Diarrhea Clinical Trial
Official title:
Mass Oral Cholera Vaccination in High-risk Populations in Zanzibar: Assessment of Effectiveness and Herd Protection
The purpose of this study is to conduct cholera vaccinations in high-risk populations in Zanzibar in order to estimate herd protection conferred by the vaccine,estimate effectiveness of the vaccine, and describe the interaction of vaccination and improved water supply on the burden of cholera and diarrhoeal diseases.
The seventh cholera pandemic began in Indonesia in 1961 and spread quickly to other Asian
countries. In 1970, the etiologic agent, Vibrio cholerae O1 El Tor, invaded sub-Saharan
Africa, whose residents had not experienced cholera for more than 100 years. Outbreaks
rapidly occurred and the disease has become endemic in several parts of the continent. In
2006, Africa reported 234,349 cholera cases to the WHO, accounting for 99% of the
officially-notified global cholera (1). Between 1995 and 2005, 66% of cholera outbreak
reports to ProMed came from sub-Saharan Africa (2). There is growing evidence of the large
and increasing burden of cholera in Africa.
One African country that is severely and repeatedly affected by cholera is Zanzibar. After
the first case of cholera was confirmed in the country in January 1978, regular outbreaks
have been reported (3). These outbreaks cause human suffering, are socially disruptive, and
divert resources from other essential services. Cholera control in Zanzibar has focused
mainly on case management, water chlorination campaigns, and dissemination of hygiene
messages. The Ministry of Health and Social Welfare (MOHSW) is eager to identify new and
effective tools, such as oral cholera vaccination, that could be implemented in Zanzibar.
In 2002, the World Health Organization (WHO) recommended the potential use of oral cholera
vaccines in endemic and epidemic situations, but it was deemed necessary to gain more
experience through demonstration projects (4). Since then, mass oral cholera vaccinations
have been conducted in Beira, Mozambique (5), in Darfour, Sudan, and in Aceh, Indonesia
which demonstrated the feasibility and effectiveness of vaccination under actual public
health conditions. The only oral cholera vaccine available in the market consists of killed
whole-cell V. cholerae O1 with purified recombinant B-subunit of cholera toxin (WC/rBS)
administered with a buffer solution as two doses, at least a week apart. The vaccine is
internationally-licensed (including in Zanzibar) for use in individuals 2 years of age and
older. This vaccine, and its predecessor (BS-WC) that contained chemically extracted rather
than recombinant cholera toxin B subunit, have been shown to be safe and protective in
several trials conducted in cholera-endemic settings in Asia and South America (6-9) and in
a sub-Saharan African setting with a high prevalence of HIV (5).
An incompletely answered question regarding this vaccine is its potential to confer herd
protection (10). The level of herd immunity would determine the minimum vaccine coverage
required to produce widespread protection against cholera in a community. A recent study
comparing cholera rates in sites in Asia and Africa has shown that the burden of cholera is
greatest in young children (11); herd immunity would provide protection for children too
young to receive the vaccine, as well as other unvaccinated members of the community.
Although recent re-analysis of data from the large placebo-controlled field trials of the
oral cholera vaccine in Bangladesh in the 1980s showed substantial herd protection from
vaccination (12,13), there may be limitations to the applicability of these findings to
other cholera endemic settings with different living conditions (14). Mathematical modelling
of the same Bangladesh data found that cholera transmission could be controlled in endemic
areas with 50% vaccine coverage. At this level of coverage, the model predicted that there
would be an 89% reduction in cholera cases among the unvaccinated, and a 93% reduction
overall in the entire population. A more modest coverage of 30% would result in a 76%
reduction in cholera incidence for the population area covered (15). If confirmed in actual
field studies, these mathematical predictions have major vaccine cost-effectiveness
implications.
We propose to carry out mass oral cholera vaccinations in populations at high risk for
cholera in Zanzibar followed by an assessment of direct and indirect protection. The WHO was
awarded a grant by the Bill and Melinda Gates Foundation entitled: "Pre-emptive use of a
cholera vaccine in vulnerable populations at risk", under which this proposal will be
funded. The 6 million US$ grant aims to address issues regarding the potential utilization
and mechanism of pre-emptive delivery of the vaccine to prevent outbreaks in endemic
regions. An important component is the potential creation of a "revolving" stock of vaccine
and the financial sustainability of maintaining such a stockpile.
The lessons learned from this project will be crucial for informed decisions about the
potential wider use of cholera vaccination in Zanzibar and other cholera-endemic sub-Saharan
African countries. The lessons learned from the effectiveness study will form part of the
evidence for the possible establishment of a sustainable vaccine stockpile. The project
would provide essential information on the vaccine coverage required to control cholera in
endemic areas and additional data on vaccine effectiveness in a different setting in Africa.
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