-Author name in bold denotes the presenting author
-Asterisk * with author name denotes a Non-ASH member
Clinically Relevant Abstract denotes an abstract that is clinically relevant.

PhD Trainee denotes that this is a recommended PHD Trainee Session.

Ticketed Session denotes that this is a ticketed session.

1939 Treatment of Chronic Graft Versus Host Disease with a Combination of B-Cell Depletion and Tyrosine Kinase Inhibition

Clinical Allogeneic Transplantation: Acute and Chronic GVHD, Immune Reconstitution
Program: Oral and Poster Abstracts
Session: 722. Clinical Allogeneic Transplantation: Acute and Chronic GVHD, Immune Reconstitution: Poster I
Saturday, December 5, 2015, 5:30 PM-7:30 PM
Hall A, Level 2 (Orange County Convention Center)

Lotte van der Wagen, MD1*, Liane CJ te Boome, MD1,2, Inger Nijhof1*, Marieke Schoordijk3*, Denise Buter1*, Ellen Meijer, MD PhD4 and Jurgen Kuball, MD PhD1

1Hematology, University Medical Center Utrecht, Utrecht, Netherlands
2Hematology, MC Haaglanden, Den Haag, Netherlands
3Hematology, VU University Medical Center, Amsterdam, Netherlands
4Hematology, VU University Medical Center, Amsterdam, Netherlands

Chronic Graft Versus Host Disease (cGVHD) affects about 60% of all patients receiving an allogeneic hematopoietic stem cell transplantation (HSCT) and surviving beyond day 100. Incidence of cGVHD is rising because of the widespread use of Peripheral Blood Stem Cells (PBSC) as stemcell source. Chronic GVHD accounts for high morbidity and mortality rates. Affected patients require long term use of immunosuppressive drugs, mainly corticosteroids, which lead to development of severe side effects. Both the manifestations of cGVHD as the side effects from immune suppressive drugs account for a decrease in quality of life when cGVHD develops. Therefor new therapeutic strategies are urgently needed.

Therapeutic approaches for cGVHD are limited. Generally recommended first line therapy consists of glucocorticoid therapy combined with a calcineurin inhibitor. Options for second line therapy are numerous but no consensus on the most favourable choice of agents has been reached.

However as both monotherapy with rituximab and monotherapy with tyrosine kinase inhibition have shown to be effective in reducing cGVHD symptoms . We aimed to test whether the sequential therapy of the anti CD20 antibody rituximab followed by a 6 month treatment period with the tyrosine kinase inhibitor nilotinib is a good treatment strategy for patients with sclerotic cGVHD (EudraCT nr 2008-004125-42).

We treated 26 patients with a combination of 4 weekly infusions of rituximab followed by a 6 month period of treatment with nilotinib (300mg b.i.d.). Patients were evaluated monthly for 13 months and sequential blood samples and skin biopsies were analyzed. All patients gave informed consent before enrollment.

3 patients experienced severe side effects from either rituximab or nilotinib treatment and therefor were taken off study. Of the remaining 13 patients who thus far have completed the study protocol, 60% showed a (partial) response (3 patients went from NIH scoring ‘severe' to ‘moderate', 1 patient went from NIH scoring ‘moderate' to ‘no cGVHD'). There is also a significant decrease in cGVHD affected body surface area (Figure 1). Moreover, two out of four patients who suffered from severe ulcerations at the start of the study had a complete resolution of ulcers at the end of the treatment period. Patients with a (partial) response also showed a decrease in self attributed severity of cGVHD and their immunosuppressive drugs could be tapered.

The sequential therapy of B-cell depletion and tyrosine kinase inhibition provides a new and interesting alternative treatment option for this difficult and heavily pretreated patient category.

Figure 1. Percentage of total body surface area affected by chronic Graft versus Host Disease is plotted against time in months after start of the study. Each dot represents 1 patient. P-values are calculated by means of Wilcoxon matched-pairs signed rank test.

 

Patients

 

 

26

 

Male sex

 

 

20

 

Mean age in years

(range)

47,5

21-70

Primary diagnosis

 

 

 

 

AML

 

7

 

 

Multiple myeloma

5

 

 

ALL

 

4

 

 

Lymphoma

 

4

 

 

MDS

 

2

 

 

CLL

 

1

 

 

Myeloproliferative disorder

2

 

 

aplastic anemia

 

1

 

Mean days after allo SCT

(range)

1368

411-3820

Ulcerative chronic GvHD at start

5

 

NIH grade severity cGVHD at start

 

 

 

severe

 

20

 

 

moderate

 

6

 

Table 1: Baseline characteristics of participants.

 

Disclosures: Off Label Use: Anti CD20 antibody rituximab is used for sclerotic chronic GVHD. Tyrosine kinase inhibitor nilotinib is used for sclerotic chronic GVHD. .

*signifies non-member of ASH