HIV Infection Clinical Trial
Official title:
A Phase II, Open-label, Multicenter Study to Evaluate the Safety, Tolerability, and Biological Activity of Single and Repeated Doses of Autologous T Cells Transduced With VRX496 in HIV-Positive Subjects
| Verified date | June 2011 |
| Source | VIRxSYS Corporation |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | United States: Food and Drug Administration |
| Study type | Interventional |
This study uses autologous (one's own) CD4 T cells modified with a viral vector expressing a genetic antisense targeting HIV, this vector is called VRX496. Study treatment is by intravenous infusion of vector modified cells and infusions will be provided every other week for a total of 4 or 8 doses. These modified cells, once infused, may provide immune support and are not destroyed by HIV, and thus may delay or reverse HIV disease progression. The study will enroll up to 40 male and female HIV-positive subjects in up to 8 centers. Subjects will be 18 years of age and over who have failed or are intolerant to at least one triple combination of antiretroviral drugs. Subjects must have a viral load between 5,000 and 200,000 copies/ml and a CD4+ count of ≥150, be in good health and have no evidence of active opportunistic infection, heart disease, or bleeding disorders. Subjects must not be on corticosteroids, immunomodulating agents or hydroxyurea. Subjects must not have received an AIDS vaccine or any investigational gene therapy product at any time. Females must not be pregnant or breastfeeding.
| Status | Active, not recruiting |
| Enrollment | 60 |
| Est. completion date | June 2023 |
| Est. primary completion date | November 2008 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 18 Years to 65 Years |
| Eligibility |
Inclusion Criteria: - Sero-positive for infection with HIV and failed, or be intolerant to, at least one triple combination of antiretroviral agent - If on antiretroviral therapy, subject must be willing to continue on current antiretroviral therapy; or if discontinues antiretroviral therapy must have a wash-out period of 6 weeks prior to screening; or if not on antiretroviral therapy must be willing to remain off antiretroviral therapy for the duration of the study (i.e. up to 1 year) - Male or female, 18 years of age and older - Karnofsky Performance score of 80 or higher - Stable HIV viral load between 5,000 and 200,000 copies/mL at the time of screening. Stable will be defined as a variation of less than 0.5 log10 in the 3 months prior to screening while on a stable regimen or no therapy - CD4 T cell count equal to or greater than 150 cells per µL at the time of screening - A body weight greater than 50 Kg - Adequate venous access and no other contraindications for leukapheresis - Subject must be willing to comply with study-mandated evaluations Exclusion Criteria: - A history of any type of cancer or malignancy, with the exception of (successfully) treated basal cell or squamous cell carcinoma of the skin - A history or any features on physical examination indicative of cardiac disease or hemodynamic instability - Any history or any features on physical examination indicative of a bleeding diathesis - Previous treatment with any HIV experimental vaccine or any gene therapy products - A positive signal for VSV-G antibodies and/or VSV-G DNA in the blood at screening - Any of the following lab results: - Hemoglobin: <10 (males); <9.5 (females) g/dL - Absolute neutrophil count: < 1000/µL - Platelet count: <100,000/mm3 - Serum creatinine: > 1.5 mg/dL (133µ mol/L) - AST or ALT: > 2.5 times the upper limit of normal - Total serum bilirubin: > 1.5 times the upper limit of normal - Proteinuria: 2+ on urine dipstick - Subjects must not be breastfeeding, be pregnant, or unwilling to use acceptable methods of birth control - Subjects must not be on chronic oral corticosteroids within 30 days of screening - (if subjects are prescribed a brief course of oral corticosteroids the use should be limited to less than 1 week), hydroxyurea, or immunomodulating agents (e.g., IL 2, interferon-gamma, granulocyte colony stimulating factors, etc.) within 30-days of screening or foreseeably need any of these within the study period - Subjects must not be using aspirin, dipyridamole, warfarin or any other medication likely to affect platelet function or other aspects of blood coagulation during the period when leukapheresis is scheduled - Subjects must not suffer from active drug or alcohol dependence or abuse, to an extent that, in the opinion of the investigator, would interfere with their ability to comply with study requirements - Any serious illnesses or acute opportunistic infection - Any other illness or condition which in the opinion of the investigator would exclude the subject from the study - Subjects unable or unwilling to give written informed consent |
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| United States | Jacobi Medical Center | Bronx | New York |
| United States | University of Kentucky | Lexington | Kentucky |
| United States | Steinhart Medical Associates | Miami | Florida |
| United States | CIRCLE Medical, LLC | Norwalk | Connecticut |
| United States | Stanford AIDS Clinical Trials Unit | Palo Alto | California |
| Lead Sponsor | Collaborator |
|---|---|
| VIRxSYS Corporation |
United States,
Humeau LM, Binder GK, Lu X, Slepushkin V, Merling R, Echeagaray P, Pereira M, Slepushkina T, Barnett S, Dropulic LK, Carroll R, Levine BL, June CH, Dropulic B. Efficient lentiviral vector-mediated control of HIV-1 replication in CD4 lymphocytes from diverse HIV+ infected patients grouped according to CD4 count and viral load. Mol Ther. 2004 Jun;9(6):902-13. — View Citation
Lu X, Humeau L, Slepushkin V, Binder G, Yu Q, Slepushkina T, Chen Z, Merling R, Davis B, Chang YN, Dropulic B. Safe two-plasmid production for the first clinical lentivirus vector that achieves >99% transduction in primary cells using a one-step protocol. J Gene Med. 2004 Sep;6(9):963-73. — View Citation
Lu X, Yu Q, Binder GK, Chen Z, Slepushkina T, Rossi J, Dropulic B. Antisense-mediated inhibition of human immunodeficiency virus (HIV) replication by use of an HIV type 1-based vector results in severely attenuated mutants incapable of developing resistance. J Virol. 2004 Jul;78(13):7079-88. — View Citation
Manilla P, Rebello T, Afable C, Lu X, Slepushkin V, Humeau LM, Schonely K, Ni Y, Binder GK, Levine BL, MacGregor RR, June CH, Dropulic B. Regulatory considerations for novel gene therapy products: a review of the process leading to the first clinical lentiviral vector. Hum Gene Ther. 2005 Jan;16(1):17-25. Review. Erratum in: Hum Gene Ther. 2006 Feb;17(2):252. Hum Gene Ther. 2005 Feb;16(2):279. — View Citation
Ni Y, Sun S, Oparaocha I, Humeau L, Davis B, Cohen R, Binder G, Chang YN, Slepushkin V, Dropulic B. Generation of a packaging cell line for prolonged large-scale production of high-titer HIV-1-based lentiviral vector. J Gene Med. 2005 Jun;7(6):818-34. Erratum in: J Gene Med. 2005 Jun;7(6):835. — View Citation
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Change in viral load | 1 Year | Yes | |
| Primary | Change in CD4 counts | 1 Year | Yes | |
| Primary | Safety | 15 Years | Yes | |
| Secondary | Immune function | 1 Year | Yes | |
| Secondary | AIDS related illness | 1 Year | Yes | |
| Secondary | Persistence of vector modified cells | 15 Years | Yes |
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