Prise en charge des lymphomes de Hodgkin avancés. O. Casasnovas Hématologie Clinique CHU Dijon, France

Prise en charge des lymphomes de Hodgkin avancés O. Casasnovas Hématologie Clinique CHU Dijon, France

Stratification Stades I -II EORTC/GELA Médiastin/Thorax > 0.35 4 aires ganglionnaires B et VS 30 ou A et VS 50 GHSG Médiastin/Thorax > 0.33 3 aires ganglionnaires B et VS 30 ou A et VS 50 Age 50 Atteinte extra-nodale Stades III -IV Aucun facteur: Favorable Facteur 1+: Défavorable LH avancé Aucun facteur: Favorable Facteur 1+: Intermédiaire Exclus: Stades IIB [M/T>0.33, AEN] + Stades IIB [M/T>0.33, AEN] LH avancé

Lymphome de Hodgkin FORMES AVANCÉES QUELLE CHIMIOTHÉRAPIE?

HL : Chemotherapy 1973 ABVD regimen Dose D1 D15 Doxorubicin 25 mg/m 2 (IV) X X Bleomycin 10 mg/m 2 (IV) X X Vinblastine 6 mg/m 2 (IV) X X Dacarbazine 375 mg/m 2 (IV) X X BEACOPPesc regimen Dose D1 D2 D3 D4 D5 D6 D7 D8 Bleomycin 10 mg/m 2 (IV) X D9 to D14 1993 Etoposide 200 mg/m 2 (IV) X X X Doxorubicin 35 mg/m 2 (IV) X Cyclophosphamide 1250 mg/m 2 (IV) X Vincristine 1,4 mg/m 2 (IV) [2mg max] X Procarbazine 100 mg/m 2 (PO) X X X X X X X Prednisone 40 mg/m 2 (PO) X X X X X X X X X

ABVD Contrôle de la maladie insuffisant pour 25 à 30 % des pts n CR 5y-PFS Follow-up Gordon JCO 2013 404 73% 74% 77 months Chisesi JCO 2011 126 89% 78% 86 months Viviani NEJM 2011 166 76% 73% 61 months Federico JCO 2009 102 84% 68% 41 months Hoskin JCO 2009 261 67% 76% 52 months Toxicité Pulmonaire Mayo clinic (n = 141): 18% des patients MSKCC (n = 152): 22% d arret précoce de la bleomycine Hoskin et al (UK) : 10% de toxicité pulmonaire g>3 RATHL: Réduction de DLCO moyenne = 11% après 6 ABVD = 4.3% après 2 ABVD + 4 AVD

HD9 10-years outcome by treatment arm Probability 1.0 0.9 0.8 0.7 0.6 0.5 0.4 0.3 0.2 0.1 0.0 p = <.001 A B C BEA esc C/ABVD 82% 64% 0 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 Pts. at Risk years A 261 194 173 146 110 75 19 0 B 469 378 332 282 222 106 26 0 C 466 412 384 321 234 92 14 0 FFTF 1.0 0.9 0.8 OS BEA esc 86% Probability 0.7 0.6 0.5 0.4 C/ABVD 75% 0.3 0.2 p = <.001 0.1 0.0 A B C 0 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 Pts. at Risk years A 261 238 218 196 147 107 30 0 B 469 436 392 344 272 134 36 0 C 466 441 412 357 270 113 18 0 Engert A, JCO 2009; 27: 2548

BEACOPP vs ABVD Stage IIB- IV BEACOPP [esc x 4 + Baseline x 2] vs ABVD x 6 Median FU = 41 months FFP OS Federico M, JCO,2009

BEACOPP vs ABVD Stage IIB- IV BEACOPP [esc x 4 + Baseline x 4] vs ABVD x 6/8 Median FU = 61 months FFP OS P = 0.004 P = 0.39 Viviani S, NEJM 2011; 365: 203

GELA H3-4 Trial IPS <3 Doxorubicine J1 et J15 : 25 Bleomycin J1 et J15 : 10 Vinblastine J1 et J15 : 6 DTIC J1 et J15 : 375 5y PFS* 5y OS 8 x ABVD N =77 N =68 8 x BEACOPP R 1 2 3 4 5 6 7 8 CT scan 1 2 3 4 5 6 7 8 75% 92% 93% 99% Bleomycin J1 10 10 Etoposide J1-3 200 100 Doxorubicine J1 35 25 Cyclophosphamide J1 1250 650 Vincristine J8 1.4 1.4 Procarbazine J1-7 100 100 Prednisone J1-14 40 40 *p= 0.008 p= 0.08 Mounier N, Cologne 2013 Abst T002

BEACOPP: Toxicité aigue Diehl et al, NEJM, 2003

BEACOPPesc : Fertilité Hommes 90% Azoospermie après 8 x BEACOPPesc Sienawski, Ann Oncol, 2008 Femmes: Aménorrhée 4 ans après fin Chimio 6-8 BEACOPPesc 2 BEACOPPesc + 2 ABVD ou 4 ABVD Behringer K, JCO, 2013

HD9 Secondary malignancy Secondary AML/MDS Engert A, JCO 2009; 27: 2548

HD15 5y FFTF: 6 Besc = 90.8% 8 Besc = 84.9% P<0.01 5y OS: 6 Besc = 96.2% 8 Besc = 91.8% P<0.01 Causes of death - N (%) BEACOPPesc x 8 (N=705) BEACOPPesc x 6 (N=711) Total 53 (7.5) 33 (4.6) Hodgkin lymphoma 13 (1.8) 11 (1.5) Toxicity of chemo 15 (2.1) 6 (0.8) 2 nd Neoplasia 13 (1.8) 5 (0.7) Toxicity of salvage treatment 2 (0.3) 2 (0.3) Other 10 (1.4) 9 (1.3) Engert A, Lancet 2012

Chimiothérapies de référence en 2014 5y-PFS 5y-OS 6 à 8 x ABVD 75% 90% 6 x BEACOPPesc 90% 96% BEACOPPesc est plus éradicateur que l ABVD, avec un meilleur contrôle de la maladie mais sans bénéfice sur la survie démontré Quel patient requière du BEACOPPesc?

Lymphome de Hodgkin FORMES AVANCÉES PATIENTS REQUÉRANT DU BEACOPP : VERS UNE STRATÉGIE ADAPTÉE

Engert A, JCO 2009; 27: 2548 HD9: IPS

PFS and DSS according to tumor microenvironment CD68+ cells Steidl C, NEJM 2010; 262: 875

Scott D, JCO 2012; 31: 692

A 23 Gene expression predictor in formalin-fixed paraffin-embedded tissue Training set Validation set Scott D, JCO 2012; 31: 692

PFS according to IL1RA IL6 CD30s signature in stages III & IV Score 0 27% Score 1-2 63% P<.0001 Score 3 10% Casasnovas O, JCO 2007; 25: 1732

Early PET PET2- PET2+ Hutchings M, Blood 2006; 107: 52 Gallamini A, JCO 2007; 25: 3746

Response adapted therapy of stages III IV Hodgkin Lymphoma based on interim FDG-PET imaging: US intergroup S0816 Objective: increase 2y-PFS from 70 % to 78 % HL Stage III-IV 18-60 y n = 357 s ABVD x 2 TEP 5PS = 4-5 5PS < 4 BEACOPP esc x 6 n = 55 (17 %) ABVD x 4 n = 277 Median FU = 16 months 100 80 79% PET2-: ABVD PFS 60 % 40 61% PET2+: BEACOPPesc 20 0 0 12 24 36 48 Mois 2y-PFS = 76% Press O, Cologne 2013 Abst T108

GITIL/FIL HD0607 ABVD x 2 N = 330 PET2 Negative N = 271 (82%) Positive N = 59 (18%) ABVD x 5 BEACOPP esc x 4 + BEACOPP b x 4 R-BEACOPP esc x 4 + R-BEACOPP b x 4 2y-PFS 85% 61% Median FU = 32 months Gallamini A, Cologne 2013 Abst P006

LYSA: AHL 2011 Standard Arm R Experimental Arm BEACOPP esc x 2 BEACOPP esc x 2 PET2 Neg / Pos Pos Neg BEACOPP esc x 2 BEACOPP esc x 2 ABVD x 2 PET4 Neg Pos Neg Pos Neg BEACOPP esc x 2 Salvage therapy BEACOPP esc x 2 Salvage therapy ABVD x 2 Non inferiority of the experimental arm

GHSG: HD18 BEACOPP esc x 2 PET2 Positive Negative BEACOPP esc x 4 BEACOPP esc x 4 BEACOPP esc x 2 End of therapy AND residual nodes > 2.5 cm: PET positive: PET negative: Rx Follow up

Lymphome de Hodgkin FORMES AVANCÉES CHIMIOTHERAPIE + ANTICORPS

MAb + ABVD in advanced HL n RC 5y-PFS Median FU ABVD Gordon JCO 2013 404 73% 74% 77 months ABVD Chisesi JCO 2011 126 89% 78% 86 months ABVD Viviani NEJM 2011 166 76% 73% 61 months R-ABVD Younes Blood 2012 78 93% 82% 68 months R-ABVD Kasamon Blood 2012 49 81% 83% 33 months BV-ABVD Ansell ASH 2012 / 22 95% - BV-AVD Cologne 2013 25 96% -

Adcetris combiné à A(B)VD 51 Hodgkin avancés (45% stade IV, 25% IPS>3, 33% Bulk) BV-ABVD BV-AVD Inclus (n) 25 26 BV 0.6mg/kg 6 0 BV 0.9mg/kg 13 0 BV 1.2mg/kg 6 26 Tox pulmonaire gr>0/ gr 3/gr=5 11 (44%)/ 6 (24%)/ 2 (8%) 0 Embolie pulmonaire gr 3 3 (12%) 0 Neuropathie gr>0 18 (73%) 20 (72%) Neutropénie fébrile gr 3 5 (20%) 2 (8%) Aucune DLT observée (Cycle 1)

ECHELON 1 Standard Arm Stage III/IV R Experimental Arm ABVD x 2 AVD-A x 2 PET2 5PS = 1-4 5PS = 5 5PS = 1-4 ABVD x 4 Protocol Therapy or Salvage therapy AVD-A x 4 Planned Accrual = 1040 pts Primary endpoint: PFS

Targeted BEACOPP Drug Day 6x BEACOPP escalated 6x BrECADD ( experimental ) 6x BrECAPP ( standard ) Bleomycin 8 10 Etoposide 1-3(2-4) 200 150 200 Adriamycin 1(2) 35 40 35 Cyclophosphamide 2 1250 1250 1250 Vincristine 8 1.4 Brentuximab vedotin 1 1.8 1.8 Procarbazine 1-7 (2-8) 100 100 Prednisone 1-14(2-15) 40 40 Dacarbazine 2-3 2x 250 Dexamethasone 2-5 40

Acute Toxicities BrECADD (n=29) Type of Toxicity NCIC-CTC Grade none I II III IV III/IV HD18* III/IV (n=447) Hematological 0% 2 (7%) 1 (3%) 2 (7%) 24 (83%) 26 (90%) 404 (90.4%) Organs 14 (48%) 10 (34%) 5 (17%) 0% 0% 0% 64 (14.3%) No severe neuropathy in > 250 cycles 31

Treatment outcome after chemotherapy (primary endpoint) Treatment Outcome BrECAPP N = 16 BrECADD N = 16 Total N = 32 CR or PET negative* PR Less than PR or PET positive* 14 (87,5%) 16 (100%) 30 (93,75%) 2 (12,5%) 0 (0%) 2 (6,25%) 10.05.2014 *PET above liver (Deauville 4) is regarded positive 32

INTERET D UNE INTENSIFICATION DE PREMIÈRE LIGNE?

Stage IIIB-IV, < 55 y HD-01 trial EBMT/SFGM/GELA High risk according to Strauss criteria M / T >0.45 Stage IV > 1 extranodal site LDH Inguinal node involvement Hb <12 (male) / 10 (female) Bone marrow involvement ABVD x 4 ABVD x 4 ASCT

HD-01 trial EBMT/SFGM/GELA 8 x ABVD 4 x ABVD ASCT n 80 80 IPS(%) 0-2 3+ 39 61 44 56 5y FFS 82 75 5y OS 88 90 Median FU 50 months Federico M, JCO 2003; 21: 2320

HD-01 trial EBMT/SFGM/GELA Federico M, JCO 2003; 21: 2320

Stage IIB,III, IV; 18-60 y High risk: M / T 0.45 H97-HR GOELAMS (1997 2004) Stage IV 2 extranodal site 5 nodal area involvement R ABVD x 4 + ASCT (BEAM) VABEM x 3 + Radiotherapy 20Gy + Boost

H97-HR GOELAMS (1997 2004) n = 158 79% 75% 87% 86% Arakelyan N, Cancer 2008; 113: 3323

Lymphome de Hodgkin FORMES AVANCÉES PLACE DE LA RADIOTHÉRAPIE

H89 8x ABVPP 6x ABVPP +STNI 6x MOPP/ABV +STNI 8x MOPP/ABV n 116 96 114 92 CR (%) 99 91 95 91 10y-EFS (%) 67 69 77 71 10y-OS (%) 90 87 82 78 Ferme C, et al. Blood 2006; 107: 4636

Advanced HL in first CR after 6-8 MOPP/ABV Aleman B, et al. NEJM 2003;348: 2396

Advanced HL (stage III-IV) after 6-8 MOPP/ABV Aleman B, et al. NEJM 2003;348: 2396

HD12 Residual disease after chemo Initial bulk without residual disease after chemo Borchmann P, et al. JCO 2011;29: 4234

HD15: study 1788 pts Dose density and reduction of toxicity A B C 8 x BEACOPP escalated Randomization 6 x BEACOPP escalated 8 x BEACOPP 14 ( baseline) Residual tumor mass? Yes PET positive: RT 30 Gy 15% of all pts! (>2.5 cm) PET-study PET negative: follow up No follow up

HD 15 Trial 8 vs 6 BEAesc vs 8 BEA-14 817 patients randomized and evaluable for outcome PET after end of chemotherapy for >2,5cm rests: Patients with rests >2,5 cm: n = 311 245 (78,8%) PET neg: no RT: 244 4,1% relapses 66 (21,2%) PET pos: IF-RT: 62 15,3% relapses

Conclusions Pas de bénéfice démontré chez les patients en 1 ère réponse: de la radiothérapie de l intensification avec autogreffe de CSH 6-8 x ABVD ou 6 x BEACOPPesc BEACOPPesc est le traitement le plus éradicateur au prix d une toxicité immédiate et retardée significative Pas d éléments pronostiques simples pour cibler les patients devant recevoir l un ou l autre des schémas Risques liés à l hématotoxicité Fertilité Les stratégies TEP guidées pourraient permettre de limiter le nombre de cycles de BEACOPPesc pour les patients répondeurs précoces (>80%?) et donc la toxicité BV-AVD futur challenger du BEACOPPesc?