HIV Infections Clinical Trial
Official title:
A Multi-Center, Double-Blind, Randomized, Placebo-Controlled Study of Orally Administered SP01A for 28 Days as Monotherapy Treatment in HIV-Infected Patients With Evidence of Resistance to Currently Available Antiretroviral Therapy
This is a 28-day, multi-center, placebo-controlled study designed to look at the dose
response, efficacy, and safety of SP01A, given as a pill to be swallowed, in the treatment
of HIV-infected subjects.
Samaritan has discovered that SP01A affects cholesterol binding, which is directly
implicated in the pathogenesis of HIV. It has also been established that drugs of this
nature exert an anti-HIV effect in-vitro. These data suggest that SP01A has the potential to
reduce HIV virus replication.
One measurement of an HIV infected person’s risk of progressing to AIDS is the number of
viral particles of HIV in their blood (called a “viral load”). This study is designed to see
if SP01A will lower the amount of HIV in an infected individual's blood. Patients will be
assigned by chance to 1 of 4 groups. Neither the patient nor the study doctor or nurse will
know which dose of the study drug the patient is taking or if he/she is receiving the
placebo (a capsule that looks like the study drug but does not contain any active
ingredient).
Study drug administration will continue for 28 days. At the end of the 28-day study, the
patient will be offered testing of his/her virus for resistance to approved drugs
(genotype).
Currently approved antiretroviral medications target either the HIV viral reverse
transcriptase (RT), (Nucleoside Reverse Transcriptase Inhibitors (NRTIs) and Non-Nucleoside
Reverse Transcriptase Inhibitors (NNRTIs)) or the viral protease, (Protease Inhibitors
(PIs)) or inhibit viral fusion with target cells (Fusion Inhibitors). A regimen using a
combination of these agents is considered the standard of care and, when effective, results
in suppression of the virus below the detection limits.
However, the long-term use of antiretroviral therapy is sometimes hampered by poor
compliance due to pill burden, food restrictions, and major side effects that impact Quality
of Life. Furthermore, one of the major reasons for therapy failure is the emergence of
resistant virus against one or more of the anti-HIV medications or, to some extent, an
entire class of drug (cross resistance).
Enfuvirtide (Fuzeon™) was recently approved as an HIV-1 fusion/entry inhibitor, a new class
of treatment that prevents fusion of the HIV-1 virus to the CD4+ cell membrane by preventing
the conformational changes required for this fusion. Since the mechanism of action of
Enfuvirtide is different from other classes of anti-HIV medication, it is effective in
patients who have failed other therapies due to emergence of resistant virus. However, a
recent study demonstrated the emergence of resistance to Enfuvirtide due to a mutation in
viral gp41.
The rapid rate of mutation of HIV-1 and conferred resistance of the virus to current
therapies continues to necessitate a need for additional therapeutic agents. To that end, a
hypothesis has been suggested regarding the immuno-modulating and anti-viral effects of
SP01A in the treatment of HIV infection.
SP01A may affect cholesterol binding, which is directly implicated in the pathogenesis of
HIV. Several observations have also established that inhibitors of cholesterol synthesis
inhibit cell fusion formation induced by HIV-l and that drugs extracting cholesterol from
the cellular membrane exert an anti-HIV-1 effect in-vitro. Taken together, these data may
suggest that procaine hydrochloride and SP01A reduces HIV-1 virus replication by modifying
the cholesterol content of the cell membrane, rendering it much more difficult for the virus
to enter and infect the cell.
There is an urgent need to develop improved new therapeutic agents. SP01A, which targets
different viral or cellular components with a new mechanism of action, is being developed
and tested by Samaritan Pharmaceuticals, Inc. as a new anti-viral therapeutic agent.
This multi-center, double-blind, randomized, placebo-controlled study of orally administered
SP01A as monotherapy in HIV-infected patients with evidence of resistance to currently
available antiretroviral therapy was designed to further evaluate the dose response,
efficacy, and safety of SP01A. HIV-positive patients will be evaluated during the pre-study
period. Following a 2-week washout period (if required), patients will be randomized into
one of four study arms and all arms will initiate the 28-day monotherapy study. The first
arm will receive 200 mg of SP01A QID. Arm Two will receive 200 mg bid. The third arm will
orally administer 400 mg bid. Finally, the fourth arm will receive placebo twice daily.
During the treatment period, patients will make five scheduled visits to the treatment
facility on or about Days 1, 8, 15, 22, and 29. During these visits patients will be
monitored for viral load and general health parameters. At the conclusion of the 28-day
monotherapy study, patients will have optimized viral testing for further treatment.
On Day 43, patients will make their final visit to the treatment facility for post-study
evaluation.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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