HIV Clinical Trial
— CUT*HIVAC001Official title:
A Phase I Clinical Trial to Assess the Safety and Immunogenicity of Three HIV GTU® MultiHIV DNA Immunisations Administered Via the Intramuscular, Intradermal and Transcutaneous Routes in Healthy Male and Female Volunteers
Our research is part of the global effort to develop a vaccine against HIV. We aim to
develop a non-invasive, needle-free 'transcutaneous' vaccine. It will be a water-based
solution which is placed on the surface of the skin of the upper arm, after the hairs have
been stripped away. The active component of the vaccine - DNA which contains genes derived
from the virus - will enter through the hair follicles from which the hair has been
stripped. The DNA will get into cells, which will use the HIV genes to make copies of virus
proteins. These proteins will stimulate the body's immune system and, we hope, make it able
to protect against HIV infection. The research is to assess the safety of this approach, and
how good it is at stimulating the immune system. We will combine the 'transcutaneous'
vaccine with an 'intramuscular' version which is injected into the muscle of the thigh, and
compare this combination with: intramuscular plus 'intradermal' (injection into the skin);
and intramuscular with added 'electroporation' - use of a pulse of electricity to increase
uptake of DNA vaccines.
We will invite healthy men and women to take part in this research. Volunteers will first be
assessed to ensure they are eligible to participate. A total of 30 will be enrolled and each
will receive three vaccinations over the course of 12 weeks. We will assess the effects of
the vaccinations by recording any symptoms experienced by the volunteers, and by analysing
samples of their blood. The research will take place at the St Mary's Hospital campus of
Imperial College London, UK. The DNA component of the vaccine is an experimental substance,
so we will monitor very closely the wellbeing of the men and women who participate in the
research.
| Status | Recruiting |
| Enrollment | 30 |
| Est. completion date | December 2015 |
| Est. primary completion date | June 2015 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | Both |
| Age group | 18 Years to 45 Years |
| Eligibility |
Inclusion Criteria: 1. Men and women aged between 18 and 45 years on the day of screening 2. BMI between 19-28 3. Available for follow-up for the duration of the study (~6 months from screening) 4. Willing and able to give written informed consent 5. At low risk of HIV and willing to remain so for the duration of the study defined as: - no history of injecting drug use in the previous ten years - no gonorrhoea or syphilis in the last six months - no high risk partner (e.g. injecting drug use, HIV positive partner) either currently or within the past six months - no unprotected anal intercourse in the last six months, outside a relationship with a regular partner known to be HIV negative - no unprotected vaginal intercourse in the last six months outside a relationship with a regular known/presumed HIV negative partner 6. Willing to undergo a HIV test 7. Willing to undergo a genital infection screen 8. If heterosexually active female, using an effective method of contraception with partner (combined oral contraceptive pill; injectable or implanted contraceptive; consistent record with condoms if using these; physiological or anatomical sterility in self or partner) from 14 days prior to the first vaccination until 4 months after the last, and willing to undergo urine pregnancy tests prior to each vaccination 9. If heterosexually active male, using an effective method of contraception with their partner from the first day of vaccination until 4 months after the last vaccination 10. Agree to abstain from donating blood for three months after the end of their participation in the trial, or longer if necessary 11. Registered with a GP for at least the past three months 12. Satisfactory response received from GP before randomisation Exclusion Criteria: 1. Pregnant or lactating 2. Use of any topical treatment on the injection or application site within the last four weeks 3. No UV tanning sessions or strong sun exposure within four weeks prior to the study and a willingness to avoid these during the study period. 4. Excessive terminal hair growth on the investigational skin areas (to be assessed by reference to a photograph which will be available during screening visit. 5. Individuals in which a skin-fold measurement (cutaneous and subcutaneous tissue) of the upper right or left thigh exceeds 40 mm. 6. Clinically relevant abnormality on history or examination including - history of grand-mal epilepsy, seizure disorder or any history of prior seizure - history of syncope or fainting episodes within 1 year of study entry. - severe eczema - liver disease with inadequate hepatic function - any skin condition which may interfere with the trial assessment on the injection site - haematological, metabolic, gastrointestinal or cardio-pulmonary disorders including an abnormal ECG. - uncontrolled infection; toxic shock syndrome - autoimmune disease, immunodeficiency or use of immunosuppressives in preceding 3 months 7. Known hypersensitivity to any component of the vaccine formulations used in this trial, or a seafood allergy or have severe or multiple allergies to drugs or pharmaceutical agents 8. History of severe local or general reaction to vaccination defined as 1. local: extensive, indurated redness and swelling involving most of the antero-lateral thigh or the major circumference of the arm, not resolving within 72 hours 2. general: fever >= 39.5oC within 48 hours; anaphylaxis; bronchospasm; laryngeal oedema; collapse; convulsions or encephalopathy within 72 hours 9. Receipt of live attenuated vaccine within 60 days or other vaccine within 14 days of enrolment 10. Receipt of an experimental vaccine containing HIV antigens at any time in the past 11. Receipt of blood products or immunoglobin within 4 months of screening 12. Participation in another trial of a medicinal product, completed less than 30 days prior to enrolment 13. HIV 1 or 2 positive or indeterminate on screening 14. Positive for hepatitis B surface antigen, hepatitis C antibody or serology indicating active syphilis requiring treatment 15. Grade 1 or above routine laboratory parameters (see study specific tables - Appendix 3 for definitions). Hyperbilirubinaemia to be considered an exclusion criterion only when confirmed to be conjugated bilirubinaemia 16. Current use of any electronic stimulation device, such as cardiac demand pacemakers, automatic implantable cardiac defibrillator, nerve stimulators, or deep brain stimulators. 17. Presence of any surgical or traumatic metal implants at the sites of administration 18. Presence of an intrauterine device. 19. Unable to read and speak English to a fluency level adequate for the full comprehension of procedures required in participation and consent. 20. Unlikely to comply with protocol. |
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
| Country | Name | City | State |
|---|---|---|---|
| United Kingdom | Imperial College London | Greater London |
| Lead Sponsor | Collaborator |
|---|---|
| Imperial College London | CUT'HIVAC Cutaneous HIV Vaccination |
United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Exploratory immunogenicity endpoint | The ratio of CD8+ to CD4+ T-cell responses to HIV peptides as measured by ICS on triplicate PBMC samples | Four weeks after final immunisation | No |
| Primary | Immunogenicity Immunogenicity | The primary immunogenicity endpoint is the presence of a T cell response measured by IFN-? ELISPOT assay using frozen PBMCs collected 2 weeks after the final vaccination. | 2 weeks after the final vaccination | No |
| Primary | Safety | Primary safety endpoint is the presence of a grade 3 or above local or systemic solicited adverse event or any adverse event that results in a clinical decision to discontinue further immunisations. | Four weeks after final immunisation | No |
| Secondary | Immunogenicity | The secondary immunogenicity endpoint is the presence of a detectable antigen specific IgG or IgA antibody response (relative to a predefined cutoff based on assay internal controls) and in those which are positive, the titre (ug/ml) according to a quantitative EIA assay. | Four weeks after final immunisation | No |
| Secondary | Safety | Grade 3 or above systemic clinical and laboratory solicited adverse event (Table 2) Any grade of adverse event that results in a clinical decision to discontinue further immunisations Any grade of adverse event that occurs in a participant that has received at least one immunisation | Four weeks after final immunisation | No |
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