Safety and Efficacy of ADAPTAVIR's Ability to Eliminate Treatment-Resistant Infectious Virus in Peripheral Blood Mononuclear Cells (PBMCs)
| Status: | Completed |
|---|---|
| Conditions: | HIV / AIDS |
| Therapuetic Areas: | Immunology / Infectious Diseases |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 4/2/2016 |
| Start Date: | July 2009 |
| End Date: | July 2010 |
| Contact: | Richard Elion, MD |
| Email: | rickelion@gmail.com |
| Phone: | 202-745-6152 |
Safety and Efficacy of ADAPTAVIR's Ability to Eliminate Treatment-Resistant Infectious Virus in the Blood Cellular Reservoir (PBMCs) of HIV Patients With Suppressed Plasma Viral Load.
This is a 24 week placebo controlled, double-blind, 2-arm study of ADAPTAVIR, Monomeric
Dala1-peptide T-amide (mDAPTA) compared to placebo, in HIV infected individuals with
suppressed plasma viral loads < 200 copies/ml by highly active antiretroviral therapy
(HAART) treatment for at least 3 months prior to entry with at least 6 continuous months of
HAART treatment preceding entry. 20 treatment and 20 placebo individuals will be enrolled in
each arm. The study duration is 24 weeks on placebo or mDAPTA administered intranasally at
0.01 mg two times a day.
The main (intent to treat) analysis is planned for the 24 week endpoint. The virological
outcomes of interest in the present study are infectious virus recoverable from cellular
(PBMC) sources and cellular viral mRNA and DNA copy numbers. Immune outcomes (plasma
cytokines) associated with HIV disease, HIV replication, or immune function will be studied.
Dala1-peptide T-amide (mDAPTA) compared to placebo, in HIV infected individuals with
suppressed plasma viral loads < 200 copies/ml by highly active antiretroviral therapy
(HAART) treatment for at least 3 months prior to entry with at least 6 continuous months of
HAART treatment preceding entry. 20 treatment and 20 placebo individuals will be enrolled in
each arm. The study duration is 24 weeks on placebo or mDAPTA administered intranasally at
0.01 mg two times a day.
The main (intent to treat) analysis is planned for the 24 week endpoint. The virological
outcomes of interest in the present study are infectious virus recoverable from cellular
(PBMC) sources and cellular viral mRNA and DNA copy numbers. Immune outcomes (plasma
cytokines) associated with HIV disease, HIV replication, or immune function will be studied.
A primary objective of this study is to assess the safety and toxicity of mDAPTA (Adaptavir)
in HIV infected individuals with suppressed viral loads with HAART treatment and assess the
proportion of study participants achieving PMBC viral culture negative status at 24weeks.
PMBC viral culture status is a direct measurement of treatment resistant, residual, active
HIV replication in the peripheral blood mononuclear cells. We hypothesize this proportion
will be significantly greater in the treatment arm relative to the placebo arm (the odds of
achieving this endpoint are significantly greater in mDAPTA- than in placebo-treated
participants).
Secondary Endpoints (all analyzed as odds ratios) are to determine
- The proportion of study participants achieving (0.5 log10) decrease in quantitative
viral mRNA in PBMCs will be significantly greater in the treatment arm relative to the
placebo arm.
- The proportion of study participants achieving (0.5 log10) decrease in quantitative
viral DNA in PBMCs will be significantly greater in the treatment arm relative to the
placebo arm.
- The proportion of study participants whose plasma viral loads were greater than 200
copies/ml on two successive measurements 6 weeks apart will be significantly greater in
the placebo arm relative to the treatment arm.
Immunological outcome hypotheses, based on 24-week data
- The proportion of study participants achieving at least greater than 50% decrease in
the inflammatory cytokines TNFa, IL-10, IL-8 or IL-6 will be significantly greater in
the treatment arm relative to the placebo arm.
- The proportion of study participants achieving at least greater than 50% increase in
the cytokines IL-2, IL-10, IL-12, IL-13 and IFNa will be significantly greater in the
treatment arm relative to the placebo arm.
- The proportion of study participants achieving at least an increase in CD4 T cells will
be significantly greater in the treatment arm relative to the placebo arm.
- The proportion of study participants whose viral load becomes greater than 200
copies/ml will be significantly greater in the placebo arm relative to the treatment
arm.
in HIV infected individuals with suppressed viral loads with HAART treatment and assess the
proportion of study participants achieving PMBC viral culture negative status at 24weeks.
PMBC viral culture status is a direct measurement of treatment resistant, residual, active
HIV replication in the peripheral blood mononuclear cells. We hypothesize this proportion
will be significantly greater in the treatment arm relative to the placebo arm (the odds of
achieving this endpoint are significantly greater in mDAPTA- than in placebo-treated
participants).
Secondary Endpoints (all analyzed as odds ratios) are to determine
- The proportion of study participants achieving (0.5 log10) decrease in quantitative
viral mRNA in PBMCs will be significantly greater in the treatment arm relative to the
placebo arm.
- The proportion of study participants achieving (0.5 log10) decrease in quantitative
viral DNA in PBMCs will be significantly greater in the treatment arm relative to the
placebo arm.
- The proportion of study participants whose plasma viral loads were greater than 200
copies/ml on two successive measurements 6 weeks apart will be significantly greater in
the placebo arm relative to the treatment arm.
Immunological outcome hypotheses, based on 24-week data
- The proportion of study participants achieving at least greater than 50% decrease in
the inflammatory cytokines TNFa, IL-10, IL-8 or IL-6 will be significantly greater in
the treatment arm relative to the placebo arm.
- The proportion of study participants achieving at least greater than 50% increase in
the cytokines IL-2, IL-10, IL-12, IL-13 and IFNa will be significantly greater in the
treatment arm relative to the placebo arm.
- The proportion of study participants achieving at least an increase in CD4 T cells will
be significantly greater in the treatment arm relative to the placebo arm.
- The proportion of study participants whose viral load becomes greater than 200
copies/ml will be significantly greater in the placebo arm relative to the treatment
arm.
Inclusion Criteria:
1. HIV positive, male or female of any race and at least 18 years of age.
2. Must have received continuous currently acceptable anti-retroviral therapy ("HAART";
highly active antiviral therapy) for at least six months prior to entry.
3. Must have HIV-1 plasma viral load RNA (PCR or bDNA) < 200 copies/mL for 90 days prior
to randomization in this study.
4. Women of childbearing potential must have a negative pregnancy test at screening
prior to randomization in this study. Upon randomization, these women must agree to
use methods of birth control or abstinence to prevent pregnancy.
5. Must have a sustained CD4+ cell count > 350 cells/mm3 for 90 days prior to
randomization in this study.
6. Must be considered clinically stable, in the opinion of the investigator, at the time
of entry into the study.
Exclusion Criteria:
1. Expected to require adjustment to their antiretroviral therapy during screening or
within 8 weeks after initiating mDAPTA therapy.
2. Current participation in other clinical trials with investigational drugs.
3. Use of any investigational agents including immunomodulatory agents (GM CSF,
interferon, interleukin etc.) within 60 days prior to study entry.
4. Use of any vaccine, including for Influenza (killed or live), Pneumovax etc., within
60 days of initiating therapy with mDAPTA.
5. Use or anticipated use of immunosuppressive therapy, including chemotherapy during
participation in the study.
6. Alcohol or substance abuse which, in the opinion of the investigator, would interfere
with patient compliance or safety.
7. Study participants with an active opportunistic infection or malignancy.
8. Pregnant or breastfeeding.
9. Any condition or history of any illness which, in the opinion of the investigator,
might confound the results of the study or pose additional risk in administering the
study drugs to the participant.
10. Participants who previously received treatment with DAPTA.
We found this trial at
1
site
Click here to add this to my saved trials
