A Clinical Trial to Evaluate Safety, Tolerability, and Immunogenicity of Adjuvanted HIV-1 Fusion Peptide Conjugate Vaccine Alone or in Prime-Boost Regimens With Adjuvanted HIV-1 Envelope Trimer 4571 and HIV-1 Trimer 6931 Vaccines in Healthy Adults

Study Description

Brief Summary

This is an open-label, dose-escalation study to examine the safety, tolerability, and immunogenicity of adjuvanted Fusion Peptide Vaccine alone or in prime-boost regimens with adjuvanted Trimer 4571 and Trimer 6931 vaccines in healthy adults. The hypothesis is that the vaccines will be safe, and well tolerated when administered alone, and when co-administered with HIV-1 Trimer 4571, in prime-boost regimens, and will induce detectable immune response.

Detailed Description

This study has two parts. Part A will evaluate the safety, tolerability, and immunogenicity of single doses of the FP conjugate, Trimer 4571 and Trimer 6931 vaccines, in a dose-escalation design. Each product must be assessed as safe prior to use in Part B. Trimer 4571 with alum adjuvant has been previously evaluated in humans but will be tested in Part A with Adjuplex. Part B will evaluate the safety, tolerability, and immunogenicity of FP conjugate prime, Trimer 4571 prime, or an FP plus Trimer 4571 prime, all followed by subsequent doses of Trimer 4571, or Trimer 6931, or both alone and then both Trimers combined.

Total study duration is 36 months (includes enrollment, planned safety holds and follow-up).

Study Design

Outcome Measures

Primary Outcome Measures

1. Local reactogenicity signs and symptoms collected for all participants [Measured for a minimum of seven days following receipt of any study product]

   Graded according to the Division of AIDS Table for Grading the Severity of Adult and Pediatric Adverse Events, Corrected Version 2.1, July 2017, except as defined in the protocol

2. Systemic reactogenicity signs and symptoms collected for all participants [Measured for a minimum of seven days following receipt of any study product]

   Graded according to the Division of AIDS Table for Grading the Severity of Adult and Pediatric Adverse Events, Corrected Version 2.1, July 2017, except as defined in the protocol

3. Adverse events collected for all participants [Collected for thirty days after any receipt of study vaccination]

   Graded according to the Division of AIDS Table for Grading the Severity of Adult and Pediatric Adverse Events, Corrected Version 2.1, July 2017, except as defined in the protocol

4. Magnitude of serum antibody binding of FP and envelope trimer antigens as measured by the MSD assay 2 weeks after the last vaccination. [36 months]

   To evaluate the ability of FP-conjugate, Trimer 4571, and Trimer 6931 vaccines to elicit FP-specific binding antibodies.

5. Response rate of serum antibody binding of FP and envelope trimer antigens as measured by the MSD assay 2 weeks after the last vaccination. [36 months]

   To evaluate the ability of FP-conjugate, Trimer 4571, and Trimer 6931 vaccines to elicit FP-specific binding antibodies.

Secondary Outcome Measures

1. Magnitude of serum antibody neutralization, as measured by the TZM-bl assay. [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

2. Response rate of serum antibody neutralization, as measured by the TZM-bl assay. [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

3. Breadth of serum antibody neutralization, as measured by the TZM-bl assay. [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

4. Magnitude of serum IgG binding antibodies to FP, Trimer 4571, and Trimer 6931. [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

5. Response rate of serum IgG binding antibodies to FP, Trimer 4571, and Trimer 6931. [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

6. Mapping of FP specific serum neutralizing activity via characterization of specific epitopes (such as base of trimers, V3, internal epitopes). [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

7. Magnitude of CD4+ T-cell responses as assessed by intracellular cytokine staining assays (ICS). [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

8. Response rate of CD4+ T-cell responses as assessed by intracellular cytokine staining assays (ICS). [36 months]

   To evaluate the peak and durability of humoral and cellular immune response to vaccination regimens including FP-conjugate vaccine, Trimer 4571, and Trimer 6931, and to compare responses between the regimens.

Eligibility Criteria

Criteria

Inclusion Criteria:

1. Able and willing to complete the informed consent process, including an Assessment of Understanding (AoU): volunteer demonstrates understanding of this study, completes a questionnaire prior to first vaccination with verbal demonstration of understanding of all questionnaire items answered incorrectly.

2. 18-50 years old, inclusive, on day of enrollment.

3. Agrees to comply with planned study procedures and be available for clinic follow-up through the last clinic visit.

4. Agrees not to enroll in another study of an investigational agent during participation in the trial, including severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) investigational agents that may subsequently obtain emergency use authorization (EUA) or undergo licensure by the FDA. If a potential participant is already enrolled in a SARS-CoV-2 clinical trial, prior approvals from the SARS-COV-2 study sponsor and HVTN 303 PSRT are required prior to enrollment in HVTN 303.

5. In good general health without clinically significant medical history.

6. Physical examination and laboratory results without clinically significant findings that would interfere with assessment of safety or reactogenicity.

7. Body Mass Index (BMI) ≤ 40.

8. Assessed as low risk for HIV acquisition.

9. Suitable injection sites in the deltoid muscle of each arm, as assessed by a clinician.

10. White blood cells (WBCs) 2,500-12,000/mm3

11. WBC differential either within institutional normal range or approved by the Investigator of Record (IoR) as "not clinically significant."

12. Platelets = 125,000 - 500,000/mm3

13. Hemoglobin

• ≥ 11.0 g/dL for volunteers who were assigned female sex at birth

• ≥ 13.0 g/dL for volunteers who were assigned male sex at birth and transgender males who have been on hormone therapy for more than 6 consecutive months

• ≥ 12.0 g/dL for transgender females who have been on hormone therapy for more than 6 consecutive months

• For transgender participants who have been on hormone therapy for less than 6 consecutive months, determine hemoglobin eligibility based on the sex assigned at birth

1. Serum creatinine ≤ 1.1 x upper limit of normal (ULN) based on the institutional normal range.

2. Alanine aminotransferase (ALT) ≤1.25 x ULN based on the institutional normal range.

3. Negative for HIV infection by an (US) Food and Drug Administration (FDA)-approved enzyme immunoassay (EIA) or chemiluminescent microparticle immunoassay (CMIA).

4. Negative for anti-Hepatitis C antibodies (anti-HCV) or negative HCV nucleic acid test (NAT) if anti-HCV antibodies are detected.

5. Negative for Hepatitis B surface antigen.

6. Agrees to use effective means of birth control from at least 21 days prior to enrollment through 12 weeks after the last product administration.

7. Negative β-HCG (beta human chorionic gonadotropin) pregnancy test (urine or serum) at screening and prior to each study product administration on the day of study product administration.

Exclusion Criteria:

1. Active duty and reserve US military personnel.

2. Breast-feeding or planning to become pregnant from at least 21 days prior to enrollment through 12 weeks after the last product administration.

3. An investigational HIV vaccine (previous placebo recipients are not excluded).

4. Immunosuppressive medications received within 168 days before first vaccination (Not exclusionary: [1] corticosteroid nasal spray; [2] inhaled corticosteroids; [3] topical corticosteroids for mild, uncomplicated dermatologic condition; or [4] a single course of oral/parenteral prednisone or equivalent at doses ≤ 60 mg/day and length of therapy < 11 days with completion at least 30 days prior to enrollment).

5. Blood products within 60 days prior to enrollment

6. Monoclonal antibodies (mAbs), whether licensed or investigational. Exceptions may be made by the HVTN 303 PSRT on a case-by-case basis

7. Receipt of any of the following:

• Within 4 weeks prior to enrollment:

• Any licensed live, attenuated vaccine

• Any adenoviral-vectored SARS-CoV-2 vaccine with FDA Emergency Use Authorization (EUA), FDA licensure or World Health Organization (WHO) Emergency Use Listing (EUL)

• Within 2 weeks prior to enrollment:

• Any licensed killed/subunit/inactivated vaccine

• Any mRNA based or protein SARS-CoV-2 vaccines with FDA EUA, FDA licensure, or WHO EUL

1. Investigational research agents with a half-life of 7 or fewer days within 4 weeks prior to enrollment. If a potential participant has received investigational agents with a half-life greater than 7 days (or unknown half-life) within the past year, PSRT approval is required for enrollment.

2. Current allergen immunotherapy with antigen injections, unless on maintenance schedule.

3. Current anti-TB prophylaxis or therapy.

4. Serious adverse reactions to vaccines or vaccine components.

5. Hereditary angioedema, acquired angioedema, or idiopathic forms of angioedema.

6. Hypertension that is not well controlled.

7. Asthma is excluded if the participant has ANY of the following:

• Required either oral or parenteral corticosteroids for an exacerbation two or more times within the past year; OR

• Needed emergency care, urgent care, hospitalization, or intubation for an acute asthma exacerbation within the past year (eg, would NOT exclude individuals with asthma who meet all other criteria but sought urgent/emergent care solely for asthma medication refills or co-existing conditions unrelated to asthma); OR

• Uses a short-acting rescue inhaler more than 2 days/week for acute asthma symptoms (ie, not for preventive treatment prior to athletic activity); OR

• Uses medium-to-high-dose inhaled corticosteroids (greater than 250 mcg fluticasone or therapeutic equivalent per day), whether in single-therapy or dual-therapy inhalers (ie, with a long-acting beta agonist [LABA]); OR

• Uses more than one medication for maintenance therapy daily. Inclusion of anyone on a stable dose of more than one medication for maintenance therapy daily for greater than two years requires PSRT approval.

1. Autoimmune disease, current or history, including psoriasis.

2. Clinically significant immunodeficiency.

3. AESIs: Volunteers who currently have, or have a history of, any condition that could be considered an AESI for the product(s) administered in this protocol.

4. History of generalized urticaria, angioedema, or anaphylaxis. (Not exclusionary: angioedema or anaphylaxis to a known trigger with at least 5 years since last reaction to demonstrate satisfactory avoidance of trigger.).

5. Diabetes mellitus type 1 or type 2.

6. Bleeding disorder diagnosed by a doctor (eg, factor deficiency, coagulopathy, or platelet disorder requiring special precautions) or significant bruising or bleeding difficulties with IM injections or blood draws.

7. Seizure disorder other than: 1) febrile seizures, 2) seizures secondary to alcohol withdrawal more than 3 years ago, or 3) seizures that have not required treatment within the last 3 years.

8. Asplenia or functional asplenia.

9. Malignancy (Not excluded from participation: Volunteer who has had malignancy excised surgically and who, in the investigator's estimation, has a reasonable assurance of sustained cure, or who is unlikely to experience recurrence of malignancy during the period of the study).

10. Any other chronic or clinically significant condition that in the clinical judgement of the investigator would jeopardize the safety or rights of the study participant, including, but not limited to: clinically significant forms of drug or alcohol abuse, serious psychiatric disorders, or cancer that, in the clinical judgement of the site investigator, has a potential for recurrence (excluding basal cell carcinoma).

Contacts and Locations

Locations

Sponsors and Collaborators

• National Institute of Allergy and Infectious Diseases (NIAID)
• National Institutes of Health (NIH)
• Department of Health and Human Services

Investigators

• Study Chair: Troy Martin, HVTN LOC, Fred Hutch
• Study Chair: Michael Keefer, M.D., Univ. of Rochester Med. Ctr., HVTU

Study Documents (Full-Text)

More Information

Publications