Classical Kaposi's Sarcoma Clinical Trial
Official title:
A Phase II Trial With the HIV Protease Inhibitor Indinavir for the Treatment of Classical Kaposi's Sarcoma
Recent studies have described a reduced incidence or the regression of Kaposi's sarcoma (KS)
in HIV-infected patients treated with the highly active anti-retroviral therapy (HAART) that
contains at least one inhibitor of the HIV protease (HIV-PI) such as Indinavir. Experimental
studies have shown that part of the anti-KS actions of HIV-PI are not related to their
antiretroviral actions, but, at least in part, to their capability of blocking angiogenesis
and tumor growth.
This study will be conducted on HIV-negative (classical) KS patients to prove that Indinavir
has anti-angiogenic and anti-KS effects in humans independently of its antiretroviral
activity.
Kaposi's sarcoma (KS) is a rare vascular tumor affecting elderly individuals from
Mediterranean countries (CKS), post transplant patients and, with increased incidence and
aggressiveness, HIV-infected individuals (AIDS-KS). No definitive cure has been established
for KS and all conventional therapies result in low response rate, high toxicity and tumor
relapse.
Antiretroviral therapies including a HIV protease inhibitor (HIV-PI) have reduced AIDS-KS
incidence and induce KS regression in treated patients. This cannot be explained solely with
drug-mediated HIV suppression and immune reconstitution. We have shown that HIV-PI such as
Indinavir or Saquinavir block KS-like lesions in mice by inhibiting angiogenesis and tumor
cell invasion through a blockade of matrix metalloprotease 2 (MMP2) proteolytic activation.
Based on these data, a proof-of-concept clinical study on HIV-negative (classic) KS (C-KS)
patients was planned to prove that Indinavir has anti-angiogenic and anti-KS effects in
humans independently of its antiretroviral activity.
Recent concepts in the evaluation of non cytotoxic anti-cancer drugs such as anti-angiogenic
agents suggest novel criteria for the design of clinical studies due to the specific
mechanism of action of these drugs. In particular, the use of the conventional evaluation
criteria based on cytotoxic actions may mislead the interpretation of the therapeutic
efficacy of non cytotoxic agents. The study was therefore designed to compare the clinical
response to Indinavir in early-stage vs. late-stage KS and by relating it to key biological
endpoints and plasmatic drug concentrations. This was also motivated by the rareness of C-KS
and by ethical reasons which prevented the inclusion of a control group.
Patients will be treated per os with 800 mg x 2/daily of Indinavir for 12 months. Follow-up
will be one year.
Primary objectives:
Evaluation of the tumor response rate (complete response, partial response, improved disease
and stable disease) to indinavir in the treatment of mild or severe classical KS patients;
Evaluation of the duration of response in indinavir-treated patients.
Secondary objectives:
Evaluation of Indinavir safety in classical KS population; Determination of the
pharmacokinetic profile of Indinavir; Evaluation of key Kaposi's sarcoma biological
endpoints including markers of angiogenesis and tumor invasion, Th1 and Th2 polarization of
the immune response, immunoactivation, and immune responses to HHV8, herpesviruses and
common pathogens.
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment