Abstract 2329

The mainstay of treatment for Chronic Graft Versus Host Disease (cGVHD) is steroids, but there are limited treatment options for steroid refractory cGVHD particularly in its sclerotic and fibrotic form (ScGVHD). We initially reported the efficacy and safety of imatinib mesylate (IM), a first generation tyrosine kinas' inhibitor, as a salvage therapy for ScGVHD patients (Magro L, et al. Blood, 2009). However, about 50% of the patients (Pts) became refractory or intolerant to IM. Nilotinib, a second generation tyrosine kinas' inhibitor, is labelled for IM resistant and advanced Chronic Myeloid leukemia and could be an attractive alternative to IM especially in refractory and intolerant patients.

We studied the clinical outcomes of 7 Pts who developed extensive ScGVHD at our institution. Among them, 5 had received prior IM. Patients' characteristics and transplantation modalities are summarised in table 1. Acute and cGVHD was scored according to standard criteria. All pts but one failed at least 3 lines of prior systemic immunosuppressive therapy.

CGVHD features, responses to nilotinib and patients' outcomes are described in table 2.

To our knowledge, this is the first report relating the impact of nilotinib on cGVHD setting. Although, tolerance to nilotinib has not been as good as we could expect, this drug appeared to be effective with manageable side-effects in some patients. One of the limitations of this study, is that nilotinib was used in patients with advanced cGVHD. Prospective studies are, therefore, warranted to investigate the efficacy and the tolerance of nilotinib in patients with less advanced disease.

Table 1.

Patients and transplantation characteristics

Case NAge, ySex, R/DdiagnosisConditioning/Stem cell sourceGVHD prophylaxiscGVHD sitesImmunosuppression before nilotinib
30.5 M/F ALL MAC/BM CSA-MTX Mouth, skin eyes,liver CS-CSA-MMF-RTX-EVE 
31 F/M AA MAC/PBSC CSA-CS-MMF Skin, mouth, eyes,bronchiolitis,joint contacture CS-TAC-MMF-EVE-IM 
51.6 M/M HODG RIC/PBSC CSA-MTX Skin, mouth CS-CSA-MMF-IM 
45.3 M/M AML MAC/BM CSA-MTX Skin, mouth, bronchiolitis, joint contracture CS-CSA-MMF-INO-ECP-RTX-AZA-IM 
57.5 M/M MDS MAC/BM CSA-MTX Skin, bronchiolitis, joint contracture CS-CSA-MMF-RTX-ECP-IM 
50.3 M/F CML MAC/BM CSA-MTX Skin, mouth, eyes, liver, joint contracture CS-CSA-MMF-ECP-IM 
53.3 M/M AML MAC/BM CSA-MTX Skin none 
Case NAge, ySex, R/DdiagnosisConditioning/Stem cell sourceGVHD prophylaxiscGVHD sitesImmunosuppression before nilotinib
30.5 M/F ALL MAC/BM CSA-MTX Mouth, skin eyes,liver CS-CSA-MMF-RTX-EVE 
31 F/M AA MAC/PBSC CSA-CS-MMF Skin, mouth, eyes,bronchiolitis,joint contacture CS-TAC-MMF-EVE-IM 
51.6 M/M HODG RIC/PBSC CSA-MTX Skin, mouth CS-CSA-MMF-IM 
45.3 M/M AML MAC/BM CSA-MTX Skin, mouth, bronchiolitis, joint contracture CS-CSA-MMF-INO-ECP-RTX-AZA-IM 
57.5 M/M MDS MAC/BM CSA-MTX Skin, bronchiolitis, joint contracture CS-CSA-MMF-RTX-ECP-IM 
50.3 M/F CML MAC/BM CSA-MTX Skin, mouth, eyes, liver, joint contracture CS-CSA-MMF-ECP-IM 
53.3 M/M AML MAC/BM CSA-MTX Skin none 

R/D: recipient/donor;

aGVHD: acute graft versus host disease;

cGVHD: chronic graft versus host disease;

CML: chronic myeloid leukemia;

MAC: myeloablative conditioning;

BM: bone marrow;

PBSC: peripheral blood stem cells;

CSA: ciclosporine A;

CS: corticosteroids, RIC: reduced intensity conditioning;

MMF: mycophenolate mofetyl;

AZA: azathioprine;

MDS: myelodysplastic syndrome;

MTX: metothrexate;

RTX: rituximab;

ECP: extracorporal photophere-sis;

INO: inolimomab; HODG, hodgkin;

AA: aplastic anemia;

TAC: tacrolimus, ALL: acute lymphoblastic leukemia;

AML: acute myeloid leukemia.;

EVE: everolimus and IM: imatinib mesylate.

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Table 2.

Outcome after nilotinib therapy

Case N°Maximal tolerate dose of nilotinib, mgNilotinb therapy duration at last follow up, moSide effects/nilotinib discontinuation at last follow upcGVHD status at 2 mo of nilotinibcGVHD response in other organs at last follow upcGVHD status at last follow upOverall follow-up, moStatus at last follow up
800 None/yes failure – PR 69 alive 
400 0.5 Pain swallowing, diarrhea/yes failure – progressive 46.8 Died of infection 
800 2.5 Nausea, diarrhea/yes PR Mouth PR (>90%) 73.1 alive 
800 7.5 None/yes MR Mouth progressive 72 alive 
800 Cough, dyspnea, muscle cramps/yes PR bronchiolitis PR 59 alive 
800 0.5 Headache, diarrhea/yes failure – PR 60.3 alive 
800 7.5 None/no PR – PR 32 alive 
Case N°Maximal tolerate dose of nilotinib, mgNilotinb therapy duration at last follow up, moSide effects/nilotinib discontinuation at last follow upcGVHD status at 2 mo of nilotinibcGVHD response in other organs at last follow upcGVHD status at last follow upOverall follow-up, moStatus at last follow up
800 None/yes failure – PR 69 alive 
400 0.5 Pain swallowing, diarrhea/yes failure – progressive 46.8 Died of infection 
800 2.5 Nausea, diarrhea/yes PR Mouth PR (>90%) 73.1 alive 
800 7.5 None/yes MR Mouth progressive 72 alive 
800 Cough, dyspnea, muscle cramps/yes PR bronchiolitis PR 59 alive 
800 0.5 Headache, diarrhea/yes failure – PR 60.3 alive 
800 7.5 None/no PR – PR 32 alive 

cGVHD indicates chronic graft versus host disease; PR, partial response and MR, minor response.

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Disclosures:

No relevant conflicts of interest to declare.

Topics:
graft-versus-host disease, chronic, nilotinib, salvage therapy, complement membrane attack complex, mac protocol, mdc protocol, mitral valve annular calcification, monitored anesthesia care, follow-up, bronchiolitis

Author notes

*

Asterisk with author names denotes non-ASH members.

© 2010 by The American Society of Hematology
2010
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