lack, until very recently, of a reliable and specific prognostic score27 that can be used in comparing data from different trials. The approach to treatment is largely based on the common belief that the disease is aggressive, although a survival of 86% at 3 years and a median overall survival of 7 years was recently described in a nonaggressively treated cohort.36 While planning treatment for a new patient with MCL, physicians face several open questions, which are addressed in the following sections.
Best combination chemotherapy regimen
The active regimens in MCL are the same that are used for other lymphoma entities: alkylators-based (COP/CVP),37-41 anthracycline-based (CHOP),37-39 cladribine-42 or fludarabine-based (FC, FCM),43 or, more recently, bendamustine-based (BOP)44 regimens, usually combined with rituximab.45 The data summarizing the outcome of the chemotherapy regimens most commonly used in first line are presented in Table 237-40,46-48 The majority of prospective data are available for CVP or CHOP-like regimens because fludarabine- or cladribine-based regimens42,43 were used only for patients not considered for autologous transplantation.
Large (≥ 30 patients) prospective studies of combination regimens for MCL in first line
| Regimen | Reference (year) | N | ORR, % | CRR, % | PFS/EFS, months | 2-Year OS, % |
|---|---|---|---|---|---|---|
| COP/CVP | Meusers et al37 (1989) | 37 | 84 | 22 | 10 | 65 |
| Teodorovic et al40 (1995) | 35 | 60 | 40 | 20 | 45 | |
| Unterhalt et al41 (1996) | 46 | 83 | 18 | — | — | |
| CHOP | Meusers et al37 (1989) | 26 | 88 | 38 | 7 | 60 |
| Lenz et al38 (2005) | 60 | 75 | 7 | 19 | 76 | |
| Nickenig et al39 (2006) | 46 | 87 | 15 | 21 | 85 | |
| MCP | Nickenig et al39 (2006) | 40 | 73 | 20 | 15 | 85 |
| Herold et al48 (2008) | 46 | 63 | 15 | 13 | — | |
| R-MCP | Herold et al48 (2008) | 44 | 71 | 32 | 18 | — |
| R-CHOP | Lenz et al38 (2005) | 62 | 94 | 34 | 20 | 76 |
| Howard et al47 (2002) | 40 | 96 | 48 | 17 | — | |
| VcR-CVAD | Kahl et al46 (2008) | 30 | 90 | 77 | 73% at 18 months | 97% at 18 months |
| Regimen | Reference (year) | N | ORR, % | CRR, % | PFS/EFS, months | 2-Year OS, % |
|---|---|---|---|---|---|---|
| COP/CVP | Meusers et al37 (1989) | 37 | 84 | 22 | 10 | 65 |
| Teodorovic et al40 (1995) | 35 | 60 | 40 | 20 | 45 | |
| Unterhalt et al41 (1996) | 46 | 83 | 18 | — | — | |
| CHOP | Meusers et al37 (1989) | 26 | 88 | 38 | 7 | 60 |
| Lenz et al38 (2005) | 60 | 75 | 7 | 19 | 76 | |
| Nickenig et al39 (2006) | 46 | 87 | 15 | 21 | 85 | |
| MCP | Nickenig et al39 (2006) | 40 | 73 | 20 | 15 | 85 |
| Herold et al48 (2008) | 46 | 63 | 15 | 13 | — | |
| R-MCP | Herold et al48 (2008) | 44 | 71 | 32 | 18 | — |
| R-CHOP | Lenz et al38 (2005) | 62 | 94 | 34 | 20 | 76 |
| Howard et al47 (2002) | 40 | 96 | 48 | 17 | — | |
| VcR-CVAD | Kahl et al46 (2008) | 30 | 90 | 77 | 73% at 18 months | 97% at 18 months |
However, both the randomized study and the interstudy comparisons suggest that no combination is superior in terms of OS. Therefore, the choice of the regimen depends chiefly on the overall goal, at which the treating physician and the patient are aiming. If an intensification with high-dose chemotherapy and peripheral blood stem cell transplantation (PBSCT) are planned and therefore a CR should be obtained, then an R-CHOP–like or even a more intensive regimen should be chosen. The CVAD regimen, including a continuous infusion of doxorubicin and hyperfractionated cyclophosphamide showed excellent results,49 which were further enhanced by the addition of rituximab and bortezomib, although at the expense of more frequent and severe neuropathy.46
Role of cytarabine (Ara-C)
As cytarabine was shown to be very active in the treatment of MCL, several investigators integrated it in first-line regimens, either as part of classic salvage combinations, such as DHAP or at high dose as used in the treatment of acute leukemia. As shown in Table 3,50-58 the addition of cytarabine improves the rate and quality of responses as well as their duration, but at the expense of a higher toxicity: approximately 5% toxic deaths, 15% severe infections, 30% severe thrombocytopenia. This option is therefore applicable only for younger patients preparing for autologous transplantation and treated in referral centers.50-57,59
Large prospective studies of cytarabine intensification for first-line MCL
| Regimen | Reference (year) | N | ORR, % | CRR, % | Toxicity grade III-IV |
|---|---|---|---|---|---|
| Hyper-CVAD/MTX-Ara-C | Khouri et al50 (1998) | 45 (20 untreated) | 93 | 38 | Thrombocytopenia 85%, infections 10% |
| Hyper-CVAD/MTX-Ara-C | Romaguera et al58 (2000) | 25 (age > 65 y) | 92 | 68 | Toxic death 8%, infections 5% |
| R-Hyper-CVAD/R-MTX-Ara-C | Romaguera et al52 (2005) | 97 | 97 | 87 | Toxic death 5%, MDS 3% |
| R-Hyper-CVAD/R-MTX-Ara-C | Epner et al53 (2007) | 49 | 88 | 58 | Toxic death 2%, hematotoxicity 87% |
| R-Hyper-CVAD/R-MTX-Ara-C | Merli et al54 (2008) | 32 | 53 | 50 | Toxic death 6%, severe infections 15% |
| R-DHAP | de Guibert et al57 (2006) | 25 | 96 | 92 | Thrombocytopenia 33% |
| CHOP × 3 + DHAP × 3 | Lefrère et al51 (2004) | 28 | 92 | 84 | — |
| R-CHOP × 3 + R-DHAP × 3 | Delarue et al55 (2008) | 60 | 95 | 61 | — |
| R-CHOP × 3 + HD-Ara-C × 1 | van't Veer et al56 (2008) | 87 | 72 | 29 | Infections 30% |
| Regimen | Reference (year) | N | ORR, % | CRR, % | Toxicity grade III-IV |
|---|---|---|---|---|---|
| Hyper-CVAD/MTX-Ara-C | Khouri et al50 (1998) | 45 (20 untreated) | 93 | 38 | Thrombocytopenia 85%, infections 10% |
| Hyper-CVAD/MTX-Ara-C | Romaguera et al58 (2000) | 25 (age > 65 y) | 92 | 68 | Toxic death 8%, infections 5% |
| R-Hyper-CVAD/R-MTX-Ara-C | Romaguera et al52 (2005) | 97 | 97 | 87 | Toxic death 5%, MDS 3% |
| R-Hyper-CVAD/R-MTX-Ara-C | Epner et al53 (2007) | 49 | 88 | 58 | Toxic death 2%, hematotoxicity 87% |
| R-Hyper-CVAD/R-MTX-Ara-C | Merli et al54 (2008) | 32 | 53 | 50 | Toxic death 6%, severe infections 15% |
| R-DHAP | de Guibert et al57 (2006) | 25 | 96 | 92 | Thrombocytopenia 33% |
| CHOP × 3 + DHAP × 3 | Lefrère et al51 (2004) | 28 | 92 | 84 | — |
| R-CHOP × 3 + R-DHAP × 3 | Delarue et al55 (2008) | 60 | 95 | 61 | — |
| R-CHOP × 3 + HD-Ara-C × 1 | van't Veer et al56 (2008) | 87 | 72 | 29 | Infections 30% |
Transplantation: when and how
Intense chemotherapy results in a high proportion of responses and CRs, but these are usually of shorter duration than in other lymphoma types. To enhance these results and with the hope of some cures, younger patients are generally consolidated with high-dose chemotherapy and PBSCT. Data of cohorts undergoing intensive induction followed by PBSCT consolidation suggest indeed a higher event-free survival (EFS) and possibly OS compared with historical controls (Table 4),50,59-65 but the only randomized study60 did not as yet reach conclusive results. All data suggest that there is no disease-free plateau and therefore probably all patients will eventually relapse. An exception is represented by the recently published Nordic trial, including 160 patients61 treated with R-maxi-CHOP alternating with HD-Ara-C and consolidation with BEAM or BEAC supported by in vivo R-purged autologous stem cells. In this study with a median observation of 4 years, a 6-year EFS of 56% was observed with no patient relapsing after 5 years. Similar data are seen for 63 patients transplanted in CR and included in bone marrow transplantation registries.66
Main prospective studies of PBSCT consolidation in first-line MCL
| Regimen | Reference (year) | N | 3-year EFS, % | 3-year OS, % | Main toxicity |
|---|---|---|---|---|---|
| Hyper-CVAD/HD-MTX-Ara-C | Khouri et al50 (1998) | 25 | 72 | 92 | — |
| Khouri et al59 (2003) | 31 | 43% at 5 years | 77% at 5 years | — | |
| 3 × APO + rituximab + sequential high-dose | Gianni et al62 (2003) | 28 | 80 | 90 | 18% CMV reactivation |
| CHOP + HD-CVB + rituximab | Mangel et al63 (2004) | 20 | 89 | 88 | Interstitial pneumonitis |
| 6xCHOP + HDdexaBEAM | Dreyling et al60 (2005) | 62 | 54 | 83 | 5% toxic deaths |
| CTAP/VMAC + HD-BuCy | Evens et al64 (2007) | 25 | 50 | 60 | |
| CHOP+HD-Ara-C +HD-R-Cy-TBI | Dreger et al65 (2007) | 34 | 80 | 100 | 79% severe mucositis |
| R-maxi-CHOP +R-HD-Ara-C+R-BEAM | Geisler et al61 (2008) | 160 | 70 | 85 | 5% toxic deaths |
| Regimen | Reference (year) | N | 3-year EFS, % | 3-year OS, % | Main toxicity |
|---|---|---|---|---|---|
| Hyper-CVAD/HD-MTX-Ara-C | Khouri et al50 (1998) | 25 | 72 | 92 | — |
| Khouri et al59 (2003) | 31 | 43% at 5 years | 77% at 5 years | — | |
| 3 × APO + rituximab + sequential high-dose | Gianni et al62 (2003) | 28 | 80 | 90 | 18% CMV reactivation |
| CHOP + HD-CVB + rituximab | Mangel et al63 (2004) | 20 | 89 | 88 | Interstitial pneumonitis |
| 6xCHOP + HDdexaBEAM | Dreyling et al60 (2005) | 62 | 54 | 83 | 5% toxic deaths |
| CTAP/VMAC + HD-BuCy | Evens et al64 (2007) | 25 | 50 | 60 | |
| CHOP+HD-Ara-C +HD-R-Cy-TBI | Dreger et al65 (2007) | 34 | 80 | 100 | 79% severe mucositis |
| R-maxi-CHOP +R-HD-Ara-C+R-BEAM | Geisler et al61 (2008) | 160 | 70 | 85 | 5% toxic deaths |
CMV indicates cytomegalovirus.
As in other indolent lymphomas, allogeneic bone marrow transplantation is the only potentially curative treatment for advanced disease, but its application is limited by the important age-dependent mortality. Even with nonmyeloablative conditioning, the transplantation-related mortality in registry data were 50% and the OS 30% at 2 years,67 although some centers of excellence present more encouraging data.68-70 The evidence of a graft-versus-lymphoma effect in MCL is weaker than for follicular lymphoma (FL)67,71 and registry data of transplanted MCL do not clearly show a plateau suggesting cure, although a few relapsed patients experienced very long remissions.
Rituximab in MCL
In MCL, rituximab has a somehow less impressive activity than in other B-cell indolent malignancies. The response rate in both untreated and pretreated patients is approximately 30% and the median duration of response 6 months.72,73 When combined with chemotherapy, it improves the CR rate47-49,52 and a comprehensive systematic review and meta-analysis of 7 randomized controlled trials indicated that rituximab plus chemotherapy may be superior to chemotherapy alone with respect to OS in MCL (hazard ratio for mortality = 0.60; 95% confidence interval, 0.37-0.98). In this meta-analysis, however, there was a strong heterogeneity among the trials, making this survival benefit not completely reliable.74 Used as maintenance after either single-agent rituximab, chemotherapy, or chemo-immunotherapy induction, rituximab marginally improves EFS but has no effect on OS.73,75
Role of radiotherapy
As MCL usually presents at an advanced stage, systemic treatment is the standard, and not much data are available on the activity of radiotherapy. Two retrospective studies suggest that radiotherapy is active in MCL, both alone or added to chemotherapy.76,77 The belief of European cooperative groups that total body irradiation regimens are more appropriate than chemotherapy as conditioning regimens before PBSCT in MCL is based on weak evidence78 and has been questioned more recently.
The recently available radioimmunotherapy (RIT) is an elegant technique to deliver radiotherapy in a targeted fashion. Anti-CD20 antibodies combined with a radioactive isotope (yttrium-90 or iodine-111) have activity in several lymphomas, including MCL. When RIT was used to consolidate remissions after (immuno)chemotherapy, it resulted in improvement of percentage, quality, and duration of responses compared with historical controls.79 RIT was also used (at either standard or high-dose) to improve on the activity of high-dose chemotherapy in the setting of autologous stem cell transplantation, showing feasibility and suggesting a possible benefit.80,81
New drugs active in MCL
Several new drugs have shown a remarkable single-agent activity in relapsed or resistant MCL and many, mainly of the so-called “molecular targeted” type, are now under investigation. Of those clinically available, the more consistent response rates are 33% for bortezomib,82 41% to 53% for lenalidomide,83,84 and 22% to 41% for temsirolimus.85-87 These compounds and others are now investigated in clinical trials for their possible role in combination with other agents active in MCL. The combination of thalidomide with rituximab88 showed remarkable activity in a small group of 16 elderly patients with relapsed disease (response rate = 81%) and the combination of bendamustine with rituximab obtained astonishingly high response rates and CR rates (75%-92% and 42%-50%, respectively).45,89
Suggested treatment algorithm
MCL is generally a systemic disease, but a small proportion of cases (10%-20%) is diagnosed with only one to 3 adjacent involved lymph node sites. In these cases, in analogy with the common practice for other lymphoma types, we treat these patients with involved field radiotherapy, preceded by 3 or 4 cycles of chemotherapy for patients who are young and fit enough for it. This strategy obtained long-term remissions in 11 of 16 patients treated in British Columbia.76
For advanced disease, considering the biologic characteristics and the treatment options illustrated in “Therapy,” the issue is whether MCL should be approached as done in diffuse large B-cell lymphoma (with which it shares the aggressive biology), that is, R-CHOP–like treatment to everybody, or rather with an approach as in FL (with which it shares the characteristic of noncurability), that is, tailored treatment based on prognostic factors and clinical characteristics of the patient.
Even though immediate combination chemotherapy for those who can tolerate it has been the far most used approach in the last decades, a watch-and-wait policy could be advocated, as we know that a fraction of patients present with a rather indolent form of MCL. Investigators at the Weill Cornell Medical College recently reported on 31 asymptomatic MCL patients with median age 58 years, who were approached by observation and treated only when clinically needed (all intervals > 3 months). Fourteen of these remained without treatment for more than 1 year, and the OS of this group was similar to an institutional comparison group (n = 66) that was treated immediately at diagnosis.90 This is an interesting observation; however, it must be noted that it comes from a retrospective analysis of a small group of cases, and to extrapolate that a watch-and-wait policy could be advocated for a selected subgroup of MCL patients may be premature.
Therefore, because MCL is to be considered a generally aggressive disease and because none of the biologic and clinical prognostic factors has been validated as a tool for the selection of therapy, our practice is to start therapy at diagnosis while tailoring treatment to the age and the general condition of the patient.
First-line treatment
Treatment of the young and fit
In several B-cell lymphomas, such as FL or diffuse large B-cell lymphoma, the advent of rituximab improved patient prognosis and changed the treatment approach, reducing the role of more aggressive treatment in front line. In MCL, in contrast, the outlook of patients has not changed significantly, and we are still facing an aggressive disease with a generally dismal prognosis, a median survival of 5 years, and a tendency to relapse early and to respond insufficiently to salvage treatment. The disease often involves the bone marrow, so that if autologous transplantation is planned, the collection of blood stem cells with the minimal amount of contaminating tumor should be performed as early as possible. For these reasons, we apply an aggressive approach for patients who are young (< 60-65 years) and fit (no relevant comorbidity). In these cases, the clinical presentation of the disease (whether involving mainly the lymph nodes, the bone marrow, and spleen or the gut) is not relevant for the choice of therapy. In our institution, we decided to use the R-hyper-CVAD/R-HD-MTX-Ara-C regimen for 4 to 6 cycles, followed by a consolidation with BEAM and PBSCT. Even though this approach was not confirmed as optimal in randomized trials, it appears to be very active and safe enough if applied in tertiary centers with sufficient expertise in high-dose therapy. Because the incidence of MCL patients with age younger than 65 years is similar to that of AML cases of the same age, we think that the suggestion to treat them all in tertiary centers with expertise in the treatment of acute leukemia should not be considered exaggerated.
Approach to the elderly and fit
Patients too old for autologous transplantation, but who are fit enough to receive intensive treatment, should be given chemotherapy with rituximab. We have chosen to treat these cases with R-CHOP or R-CVP (depending on the cardiac comorbidities), but regimens such as R-BOP or R-FCM have as well shown to be suitable for this purpose and should be selected based on their side effect profile and the physician confidence with the regimen. Because of its toxicity profile, we do not add HD-Ara-C to these patients. On the other hand, it could be an option to consolidate these remissions with radioimmunotherapy, as it significantly improves the duration of remission without hampering the quality of life. Because of problems in obtaining payment of this expensive treatment by insurances, we are not routinely applying this option to our patients.
Treatment of the unfit
Patients who, either because of age or of comorbidities, are unable to tolerate aggressive treatment, are treated with palliative chemotherapy of reduced intensity, usually with single agents. Of all the possible options, because of the favorable toxicity and cost profile, we often still choose to give oral chlorambucil, eventually combined with rituximab. The response rate and duration of this combination are satisfactory, as is the minimal impact on the quality of life.91
Second-line treatments
It has been proposed that the improvement in survival observed in the last decade is not the result of better first-line treatments but rather to improved second-, third-, and fourth-line therapeutic options.92 Whether this is true or not, when patients relapse after an aggressive approach, the goal of treatment becomes palliation of symptoms, and second-line treatments with few side effects should be preferred. An exception is the relatively rare case of young and motivated patients with a compatible donor: here we consider the possibility of an allogeneic transplantation and the pros and cons of such a procedure are discussed. If an allogeneic transplantation is foreseen, we induce remission with a cisplatin-based regimen (etoposide, Solu-Medrol, high-dose Ara-C, Platinol-ESHAP) as done for other lymphomas.
A variety of treatments have shown a good therapeutic index at relapse. They are composed of single agents as thalidomide,88 chlorambucil,91 bendamustine,45,89 and cladribine,42 or newer agents such as bortezomib,82 lenalidomide,93 or temsirolimus.85 Combination treatments, such as R-FC,94 R-FCM,75 and gemcitabine/dexamethasone plus or minus cisplatin,95 obtain a higher response rate but have probably no impact on survival and are at risk of causing major side effects. Low-dose metronomic PEP-C96 is a new combination of orally administered drugs, which is both well tolerated and active.
Despite the clinical activity of many compounds and regimens, the treatment outcome of relapsing MCL patients who are not suitable for allogeneic transplantation remains dismal, and no curative options are available. Therefore, we think that, whenever possible, these patients should be offered the possibility of entering clinical trials testing new agents. When this is not possible, for practical reasons, we usually try chlorambucil first, or CVP if a rapid response is needed for symptom palliation. Bortezomib is our next choice, followed by lenalidomide, each of these eventually combined with rituximab.
Even though in some countries it is customary to add rituximab to any line of therapy for any B-cell neoplasia, we consider MCL as one of the lymphomas less sensitive to this antibody. We therefore do not add rituximab to subsequent treatments if progression occurred within 6 months from the termination of a previous R-containing therapy.
Finally, radiotherapy, either in the form of irradiation of symptomatic localizations or in the form of radio-immunotherapy, can be a good choice in selected patients. A problem with this latter form of treatment is that a bone marrow infiltration less than 25% and a normal platelet count are needed, both conditions that are not often met in relapsed MCL.
Acknowledgments
We thank our colleagues Franco Cavalli and Francesco Bertoni for critically reading the manuscript and for their fruitful feedback and thoughtful discussion, and Dr Monica Taborelli for kindly providing the photographs included in Figure 1.
Authorship
Contribution: M.G. and E.Z. wrote the paper.
Conflict-of-interest disclosure: The authors declare no competing financial interests.
Correspondence: Michele Ghielmini, Medical Oncology Departement, Oncology Institute of Southern Switzerland, Ospedale San Giovanni 6500 Bellinzona, Switzerland; e-mail: michele.ghielmini@eoc.ch.
