HIV Clinical Trial
Official title:
Safety of Reduced Dose Zidovudine (AZT) Compared With Standard Dose AZT in Antiretroviral-naïve HIV-infected Patients: A Randomized Controlled Trial
The primary objective of the study is to compare the tolerance and safety between a low-dose
Zidovudine (AZT) containing regimen (200 mg BID) and a standard dosage (300 mg BID) in HIV
patients initiating a first line antiretroviral therapy. The investigators expect that the
low-dose regimen will show improved tolerability and safety compared to the standard dosage,
with significant reduction in number of patients experiencing a new grade 1 to 4 anaemia or
increasing their anaemia grade during the first 6 months of treatment.
The secondary objectives of the study is to compare the efficacy of the two dosing regimen,
as measured by classical clinical and biological markers: the number of new AIDS defining
illness, the mortality rate, the proportion of patients achieving virological success and
the mean CD4 cell count increase from baseline.
Existing formulations for adults include zidovudine 100mg capsule, zidovudine/3TC 300/150mg,
zidovudine/3TC/NVP 300/150/200mg, zidovudine/3TC/ABC 300/150/300. Currently, international
guidelines recommend a daily dose of 600 mg in 2 divided doses. Pharmacokinetic studies on
zidovudine showed a twice daily regimen resulted in higher predose zidovudine-triphosphates
(TP) concentrations, the active intracellular metabolite, when compared to the same daily
dose given once daily. Further, a small study in Thailand study found doses of zidovudine
200 mg twice daily achieved plasma levels equivalent to the standard international 300 mg
twice daily dose in individuals weighing less than 60 kg.
The clinical efficacy of zidovudine has been evaluated in randomized clinical trials using a
range of doses from 300 to 1500 mg/day. In an early trial (Nordic Medical Research Councils'
HIV Therapy Group 1992) comparing different dosing of zidovudine monotherapy in advanced HIV
infection found no differences in death rate, or new AIDS defining events. The incidence of
anaemia and leucopenia comparing 400 mg and 1200 mg daily showed a direct dose relationship:
4% to 24% (anaemia) and 3% to 22% (leucopenia) respectively. Another early trial (Fischl
1990) demonstrated an improved survival with the lower dose of zidovudine (63%) versus the
high dose (52%), again with significantly more anaemia and neutropenia in the high dose
zidovudine arm (p < 0.001).
High doses of zidovudine have led to increased incidence of anaemia and neutropenia, with no
impairment in treatment efficacy as measured by CD4 cell count, HIV RNA level or clinical
progression. In the context of new recommendations favouring the use of zidovudine over
stavudine as first line treatment in resource limited settings, the investigators aim at
evaluating the impact of reduced zidovudine (200 mg BID) treatment.
API (active product ingredient) production costs are the most important determinant of
antiretroviral drug prices among generic manufacturers. A given percentage reduction in
dosage will thus translate into a virtually equivalent percentage in drug pricing. As cART
will continue to expand in Least Developed Countries, it is predicted that around 1.5
million people will take zidovudine-based regimen by 2010. Small reductions in the annual
per-patient cost of AZT-based regimen could lead to significant reductions in the global
cost of HIV treatment: it is estimated a 47 million US dollars savings if 9 million patients
will be treated in 2014.
The present study is a prospective, randomised, 48 weeks, phase II trial. Subjects will be
recruited through one site: the HIV outpatient clinic of Internal Medicine Department, CNPS
Hospital, Yaoundé, Cameroun. Randomisation will be performed at initiation of ART. Patients
will be randomised in one of the following treatments arms, in combination with lamivudine
and an NNRTI regimen: a low-dose AZT arm (200 mg twice daily)or a standard-dose AZT arm (300
mg twice daily).
The primary endpoint is the comparison of proportions of patients experiencing a new grade 1
to 4 anaemia or increasing their anaemia grade between the two dosing AZT regimen during the
first six months of treatment.
The secondary endpoints are:
- Mean haemoglobin concentration and leukocyte count changes, laboratory grade 3 and 4
adverse events rate leading or not to switch for another cART regimen.
- Differences in proportion of patients achieving virological success (VL <50 cop/ml)
between the two dosing zidovudine regimen at week 24.
- Difference in proportion of patients achieving virological success ( VL <400 cop/ml)
between the two dosing zidovudine regimen at week 24.
- Difference in mean viral load decline between the two groups at week 4 and 8
- Difference in mean CD4 cell count increase from baseline between the two dosing
zidovudine regimen at week 8, 24.
- Difference in proportion of patients with genotype mutations in patient with detectable
viral load at week 24.
- Number of new AIDS defining illness, mortality rate, drop-out rate will be compared
between the two groups.
Patients will be followed individually 24 weeks for the entire period of experimental
treatment. After the follow-up period, all patients included in the low dose AZT arm will be
treated with standard AZT dose. They will keep their routine follow-up at the CNPS hospital.
For the first 68 patients included (half of the total cohort) in the study, the Data Safety
Monitoring Board (DSMB, independently of the clinical investigators) will undergo an interim
analysis at week 8 of follow-up before continuing enrollment. In this sample of patients,
the efficacy of two treatment groups will be compared: an excess of 15% virological
treatment failure in the low-dose AZT arm will be considered as significant. Virological
treatment failure at this point is defined as a decline in viral load from baseline to the
8th week of less than 2log.
An incidence of 30% of patients experiencing new grade 1 to 4 anaemia or increasing their
anaemia grade during the first 6 months of treatment is expected with the standard AZT dose
regimen. A reduction of this adverse event to 10% of the patients treated by the low dose
regimen would be considered as clinically significant. Thus, with a 10% of LFU expected
during the follow-up period, the investigators calculate a sample size of 68 patients in
each arm to detect a clinically significant difference between the two arms.
The percentage of patients experiencing a new grade 1 to 4 anaemia or increasing their
anaemia grade will be compared between both treatment arms using the difference of
proportion observed (Chi2 test or Fisher exact test).
The same method will be used to compare all the efficacy and safety indicators. Multivariate
analysis will be used to obtain adjusted estimates of risk factors for treatment failure and
for clinically significant adverse events.
Analysis on treatment safety and efficacy will be performed both in 'intention to treat" and
in "per protocol".
An "intention to treat" analysis will include patients enrolled in the study who received at
least one dose of study medication to which they were randomly allocated.
A "per protocol" analysis will include patients enrolled in the study who received at least
one dose of study medication to which they were randomly allocated AND have reached one of
the protocol defined treatment failure endpoints (death, lost to follow-up, virological
failure) on the treatment they were randomly allocated or have completed the trial follow-up
on the treatment they were randomly allocated.
Criteria for the termination of the trial are:
- Too low enrollment rate.
- Unsafe or unethical practices.
- Following the recommendation of the DSMB. The sponsor and investigators will ensure
that this study is conducted in full compliance with the principles of the "Declaration
of Helsinki" or with the laws and regulations of the country in which the research is
conducted, whichever affords the greater protection to the individual. The study must
fully adhere to the principles outlined in "Guideline for Good Clinical Practice" ICH
Tripartite Guideline (E6, June 1996) or with local law if it affords greater protection
to the subject.
This study will be conducted in accordance with the ethical principles laid out in the
Declaration of Helsinki and the National Statement on Ethical Conduct in Research Involving
Humans.
Investigators will obtain written informed consent from each subject participating in this
study, after adequate explanation of the aims, methods, anticipated benefits, and potential
hazards of the study.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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