Nasopharyngeal Cancer Clinical Trial
Official title:
Administration of EBV-Specific Cytotoxic T Lymphocytes Following CD45 Antibody to Patients With EBV Positive Nasopharyngeal Carcinoma
To determine the safety of the combination of CD45 monoclonal antibody (Mab) followed by
intravenous injection of EBV specific CTL in patients with nasopharyngeal cancer.
To compare the expansion, persistence and anti-tumor effects of the EBV specific CTL given
after CD45 Mab administration with that observed in our first study.
To obtain preliminary information on the safety and response to an extended dosage regimen
of EBV-specific CTL in patients, who have stable disease or a partial response after the
initial dose of EBV-specific CTL.
Three different doses of CTL will be evaluated: dose level I: 2 x 10e7/m2; dose level II: 5
x 10e7/m2; dose level III: 1 x 10e8/m2
Day 1 YTH 24/54 800ug/kg over 8 hr; Day 2 YTH 24/54 800ug/kg over 8 hr; Day 3 Rest; Day 4-6
CTL Infusion (provided CD45 Mab level <100 ug/ml).
Generation of EBV-specific CTL
After consent on the separate procurement protocol for CTL preparation the patient will
donate up to 60-70cc of peripheral blood. 10-20cc of this will be used for the establishment
of an EBV transformed lymphoblastoid cell line (EBV-LCL) by infection with virus produced
from the B95-8 master cell line. The EBV-LCLs will take approximately four to six weeks to
establish. 30-40cc of peripheral blood will be used to generate EBV specific CTLs. The CTL
line will be prepared by co-cultivation of the irradiated EBV-LCL with patient PBMC. After
establishment, the CTL lines will be checked for identity, phenotype and microbiological
culture and cryopreserved prior to administration according to SOPs. The antigen specificity
of each CTL line will be determined in cytotoxicity assay and when possible with tetramer
reagents.
CD45 monoclonal antibodies
Anti-CD45 is a combination in equal amounts (weight for volume) of two monoclonal antibodies
that are directed to non-overlapping epitopes on human CD45. It is a purified, concentrated,
and sterile gamma globulin, primarily monomeric IgG, produced from the supernatant of the
two rat IgG2b hybridoma clones, YTH 24 and YTH 54. The hybridomas were produced as fusions
between splenocytes from DA rats immunized with human leukocytes and the rat myeloma line
Y3. The combination of the two MAbs exerts a synergistic effect in vitro on
complement-mediated cytotoxicity of white cells and it has been demonstrated to clear almost
all passenger leukocytes from donor kidneys before transplant. Anti-CD45 Mabs have been made
under cGMP conditions at the Therapeutic Antibody Center at Oxford and at Baylor College of
Medicine and will pass the safety tests required by the FDA.
Cell administration
Patients will be pre-medicated with Diphenhydramine 1mg/kg IV (max 50 mg) and Acetaminophen
10mg/kg po (max 650 mg). EBV specific T cells will be given by intravenous injection over
1-10 minutes through either a peripheral or a central line. Outpatients may be treated in
the clinic. Monitoring will be undertaken according to institutional standards for
administration of blood products with the exception that the injection will be given by a
physician. Anti-emetics in appropriate dosage for each patient will be prescribed as
necessary. Patients will receive supportive care for acute or chronic toxicity, including
blood components or antibiotics, and other intervention as appropriate.
Antibody administration
Patients will be pre-medicated with Diphenhydramine 1mg/kg IV (max 50 mg) and Acetaminophen
10mg/kg po (max 650 mg). 800ug/kg CD45 Mabs will be given as 2 daily intravenous infusions
over 8 hours. The antibody aliquot to be infused will arrive in the treatment area
hand-carried by the attending physician or appointed designate. The antibody aliquot will be
diluted in minimal amounts of normal saline. The resulting solution is stable for 24 hours.
The antibody solution is administered by a syringe pump in incremental doses, 0.2-0.8 mg in
the first hour and up to 10 mg/hr thereafter, for a total infusion time of a maximum of 6
hrs. A registered nurse and a physician must be readily available.
;
Endpoint Classification: Safety Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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