HIV-1 Infection Clinical Trial
Official title:
Immunotherapy of HIV-infected Patients An Open, Dose-escalating Assessment of Vacc-C5 With Either GM-CSF or Alhydrogel as Adjuvant in HIV-1-infected Subjects on Antiretroviral Therapy (ART)
Background:
Despite the introduction of highly effective antiretroviral therapy (ART) regimes, which
control the HIV infection and results in increases in CD4 cell counts and an undetectable
viral load, many patients suffer from increased morbidity. There is evidence that presence
of antibodies against the C5 region of gp120 strongly correlates with slower disease
progression, and that loss of antibody responses to this region are associated with
progression.
Investigational product:
Vacc-C5 is a single heterodimeric peptide-based HIV therapeutic vaccine corresponding to the
C5 region on gp120 and the external domain of gp41. The vaccine is intended to create a
non-neutralizing antibody against C5 region.
Study objectives:
1. To evaluate safety of the vaccination regimens
2. To evaluate C5-specific humoral immune responses (antibodies), T cell responses, T cell
activation markers and other immune markers.
Background:
Despite the introduction of highly effective antiretroviral therapy (ART) regimes, which
control the HIV infection and results in increases in CD4 cell counts and an undetectable
viral load, many patients suffer from increased morbidity. There is evidence that presence
of antibodies against the C5 region of gp120 strongly correlates with slower disease
progression, and that loss of antibody responses to this region are associated with
progression.
Investigational product:
Vacc-C5 is a single heterodimeric peptide-based HIV therapeutic vaccine corresponding to the
C5 region on gp120 and the external domain of gp41. The rationale behind the Vacc-C5 is the
finding that long-term non-progressors (LTNP) subjects have more antibodies towards the C5
part of gp120 than HIV infected subjects with a more rapid disease progression.
The primary objective of Vacc-C5 immunotherapy is to induce a humoral immune response. The
vaccine is intended to create a non-neutralizing antibody against the C5 region and to
thereby mimic a natural process in HIV-infected long-term non-progressors (LTNP) subjects.
Use of adjuvant:
Peptide vaccines are poorly immunogenic by themselves. To induce measurable levels of T
helper cell type 1 (Th1) or type 2 (Th2) immune responses against these peptides, an
adjuvant is often required.
Two different adjuvants are to be used in this study:
1. GM-CSF which facilitates dendritic cell maturation and migration to the lymph nodes for
antigen presentation. The regimen when using this adjuvant is intradermal
administration.
2. Aluminum-containing adjuvants is well known. They have been administered to human
beings and animals in millions of doses of vaccines. This type of vaccine is usually
administered intramuscularly or subcutaneously. In this study intramuscular
administration will be used.
Primary objective:
It is to evaluate the safety of Vacc-C5 at three different dose levels given intradermally
with GM-CSF as adjuvant or given intramuscularly with Alhydrogel as adjuvant.
Secondary objectives:
1. To evaluate C5-specific humoral immune responses (antibodies).
2. To evaluate the C5-specific T cell responses by ELISPOT and T cell proliferation.
3. To evaluate T cell activation markers (e.g. CD38, HLA-DR) and other immune markers.
Study design:
The study is an open, dose-escalating, single centre study in HIV-positive subjects on
treatment (ART). Two different vaccine regimens will be tested:
1. Arm A: Vacc-C5 with GM-CSF as adjuvant administered intradermally.
2. Arm B: Vacc-C5 with Alhydrogel as adjuvant administered intramuscularly.
Three dose levels of Vacc-C5 (100, 300 and 900 microgram will be tested for each of the two
vaccination regimen. A dose escalation design (3+3) will be used, and if no dose limiting
toxicity (DLT) is detected 18 subjects will be included in each arm.
Subjects who have been HIV-positive and stable on ART for the last 6 months with CD4 cell
counts ≥400x 10 6 /L and who meet the other inclusion and exclusion criteria will be
eligible for the study. The duration of the study is 26 weeks plus a screening period of up
to 12 weeks.
During the Treatment Period, all subjects will remain on their ART and receive three
immunizations; at Weeks 1, 2 and 4, with Vacc C5 including either GM-CSF or Alhydrogel as
adjuvant.
The study is sequential, meaning that the first three subjects in each arm receive the
lowest dose (three subjects) 100 µg Vacc-C5. If no dose limiting toxicity has been detected
after week 4 vaccination, three more subjects will be added and the next dose level will be
started.
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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