Shigellosis Clinical Trial
Official title:
Phase 3 Study (Safety, Immunogenicity and Efficacy) of Improved Shigella Conjugate Vaccines in 1-4 Year Olds in Israel
Shigellosis remains a serious and frequent disease throughout the world. Development of
vaccines has been difficult because shigellae are habitants of and pathogens for humans only
and there is no consensus about the mechanism(s) of immunity to this pathogen.
Incomplete, but compelling evidence, indicates that a critical level of serum IgG anti-LPS
confers immunity to shigellosis. Important data come from our clinical trial in the Israel
Defense Forces (IDF) recruits. A randomized, double-blind, vaccine-controlled study showed
that the S. sonnei-rEPA elicited 74% protection against shigellosis occurring about 3 months
after vaccination (p=0.001). This vaccine conferred 43% (p=0.04) protection in one company
during an outbreak up to 14 days following vaccination suggesting that our Shigella
conjugates might be of value in epidemics. The efficacy of S. sonnei-rEPA was correlated
with the level of vaccine-induced IgG antibodies.
The highest incidence, morbidity, and mortality of shigellosis is in young children. But
serum antibody responsiveness to polysaccharide-based vaccines is age-dependent and infants
and young children respond poorly or not at all to both disease and vaccination. The safety
and immunogenicity of these Shigella conjugates in 4 to 6 years-old children in Israel was
demonstrated. But although the fold rise in anti-LPS was similar in the children, the level
of anti-LPS elicited by the conjugates was lower than in adults. We improved the
immunogenicity of Shigella conjugates as shown in mice and then in adult humans. Now we
apply to evaluate the safety, immunogenicity and efficacy of these improved conjugates in 1
to 4 years-old children in Israel.
In Israel, shigellosis is common especially in children. S. sonnei (Group D) comprise about
60% of the isolates followed by S. flexneri (Group B): Shigella dysenteriae type 1 (Group A)
is not found. We propose to administer 2 injections of either S. sonnei-CRM9 or S. flexneri
type 2a-rEPAsucc 6 weeks apart in a random double-blind fashion to about 6,000 1 to 4
year-olds. Active surveillance of the vaccinees for enteric infections will be maintained
for at least 2 years to evaluate the effect of vaccination.
Shigellosis remains a serious and frequent disease throughout the world. Development of
vaccines has been difficult because shigellae are habitants of and pathogens for humans only
and there is no consensus about the mechanism/s of immunity to this pathogen.
Incomplete, but compelling evidence, indicates that a critical level of serum IgG anti-LPS
confers immunity to shigellosis. A randomized, double-blind, vaccine-controlled study in
Israel Defense Force (IDF) recruits showed that the S. sonnei-rEPA elicited 74% protection
against shigellosis occurring about 3 months after vaccination (p=0.001). This vaccine also
conferred 43% (p=0.04) protection in one company during an outbreak up to 17 days following
vaccination suggesting that our Shigella conjugates might be of value in epidemics. The
efficacy of S. sonnei-rEPA was correlated with the level of vaccine-induced IgG antibodies.
The highest incidence, morbidity, and mortality of shigellosis is in young children. But
serum antibody responsiveness to it is age dependent and infants and young children respond
poorly or not at all to polysaccharide antigens following disease, administration of
attenuated strains of Shigella or vaccination with whole cell vaccines. The safety and
immunogenicity of similar Shigella conjugates in 4 to 7 years-old children in Israel was
demonstrated. But, although the fold rise in anti-LPS was similar in the children, the level
of anti-LPS elicited by the conjugates was lower than in adults. We improved the
immunogenicity of Shigella conjugates as shown in mice and then in adult humans. Now we
apply to evaluate the safety, immunogenicity and efficacy of these improved conjugates in 1
to 4 years-old children in Israel. In addition to monitoring the safety and immunogenicity
of the two investigational Shigella vaccines, active surveillance of the vaccines for
enteric infections wil be maintained for at lest 2 years to evaluate the effect of
vaccination.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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