Rabbit Antithymocyte Globulin Versus Campath-1H for Treating Severe Aplastic Anemia



Status:Completed
Conditions:Anemia
Therapuetic Areas:Hematology
Healthy:No
Age Range:2 - Any
Updated:4/21/2016
Start Date:July 2003
End Date:March 2015

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A Randomized Trial of Immunosuppression in Aplastic Anemia Patients With Refractory Pancytopenia or Suboptimal Hematologic Response After h-ATG/CsA Treatment

Severe aplastic anemia, characterized by pancytopenia and a hypocellular bone marrow, is
effectively treated by immunosuppressive therapy, usually a combination of antithymocyte
globulin (ATG) and cyclosporine (CsA). Survival rates following this regimen are equivalent
to those achieved with allogeneic stem cells transplantation. However, approximately 1/3 of
patients will not show blood count improvement after ATG/CsA. General experience and small
pilot studies have suggested that such patients may benefit from further immunosuppression.
Furthermore, analysis of our own clinical data suggest that patients with poor blood count
responses to a single course of ATG, even when transfusion-independence is achieved, have a
markedly worse prognosis than patients with robust hematologic improvement. The management
of such cases is uncertain.

This study will enroll patients who are either refractory to h-ATG (continued severe
pancytopenia) or who have only modest improvement in blood counts (weak hematologic
responders) to receive a further immunosuppressive therapy, delivered either as rabbit ATG
(Thymoglobulin, r-ATG) or a humanized monoclonal antibody to T-cells, alemtuzumab
(Campath-1H ). Primary endpoint will be response rate at 3 months defined as no longer
meeting criteria for severe aplastic anemia. Relapse, robustness of hematopoietic recovery
at 3 months, survival and clonal evolution to paroxysmal nocturnal hemoglobinuria (PNH),
myelodysplasia and acute leukemia will be the secondary endpoints.

Severe aplastic anemia, characterized by pancytopenia and a hypocellular bone marrow, is
effectively treated by immunosuppressive therapy, usually a combination of antithymocyte
globulin (ATG) and cyclosporine (CsA). Survival rates following this regimen are equivalent
to those achieved with allogeneic stem cells transplantation. However, approximately 1/3 of
patients will not show blood count improvement after ATG/CsA. General experience and small
pilot studies have suggested that such patients may benefit from further immunosuppression.
Furthermore, analysis of our own clinical data suggest that patients with poor blood count
responses to a single course of ATG, even when transfusion-independence is achieved, have a
markedly worse prognosis than patients with robust hematologic improvement. The management
of such cases is uncertain.

This study will enroll patients who are either refractory to h-ATG (continued severe
pancytopenia) or who have only modest improvement in blood counts (weak hematologic
responders) to receive further immunosuppressive therapy, delivered either as rabbit ATG
(Thymoglobulin , r-ATG) or a humanized monoclonal antibody to T-cells, alemtuzumab
(Campath-1H ). Primary endpoint will be response rate at 6 months defined as no longer
meeting criteria for severe aplastic anemia. Relapse, robustness of hematopoietic recovery
at 6 months, survival and clonal evolution to paroxysmal nocturnal hemoglobinuria (PNH),
myelodysplasia and acute leukemia will be the secondary endpoints.

- INCLUSION CRITERIA:

Severe aplastic anemia confirmed at NIH by:

Bone marrow cellularity less than 30% (excluding lymphocytes)

At least two of the following:

Absolute neutrophil count less than 500/microL;

Platelet count less than 20,000/ microL;

Reticulocyte count less than 60,000/ microL.

Severe aplastic anemia refractory to prior course(s) of h-ATG/CsA defined after 3 months
from treatment with less or equal to 4 years from receiving h-ATG.

OR

Suboptimal response to initial immunosuppression with h-ATG/CsA as defined by platelet and
reticulocyte count less than 50,000 /microL at 3 months.

Age greater than or equal to 2 years of age

EXCLUSION CRITERIA:

Diagnosis of Fanconi anemia.

Evidence of a clonal disorder on cytogenetics. Patients with super severe neutropenia (ANC
less than 200/microL) will not be excluded initially if results of cytogenetics are not
available or pending. If evidence of a clonal disorder is later identified, the subject
will go off study.

Prior treatment courses with rabbit ATG or high dose cyclophosphamide (200 mg/kg or
equivalent).

Infection not adequately responding to appropriate therapy.

Underlying immunodeficiency state including seropositivity for HIV.

Failure to discontinue the herbal supplements Echinacea purpurea or Usnea barbata (Old
Man's Beard) within two weeks of enrollment.

Previous hypersensitivity to Campath-1H or its components.

Moribund status or concurrent hepatic, renal, cardiac, neurologic, pulmonary, infectious,
or metabolic disease of such severity that it would preclude the patient s ability to
tolerate protocol therapy or that death within 7-10 days is likely.

Potential subjects with cancer who are on active chemotherapeutic treatment or who take
drugs with hematological effects will not be eligible.

Serum creatinine greater than 2.5 mg/dL.

Current pregnancy or lactation or unwillingness to take contraceptives.

Inability to understand the investigational nature of the study or give informed consent.
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
?
mi
from
Bethesda, MD
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