Latent Tuberculosis Infection Clinical Trial
Official title:
A Randomized Trial to Compare Effectiveness of 4 Months Rifampin (4 RIF) With 9 Months Isoniazid (9 INH) in the Prevention of Active TB in Children: The P4v9 Trial
Tuberculosis (TB) is spread by airborne transmission from adults with active contiguous TB to
children, especially those living in the same household. Once children are exposed and
infected they are at very high risk to develop active TB - which can be lethal if not
detected and treated promptly. This makes it very important to detect TB infection as soon as
possible, and treat this while it is still latent or dormant. Current therapy for latent TB
infection is 9 months of Isoniazid; this is very effective if taken properly but because
treatment is so long many children do not finish this. Four months of Rifampin is a
recommended alternative. In adults this has been shown to be safer with much higher
completion rates. However the effectiveness of this treatment is unclear, and is being
studied in an ongoing study. The investigators plan to compare the safety as well as the
acceptability and effectiveness of 4 months Rifampin with 9 months Isoniazid (standard
treatment) in children in several sites in Canada and other countries.
It is hypothesized that among children at high risk for development of active TB,
intolerance/adverse events will not be worse (non-inferiority), among those randomized to
4RIF compared to those randomized to 9INH. In addition completion of latent tuberculosis
infection (LTBI) therapy will be significantly greater (superiority), and subsequent rates of
active TB will not be significantly higher (non-inferiority) in children taking 4RIF.
On a global scale tuberculosis (TB) is the single most important infectious cause of
morbidity and mortality in individuals aged 15-49. The World Health Organization has
estimated that one third of the entire population of the world carries dormant or latent TB
infection (LTBI). Of these, 9 million develop active disease and 2 million die from TB each
year. In Canada and other industrialized countries, TB continues to cause significant
morbidity and mortality, particularly in minorities, immigrants and other disadvantaged
populations.
A key TB control strategy is therapy of LTBI. The current standard regimen is 9 months of
daily Isoniazid (9INH). This has excellent efficacy if taken regularly, but the long duration
of treatment as well as potential for serious side effects, substantially reduces provider
prescription, patient acceptance, and completion. A shorter alternative of 4 months of daily
Rifampin (4RIF) has been recommended based on limited evidence in LTBI, but extensive
experience using Rifampin for treatment of active TB. However the efficacy of 4RIF in
preventing active TB is not known, especially in children.
The investigators have initiated a research program to evaluate 4RIF for the treatment of
LTBI. In a first study, 4RIF was associated with significant higher completion rates than
9INH. In a second study, all suspected adverse events were judged by an independent 3-member
review panel, who were blinded to study drug. Incidence of Grade 3-4 serious adverse events
was significantly lower among the 420 subjects randomized to 4RIF then among the 427
randomized to 9INH (2.4 % vs. 5.6%, P=.02). Grade 3-4 hepatotoxicity was also significantly
lower with 4RIF than 9INH (0.7% vs. 3.8%, P=.003), and completion rates were significantly
higher with 4RIF.
Therefore, a large scale multi-center trial was launched, with CIHR funding, to compare the
efficacy and effectiveness in preventing active TB of 4RIF and 9INH in adults (see
NCT00931736). In total 5,850 adults will be randomized at 4 sites in Canada as well as sites
in Australia, Brazil, Benin, Ghana, Indonesia, Korea and Saudi Arabia. The primary outcome of
this trial is the occurrence of microbiologically confirmed active TB within 28 months after
randomization.
As an addition to this ongoing study, the investigators are conducting an open label
randomized trial in children at some of these same sites with the primary objectives of
comparing tolerability and safety. Secondary outcomes will be completion of therapy (defined
as taking more than 80% of planned doses), and active TB. Eligible children will be HIV
infected, household contacts of active pulmonary TB cases, or other high risk group, with a
positive Tuberculin skin test (TST) reaction. Active TB must be excluded before enrollment.
A total of 822 children will be randomized in equal numbers to receive daily and
self-administered 9INH or 4RIF. Children will be followed by their usual providers during
therapy.
Intolerability and adverse events during therapy will be investigated according to a
standardized protocol, and reported in non-nominal fashion, using a web-based system. These
reports will be reviewed by an independent 3-member panel, blinded to study drug, to judge
severity and likely relationship to study drug. Completion of therapy will be ascertained by
dosage counts (of pills or suspension) at each follow-up visit, and defined as taking > 80%
of doses within a defined maximum time.
After therapy, children will be followed every 3 months up to 16 months post-randomization
for the occurrence of clinically diagnosed active TB; this will also be detected and
investigated following a standardized protocol. The final diagnosis of active TB will be
based on the judgment of an independent panel of two expert pediatricians who will review all
clinical radiographic and microbiologic information while remaining blinded to study drug.
The primary analysis will compare rates of Grade 1-5 adverse events judged probably due to
study drug. Planned secondary analysis will compare rates of study drug completion as well as
rates of clinically diagnosed active TB in all children randomized to the two regimens
(intention to treat=effectiveness) and rates of clinical active TB in children who take more
than 80% of planned doses (per protocol-efficacy analysis).
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