Maintenance therapy with thalidomide improves survival in patients with multiple myeloma

doi:10.1182/blood-2006-05-022962

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Blood, 15 November 2006, Vol. 108, No. 10, pp. 3289-3294.
Prepublished online as a Blood First Edition Paper on July 27, 2006; DOI 10.1182/blood-2006-05-022962.

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CLINICAL TRIALS AND OBSERVATIONS
Maintenance therapy with thalidomide improves survival in patients with multiple myeloma
Michel Attal, Jean-Luc Harousseau, Serge Leyvraz, Chantal Doyen, Cyrille Hulin, Lofti Benboubker, Ibrahim Yakoub Agha, Jean-Henri Bourhis, Laurent Garderet, Brigitte Pegourie, Charles Dumontet, Marc Renaud, Laurent Voillat, Christian Berthou, Gerald Marit, Mathieu Monconduit, Denis Caillot, Bernard Grobois, Herve Avet-Loiseau, Philippe Moreau, Thierry Facon, for the Inter-Groupe Francophone du Myélome (IFM)
From the Department of Hematology, Hôpital Purpan, Toulouse, France; the Department of Biostatistics, Hôpital Purpan, Toulouse, France; the Hôtel Dieu, Nantes, France; the Centre Hospitalier Universitaire, Lausanne, Switzerland; the Cliniques Universitaires de Mont-Godinne, Yvoir, Belgium; the Centre Hospitalier Brabois, Nancy, France; the Hôpital Bretonneau, Tours, France; the Hôpital C. Huriez, Lille, France; the Institut Gustave Roussy, Villejuif, France; the Hôpital St-Antoine, Paris, France; the Hôpital Albert Michallon, Grenoble, France; the Hôpital Edouard Herriot, Lyon, France; the Centre Hospitalier la Mileterie, Poitiers, France; the Hôpital Jean Minjoz, Besançon, France; the Hôpital A. Morvan, Brest, France; the Hôpital Haut-Lévèque, Bordeaux Pessac, France; the Centre Henri Becquerel, Rouen, France; the Centre Hospitalier Le Bocage, Dijon, France; and the Hôpital Sud, Rennes, France.

   Abstract

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

Newer chemotherapeutic protocols as well as high-dose chemotherapyhave increased the response rate in myeloma. However, thesetreatments are not curative. Effective maintenance strategiesare now required to prolong the duration of response. We conducteda randomized trial of maintenance treatment with thalidomideand pamidronate. Two months after high-dose therapy, 597 patientsyounger than age 65 years were randomly assigned to receiveno maintenance (arm A), pamidronate (arm B), or pamidronateplus thalidomide (arm C). A complete or very good partial responsewas achieved by 55% of patients in arm A, 57% in arm B, and67% in arm C (P = .03). The 3-year postrandomization probabilityof event-free survival was 36% in arm A, 37% in arm B, and 52%in arm C (P < .009). The 4-year postdiagnosis probabilityof survival was 77% in arm A, 74% in arm B, and 87% in arm C(P < .04). The proportion of patients who had skeletal eventswas 24% in arm A, 21% in arm B, and 18% in arm C (P = .4). Thalidomideis an effective maintenance therapy in patients with multiplemyeloma. Maintenance treatment with pamidronate does not decreasethe incidence of bone events.

   Introduction

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

During the past 10 years, major advances in the treatment haveimproved the outlook in myeloma. The antitumor activity of thalidomide,¹bortezomib,² and lenalidomide³ has been discovered, and thecombination of these new drugs with conventional cytotoxic agentshas been reported to induce a high complete response rate.^4-8High-dose therapy followed by autologous stem cell transplantation(ASCT) has been shown to improve response rate,^9-13 event-freesurvival,^9-11,13 and overall survival^9,10,13 as compared withconventional chemotherapy. ASCT is now recommended for youngpatients as part of the initial therapy or at time of the diseaseprogression.¹⁴ However, the median duration of response afterthe newer chemotherapeutic protocols and ASCT does not exceed3 years, and almost all patients relapse.
To prolong the duration of response, maintenance therapy wasa logical approach. Maintenance therapy might prolong responseand survival by inhibiting proliferation and inducing apoptosisof malignant cells that have not been eliminated by chemotherapy.However, this hypothesis is not supported by controlled trials,and the role of maintenance therapy in myeloma remains controversial.Maintenance chemotherapy has failed to demonstrate any benefit.^15,16Most randomized studies and meta-analyses evaluating maintenanceinterferon showed a modest increase in progression-free survivalwithout any, or with minimal, survival benefit after conventionalor high-dose therapy.^17-19 Corticosteroid maintenance was foundto prolong the duration of response; however, the effect onsurvival was controversial.^20,21
Thalidomide is an agent with immunomodulatory and antiangiogenicproperties. In 1999, Singhal et al¹ reported that thalidomideinduced responses in one third of patients with refractory disease.Several studies confirmed the activity of this oral agent amongpatients who had failed high-dose therapy, with doses as lowas 50 mg, without myelosuppressive toxicity.^22,23 Thus, thalidomidewas an attractive candidate for use in maintenance situations,particularly after high-dose therapy. Biphosphonates inhibitosteoclastic activity and are effective in the treatment ofcancer-associated hypercalcemia.²⁴ Pamidronate, a second-generationbiphosphonate, was found to decrease the incidence of osteolyticbone lesion in myeloma, when added to conventional chemotherapy.²⁵However, the efficacy of pamidronate in reducing skeletal eventshas never been evaluated when used as maintenance treatmentafter conventional or high-dose therapy. In 1999, the IntergroupeFrancophone du Myélome (IFM) initiated the first randomizedtrial designed to evaluate the role of thalidomide and pamidronateas maintenance treatment.

   Patients, materials, and methods

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

Requirements for patient enrollment
Patients younger than 65 years of age were eligible for theIFM 99 trials. Patients with 2 adverse prognostic factors ( $beta$ -2microglobulin > 3 mg/L and deletion of chromosome 13 by fluorescencein situ hybridization [FISH] analysis) were enrolled in theIFM 99 03-04 trials (reported elsewhere). Patients without orwith only 1 adverse prognostic factor were enrolled in the presentIFM 99 02 protocol. The criteria for exclusion were prior treatmentfor myeloma, another malignancy, abnormal cardiac function (systolicejection fraction < 50%), chronic respiratory disease (vitalcapacity or carbon monoxide diffusion < 50% of normal), abnormalliver function (serum bilirubin > 35 µM or ALAT, ASAT> 4 times normal), psychiatric disease. Between April 2000and October 2003, 1019 patients from 74 centers were registeredin the IFM 99 trials. Two hundred thirty-nine patients (23%)were enrolled in the IFM 99 03-04 trials and 780 patients (77%)were enrolled in the present IFM 99 02 protocol. The study wasapproved by the institutional ethics committees of Purpan Hospital(Toulouse, France), and the patients gave written informed consentin accordance with the Declaration of Helsinki.
Study protocol
Initial enrollment. Patients were registered by the coordinatingcenter (Toulouse), and a centralized analysis of $beta$ -2 microglobulinand deletion of chromosome 13 were performed (Nantes).
Initial chemotherapy. Patients were initially treated with acontinuous intravenous infusion of 0.4 mg vincristine/m² bodysurface area and 9 mg doxorubicin/m² over a 24-hour period for4 days, with 40 mg oral dexamethasone/day on days 1 through4 (the VAD regimen). Three to 4 cycles of VAD were administeredat 3-week intervals.
Stem-cell transplantation. After initial chemotherapy, patientswith a performance status below World Health Organization grade3 and a serum creatinine level less than 150 µM underwentblood stem-cell collection. Double ASCT was performed. Melphalanalone was given before each ASCT (140 mg/m² before the firsttransplantation and 200 mg/m² before the second).
Randomization. Two months after the second ASCT, patients withoutprogressive disease were randomly assigned to receive one ofthe following treatment arms until disease progression: armA, no maintenance treatment; arm B, maintenance treatment withpamidronate (intravenous infusion of 90 mg pamidronate at 4-weekintervals); arm C, maintenance treatment with pamidronate andthalidomide (400 mg orally, dose reduction to a minimum doseof 50 mg was allowed for treatment-related toxicity). Patientsenrolled in arm C did not receive any prophylaxis of thromboemboliccomplications. The sequence of randomization was determinedby the coordinating center (Toulouse), which made the treatmentassignment by Fax after each patient's eligibility was confirmed.
Assessments
The response criteria of the European Group for Blood and MarrowTransplantation²⁶ proposed in 1998 were not used in this studysubmitted to the French authorities in 1998. A complete remissionwas defined as the lack of detectable paraprotein by serum andurine electrophoresis and 5% or fewer plasma cells with normalmorphology in a bone marrow aspirate. A very good partial responsewas defined as a decrease of 90% in the serum paraprotein level,a partial response as a decrease of 50% in the serum paraproteinlevel or a 90% decrease in the level of Bence Jones protein(including patients with Bence Jones protein only) or both,a minimal response as a decrease of 25% in the serum paraproteinlevel, stable disease as no change in the paraprotein level,progressive disease as an increase of 25% in the serum paraproteinlevel after 2 cycles of the initial chemotherapy, and a relapseas the reappearance of the paraprotein and/or the recurrenceof bone marrow infiltration in a patient with a complete responseand a 50% increase in paraprotein above the "plateau" levelin 2 samples obtained 4 weeks apart in a patient with a response.A skeletal event was defined as a bone lesion requiring a specifictherapy (chemotherapy, irradiation, or surgery).
Statistical analysis
The proportions of patients with a given characteristic werecompared by chi-square test or Fisher exact test. Differencesin the means of continuous measurements were tested by Studentt test and checked with the use of the Mann-Whitney U test.All tests were 2-tailed. The duration of event-free survivalwas calculated for patients randomly assigned from the dateof random assignment to the time of progression, relapse, ordeath. The duration of relapse-free survival was calculatedfor patients achieving at least a minimal response, from thedate of random assignment to the date of progression. The timeto skeletal event was calculated from the date of random assignmentto the date of the first occurrence of a skeletal event. Kaplan-Meiercurves for event-free survival, relapse-free survival, timeto skeletal event, and overall survival were compared by theuse of the log-rank test. Prognostic factors for event-freesurvival were determined by means of the Cox proportional hazardmodel for covariate analysis. The objectives were to comparethe arm A and arm B with respect to the 3-year risk of skeletalevents, and to compare the arm B and arm C with respect to the3-year risk of events. Two hundred patients were required ineach group to ensure a significance level of 5% and a powerof 95% if the true 3-year risk of skeletal events were 25% inarm A and 10% in arm B, and if the true 3-year risk of eventswere 50% in arm B and 38% in arm C. The study was completedafter 597 patients had been randomly assigned.

   Results

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

Patient flow
Seven hundred eighty patients were enrolled. Five hundred ninety-sevenpatients (77%) were randomly assigned: 200 in arm A, 196 inarm B, and 201 in arm C. The median time from enrollment torandomization was 9 months (range, 6-21 months). One hundredeighty-three patients were not randomly assigned: 40 becauseof protocol violation, 26 because of early death, 40 becauseof early progression, and 77 because they did not undergo doubletransplantation.
Baseline characteristics
The baseline characteristics of the 597 patients randomly assignedis shown in Table 1. No significant differences were found betweenthe treatment groups.

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Table 1.. Baseline characteristics of the patients

Response rate
The response rate at each step of the study is shown in Table 2.Thalidomide was found to improve the best response achievedafter randomization (P < .001). Sixty-seven percent of thepatients enrolled in arm C had a complete or a very good partialresponse, as compared with 55% in arm A and 57% in arm B (P= .03).

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Table 2.. Response rate

Event-free, relapse-free, and overall survival
In arm A, the median follow-up was 40 months (range, 28-63 months)from the time of enrollment and 30 months (range, 18-50 months)from the time of randomization. The 3-year probabilities ofevent-free and relapse-free survival after randomization were36% and 38%, respectively. The probability of overall survival4 years after enrollment was 77%.
In arm B, the median follow-up was 39 months (range, 29-64 months)from the time of enrollment and 29 months (range, 19-52 months)from the time of randomization. The 3-year probabilities ofevent-free and relapse-free survival after randomization were37% and 39%, respectively. The probability of overall survival4 years after enrollment was 74%.
In arm C, the median follow-up was 39 months (range, 30-63 months)from the time of enrollment and 29 months (range, 20-53 months)from the time of randomization. The 3-year probabilities ofevent-free and relapse-free survival after randomization were52% and 51%, respectively. The probability of overall survival4 years after enrollment was 87%.
The event-free survival (P < .009), relapse-free survival(P < .008), and overall survival (P < .04) were significantlydifferent between the 3 treatment arms. The event-free survival(P = .6), relapse-free survival (P = .7), and overall survival(P = .7) of patients randomly assigned to arms A and B weresimilar (without thalidomide). The event-free survival (P <.01), relapse-free survival (P <0.01), and overall survival(P <0.03) were significantly improved in arm C as comparedwith arm B. Thalidomide (arm C/arms A + B) was found to significantlyimprove the event-free survival (P = .002) (Figure 1), relapse-freesurvival (P = .003), and overall survival (P = .04) (Figure 2).

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Figure 1.. Event-free survival according to treatment arm. The probabilities of event-free survival (95% confidence interval) are shown below each time point. Without thalidomide (dotted line); with thalidomide (solid line). The probability of event-free survival (95% CI) after randomization at 2 years, 3 years, and 4 years with thalidomide is 71 (63-78), 52 (43-62), and 36 (22-55), respectively, and without thalidomide is 58 (53-64), 37 (31-44), and 26 (14-41), respectively.

Salvage therapy
In arm A, 96 patients had a relapse: 6 patients received nosalvage therapy, 10 received conventional chemotherapy, 2 receivedstem-cell transplantation, 61 received thalidomide, and 17 receivedbortezomib or lenalidomide. With a median follow-up of 13 monthsfrom the time of relapse, the probability for 1-year survivalafter relapse was 78%.
In arm B, 92 patients had a relapse: 8 patients received nosalvage therapy, 11 received conventional chemotherapy, 61 receivedthalidomide, and 12 received bortezomib or lenalidomide. Witha median follow-up of 12 months from the time of relapse, theprobability for 1-year survival after relapse was 73%.
In arm C, 72 patients had a relapse: 5 patients received nosalvage therapy, 19 received conventional chemotherapy, 1 receivedstem-cell transplantation, 20 received thalidomide plus dexamethasone,and 27 received bortezomib or lenalidomide. With a median follow-upof 11 months from the time of relapse, the probability for 1-yearsurvival after relapse was 75%. The survival rates after relapsewere similar in the 3 treatment groups (P = .7).

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Figure 2.. Overall survival according to treatment arm. The probabilities of overall survival (95% confidence interval) are shown below each time point. Without thalidomide (dotted line); with thalidomide (solid line). The probability of overall survival (95% CI) after enrollment at 2 years, 3 years, and 4 years with thalidomide is 97 (93-98), 93 (87-96), and 87 (80-93), respectively, and without thalidomide is 94 (91-96), 87 (83-90), and 75 (69-82), respectively.

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Figure 3.. Survival without skeletal event according to treatment arm. The probabilities of survival without skeletal event (95% confidence interval) are shown below each time point. Arm A received no maintenance (dotted line); arm B received maintenance with pamidronate (gray line); arm C received maintenance with pamidronate and thalidomide (solid line). The probability of survival without skeletal event (95% CI) after randomization at 1 year, 2 years, and 3 years in arm A is 89 (83-93), 78 (70-83), and 63 (52-74), respectively; in arm B is 91 (87-95), 79 (71-86), and 66 (55-76), respectively; and in arm C is 95 (91-98), 84 (78-90), and 69 (59-79), respectively.

Prognostic factors for event-free survival
In a multivariate analysis of all 597 patients randomly assigned,event-free survival was significantly related to deletion ofchromosome 13 (P < .05), $beta$ -2 microglobulin (P < .009),response at time of randomization (P < .009), and treatmentassignment (with or without thalidomide) (P < .001).
We compared the event-free survival according to the treatmentgroup (with or without thalidomide) in different subsets ofpatients. Thalidomide prolonged the event-free survival in eachof the following subsets: patients with $beta$ -2 microglobulin levelof 3 mg/L or less, with $beta$ -2 microglobulin level of greater than3 mg/L, with LDH level of 330 IU or less, with LDH level greaterthan 330 IU, with stage I or II DS, with stage III DS, patientsaged 50 years or younger, and patients aged 50 years or older.The effect of thalidomide on event-free survival differed accordingto the deletion of chromosome 13. Patients who did not havea deletion of chromosome 13 had a significant benefit from thalidomide(P < .006). Patients who had a deletion of chromosome 13did not benefit from thalidomide (P = .2). The effect of thalidomideon event-free survival differed according to the response achievedat time of randomization. Patients who had at least a very goodpartial response did not benefit from thalidomide (P = .4).Patients who did not have at least a very good partial responsehad a significant benefit from thalidomide (P < .004). Thelack of benefit in the patients with deletion 13 was independentfrom the response.
Risk of skeletal events
The proportion of patients who had skeletal events was 24% inarm A, 21% in arm B, and 18% in arm C (P = .4). The survivalwithout skeletal event was not significantly different betweenthe treatment groups (P = .2) (Figure 3).
Treatment-related toxicity
Patients received thalidomide for a median of 15 months (range,0.1-50 range). Drug-related adverse events led to discontinuationof thalidomide in 78 patients (39%). The median time elapsedbetween randomization and the onset of the adverse event thatled to the discontinuation of thalidomide was 8 months. Peripheralneuropathy was the main reason for discontinuation. The meandose of thalidomide received by the patients (calculated frominitiation to definite discontinuation) was 200 mg/day (range,50-400 mg/day), and 30 patients tolerated the maximum thalidomidedose for 12.6 months. Patients received pamidronate for a medianof 21 months (range, 0.2-51 months). A total of 16 patients(4%) had drug-related adverse effects necessitating discontinuationof pamidronate.
The adverse events (as defined by the National Cancer InstituteCommon Toxicity Criteria, version 2) in each treatment groupare shown in Table 3. Certain toxicities were more prominentin the thalidomide group, including neuropathy (68%), fatigue(34%), constipation (20%), neutropenia (7%), and cardiac (4%).The incidence of venous symptomatic thrombotic events was notsignificantly different between the 3 treatment groups.

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Table 3.. Adverse events according to treatment arm

   Discussion

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

We found that maintenance treatment with thalidomide after high-dosechemotherapy improves the response rate, the event-free survival,and the overall survival in patients with myeloma. Barlogieet al²⁷ recently reported that high-dose thalidomide improvedthe complete response rate and prolonged the event-free survivalwhen added to each phase of an intensive combined therapy (includinginduction, tandem transplantation, consolidation, and maintenance).However, in this study, thalidomide failed to improve survivalbecause of considerable adverse effects and to the occurrenceof drug resistance at time of relapse. Our results stronglysuggest that reserving the use of low-dose thalidomide for maintenanceafter transplantation is an effective strategy: toxicity isacceptable, drug resistance at time of relapse is not observed,and survival is improved. We also found that maintenance treatmentwith pamidronate, a second-generation biphosphonate, does notdecrease or delay the risk of skeletal events. Whether newerthird-generation biphosphonates, which are more potent thanpamidronate in preclinical models, will achieve this goal remainsto be answered.
An important objective of our trial was to evaluate the feasibilityand tolerance of maintenance treatment with thalidomide. Peripheralneuropathy (68%), fatigue (34%), and constipation (20%) werefrequently encountered adverse events. However, the incidenceof severe neuropathy (grade 3-4) was acceptable (7%). In ourtrial, maintenance therapy with thalidomide was not found toincrease the risk of thromboembolic complications. We thus confirmthat this risk is mainly observed if thalidomide is given duringinduction therapy when the tumor burden is high.^4,27 Thirty-ninepercent of patients had to discontinue thalidomide because ofdrug-related adverse events, and peripheral neuropathy was themain reason for discontinuation. Thus, lenalidomide,^3,7-8 ananalog of thalidomide without neurologic toxicities, might bean attractive candidate for use in maintenance situations. Theplanned starting dose of thalidomide was 400 mg/day. Becauseof drug-related toxicities, patients received a mean dosageof 200 mg/day for a median of 15 months. Stewart et al²⁸ reportedthat the adverse effects of thalidomide, when used as maintenancetherapy after transplantation, were dose related. Because responsesmay occur with doses of 50 to 100 mg/day,²³ maintenance therapywith these low doses should be proposed.
Our trial shows that thalidomide improves the quality of responseafter randomization. We have previously reported that the attainmentof a very good partial response was an important prognosticfactor for survival after high-dose therapy in patients withmyeloma.⁹ The best quality of response, observed in the thalidomidegroup, could explain the difference in event-free and overallsurvival. This hypothesis is supported by the observation thatthalidomide could benefit patients who do not have a very goodpartial response at time of randomization but has a limitedeffect among patients already in very good partial responseat time of randomization. Thus, thalidomide may improve thesurvival by reducing the tumor mass after high-dose therapyrather than by a pure maintenance effect. This result also suggeststhat stopping thalidomide as soon as a very good partial responsehas been reached could be an effective strategy to reduce theside effects and to avoid thalidomide resistance at time ofrelapse. The combination of thalidomide and corticosteroidswas reported to be synergistic in term of response rate.^29,30A phase 2 trial showed that this combination was tolerable whenused after high-dose therapy.²⁸ Whether this association ofthalidomide and corticosteroids would further improve the responserate and the overall survival of patients failing to achievea very good partial response after high-dose therapy will beclarified in ongoing trials.
The toxicity and costs of thalidomide justify the use of anapproach in which patients who could benefit the most from thistreatment are selected. Our results indicate that thalidomidecould benefit patients who do not have a very good partial responseat time of randomization. Our results also indicate that thalidomidecould benefit patients who do not have a deletion of chromosome13. Deletion of chromosome 13 is observed in 50% of multiplemyeloma tumors and is associated with a poor prognosis.³¹ Singhalet al¹ have also reported a poor response rate to thalidomidein patients with this deletion. Another strategy for patientswith the chromosome 13 deletion could be maintenance therapywith bortezomib² or lenalidomide,³ because responsiveness tothese agents did not correlate with the deletion.
Finally, our trial shows that maintenance treatment with thalidomideafter transplantation significantly improves the overall survivalin patients with multiple myeloma. However, the absence of plateauin the curve for event-free survival justifies the evaluationof novel agents to decrease the tumor mass before and aftertransplantation. Analogs of thalidomide, proteasome inhibitors,agents targeting cell-signaling cascades, or surface receptorsare being investigated.

   Appendix

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Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

The following centers and investigators from the IFM participatedin this study: Amiens, Hôpital Sud (B. Desablens, R. Garidi,V. Salle); Angers, Centre Hospitalier Régional et Universitaire(N. Ifrah, M. Dib, M. Gardembas); Annecy, Centre Hospitalier(B. Corront, C. Martin, P. Cony-Makhoul); Arlon, Clinique StJoseph (P. Pierre); Avignon, Hôpital Henri Duffaut (G.Lepeu); Bâle, Hôpital Cantonal (J.R. Passweg); Besançon,Hôpital Jean Minjoz (L. Voillat); Blois, Centre Hospitalier(D. Rodon); Bobigny, Hôpital Avicenne (P. Casassus); Bordeaux,Hôpital du Haut-Lévêque (G. Marit, A. DeSaint Marc); Bordeaux Institut Bergonie (H. Eghbali); Bordeaux,Polyclinique Bordeaux Nord Aquitaine (O. Fitoussi); Boulogne/Mer,Centre Hospitalier (P. Agape); Bourg En Bresse, Centre Hospitalier(H. Orfeuvre); Brest, Hôpital Augustin Morvan (J.F. Abgrall,C. Berthou, M. Escoffre Barbe, G. Guillerm); Bruxelles, HôpitalErasme (W. Feremans); Brugge, AZ Sint Jan AV (A.C. Louwdagie);Bruxelles, Clinique Universitaire Saint-Luc (J.L. Michaux, A.Ferrant, Drs Straetmans et Vandeneste); Bruxelles, InstitutJules Bordet (D. Bron); Caen, Center F. Baclesse (A.M. Peny);Caen, Centre Hospitalier Universitaire (M. Leporrier); Châlonsur Saône, Centre Hospitalier (B. Salles); Clamart, HôpitalPercy (T. De Revel); Clermont Ferrand, Hôpital HôtelDieu (A.C. Fouilhoux, P. Travade); Colmar, Centre HospitalierLouis Pasteur (B. Audhuy); Dijon, Centre Hospitalier du Bocage(D. Caillot, R.O. Casasnovas); Dunkerque, Centre HospitalierGénéral (M. Wetterwald); Genève, HôpitalCantonal (T. Matthes); Gilly, Hôpital St Joseph (P. Mineur);Grenoble, Hôpital Albert Michallon (J.J. Sotto, J.Y. Cahn,B. Pegourié, L. Molina, F. Garban, C.E. Bulabois, R.Gressin, C. Makowski, F. Courby); Haine St Paul, Centre HospitalierJolimont (A. Delannoy); La Roche sur Yon, Centre HospitalierDépartemental (H. Maisonneuve); Lausanne, Centre HospitalierUniversitaire (S. Leyvraz, N. Ketterer, T. Kowacsovics); Laval,Center Hospitalier Général (M. Jacomy); Le Havre,Groupe Hospitalier (C. Zarnitsky); Le Mans, Centre Hospitalier(J. Dugay); Le Mans, Centre J. Bernard (P. Solal Celigny, E.Voog); Liège Centre Hospitalier de la Citadelle (Pr DePrijck); Lille, Hôpital C. Huriez (T. Facon, I. Yakoub-Agha,X. Leleu); Lorient, Centre Hospitalier Bodélio (P. Moreau);Lyon, Centre Léon Bérard (C. Sebban); Lyon, HôpitalEdouard Herriot (D. Fiere, M. Michallet, C. Dumontet, X.G. Thomas,J. Troncy, F. Nicolini, A.S. Micallet, A. Thiebaut, E. Tavernier,H. Le Quoc); Lyon, Centre Hospitalier Lyon Sud (B. Coiffier,G. Salles, C. Thieblemont, S. Tartas, C. Traulle, D. Espinouse,F. Bouafia-Sauvy); Marseille, Institut Paoli Calmettes (A.M.Stoppa, R. Bouabdallah, D. Blaise, A. Charbonnier, D. Coso,R. Costello, J.M. Schiano De Colella); Marseille, HôpitalNord (G. Sebahoun); Metz, Hôpital Notre Dame de Bon Secours(B. Christian, V. Dorvaux); Nancy, Centre Hospitalier Brabois(C. Hulin, P. Lederlin, P. Delaby, F. Witz); Nantes, HôpitalHôtel Dieu (J.L. Harousseau, P. Moreau, R. Bataille, N.Juge-Morineau, V. Dubruille, B. Mahe, T. Guillaume); Nice, Hôpitalde l'Archet (J.G. Fuzibet, L. Euller-Ziegler); Nice, CentreAntoine Lacassagne (A. Thyss); Orléans, Hôpitalde la Source (V. Lucas, M. Schoenwald, K. Seyeffedine, S. Letortorec);Paris, Hôpital Saint-Antoine (A. Najman, L. Garderet);Paris, Hôtel Dieu (Pr Marie); Paris, Institut Curie (D.Decaudin, C. Mathiot); Poitiers, Centre Hospitalier La Mileterie(F. Guilhot, M. Renaud, E. Randriamala); Quimper, Centre Hospitalierde Cornouaille (J.P. Vilque); Reims, Hôpital Robert Debré(B. Pignon, B. Kolb); Rennes, Hôpital sud (B. Grobois,M. Sebillot); Rennes, Hôpital Ponchaillou (P.Y. Le Prise,T. Lamy, M. Escoffre-Barbe); Roselaere, H. Hart Ziekenhuis (H.Demuyck); Rouen, Centre Henri Becquerel (M. Monconduit); Saint-Cloud,Centre René Huguenin (F. Turpin); Saint Etienne, HôpitalNord (J. Jaubert); Saint Etienne, Hôpital de Bellevue(P. Collet); Saumur, Centre Hospitalier (Dr Maigre); Strasbourg,Hôpital de Hautepierre (F. Maloisel); Toulouse, HôpitalPurpan (M. Attal, A. Huynh, F. Huguet, C. Nouvel, C. Recher,X. Carles, G. Laurent); Toulouse, Hôpital Rangueil (M.Laroche); Tours, Hôpital Bretonneau (Ph Colombat, L. Benboubker);Vannes, Centre Hospitalier Prosper Chubert (H. Jardel); Villejuif,Institut Gustave Roussy (J.H. Bourhis, P.L. Arnaud, P. Brault);Yvoir, Cliniques Universitaires de Mont-Godinne (A. Bosly, C.Doyen, Drs Chatelain and Sonet).

   Acknowledgements

We thank Mr Ian Eustace for his critical reading of the manuscript.

   Footnotes

Submitted May 25, 2006; accepted July 6, 2006.
Prepublished online as Blood First Edition Paper, July 27, 2006;DOI 10.1182/blood-2006-05-022962.

A complete list of the members of the Inter-Groupe Francophonedu Myélome appears in the "Appendix."

Supported by a major grant from the Programme Hospitalier deRecherche Clinique and by the Swiss Group for Clinical CancerResearch (SAKK).

The authors declare no competing financial interests.

M.A., J.-L.H., S.L., C.D., C.H., L.B., I.Y.A., J.-H.B., L.G.,B.P., C.D., M.R., L.V., C.B., G.M., M.M., D.C., B.G., H.A.-L.,P.M., and T.F. participated in designing and performing theresearch; M.A. analyzed the data and wrote the paper; and allauthors checked the final version of the manuscript.

The publication costs of this article were defrayed in partby page charge payment. Therefore, and solely to indicate thisfact, this article is hereby marked "advertisement" in accordancewith 18 USC section 1734.

Reprints: Michel Attal, Service d'Hématologie, Hôpital Purpan, Place du Dr Baylac, 31059 Toulouse, France; e-mail: attal.m{at}chu-toulouse.fr.

   References

Top
Abstract
Introduction
Patients, materials, and methods
Results
Discussion
Appendix
References

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