HIV-CORE 004: Safety & Immunogenicity of HIV Vaccines in Healthy Kenyan Adults

Sponsor

University of Oxford (Other)

Overall Status

Completed

CT.gov ID

NCT02099994

Collaborator

European and Developing Countries Clinical Trials Partnership (EDCTP) (Other), International AIDS Vaccine Initiative (Other), Karolinska Institutet (Other), University of Nairobi (Other), Ichor Medical Systems Incorporated (Industry)

Enrollment

Location

Arms

Duration (Months)

4.2

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The study is part of a long-term aim to develop an effective HIV-1 vaccine and will evaluate safety and immunogenicity of vaccines focusing T cell responses on the conserved region of the HIV-1 proteome. The vaccines used are pSG2.HIVconsv DNA (D), MVA.HIVconsv (M) and Ad35-GRIN (A), delivered in regimens AM, DDDAM and DeDeDeAM, where e indicates electroporation.

Condition or Disease	Intervention/Treatment	Phase
AIDS	Biological: Ad35-GRIN Biological: MVA.HIVconsv Biological: pSG2.HIVconsv DNA Biological: Electroporated pSG2.HIVconsv	Phase 1/Phase 2

Detailed Description

The main objectives of this study are to determine the vaccines' safety and immunogenicity in an African population, and further strengthen the vaccine trial capacity in the South.

HIV-CORE 004 is a double blind, placebo controlled randomized Phase I/IIa study designed to evaluate the safety and immunogenicity of different delivery regimens using three novel HIV-1 vaccines pSG2.HIVconsv DNA (D) with and without electroporation (e), adenovirus Ad35-GRIN (A) and poxvirus MVA.HIVconsv (M) administered by intramuscular needle injection in heterologous prime-boost regimens.

72 healthy, low-risk, HIV-1-uninfected adult volunteers in Nairobi will be randomly assigned to one of three groups, AM, DDDAM and DeDeDeAM each containing 20 vaccinees and 4 placebo recipients.

Firstly, this study aims to evaluate the safety and tolerability of the vaccines pSG2.HIVconsv DNA (D) with and without electroporation (e), adenovirus Ad35-GRIN (A) and poxvirus MVA.HIVconsv (M).

Secondly, we shall determine the effect of electroporation during DNA priming on the frequency, durability and/or quality of T cell responses (DDDAM vs DeDeDeAM).

Thirdly, we shall determine whether priming with three DNA vaccinations with or without electroporation affects the frequency, durability and/or quality of T cell responses to the HIVconsv immunogen compared to that seen in the AM regimen (AM vs DDDAM/DeDeDeAM).

As this is the first study of the combined HIVconsv vaccines in an African population, of the pSG2.HIVconsv DNA with electroporation, and the combination of the two HIVconsv vaccines with Ad35-GRIN, this trial has been designed as a pilot study to compare different vector combinations. The sample sizes will only allow detection of large response differences between volunteers in the three groups, thus, yielding data that are primarily descriptive.

Study Design

Study Type:

Interventional

Actual Enrollment :

72 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

Double (Participant, Investigator)

Primary Purpose:

Prevention

Official Title:

A Phase I/IIa Clinical Trial of HIV-1 Vaccines pSG2.HIVconsv DNA, MVA.HIVconsv and Ad35-GRIN in Combined Regimens in Healthy HIV-1/2-negative Adults in Nairobi.

Study Start Date :

Mar 1, 2014

Actual Primary Completion Date :

Aug 1, 2015

Actual Study Completion Date :

Aug 1, 2015

Arms and Interventions

Arm	Intervention/Treatment
Experimental: A - AM Ad35-GRIN 5 x 10^10 vp IM at week 0, MVA.HIVconsv 2 x 10^8 pfu IM at week 8.	Biological: Ad35-GRIN intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo Biological: MVA.HIVconsv IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo
Experimental: B - DDDAM pSG2.HIVconsv DNA 4 mg or saline placebo at weeks 0, 4 and 8. Ad35-GRIN 5 x 10^10 vp or saline placebo at week 12. MVA.HIVconsv 2 x 10^8 pfu or saline placebo at week 20.	Biological: Ad35-GRIN intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo Biological: MVA.HIVconsv IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo Biological: pSG2.HIVconsv DNA IM administration of pSG2.HIVconsv DNA 4 mg or saline placebo
Experimental: C - DeDeDeAM Electroporated pSG2.HIVconsv 4 mg or electroporated saline placebo at weeks 0, 4 and 8. Ad35-GRIN 5 x 10^10 vp or saline placebo at week 12. MVA.HIVconsv 2 x 10^8 pfu or saline placebo at week 20.	Biological: Ad35-GRIN intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo Biological: MVA.HIVconsv IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo Biological: Electroporated pSG2.HIVconsv IM administration of electroporated pSG2.HIVconsv 4mg or saline placebo

Arm

Intervention/Treatment

Experimental: A - AM

Ad35-GRIN 5 x 10^10 vp IM at week 0, MVA.HIVconsv 2 x 10^8 pfu IM at week 8.

Biological: Ad35-GRIN

intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo

Biological: MVA.HIVconsv

IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo

Experimental: B - DDDAM

pSG2.HIVconsv DNA 4 mg or saline placebo at weeks 0, 4 and 8. Ad35-GRIN 5 x 10^10 vp or saline placebo at week 12. MVA.HIVconsv 2 x 10^8 pfu or saline placebo at week 20.

Biological: Ad35-GRIN

intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo

Biological: MVA.HIVconsv

IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo

Biological: pSG2.HIVconsv DNA

IM administration of pSG2.HIVconsv DNA 4 mg or saline placebo

Experimental: C - DeDeDeAM

Electroporated pSG2.HIVconsv 4 mg or electroporated saline placebo at weeks 0, 4 and 8. Ad35-GRIN 5 x 10^10 vp or saline placebo at week 12. MVA.HIVconsv 2 x 10^8 pfu or saline placebo at week 20.

Biological: Ad35-GRIN

intramuscular administration of Ad35-GRIN 5 x 10^10 vp or saline placebo

Biological: MVA.HIVconsv

IM administration of MVA.HIVconsv 2 x 10^8 pfu or saline placebo

Biological: Electroporated pSG2.HIVconsv

IM administration of electroporated pSG2.HIVconsv 4mg or saline placebo

Outcome Measures

Primary Outcome Measures

Vaccine Safety [44 weeks]
Proportion of volunteers who develop a grade 3 or 4 local reaction. Proportion of volunteers who develop a grade 3 or 4 systemic reaction

Secondary Outcome Measures

Vaccine immunogenicity [44 weeks]
T cell responses will be determined initially by interferon-gamma enzyme-linked immunospot assay
Vaccine Safety [44 weeks]
A descriptive summary of grade 3 of 4 local and systemic events including laboratory abnormalities. A descriptive summary of serious adverse events, including laboratory abnormalities

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 50 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Yes

Inclusion Criteria:

Healthy adults aged 18-50
Willing to comply with the requirements of the protocol and available for follow-up for the planned duration of the study.
Written informed consent.
Willing to undergo HIV-1 testing, counselling and receive test results.
All female volunteers must be willing to undergo urine pregnancy tests
If sexually active using an effective method of contraception until at least 4 months after the last vaccination.
Willing to forgo donating blood during the study.

Exclusion Criteria:

Any relevant abnormality on history or examination including history of immunodeficiency or autoimmune disease, or use of systemic corticosteroids, immunosuppressive, antiviral, anticancer or other medication that, in the opinion of the Principal Investigator or designee, is clinically significant, within the previous 6 months. (Note: use of inhaled steroids for asthma or use of topical steroids for localized skin conditions will not exclude a volunteer from participation.)
Any clinically significant acute or chronic medical condition that is considered progressive or, in the opinion of the Principal Investigator or designee, would make the volunteer unsuitable for the study.
Any of the following abnormal laboratory parameters (1 abnormal test may be repeated once if thought to be due to a temporary condition):
Haematology
Haemoglobin < 9.0 g/dl for women and <11.0 g/dl for men
Absolute Neutrophil Count (ANC) ≤ 1000 /mm3 (≤ 1 x 109 /l)
Absolute Lymphocyte Count (ALC) ≤ 600 /mm3 (≤0.6 x 109 /l)
Platelets ≤100,000 /mm3, ≥ 550,000 /mm3 (≤ 100 /l, ≥ 550 /l)
Biochemistry
Creatinine > 1.3 x upper limit of normal (ULN)
Aspartate aminotransferase (AST) > 2.5 x ULN
Alanine aminotransferase (ALT) > 2.5 x ULN
Urinalysis- Clinically significant abnormal dipstick confirmed by microscopy:
Protein = 2+ or more
Blood = 2+ or more (for women: before or after menses)
Confirmed HIV-1 or HIV-2 infection.
If female, pregnant or planning a pregnancy any time from enrolment to 4 months after the last vaccination; or lactating.
Receipt of live attenuated vaccine within the previous 60 days or planned receipt at any time until 60 days after vaccination with Investigational Medicinal Product (IMP) or receipt of other vaccine, including influenza vaccine, within the previous 14 days or planned receipt at any time until 14 days after vaccination with the IMP.
Receipt of blood transfusion or blood products within the previous 6 months.
Participation in another clinical trial of an IMP currently or within the previous 3 months or expected participation during this study.
Receipt of any investigational HIV-1 vaccine within the last 6 years.
History of severe or very severe local or systemic reactogenicity events after vaccination, or history of severe or very severe allergic reactions.
Confirmed diagnosis of acute or chronic hepatitis B virus infection (spontaneous clearance leading to natural immunity, indicated by antibodies to core + antigens, is not an exclusion criterion); confirmed diagnosis of hepatitis C virus infection; untreated syphilis.
Smallpox vaccination within the previous 3 years.
Major psychiatric illness in the previous 3 years.
History of allergy or hypersensitivity to latex, chronic skin problems such as eczema or psoriasis, or skin and subcutaneous tissue thickness > 40 mm as assessed by skin pinch test in either deltoid region.
Presence of an implantable device
Current use of any electronic stimulation device. Therapeutic or traumatic metal implant in either deltoid region.
History of, or known active cardiac disease or a heart condition under the care of a doctor. Note: Slight physiological variation of normal resting heart rate (60 - 100 beats/minute) with respiration is NOT excluded.
History of syncope or fainting episode within 1 year of study entry.
Seizure disorder or any history of prior seizure.

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	KAVI-Kangemi clinic	Nairobi		Kenya

Sponsors and Collaborators

University of Oxford
European and Developing Countries Clinical Trials Partnership (EDCTP)
International AIDS Vaccine Initiative
Karolinska Institutet
University of Nairobi
Ichor Medical Systems Incorporated

Investigators

Principal Investigator: Walter Jaoko, University of Nairobi

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

University of Oxford

ClinicalTrials.gov Identifier:

NCT02099994

Other Study ID Numbers:

HIV-CORE 004/IAVI N004

First Posted:

Mar 31, 2014

Last Update Posted:

May 30, 2016

Last Verified:

May 1, 2016

Keywords provided by University of Oxford

HIV

vaccine

Study Results

No Results Posted as of May 30, 2016