Cytomegalovirus Infections Clinical Trial
Official title:
Phase III Study Evaluating the Safety and Efficacy of Artesunate in Preemptive Treatment of Human Cytomegalovirus Disease in Stem Cell Transplant Recipients
Human cytomegalovirus (HCMV) has remained a major cause of morbidity and mortality following
allogeneic bone marrow or peripheral blood stem cell transplantation (SCT). The most
reliable virological predictive marker for disease development is the presence of HCMV
viremia. It has been further recognized that viral load, and viral load kinetics are
important determinants of pathogenesis. Prior to the preventive use of antiviral agents, CMV
disease occurred in 15-45% of at-risk patients and carried a high mortality rate. In the
last decade, major advances in the prevention of CMV disease have occurred with the
application of pp65 antigenemia and qualitative/quantitative polymerase chain reaction (PCR)
assays for the rapid and sensitive diagnosis of HCMV infection, combined with preemptive
antiviral treatment targeted to patients with viremia. The prevalence of early CMV disease
has declined to 3% to 6% with intense antiviral drug use. All antiviral drugs currently used
for the treatment of systemic HCMV infection, including ganciclovir, foscarnet, and
cidofovir, target the HCMV DNA polymerase. Ganciclovir is the most widely used drug for
preemptive treatment. However, ganciclovir treatment is often complicated by bone marrow
toxicity with the occasional development of potentially life-threatening thrombocytopenia,
granulocytopenia, and graft failure, associated with secondary bacterial and fungal
infection. Another limitation of preemptive ganciclovir therapy is the requirement for
intravenous administration. The currently available oral valganciclovir is not yet approved
for preemptive therapy in SCT recipients, and is associated with high treatment cost.
Additionally, prolonged or repeated ganciclovir treatment may lead to the development of
drug resistance. The use of foscarnet and cidofovir is limited by considerable
nephrotoxicity, low oral bioavailability, and high cost. Thus, there is an increasing need
for new effective non-toxic, low-cost anti-HCMV drugs with high oral bioavailability.
Recently, the anti-malaria drug artesunate, which is widely used in the treatment of severe
malaria, has been shown to be a highly effective inhibitor of HCMV in vitro. Artesunate
exhibited similar antiviral activity (same micromolar range) to that of ganciclovir, while
demonstrating no cytotoxicity. Importantly, its antiviral activity has been further
demonstrated in vivo in a rat CMV model. No significant side effects were demonstrated in a
number of pre-clinical and clinical studies, and artemisinin and its derivatives have been
shown to be well-tolerated and safe in adults and children. Several million people have
taken artemisinins to date, with no significant adverse or treatment-limiting effects being
reported. Although neurotoxicity has been reported with supraphysiological doses in animals,
it has not been documented in humans. Meta-analyses of malaria patients treated with
artemisinins demonstrated that this drug class is safe. In rare cases, however, slight
changes to haematology values have been seen, including a reduction in the number of
reticulocytes as well as a slight increase in transaminase levels. These signs, however, do
not generally give rise to any noticeable clinical manifestations. In rare cases, a slight
but transient reduction in sinus heart rate has been observed. Abdominal cramps and mild
diarrhoea have been reported at elevated doses.
Thus, one might expect a similarly high degree of safety for the potential use of artesunate
as an antiviral drug for HCMV infection. Thus, oral therapy with artesunate could be a
beneficial option to the current therapies for the preemptive treatment of HCMV disease in
SCT recipients.
n/a
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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