Diarrhea Clinical Trial
Official title:
A Multi-site, Randomized, Double-blind, Placebo-controlled Study to Evaluate the Safety and Immunogenicity of Trehalose-reformulated Peru-15 (Choleragarde)Vaccine Given Simultaneously With Measles Vaccine in Healthy Indian and Bangladeshi Infants
The purpose of this study is to confirm the safety and immunogenicity of Peru-15 vaccine in infants when given simultaneously with measles vaccine.
Cholera is an important public health problem worldwide, remaining endemic in most of the
developing world at the same time causing outbreaks in areas where lapses in sanitation
occur. In 2005, 131 943 cholera cases and 2272 deaths were reported to the World Health
Organization (WHO) with more countries reporting cholera outbreaks. Overall, this represents
a 30% increase in the number of cases reported compared to 2004. The cholera case fatality
rate during that year was 1.72%; however, recent outbreaks in West Africa resulted in
case-fatality rates of as high as 12% [1, 2]. These figures are believed to be
underestimates and that as much as 120 000 deaths due to cholera are estimated to occur each
year [3]. Aside from this high mortality, cholera outbreaks cause economic and social
disruptions.
The states of West Bengal in India together with neighboring Bangladesh have been considered
by many as the "homeland of cholera". In India, 4695 cases of cholera were reported to the
WHO [1] with states such as West Bengal, Maharashtra, Andra Pradesh, Tamil Nadu, Karnataka
and Delhi long been reporting outbreaks [4]. Although no country-wide data is available from
Bangladesh, a 4 - year surveillance in 4 different geographical areas in Bangladesh reveal
that cholera is widely distributed even in an area with no reported outbreaks for 10 years
[5]. Cholera in these 2 countries affects all age groups, with the youngest age group being
the most affected. In Kolkata, children <5 years of age had a 30% higher risk of having
cholera compared to older individuals [6] and in Bangladesh, 53% of 5670 cholera-infected
patients in the 4-year surveillance were children <5 years of age [5]. Further analysis of a
3 year prospective surveillance of cholera in Kolkata shows that infants less than 2 years
of age had a cholera incidence rate of 4.20 per 1000 person-years whereas the over-all rate
in the study population was 1.41 per 1000 person-years (Data on file).
Provision of safe water and food, establishment of adequate sanitation, and implementation
of personal and community hygiene constitute the main public health interventions against
cholera. These measures cannot be fully implemented in the near future in most
cholera-endemic areas. A safe, effective, and affordable vaccine would be a useful tool for
cholera prevention and control.
Considerable progress has been made during the last decade in the development of new
generation oral vaccines against cholera. These have already been licensed in some countries
and are now being considered for wider public health application. The World Health
Organization recently recommended that the newer generation cholera vaccines be considered
in certain endemic and epidemic situations, but indicated that demonstration projects are
needed to provide more information about the costs, feasibility, and impact of using these
vaccines [7].
A killed oral cholera vaccine (Dukoral™) has long been available internationally, however
its 2-dose schedule, the use of a buffer and the cost of the vaccine have impeded its use in
public health settings. A live oral vaccine, CVD-103 HgR (Orochol™), although
internationally licensed is currently not available in the market. This vaccine is only
available for use in children older than 6 years old and adults. Despite the immunogenicity
and efficacy in challenge studies in North American volunteers [8], in a field trial of this
vaccine in an endemic area in Indonesia, no protective efficacy was detected during the
period of observation [9].
A need exists for an improved cholera vaccine that is more thermostable and may be used in
endemic countries in younger age groups. This new generation oral cholera vaccine must be
administered in a single-dose regimen, be thermostable, confer high grade long-term
protection and may be given to children below 2 years of age through mass immunization
campaigns or through the expanded programme on immunization (EPI). In the Diseases of the
Most Impoverished Programme (DOMI) of the IVI, Peru-15 was identified as the most promising
of all the vaccine candidates. It is a live oral attenuated cholera vaccine derived from V.
cholerae O1 El Tor Inaba strain that was first isolated in Peru in 1991 [10]. This has the
advantage of being given in a single dose and of having the same biotype as the current
pandemic strain (biotype El tor), unlike CVD-103 HgR which is a classical biotype. Peru-15
has been attenuated by several genetic modifications and deletions. By the deletion of the
ctx A and the rtxA genes, it has been rendered unable to encode for cholera toxin subunit A
and RTX toxin making it non-toxigenic and by insertion of the cholera toxin B gene to the
recA gene, it enabled the strain to produce cholera toxin B. This insertion has inactivated
the recA gene, and this together with the deletion of the attRS1 sequences, has decreased
the ability of the strain to integrate exogenous DNA making it non-recombinational. Lastly,
by the absence of the potentially inflammatory flagella it has been rendered non-motile [10,
11]. In addition, Phase I and II studies have been performed in North American volunteers
where it was found to be safe and immunogenic [11-12]. Furthermore, the vaccine strain
isolated from the stools of volunteers retained its non-motile characteristic. In a
challenge study among North American volunteers, Peru-15 provided 100% protection against
moderate and severe diarrhoea, and 93% against any diarrhoea [13].
This vaccine underwent phase I and II studies in a cholera-endemic area in Dhaka, Bangladesh
in three age groups: adults aged 18 - 45 years, children aged 2 - 5 years and infants aged 9
- 23 months [14, 15]. In these studies, a 2 x108 CFU dose of the vaccine was shown to be
safe and able to elicit vibriocidal responses among all age groups. 75% of adults, 84% of
children aged 2-5 years and 70% of infants aged 9-23 months developed a 4-fold rise from
baseline in their vibriocidal titres. Only 1 of 20 adults and 8 of 140 children who received
vaccine excreted the vaccine strain up to 4 days after vaccination. Analysis of the strains
isolated revealed that the strains remained unchanged in phenotypic and genotypic properties
after passage in the stool.
To date, the vaccine has been tested on more than 400 volunteers. The freshly harvested
product, tested on 23 volunteers and the frozen lyophilized preparation, tested on 381
volunteers were both shown to be safe and immunogenic in all age groups. The most frequently
reported adverse events were gastrointestinal symptoms (diarrhea, nausea, abdominal
cramping, gas, decreased appetite) and headache and in controlled studies were reported in
similar frequencies in subjects who received Peru-15 and placebo. The optimal dose for
healthy adult travelers was a single, oral dose of 1 x 108 CFU. The study in Bangladesh
further confirmed that a 108 dose was safe and immunogenic in all age groups including
infants among residents of a cholera endemic area.
Avant Immunotherapeutics Inc., manufacturers of Peru-15, are in the process of reformulating
the vaccine with the long-term stabilizing ability of trehalose in order to make Peru-15
more thermostable at elevated temperatures, i.e. 2-8ºC. If this reformulation is proven as
safe and at least as immunogenic as the previous version, then this will make vaccine
storage easier and more easily deployable in field conditions in Africa, in refugee settings
and in endemic countries in South Asia.
The International Vaccine Institute (IVI) through the Cholera Vaccine Initiative (CHOVI)
together with Avant Immunotherapeutics Inc., manufacturers of the Peru-15 vaccine, have
negotiated an agreement that allow clinical trials on this reformulated vaccine to be
performed in 2 cholera-endemic countries - India and Bangladesh. This will eventually enable
licensure and facilitate the international use of this vaccine by obtaining a WHO
recommendation for its global use. This single dose vaccine may easily be used in endemic
countries and deployed at times when outbreaks are likely to occur. Furthermore, this
vaccine may potentially be used in infants and young children who have the highest risk of
cholera, potentially being included as part of the EPI in endemic areas.
The previous formulations of the vaccine were shown to be safe and immunogenic in all age
groups, including infants, in a cholera endemic area [12 - 15] and efficacious in preventing
cholera diarrhea in healthy adult volunteers [13]. In view of this, the current dose of up
to 109 of the current formulation will be directly tested among infants.Data regarding the
safety and immunogenicity of the trehalose-reformulated Peru-15 vaccine among infants need
to be confirmed in order to pave the way for the possible use of this vaccine in
cholera-endemic areas where infants and children are most at risk. Furthermore, if this
vaccine will be used in the context of the EPI to be given together with measles vaccine, it
would be important to determine if immune interference exists between these 2 live
attenuated vaccines.
;
Allocation: Randomized, Endpoint Classification: Safety Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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