A Randomized Phase I Safety and Immunogenicity Trial of Live Recombinant Canarypox ALVAC-HIV vCP205 Delivered by Alternate Mucosal Routes in HIV-1 Uninfected Adult Volunteers
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To compare the safety of ALVAC-HIV vCP205 to that of ALVAC-RG vCP65 rabies glycoprotein, delivered by a variety of mucosal routes. To evaluate the antibody, humoral, and cellular immune responses resulting from ALVAC-HIV vCP205. [AS PER AMENDMENT 8/3/98: To obtain safety data on AIDSVAX B/B boosting administered by the intramuscular and intranasal routes in the context of previous immunization via alternate mucosal routes or intramuscularly with a canarypox vector expressing HIV-1 antigens (vCP205). To obtain immunogenicity data on AIDSVAX B/B boosting.] One of the earliest observations in the HIV epidemic was the demonstration of HIV infection at mucosal surfaces of cells in the genital tract. These data suggest that priming of immune defenses of viral infected cells may be an important component in the strategy of developing an effective HIV vaccine. Direct immunization of relevant mucosal surfaces with a vectored vaccine may stimulate mucosal immunity. The ALVAC-HIV vCP205 immunogen is constructed from a live recombinant canarypox vector that has a good safety profile in volunteers and should allow mucosal induction of immunity.
Condition | Intervention | Phase |
---|---|---|
HIV Infections |
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1 Biological: ALVAC-HIV MN120TMG (vCP205) Biological: ALVAC-RG Rabies Glycoprotein (vCP65) |
Phase 1 |
Study Type: | Interventional |
Study Design: | Allocation: Randomized Endpoint Classification: Safety Study Intervention Model: Parallel Assignment Masking: Double Blind (Subject, Investigator) Primary Purpose: Prevention |
Official Title: | A Randomized Phase I Safety and Immunogenicity Trial of Live Recombinant Canarypox ALVAC-HIV vCP205 Delivered by Alternate Mucosal Routes in HIV-1 Uninfected Adult Volunteers |
- To compare the safety of ALVAC-HIV vCP205 to that of ALVAC-RG vCP65 rabies glycoprotein, delivered by a variety of mucosal routes [ Time Frame: Throughout study ] [ Designated as safety issue: Yes ]
- To evaluate the antibody, humoral, and cellular immune responses resulting from ALVAC-HIV vCP205 [ Time Frame: Throughout study ] [ Designated as safety issue: No ]
- To obtain safety data on AIDSVAX B/B boosting administered by the intramuscular and intranasal routes in the context of previous immunization via alternate mucosal routes or intramuscularly with a canarypox vector expressing HIV-1 antigens (vCP205) [ Time Frame: Throughout study ] [ Designated as safety issue: Yes ]
- To obtain immunogenicity data on AIDSVAX B/B boosting [ Time Frame: Throughout study ] [ Designated as safety issue: No ]
Enrollment: | 84 |
Study Completion Date: | October 2000 |
Arms | Assigned Interventions |
---|---|
Experimental: 1
Participants will undergo treatment intramuscularly
|
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 2
Participants will undergo treatment orally
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 3
Participants will undergo treatment intranasally
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 4
Participants will undergo treatment intrarectally
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 5
Participants will undergo treatment intravaginally
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 6
Participants will undergo treatment intranasally and intramuscularly
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Experimental: 7
Participants will undergo treatment intrarectally and intramuscularly
|
Biological: MN rgp120/HIV-1 and GNE8 rgp120/HIV-1
Dosage will vary based on route of administration
Biological: ALVAC-HIV MN120TMG (vCP205)
Dosage will vary based on route of administration
Biological: ALVAC-RG Rabies Glycoprotein (vCP65)
Dosage will vary based on route of administration
|
Detailed Description:
One of the earliest observations in the HIV epidemic was the demonstration of HIV infection at mucosal surfaces of cells in the genital tract. These data suggest that priming of immune defenses of viral infected cells may be an important component in the strategy of developing an effective HIV vaccine. Direct immunization of relevant mucosal surfaces with a vectored vaccine may stimulate mucosal immunity. The ALVAC-HIV vCP205 immunogen is constructed from a live recombinant canarypox vector that has a good safety profile in volunteers and should allow mucosal induction of immunity.
This randomized, double-blind trial evaluates the safety of and immune response to vaccination with ALVAC-HIV vCP205 given at 0, 1, 3, and 6 months. Patients are randomly assigned to 1 of 7 drug administration routes as follows:
Group A: Intramuscular Group B: Oral Group C: Intranasal Group D: Intrarectal Group E: Intravaginal Group F: Intranasal/intramuscular Group G: Intrarectal/intramuscular Twelve patients are randomized to each group, 8 of whom receive experimental therapy with ALVAC-HIV vCP205 and 4 of whom receive control therapy with ALVAC-RG vCP2058 (rabies vaccine). Women are preferentially enrolled, with a goal of 60% women (minimum of 4 women per treatment arm); only women are randomized to Group E. Blinding is maintained with respect to drug assignment rather than route of administration, after randomization. NOTE: The protocol will be amended to add 2 boost vaccinations with subunit products at approximately Months 9 and 12 when a suitable boost product is identified. [AS PER AMENDMENT 8/3/98: The protocol has been modified to include 2 booster vaccinations to be administered at 9 and 12 months. Patients in Group A receive booster vaccination with ALVAC-HIV VCP205 or ALVAC-RG intranasally. Patients in Groups B through G are boosted with AIDSVAX B/B vaccine (a bivalent vaccine consisting of MN rgp120/HIV-1 antigen and GNE8 rgp120/HIV-1 antigen in alum adjuvant) or with Imovax diploid cell rabies vaccine; vaccinations for these patients are given intramuscularly.] [AS PER AMENDMENT 11/19/98: The second booster vaccination for group A will be administered at study Month 15.]
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Ages Eligible for Study: | 18 Years to 50 Years |
Genders Eligible for Study: | Both |
Accepts Healthy Volunteers: | Yes |
Inclusion Criteria
Volunteers must have:
- Negative ELISA for HIV within 8 weeks of immunization.
- No envelope bands in Western blot for HIV-1 within 8 weeks of immunization.
- Normal history and physical examination.
Exclusion Criteria
Co-existing Condition:
Volunteers with the following conditions are excluded:
- Medical or psychiatric condition or occupational responsibilities that preclude compliance with the protocol, including recent suicidal attempt or ideation or present psychosis.
- Active syphilis (if the serology is documented to be a false positive or due to a remote [more than 6 months] treated infection, the volunteer is eligible).
- Active tuberculosis (volunteers with a positive PPD and a normal chest x-ray showing no evidence of TB and not requiring INH therapy are eligible).
- Allergy to egg products or neomycin (used to prepare ALVAC vaccines).
- Occupational or household exposure to birds (no known pathogenicity of avipox for birds).
- Episode of severe diarrhea within 1 week prior to immunization.
- Abnormal pelvic exam with evidence of sexually transmitted disease or other genital tract infection or trauma, including vaginitis, cervicitis, ecchymosis, vulvar or cervicovaginal lesions or abrasions, or chronic cervical and/or abnormal PAP smear changes.
- Recent history of rectal bleeding or repeatedly positive hemocult test (within 1 month).
- Positive for Hepatitis B surface antigen.
Volunteers with the following prior conditions are excluded:
- History of immunodeficiency, chronic illness (in particular, chronic inflammatory disease or gastroenteritis), malignancy, or autoimmune disease.
- History of cancer unless there has been surgical excision followed by a sufficient observation period to give a reasonable assurance of cure.
- History of anaphylaxis or history of other serious adverse reactions to vaccines.
- History of serious allergic reaction to any substance, requiring hospitalization or emergent medical care (e.g., Stevens-Johnson syndrome, bronchospasm, or hypotension).
Prior Medication:
Excluded:
- Live attenuated vaccines within 60 days of study. NOTE: Medically indicated subunit or killed vaccines (e.g., influenza, pneumococcal) are not exclusionary, but should be given at least 2 weeks away from HIV immunizations.
- Experimental agents within 30 days prior to study.
- HIV-1 vaccines or placebo received in a previous HIV vaccine trial.
- Previous immunization against rabies.
Prior Treatment:
Excluded:
- Prior hysterectomy.
- Blood products or immunoglobulin in the past 6 months.
Risk Behavior:
Excluded:
Volunteers with identifiable higher-risk behavior, or whose partners have an identifiable higher-risk behavior for HIV infection as determined by screening questions designed to identify risk factors for HIV infection (i.e., AVEG Risk Groups C or D); specific exclusions include:
- history of injection drug use within the last 12 months prior to enrollment or higher-risk sexual behavior as defined by the AVEG.
![](https://webarchive.library.unt.edu/web/20130315212028im_/http://clinicaltrials.gov/ct2/html/images/frame/triangle.gif)
United States, Alabama | |
UAB AVEG | |
Birmingham, Alabama, United States, 35294 | |
United States, Maryland | |
JHU AVEG | |
Baltimore, Maryland, United States | |
United States, Missouri | |
St. Louis Univ. School of Medicine AVEG | |
St Louis, Missouri, United States, 63104 | |
United States, New York | |
Univ. of Rochester AVEG | |
Rochester, New York, United States, 14642 | |
United States, Tennessee | |
Vanderbilt Univ. Hosp. AVEG | |
Nashville, Tennessee, United States, 37232 | |
United States, Washington | |
UW - Seattle AVEG | |
Seattle, Washington, United States, 98144 |
Study Chair: | P Wright |
![](https://webarchive.library.unt.edu/web/20130315212028im_/http://clinicaltrials.gov/ct2/html/images/frame/triangle.gif)
No publications provided
Responsible Party: | National Institute of Allergy and Infectious Diseases (NIAID) |
ClinicalTrials.gov Identifier: | NCT00000884 History of Changes |
Other Study ID Numbers: | AVEG 027, 10577 |
Study First Received: | November 2, 1999 |
Last Updated: | May 16, 2012 |
Health Authority: | United States: Federal Government |
Keywords provided by National Institute of Allergy and Infectious Diseases (NIAID):
Vaccines, Synthetic Injections, Intramuscular HIV-1 Immunity, Cellular AIDS Vaccines HIV Seronegativity Mucous Membrane |
Antibodies, Viral Avipoxvirus Genetic Vectors HIV Envelope Protein gp120 Immunity, Mucosal Rabies Vaccines HIV Preventive Vaccine |
Additional relevant MeSH terms:
HIV Infections Acquired Immunodeficiency Syndrome Lentivirus Infections Retroviridae Infections RNA Virus Infections Virus Diseases Sexually Transmitted Diseases, Viral Sexually Transmitted Diseases Immunologic Deficiency Syndromes Immune System Diseases Slow Virus Diseases Krestin |
Antibiotics, Antineoplastic Antineoplastic Agents Therapeutic Uses Pharmacologic Actions Antiviral Agents Anti-Infective Agents Adjuvants, Immunologic Immunologic Factors Physiological Effects of Drugs Interferon Inducers Radiation-Protective Agents Protective Agents |
ClinicalTrials.gov processed this record on March 14, 2013