Safety and Immunogenicity of Oral Cholera Vaccine in Kolkata

Phase 2CompletedNCT00119197

International Vaccine Institute200 enrolled

Overview

The purpose of the study is to confirm the safety and immunogenicity of the oral killed bivalent cholera vaccine in adult and pediatric volunteers in Eastern Kolkata, West Bengal, India.

Cholera remains to be a serious public health problem worldwide. In the mid-1980s following technology transfer from Sweden, Vietnamese scientists developed and produced an oral killed monovalent cholera vaccine for Vietnam's public health programs. A 2-dose regimen of this vaccine has been shown to be safe and efficacious. Subsequently, a bivalent vaccine was developed containing the newly emergent O139 V. cholerae. This vaccine has several advantages over the existing Swedish vaccine. It confers protection against the El Tor biotype in younger children, is considerably less expensive, does not require a buffer during administration and does not require strict cold chain requirements. However, this vaccine is not licensed for use in countries other than Vietnam. Through IVI, an agreement between VABIOTECH in Hanoi and Shantha Biotechnics PVT, LTD in India has been reached that will make the bivalent vaccine available in India. A double-blind randomized phase III trial in a cholera-endemic area would be necessary to demonstrate the efficacy of this vaccine in other settings. This would pave the way for the introduction of the vaccine into the national immunization programme in India and the internationalization of this vaccine and licensure in other countries where it is needed. Prior to the phase III trial, a phase II study will be performed among adults and children.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

PREVENTION

Masking

QUADRUPLE

Enrollment

200

Conditions

Cholera

Interventions

killed whole cell oral cholera vaccineBIOLOGICAL

Bivalent oral killed cholera vaccine: each dose of this vaccine contains: * Inactivated V.Cholerae Inaba (569B), Classical biotype - 25.109 cells * Inactivated V.Cholerae Ogawa (Cairo 50) Classical biotype - 25.109 cells * Inactivated V.Cholerae Inaba (Phil 6973) El Tor biotype - 50.109 cells * Inactivated V.Cholerae O139 - 50.109 cells each 1.5 mL dose given orally, two doses given 14 days apart

Heat Killed E. coliBIOLOGICAL

Escherichia coli K12 strain placebo: each dose of placebo contains heat-killed E. coli K12 strain in an amount whose optical turbidity is identical to that for the cholera vaccine. Each 1.5 mL dose given orally, two doses given 14 days apart

Eligibility

Sex: ALLMin age: 12 MonthsMax age: 40 YearsHealthy volunteers:

Medical Language ↔ Plain English

Inclusion Criteria: * Healthy non-pregnant adults aged 18-40 years and children aged 1-17 years Exclusion Criteria: * Diarrhea during the past week * Antibiotic and anti-diarrheal medicine use during the past week * One or more episodes of diarrhea or abdominal pain lasting for 2 weeks during the past 6 months * Abdominal pain, nausea, vomiting, loss of appetite or generalized ill feeling for the past 24 hours * Pregnancy

Locations (1)

National Institute of Cholera and Enteric Diseases

Kolkata, West Bengal, India

Outcomes

Primary Outcomes

adverse events

Time frame: immediate events - 30 minutes after each dose, adverse events - for 3 days following dose, serious adverse events throughout study - 28 days

Secondary Outcomes

serum vibriocidal antibody response

Time frame: baseline and 14 days after second dose

Data from ClinicalTrials.gov

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