Fludarabine and lenalidomide are essential drugs in the front-line treatment of non-Hodgkin lymphoma (NHL) and multiple myeloma (MM), respectively. Data suggests that fludarabine and lenalidomide therapy may have a deleterious effect on stem cell mobilization. In the European compassionate use program, 48 patients (median age 57 years) previously treated with fludarabine (median 5 cycles; range: 1-7 cycles) were given plerixafor plus granulocyte colony-stimulating factor (G-CSF) for remobilization following a primary mobilization attempt. The overall median number of CD34+ cells collected was 2.3 × 10(6)/kg (range: 0.3-13.4). The minimum required number of CD34+ cells (≥2.0 × 10(6)/kg) was collected from 58% of patients in a median of 2 days. Thirty-five patients (median age = 57 years) previously treated with lenalidomide (median 5 cycles; range: 1-10 cycles) were given plerixafor plus G-CSF for remobilization. The overall median number of CD34+ cells collected was 3.4 × 10(6)/kg (range: 1.1-14.8). The minimum required number of CD34+ cells (≥2.0 × 10(6) per kg) was collected from 69% of patients in a median of 2 days. In conclusion, salvage mobilization with plerixafor plus G-CSF is successful in the majority of patients with MM previously treated with lenalidomide. In fludarabine-exposed patients, only 58% of patients will achieve successful salvage mobilization with plerixafor plus G-CSF, suggesting the need for novel mobilization regimens algorithms in this subgroup of patients

Apperley, Jane F.

Basak, Grzegorz W.

Douglas, Kenneth W.

Duarte, Rafael F.

Gabriel, Ian H.

Geraldes, Catarina

Hübel, Kai

Jaksic, Ozren

Koristek, Zdenek

Kröger, Nicolaus

Lanza, Francesco

Lemoli, Roberto

Malard, Florent

Mikala, Gabor

Mohty, Mohamad

Selleslag, Dominik

Worel, Nina

English

Malard F.

Kröger N.

Gabriel I. H.

Hübel K.

Apperley J. F.

Basak G. W.

Douglas K. W.

Geraldes C.

Jaksic O.

Koristek Z.

Lanza F.

Mikala G.

Selleslag D.

Worel N.

Mohty M.

Duarte R. F.

LEMOLI, ROBERTO MASSIMO

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Plerixafor for autologous peripheral blood stem cell mobilization in patients previously treated with fludarabine or lenalidomide.

Fludarabine and lenalidomide are essential drugs in the front-line treatment of non-Hodgkin lymphoma (NHL) and multiple myeloma (MM), respectively. Data suggests that fludarabine and lenalidomide therapy may have a deleterious effect on stem cell mobilization. In the European compassionate use program, 48 patients (median age 57 years) previously treated with fludarabine (median 5 cycles; range: 1-7 cycles) were given plerixafor plus granulocyte colony-stimulating factor (G-CSF) for remobilization following a primary mobilization attempt. The overall median number of CD34+ cells collected was 2.3 × 106/kg (range: 0.3-13.4). The minimum required number of CD34+ cells (≥2.0 × 106/kg) was collected from 58% of patients in a median of 2 days. Thirty-five patients (median age = 57 years) previously treated with lenalidomide (median 5 cycles; range: 1-10 cycles) were given plerixafor plus G-CSF for remobilization. The overall median number of CD34+ cells collected was 3.4 × 106/kg (range: 1.1-14.8). The minimum required number of CD34+ cells (≥2.0 × 106 per kg) was collected from 69% of patients in a median of 2 days. In conclusion, salvage mobilization with plerixafor plus G-CSF is successful in the majority of patients with MM previously treated with lenalidomide. In fludarabine-exposed patients, only 58% of patients will achieve successful salvage mobilization with plerixafor plus G-CSF, suggesting the need for novel mobilization regimens algorithms in this subgroup of patients

Malard F

Kroger N

Gabriel IH

Hubel K

Apperley JF

Basak GW

Douglas KW

Geraldes C

Jaksic O

Koristek Z

Lanza F

Lemoli R

Mikala G

Selleslag D

Worel N

Mohty M

Duarte RF.

Archivio istituzionale della ricerca - Università di Ferrara

314 Biol Blood Marrow Transplant 18:309-329, 2012F. Malard et al.From theServicCentrINSEHosp3ImpeLondI, UnHemasity ogrammUnitegal; 8hemaCzechCremPlerixafor for Autologous Peripheral Blood Stem CellMobilization in Patients Previously Treatedwith Fludarabine or LenalidomideFlorent Malard,1 Nicolaus Kr€oger,2 Ian H. Gabriel,3 Kai H€ubel,4Jane F. Apperley,3 Grzegorz W. Basak,5 Kenneth W. Douglas,6 Catarina Geraldes,7Ozren Jaksic,8 Zdenek Koristek,9 Francesco Lanza,10 Roberto Lemoli,11 Gabor Mikala,12Dominik Selleslag,13 Nina Worel,14 Mohamad Mohty,1,* Rafael F. Duarte15,*1Cene d’He d’RMitalrialon, Uiversitologf We, Bd KinDubrtoonkRepona,Fludarabine and lenalidomide are essential drugs in the front-line treatment of non-Hodgkin lymphoma(NHL) and multiple myeloma (MM), respectively. Data suggests that fludarabine and lenalidomide therapymay have a deleterious effect on stem cell mobilization. In the European compassionate use program, 48 pa-tients (median age 57 years) previously treated with fludarabine (median 5 cycles; range: 1-7 cycles) weregiven plerixafor plus granulocyte colony-stimulating factor (G-CSF) for remobilization following a primarymobilization attempt. The overall median number of CD341 cells collected was 2.3  106/kg (range:0.3-13.4). The minimum required number of CD341 cells ($2.0  106/kg) was collected from 58% ofpatients in a median of 2 days. Thirty-five patients (median age5 57 years) previously treated with lenalido-mide (median 5 cycles; range: 1-10 cycles) were given plerixafor plus G-CSF for remobilization. The overallmedian number of CD341 cells collected was 3.4 106/kg (range: 1.1-14.8). The minimum required numberof CD341 cells ($2.0 106 per kg) was collected from 69% of patients in a median of 2 days. In conclusion,salvage mobilization with plerixafor plus G-CSF is successful in the majority of patients with MM previouslytreated with lenalidomide. In fludarabine-exposed patients, only 58% of patients will achieve successfulsalvage mobilization with plerixafor plus G-CSF, suggesting the need for novel mobilization regimensalgorithms in this subgroup of patients.Biol Blood Marrow Transplant 18: 314-317 (2012)  2012 American Society for Blood and Marrow TransplantationKEY WORDS: Autologous stem cell mobilization, Plerixafor, Salvage mobilization, FludarabineINTRODUCTIONHigh-dose chemotherapy with or without radio-therapy followed by autologous hematopoietic stemcell transplantation (HSCT) is an effective treatmentfor patients with non-Hodgkin lymphoma (NHL)[1,2] and multiple myeloma (MM) [3]. At present,granulocyte colony-stimulating factor (G-CSF)-mobi-lized peripheral blood stem cells are the preferred stemtre Hospitalier et Universitaire (CHU) de Nantes,ematologie Clinique, Nantes, Universite de Nantes,Investigation Clinique en Cancerologie (CI2C),CRNCA UMR 892, Nantes, France; 2Universityof Hamburg-Eppendorf, Hamburg, Germany;College London, Department of Haematology,nited Kingdom; 4Department of Internal Medicinety Hospital of Cologne, Germany; 5Department ofy, Oncology & Internal Diseases, Medical Univer-arsaw, Warsaw, Poland; 6HPC Transplant Pro-eatson West of Scotland Cancer Centre, Glasgow,gdom; 7Hospitais da Universidade, Coimbra, Portu-ava University Hospital, Zagreb, Croatia; 9Internıologicka klinika Lekarske Fakulty MU a FN Brno,ublic; 10Cremona Hospital, Section of Hematology,Italy; 11Department of Hematology and Oncologicalcell source for autologous HSCT [4]. The success ofHSCmobilization is usually assessed by the total num-ber of CD341 stem cells collected, with a cutoff of 2.0 106 CD341 cells/kg recipient body weight beingconsidered as a minimum requirement for transplant.Higher cell dose in the range of 4-5  106 CD341cells/kg, however, are associated with faster neutro-phils and platelets recovery [5]. Traditionally, HSCSciences ‘‘L&A Seragnoli,’’ Institute of Hematology, Universityof Bologna, Bologna, Italy; 12St. Laszlo Hospital, Departmentof Haematology & SCT, Budapest, Hungary; 13AlgemeenZiekenhuis Sint-Jan, Brugge, Belgium; 14Medical Universityof Vienna, Austria; and 15Catalan Institute of Oncology,IDIBELL, L’Hospitalet de Llobregat, Barcelona, Spain.Financial disclosure: See Acknowledgments on page 316.*These two authors share senior authorship.Correspondence and reprint requests: MohamadMohty, MD, PhD,Hematologie Clinique, CHUdeNantes, Place A. Ricordeau, F-44093 Nantes Cedex, France (e-mail: mohamad.mohty@univ-nantes.fr).Received August 2, 2011; accepted October 1, 2011 2012 American Society for Blood and Marrow Transplantation1083-8791/$36.00doi:10.1016/j.bbmt.2011.10.003Biol Blood Marrow Transplant 18:309-329, 2012 315Plerixafor after Fludarabine/Lenalidomidemobilization has been achieved using G-CSF alone orin combination with chemotherapy, with a failure ratereported in 5% to 30% of cases [6]. The main risk fac-tors for failure or suboptimal mobilization are ad-vanced age (.60 years), progressive disease, bonemarrow involvement, or previous chemotherapyincluding drugs such as fludarabine [7] or lenalidomide[8]. Indeed, given the increasing use of fludarabine aspart of the treatment armamentarium of differentlymphoma subtypes, and the wide use of lenalidomidein MM treatment regimens, collection of adequatenumbers of autologous CD341 stem cells in patientswho are candidates for autologous HSCT is becominga matter of concern [9]. Plerixafor (previouslyAMD3100) reversibly and selectively antagonizes theCXCR4 chemokine receptor resulting in mobilizationof CD341 cells to the peripheral blood [10]. Before thedrug approval in Europe, a plerixafor compassionateuse program (CUP) was available from July 2008 toAugust 2010 to provide access to the drug for patientswith MM or lymphoma who had previously faileda mobilization attempt, and who were not eligible foranother specific plerixafor trial. In this report, we pres-ent the efficacy data of plerixafor in a subgroup ofpatients in the CUP who were previously treatedwith fludarabine or lenalidomide.PATIENTS AND METHODSFrom June 2008 to August 2010, over 1400 pa-tients were enrolled in the European CUP, anda European Consortium for Stem Cell Collection(ECOSM) collected data in one-half of patientstreated. Eligibility criteria for the CUP were age.18 years, a diagnosis of NHL, Hodgkin’s disease,or MM, and candidate for autologous HSCT butwho had previously failed to collect a minimum of2.0  106 CD341 cells/kg or did not even proceed toapheresis based on a low peripheral blood CD341count (usually\10 cells/mL) after a conventional mo-bilization procedure. The current analysis focused on83 patients included in this CUP who were previouslytreated with fludarabine or lenalidomide (for at least 1treatment course including fludarabine or lenalido-mide) before autologous stem cell collection, and forwhom adequate data for analysis were available. Allpatients signed informed consents for inclusion inthe CUP and for collection of their data.The salvage mobilization protocol included non-pegylated G-CSF, administered at a dose of 10 mg/kgdaily by subcutaneous injection on 4 consecutivedays. In the evening of the fourth day, patients receivedsubcutaneous plerixafor at a dose of 240 mg/kg. Apher-esis was usually initiated on the fifth day, 10 to 12 h af-ter plerixafor and 1 h after G-CSF administration.Apheresis and daily administration of G-CSF and pler-ixafor were continued until the patient collectedenough CD341 cells for auto-HSCT (minimum of2.0  106/kg), and a maximum of 7 plerixafor injec-tions was allowed. The apheresis procedures were per-formed according to the standard protocols at eachinstitution.Theprimary endpoint for the current analysiswas toassess the rate of successful mobilization defined as col-lection of a total number$2.0 106 CD341 cells/kg ofbody weight. Descriptive statistics were used to definecharacteristics of patients.RESULTS AND DISCUSSIONThis retrospective analysis included a total of83 patients. Patients’ characteristics and mobilizationfeatures are summarized in Table 1. A total of 48 pa-tients were previously treated with fludarabine (‘‘Flugroup’’), whereas 35 patients received lenalidomide(‘‘Len group’’). All 48 patients from the ‘‘Flu group’’had a diagnosis of NHL, whereas all patients fromthe ‘‘Len group’’ hadMM. In the Flu group, the overallmedian number of CD341 cells collected after salvagemobilization with plerixafor was 2.3  106/kg (range:0.3-13.4). Of the 48 patients, 28 (58%) reached theminimum number of 2.0  106 CD341 cells/kg,whereas only 3 patients (6%) collected $5.0  106CD341 cells. The collection target of 2.0  106/kgwas reached in a median of 2 apheresis sessions (range:1-3).The overall median number of CD341 cells col-lected in the Len group was 3.4  106/kg (range:1.1-14.8). Among these 35 patients, 24 patients(69%) collected the minimum number of CD341 cells($2.0  106/kg), including 12 patients (34%) whowere able to collect $5.0  106 cells/kg. In the Lengroup, 7 patients (20%) had received a prior autolo-gous HSCT before salvage mobilization with plerixa-for. Both targets were reached with a median of 2apheresis sessions (range: 1-4).In this salvage CUP program, 58% of patients pre-viously exposed to fludarabine successfully mobilized$2.0  106 CD341 cells/kg using plerixafor plusG-CSF, among them only 3 patients (6%) were ableto collect an optimal graft of $5.0  106 CD341/kg,allowing for at least 2 HSCT procedures. Interest-ingly, previously published data suggested that first-line mobilization success rates in patients pretreatedwith fludarabine can range from 46% to 63% [11-13]with G-CSF alone, G-CSF plus chemotherapy, orG-CSF plus stem cell factor. Furthermore, second-line mobilization regimens are considered to be oflittle effect in this subgroup of patients [14,15].Therefore, results observed in the current analysis inTable 1. Study Population CharacteristicsCharacteristic (%)Fludarabine(n 5 48)Lenalidomide(n 5 35)Patient age, median (range) 57 (36-69) 57 (34-66)Patient genderMale 26 (54) 18 (51)Female 22 (46) 17 (42)Fludarabine or lenalidomide cycles,median (range)5 (1-7) 5 (1-10)Diagnosis and disease statusNHL 48 (100) 0Multiple myeloma 0 35 (100)Previous chemotherapy: number of lines,median (range)3 (1-6) 4 (1-9)Previous autograftYes 0 7 (20)No 43 (90) 20 (57)Data missing 5 (10) 8 (23)RadiotherapyYes 5 (10) 3 (9)No 36 (75) 24 (68)Data missing 7 (15) 8 (23)Mobilization strategy with plerixaforSteady-state G-CSF mobilization 38 (79) 27 (77)Chemotherapy + G-CSF mobilization 10 (21) 8 (23)No. of patients collected 44 (92) 34 (97)CD34+ cells collected/kg, median (range) 2.3 (0.3-13.4) 3.4 (1.1-14.8)No. of patients who reached$2.106 CD34+28 (58) 24 (69)No. of apheresis days to reach$2.106 CD34+2 (1-3) 2 (1-4)No. of patients who reached$5.106 CD34+3 (6) 12 (34)No. of apheresis days to reach$5.106 CD34+2 (1-3) 2 (1-3)316 Biol Blood Marrow Transplant 18:309-329, 2012F. Malard et al.a salvage setting can be viewed as encouraging.However, one cannot ignore that nearly one-half offludarabine-treated patients failed to be rescued aftersalvage remobilization with plerixafor, raising the issueof the use of this drug as front-line therapy in order tooptimize the overall results in this subgroup predictedto be very poor mobilizers and thus improve treatmentoptions [9].In contrast, in patients previously treated withlenalidomide, salvage remobilization with plerixaforplus G-CSF was significantly more effective with 69%of the 38 patients successfully mobilizing $2.0  106CD341 cells/kg, including 34% of cases achieving$5.0 106 CD341 cells/kg. In the literature, mobiliza-tion failure rates in patients pretreated with lenalido-mide ranged from 7% to 45% [8,16,17], suggestingthat second-line agents are likely to be needed forthese patients. In patients with MM, chemotherapy-based mobilization has been shown to be effective forremobilization, especially in patients treatedwith lenali-domide but at the cost of increased toxicity [17]. Resultsfrom this current analysis after lenalidomide therapy arecomparable to the results published by Micallef et al.[18] as part of the U.S. CUP, who reported, in 40 pa-tients previously treated with lenalidomide undergoinga remobilization attempt after primarymobilization fail-ure, achievement of the minimum required number ofCD341 cells in 80%. With this background, theInternational Myeloma Working Group recentlypublished comprehensive recommendations for stemcell mobilization in patients with MM in the era ofnovel therapeutic agents. In patients treated withlenalidomide-based regimens, collection of autologousstem cells is recommended within the first 4 cycles. Incase of failure of the front-line collection procedureusing G-CSF, second-line collection with G-CSF plusplerixafor is 1 of the recommended options [19].In terms of postautologous HSCT outcome, thedesign of this CUP-based analysis did not allow assessto such data, especially engraftment kinetics. How-ever, based on previously published data [20], it hasalready been well established that engraftment featureswhen using autologous CD341 stem cells mobilizedwith G-CSF and plerixafor are at least as good as thoseof patients transplanted with stem cells mobilizedwithout plerixafor.In conclusion, the majority of patients treatedwith lenalidomide can undergo successful salvagesecond-line mobilization with plerixafor plus G-CSF.However, in patients treated with fludarabine, resultsare less appealing in the salvage setting,warranting largerprospective studies evaluating the efficacy of plerixaforfor front-line mobilization in this subgroup of patients.ACKNOWLEDGMENTSFinancial disclosure:The authors acknowledge the fi-nancial support ofGenzymeCorp. for their help in datacollection. However, Genzyme Corp. did not partici-pate in either the definition or data analysis. M.M.thanks C. Chabannon (Institut Paoli-Calmettes,Marseille, France) for helpful discussions. All authorshave received honoraria or educational grants supportfrom GENZYME whose product was discussed inthis manuscript.AUTHORSHIP STATEMENTF. Malard analyzed data and wrote the manuscript;M. Mohty recruited patients, supervised research, ana-lyzed data, and wrote the manuscript; N. Kr€oger, I. Ga-briel, K. H€ubel, J. Apperley, G. Basak, K. Douglas, C.Geraldes, O. Jaksic, Z. Koristek, F. Lanza, R. Lemoli,G. Mikala, D. Selleslag, and N.Worel recruited patientsand commented on the manuscript; R.F. Duarte re-cruited patients, supervised research, analyzed data, andhelped write the manuscript. All authors approved sub-mission of the manuscript for publication purposes.REFERENCES1. FreedmanAS,NeubergD,Mauch P, et al. Long-term follow-upof autologous bone marrow transplantation in patients withrelapsed follicular lymphoma. Blood. 1999;94:3325-3333.Biol Blood Marrow Transplant 18:309-317, 2012 317Plerixafor after Fludarabine/Lenalidomide2. van Besien K, Keralavarma B, Devine S, Stock W. Allogeneicand autologous transplantation for chronic lymphocytic leuke-mia. Leukemia. 2001;15:1317-1325.3. Attal M, Harousseau JL, Stoppa AM, et al. A prospective, ran-domized trial of autologous bone marrow transplantation andchemotherapy in multiple myeloma. Intergroupe Francais duMyelome. N Engl J Med. 1996;335:91-97.4. Beyer J, SchwellaN, Zingsem J, et al.Hematopoietic rescue afterhigh-dose chemotherapy using autologous peripheral-bloodprogenitor cells or bone marrow: a randomized comparison.J Clin Oncol. 1995;13:1328-1335.5. Siena S, Schiavo R, Pedrazzoli P, Carlo-Stella C. Therapeuticrelevance of CD34 cell dose in blood cell transplantation forcancer therapy. J Clin Oncol. 2000;18:1360-1377.6. Pusic I, Jiang SY, Landua S, et al. Impact of mobilization andremobilization strategies on achieving sufficient stem cell yieldsfor autologous transplantation. Biol Blood Marrow Transplant.2008;14:1045-1056.7. Tournilhac O, Cazin B, Lepretre S, et al. Impact of frontlinefludarabine and cyclophosphamide combined treatment onperipheral blood stem cell mobilization in B-cell chroniclymphocytic leukemia. Blood. 2004;103:363-365.8. Kumar S, Dispenzieri A, LacyMQ, et al. Impact of lenalidomidetherapy on stem cell mobilization and engraftment post-peripheral blood stem cell transplantation in patients with newlydiagnosed myeloma. Leukemia. 2007;21:2035-2042.9. Mohty M, Duarte RF, Croockewit S, Hubel K, Kvalheim G,Russell N. The role of plerixafor in optimizing peripheral bloodstem cell mobilization for autologous stem cell transplantation.Leukemia. 2011;25:1-6.10. Devine SM, Flomenberg N, Vesole DH, et al. Rapid mobili-zation of CD341 cells following administration of theCXCR4 antagonist AMD3100 to patients with multiple mye-loma and non-Hodgkin’s lymphoma. J Clin Oncol. 2004;22:1095-1102.11. Morgan SJ, Seymour JF, Grigg A, et al. Predictive factors forsuccessful stem cell mobilization in patients with indolent lym-phoproliferative disorders previously treated with fludarabine.Leukemia. 2004;18:1034-1038.12. Michallet M, Thiebaut A, Dreger P, et al. Peripheral blood stemcell (PBSC) mobilization and transplantation after fludarabinetherapy in chronic lymphocytic leukaemia (CLL): a report ofthe European Blood and Marrow Transplantation (EBMT)CLL subcommittee on behalf of the EBMT Chronic Leukae-mias Working Party (CLWP). Br J Haematol. 2000;108:595-601.13. Herbert KE, Morgan S, Prince HM, et al. Stem cell factor andhigh-dose twice daily filgrastim is an effective strategy for pe-ripheral blood stem cell mobilization in patients with indolentlymphoproliferative disorders previously treated with fludara-bine: results of a Phase II study with an historical comparator.Leukemia. 2009;23:305-312.14. Lysak D, Koza V, Steinerova K, Jindra P, Vozobulova V,Schutzova M. Mobilization of peripheral blood stem cells inCLL patients after front-line fludarabine treatment. Ann Hema-tol. 2005;84:456-461.15. Montillo M, Tedeschi A, Rossi V, et al. Successful CD341 cellmobilization by intermediate-dose Ara-C in chronic lympho-cytic leukemia patients treated with sequential fludarabine andCampath-1H. Leukemia. 2004;18:57-62.16. Paripati H, Stewart AK, Cabou S, et al. Compromised stem cellmobilization following induction therapy with lenalidomide inmyeloma. Leukemia. 2008;22:1282-1284.17. Popat U, Saliba R, Thandi R, et al. Impairment of filgrastim-induced stem cell mobilization after prior lenalidomide inpatients with multiple myeloma. Biol Blood Marrow Transplant.2009;15:718-723.18. Micallef IN, Ho AD, Klein LM, Marulkar S, Gandhi PJ,McSweeney PA. Plerixafor (Mozobil) for stem cell mobili-zation in patients with multiple myeloma previously treatedwith lenalidomide. Bone Marrow Transplant. 2011;46:350-355.19. Kumar S, Giralt S, Stadtmauer EA, et al. Mobilization inmyeloma revisited: IMWG consensus perspectives on stemcell collection following initial therapy with thalidomide-, lena-lidomide-, or bortezomib-containing regimens. Blood. 2009;114:1729-1735.20. DiPersio JF, Stadtmauer EA, Nademanee A, et al. Plerixaforand G-CSF versus placebo and G-CSF to mobilize hemato-poietic stem cells for autologous stem cell transplantationin patients with multiple myeloma. Blood. 2009;113:5720-5726.

Plerixafor for autologous peripheral blood stem cell mobilization in patients previously treated with fludarabine or lenalidomide

Kröger N

Hübel K

Duarte RF

Archivio istituzionale della ricerca - Università di Genova

Open Access Repository

Elsevier - Publisher Connector 

314 Biol Blood Marrow Transplant 18:309-329, 2012F. Malard et al.From the
Servic
Centr
INSE
Hosp
3Impe
Lond
I, Un
Hema
sity o
gramm
Unite
gal; 8
hema
Czech
CremPlerixafor for Autologous Peripheral Blood Stem Cell
Mobilization in Patients Previously Treated
with Fludarabine or Lenalidomide
Florent Malard,1 Nicolaus Kr€oger,2 Ian H. Gabriel,3 Kai H€ubel,4
Jane F. Apperley,3 Grzegorz W. Basak,5 Kenneth W. Douglas,6 Catarina Geraldes,7
Ozren Jaksic,8 Zdenek Koristek,9 Francesco Lanza,10 Roberto Lemoli,11 Gabor Mikala,12
Dominik Selleslag,13 Nina Worel,14 Mohamad Mohty,1,* Rafael F. Duarte15,*1Cen
e d’H
e d’
RM
ital
rial
on, U
iversi
tolog
f W
e, B
d Kin
Dubr
toonk
Rep
ona,Fludarabine and lenalidomide are essential drugs in the front-line treatment of non-Hodgkin lymphoma
(NHL) and multiple myeloma (MM), respectively. Data suggests that fludarabine and lenalidomide therapy
may have a deleterious effect on stem cell mobilization. In the European compassionate use program, 48 pa-
tients (median age 57 years) previously treated with fludarabine (median 5 cycles; range: 1-7 cycles) were
given plerixafor plus granulocyte colony-stimulating factor (G-CSF) for remobilization following a primary
mobilization attempt. The overall median number of CD341 cells collected was 2.3  106/kg (range:
0.3-13.4). The minimum required number of CD341 cells ($2.0  106/kg) was collected from 58% of
patients in a median of 2 days. Thirty-five patients (median age5 57 years) previously treated with lenalido-
mide (median 5 cycles; range: 1-10 cycles) were given plerixafor plus G-CSF for remobilization. The overall
median number of CD341 cells collected was 3.4 106/kg (range: 1.1-14.8). The minimum required number
of CD341 cells ($2.0 106 per kg) was collected from 69% of patients in a median of 2 days. In conclusion,
salvage mobilization with plerixafor plus G-CSF is successful in the majority of patients with MM previously
treated with lenalidomide. In fludarabine-exposed patients, only 58% of patients will achieve successful
salvage mobilization with plerixafor plus G-CSF, suggesting the need for novel mobilization regimens
algorithms in this subgroup of patients.
Biol Blood Marrow Transplant 18: 314-317 (2012)  2012 American Society for Blood and Marrow TransplantationKEY WORDS: Autologous stem cell mobilization, Plerixafor, Salvage mobilization, FludarabineINTRODUCTION
High-dose chemotherapy with or without radio-
therapy followed by autologous hematopoietic stem
cell transplantation (HSCT) is an effective treatment
for patients with non-Hodgkin lymphoma (NHL)
[1,2] and multiple myeloma (MM) [3]. At present,
granulocyte colony-stimulating factor (G-CSF)-mobi-
lized peripheral blood stem cells are the preferred stemtre Hospitalier et Universitaire (CHU) de Nantes,
ematologie Clinique, Nantes, Universite de Nantes,
Investigation Clinique en Cancerologie (CI2C),
CRNCA UMR 892, Nantes, France; 2University
of Hamburg-Eppendorf, Hamburg, Germany;
College London, Department of Haematology,
nited Kingdom; 4Department of Internal Medicine
ty Hospital of Cologne, Germany; 5Department of
y, Oncology & Internal Diseases, Medical Univer-
arsaw, Warsaw, Poland; 6HPC Transplant Pro-
eatson West of Scotland Cancer Centre, Glasgow,
gdom; 7Hospitais da Universidade, Coimbra, Portu-
ava University Hospital, Zagreb, Croatia; 9Internı
ologicka klinika Lekarske Fakulty MU a FN Brno,
ublic; 10Cremona Hospital, Section of Hematology,
Italy; 11Department of Hematology and Oncologicalcell source for autologous HSCT [4]. The success of
HSCmobilization is usually assessed by the total num-
ber of CD341 stem cells collected, with a cutoff of 2.0
 106 CD341 cells/kg recipient body weight being
considered as a minimum requirement for transplant.
Higher cell dose in the range of 4-5  106 CD341
cells/kg, however, are associated with faster neutro-
phils and platelets recovery [5]. Traditionally, HSCSciences ‘‘L&A Seragnoli,’’ Institute of Hematology, University
of Bologna, Bologna, Italy; 12St. Laszlo Hospital, Department
of Haematology & SCT, Budapest, Hungary; 13Algemeen
Ziekenhuis Sint-Jan, Brugge, Belgium; 14Medical University
of Vienna, Austria; and 15Catalan Institute of Oncology,
IDIBELL, L’Hospitalet de Llobregat, Barcelona, Spain.
Financial disclosure: See Acknowledgments on page 316.
*These two authors share senior authorship.
Correspondence and reprint requests: MohamadMohty, MD, PhD,
Hematologie Clinique, CHUdeNantes, Place A. Ricordeau, F-
44093 Nantes Cedex, France (e-mail: mohamad.mohty@
univ-nantes.fr).
Received August 2, 2011; accepted October 1, 2011
 2012 American Society for Blood and Marrow Transplantation
1083-8791/$36.00
doi:10.1016/j.bbmt.2011.10.003
Biol Blood Marrow Transplant 18:309-329, 2012 315Plerixafor after Fludarabine/Lenalidomidemobilization has been achieved using G-CSF alone or
in combination with chemotherapy, with a failure rate
reported in 5% to 30% of cases [6]. The main risk fac-
tors for failure or suboptimal mobilization are ad-
vanced age (.60 years), progressive disease, bone
marrow involvement, or previous chemotherapy
including drugs such as fludarabine [7] or lenalidomide
[8]. Indeed, given the increasing use of fludarabine as
part of the treatment armamentarium of different
lymphoma subtypes, and the wide use of lenalidomide
in MM treatment regimens, collection of adequate
numbers of autologous CD341 stem cells in patients
who are candidates for autologous HSCT is becoming
a matter of concern [9]. Plerixafor (previously
AMD3100) reversibly and selectively antagonizes the
CXCR4 chemokine receptor resulting in mobilization
of CD341 cells to the peripheral blood [10]. Before the
drug approval in Europe, a plerixafor compassionate
use program (CUP) was available from July 2008 to
August 2010 to provide access to the drug for patients
with MM or lymphoma who had previously failed
a mobilization attempt, and who were not eligible for
another specific plerixafor trial. In this report, we pres-
ent the efficacy data of plerixafor in a subgroup of
patients in the CUP who were previously treated
with fludarabine or lenalidomide.PATIENTS AND METHODS
From June 2008 to August 2010, over 1400 pa-
tients were enrolled in the European CUP, and
a European Consortium for Stem Cell Collection
(ECOSM) collected data in one-half of patients
treated. Eligibility criteria for the CUP were age
.18 years, a diagnosis of NHL, Hodgkin’s disease,
or MM, and candidate for autologous HSCT but
who had previously failed to collect a minimum of
2.0  106 CD341 cells/kg or did not even proceed to
apheresis based on a low peripheral blood CD341
count (usually\10 cells/mL) after a conventional mo-
bilization procedure. The current analysis focused on
83 patients included in this CUP who were previously
treated with fludarabine or lenalidomide (for at least 1
treatment course including fludarabine or lenalido-
mide) before autologous stem cell collection, and for
whom adequate data for analysis were available. All
patients signed informed consents for inclusion in
the CUP and for collection of their data.
The salvage mobilization protocol included non-
pegylated G-CSF, administered at a dose of 10 mg/kg
daily by subcutaneous injection on 4 consecutive
days. In the evening of the fourth day, patients received
subcutaneous plerixafor at a dose of 240 mg/kg. Apher-
esis was usually initiated on the fifth day, 10 to 12 h af-
ter plerixafor and 1 h after G-CSF administration.Apheresis and daily administration of G-CSF and pler-
ixafor were continued until the patient collected
enough CD341 cells for auto-HSCT (minimum of
2.0  106/kg), and a maximum of 7 plerixafor injec-
tions was allowed. The apheresis procedures were per-
formed according to the standard protocols at each
institution.
Theprimary endpoint for the current analysiswas to
assess the rate of successful mobilization defined as col-
lection of a total number$2.0 106 CD341 cells/kg of
body weight. Descriptive statistics were used to define
characteristics of patients.RESULTS AND DISCUSSION
This retrospective analysis included a total of
83 patients. Patients’ characteristics and mobilization
features are summarized in Table 1. A total of 48 pa-
tients were previously treated with fludarabine (‘‘Flu
group’’), whereas 35 patients received lenalidomide
(‘‘Len group’’). All 48 patients from the ‘‘Flu group’’
had a diagnosis of NHL, whereas all patients from
the ‘‘Len group’’ hadMM. In the Flu group, the overall
median number of CD341 cells collected after salvage
mobilization with plerixafor was 2.3  106/kg (range:
0.3-13.4). Of the 48 patients, 28 (58%) reached the
minimum number of 2.0  106 CD341 cells/kg,
whereas only 3 patients (6%) collected $5.0  106
CD341 cells. The collection target of 2.0  106/kg
was reached in a median of 2 apheresis sessions (range:
1-3).
The overall median number of CD341 cells col-
lected in the Len group was 3.4  106/kg (range:
1.1-14.8). Among these 35 patients, 24 patients
(69%) collected the minimum number of CD341 cells
($2.0  106/kg), including 12 patients (34%) who
were able to collect $5.0  106 cells/kg. In the Len
group, 7 patients (20%) had received a prior autolo-
gous HSCT before salvage mobilization with plerixa-
for. Both targets were reached with a median of 2
apheresis sessions (range: 1-4).
In this salvage CUP program, 58% of patients pre-
viously exposed to fludarabine successfully mobilized
$2.0  106 CD341 cells/kg using plerixafor plus
G-CSF, among them only 3 patients (6%) were able
to collect an optimal graft of $5.0  106 CD341/kg,
allowing for at least 2 HSCT procedures. Interest-
ingly, previously published data suggested that first-
line mobilization success rates in patients pretreated
with fludarabine can range from 46% to 63% [11-13]
with G-CSF alone, G-CSF plus chemotherapy, or
G-CSF plus stem cell factor. Furthermore, second-
line mobilization regimens are considered to be of
little effect in this subgroup of patients [14,15].
Therefore, results observed in the current analysis in
Table 1. Study Population Characteristics
Characteristic (%)
Fludarabine
(n 5 48)
Lenalidomide
(n 5 35)
Patient age, median (range) 57 (36-69) 57 (34-66)
Patient gender
Male 26 (54) 18 (51)
Female 22 (46) 17 (42)
Fludarabine or lenalidomide cycles,
median (range)
5 (1-7) 5 (1-10)
Diagnosis and disease status
NHL 48 (100) 0
Multiple myeloma 0 35 (100)
Previous chemotherapy: number of lines,
median (range)
3 (1-6) 4 (1-9)
Previous autograft
Yes 0 7 (20)
No 43 (90) 20 (57)
Data missing 5 (10) 8 (23)
Radiotherapy
Yes 5 (10) 3 (9)
No 36 (75) 24 (68)
Data missing 7 (15) 8 (23)
Mobilization strategy with plerixafor
Steady-state G-CSF mobilization 38 (79) 27 (77)
Chemotherapy + G-CSF mobilization 10 (21) 8 (23)
No. of patients collected 44 (92) 34 (97)
CD34+ cells collected/kg, median (range) 2.3 (0.3-13.4) 3.4 (1.1-14.8)
No. of patients who reached
$2.106 CD34+
28 (58) 24 (69)
No. of apheresis days to reach
$2.106 CD34+
2 (1-3) 2 (1-4)
No. of patients who reached
$5.106 CD34+
3 (6) 12 (34)
No. of apheresis days to reach
$5.106 CD34+
2 (1-3) 2 (1-3)
316 Biol Blood Marrow Transplant 18:309-329, 2012F. Malard et al.a salvage setting can be viewed as encouraging.
However, one cannot ignore that nearly one-half of
fludarabine-treated patients failed to be rescued after
salvage remobilization with plerixafor, raising the issue
of the use of this drug as front-line therapy in order to
optimize the overall results in this subgroup predicted
to be very poor mobilizers and thus improve treatment
options [9].
In contrast, in patients previously treated with
lenalidomide, salvage remobilization with plerixafor
plus G-CSF was significantly more effective with 69%
of the 38 patients successfully mobilizing $2.0  106
CD341 cells/kg, including 34% of cases achieving
$5.0 106 CD341 cells/kg. In the literature, mobiliza-
tion failure rates in patients pretreated with lenalido-
mide ranged from 7% to 45% [8,16,17], suggesting
that second-line agents are likely to be needed for
these patients. In patients with MM, chemotherapy-
based mobilization has been shown to be effective for
remobilization, especially in patients treatedwith lenali-
domide but at the cost of increased toxicity [17]. Results
from this current analysis after lenalidomide therapy are
comparable to the results published by Micallef et al.
[18] as part of the U.S. CUP, who reported, in 40 pa-
tients previously treated with lenalidomide undergoing
a remobilization attempt after primarymobilization fail-
ure, achievement of the minimum required number ofCD341 cells in 80%. With this background, the
International Myeloma Working Group recently
published comprehensive recommendations for stem
cell mobilization in patients with MM in the era of
novel therapeutic agents. In patients treated with
lenalidomide-based regimens, collection of autologous
stem cells is recommended within the first 4 cycles. In
case of failure of the front-line collection procedure
using G-CSF, second-line collection with G-CSF plus
plerixafor is 1 of the recommended options [19].
In terms of postautologous HSCT outcome, the
design of this CUP-based analysis did not allow assess
to such data, especially engraftment kinetics. How-
ever, based on previously published data [20], it has
already been well established that engraftment features
when using autologous CD341 stem cells mobilized
with G-CSF and plerixafor are at least as good as those
of patients transplanted with stem cells mobilized
without plerixafor.
In conclusion, the majority of patients treated
with lenalidomide can undergo successful salvage
second-line mobilization with plerixafor plus G-CSF.
However, in patients treated with fludarabine, results
are less appealing in the salvage setting,warranting larger
prospective studies evaluating the efficacy of plerixafor
for front-line mobilization in this subgroup of patients.ACKNOWLEDGMENTS
Financial disclosure:The authors acknowledge the fi-
nancial support ofGenzymeCorp. for their help in data
collection. However, Genzyme Corp. did not partici-
pate in either the definition or data analysis. M.M.
thanks C. Chabannon (Institut Paoli-Calmettes,
Marseille, France) for helpful discussions. All authors
have received honoraria or educational grants support
from GENZYME whose product was discussed in
this manuscript.AUTHORSHIP STATEMENT
F. Malard analyzed data and wrote the manuscript;
M. Mohty recruited patients, supervised research, ana-
lyzed data, and wrote the manuscript; N. Kr€oger, I. Ga-
briel, K. H€ubel, J. Apperley, G. Basak, K. Douglas, C.
Geraldes, O. Jaksic, Z. Koristek, F. Lanza, R. Lemoli,
G. Mikala, D. Selleslag, and N.Worel recruited patients
and commented on the manuscript; R.F. Duarte re-
cruited patients, supervised research, analyzed data, and
helped write the manuscript. All authors approved sub-
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Plerixafor for Autologous Peripheral Blood Stem Cell Mobilization in Patients Previously Treated with Fludarabine or Lenalidomide 

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Plerixafor for autologous peripheral blood stem cell mobilization in patients previously treated with fludarabine or lenalidomide.

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