Phase I, Initial Safety/Toxicity Study on the Transfer of Adenovirus With the CD40 Ligand Gene (AdCUCD40L) to Patients With Stage III or IV Esophageal Carcinoma
Overview
- Phase
- Phase 1
- Intervention
- Not specified
- Conditions
- Esophageal Neoplasms
- Sponsor
- Weill Medical College of Cornell University
- Locations
- 2
- Primary Endpoint
- Since this is a dose escalation, phase I design to evaluate toxicity, the analysis for this section will be purely descriptive. Adverse events will be considered on an individual basis.
- Status
- Withdrawn
- Last Updated
- 10 years ago
Overview
Brief Summary
This a pilot clinical study focused on enhancing the patient's anti-tumor immune response in individuals with esophageal cancer by altering the genetic repertoire of the tumors to express CD40L, an activator of dendritic cells. This will be accomplished by endoscopic administration to the tumors of AdcuCD40L, an adenovirus gene transfer vector expressing the coding sequence of the human CD40L cDNA. This study is designed to assess the hypothesis that it is safe to administer the AdcuCD40L vector to individuals with esophageal cancer.
Detailed Description
Esophageal cancer is a deadly disease, with only slow advances in therapy over several decades, despite a rapid increase in incidence. Esophageal cancer is estimated to be the seventh most common malignancy worldwide, with incidence rates reaching epidemic proportions in select regions in Asia and Africa. In the United States, it is estimated that 12,300 new cases were diagnosed in 2000, however, the incidence of adenocarcinoma of the esophagus is currently rising faster than that of any other human malignant tumor in this country. Despite advances in surgical technique, chemotherapy, radiotherapy and early detection, only 12% of patients diagnosed with esophageal cancer will survive more than five years, a cure rate more dismal than that seen with cancers of the breast, prostate, colon, and even lung. Survival following treatment for esophageal cancer is stage dependent. This study is directed towards augmenting host anti-tumor immunity by using gene transfer to activate dendritic cells (DC; cells of our immune system that play a central role in initiating immune responses) in tumors of patients with esophageal cancer. Based on extensive pre-clinical data, two proposed clinical trial protocols will evaluate the concept that transient modification of the genetic repertoire of esophageal tumors to express CD40 Ligand (CD40L; a potent activator of DC) will induce the accumulation of activated DC within the tumor, and the in vivo interaction of DC with the tumor cells/tumor antigens will induce tumor-specific immunity. To assess this concept, an adenovirus (Ad) vector (AdcuCD40L) will be used to transfer and transiently express the human CD40L cDNA in esophageal carcinoma by direct injection into the tumor. Phase I represents a dose escalation study to determine the maximum tolerated dose of the vector and will include 12 individuals with unresectable, stage III or IV esophageal cancer. Phase II is a randomized, double-blinded assessment of biologic efficacy and will include 24 individuals with resectable, stage I-III disease who will be undergoing potentially curative resection. Together, both protocols are designed to assess two hypotheses. First, that it is safe to administer the AdcuCD40L vector to individuals with esophageal cancer. Second, that intratumoral administration of the AdCUCD40L vector will induce both the accumulation, in the tumor and in regional lymph nodes, of activated DC, and CD8+ T cells (and other inflammatory cells), including T cells exhibiting tumor-specific responses, as well as systemic antitumor immunity.
Investigators
Eligibility Criteria
Inclusion Criteria
- •Must be capable of providing informed consent
- •Males and females, age 18 to 75 years
- •Hematocrit \> 30%
- •WBC \< 10,000
- •Normal prothrombin, partial thromboplastin time; platelet count \> 100,000
- •Normal liver-related serum parameters
- •Blood urea nitrogen \< 60 mg/dL, creatinine \< 2.5 mg/dl
- •No evidence of active infection of any type, including with adenovirus, hepatitis virus (A, B or C) or human immunodeficiency virus
- •No evidence of central nervous system, major psychiatric, musculoskeletal or immune disorder
- •No allergy to the vehicle used to suspend the virus or contrast materials used in radiographic procedures
Exclusion Criteria
- •Individuals who do not meet the inclusion criteria will be unable to participate in the protocol
- •Individuals in whom participation in the study would compromise the normal care and expected progression of their disease
- •Individuals receiving corticosteroids or other immunosuppressive medications; previous splenectomy or radiation to the spleen; autoimmune disease
- •Recent (less than 6 wk) cerebral vascular accident
- •Recent (less than 6 wk) transmural myocardial infarction
- •Evidence of infection defined by elevated white blood cell count, temperature \> 38.5oC or infiltrate on chest x-ray
- •Cervical esophageal cancer
- •Gastric cancer (tumor more than 50% in the stomach as determined by endoscopy)
- •Lack of viable esophageal tumor (applies only to pretreated patients)
- •Pathology other than squamous cell or adenocarcinoma
Outcomes
Primary Outcomes
Since this is a dose escalation, phase I design to evaluate toxicity, the analysis for this section will be purely descriptive. Adverse events will be considered on an individual basis.
Time Frame: 8 months