Serological Evaluation of Varicella and Hepatitis A Vaccines Using Injector Delivery

Serological Evaluation of Chickenpox (Varicella) and Hepatitis A Vaccines Using Disposable Needle-Free Syringe Jet Injector (DSJI) Delivery

Status

UNKNOWN

Phases

Phase 2Phase 3

Study type

Interventional

Source

ClinicalTrials.gov

Registry ID

NCT00926419

Acronym

InjHepAVar

Enrollment

600

Registered

2009-06-23

Start date

2009-06-30

Completion date

2010-05-31

Last updated

2009-06-23

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Varicella, Hepatitis A

Keywords

Varicella, Hepatitis A, Vaccine, Injector, Fractional dose, Intradermal, Children

Brief summary

This study aims to assess immunogenicity and safety of nd influence of the delivery system (needle-free injector or syringe with needle) of fractional doses (dose sparing) of two vaccines (Varicella and Hepatitis A vaccines) in children aged 13 to 30 months.

Detailed description

The purpose of this study is to evaluate the immunogenicity, safety and influence of the delivery system (needle-free injector or syringe with needle) of fractional doses (dose sparing) (23,3 and 43,3 PFU - plaque-forming units - of live attenuated OKA strain of Varicella-zoster virus and 100 radioimmunoassay units HAV) of chickenpox and Hepatitis A ( vaccines, intradermally administered, compared with full dose of 103,3 PFU, subcutaneously administered, in 600 primo (first) vaccinated children aged 13 to 30 months selected at random at day care centers in São Paulo. Vaccines will be tested sequentially (Varicella on day 0 and Hepatitis A on day 45). Only 400 children will be randomized again for Hepatitis A vaccine testing, the remaining 200 children will receive the regular dose of Hepatitis A vaccine without further assessment. Doses will be administered using two systems: Disposable Needle-free Syringe Jet Injector (DSJI), compared with the conventional procedure using syringes and needles. Serial blood samples will be blindly analyzed to detect antibody seroconversion. Local and systemic adverse events will be assessed according to definition established by Brighton Collaboration Group, 24 and 72 hours, 7 days, 14 days, 21 days and 45 days after each vaccination, through clinical evaluation and telephone calls.

Interventions

BIOLOGICALVaricella Vaccine

Lyophilized Varicella virus vaccine, live, attenuated (Oka-strain)

BIOLOGICALHepatitis A Vaccine

Hepatitis A virus vaccine, inactivated, Single dose

Study design

Allocation

RANDOMIZED

Intervention model

PARALLEL

Primary purpose

PREVENTION

Masking

SINGLE (Outcomes Assessor)

Eligibility

Sex/Gender

ALL

Age

13 Months to 30 Months

Healthy volunteers

Yes

Inclusion criteria

* Children of both genders older than 13 months and younger than 30 months of age. * Available for follow-up for at least 45 days at public day care centers funded by São Paulo City local government. * Written informed consent signed by parents or legal guardians after reading and explanation

Exclusion criteria

* Suspect/verified diagnosis of congenital or acquired immunodeficiency syndrome (AIDS) * Suspect/verified diagnosis of malign neoplasia * Children on treatment with high-dose systemic corticosteroids (equivalent to prednisone 2 mg/kg/day, for two or more weeks), or immunosuppressive therapy. * Received a vaccine with live attenuated strain of virus within less than 30 days * Suspect/verified diagnosis of chickenpox or has already been immunized against chickenpox (varicella). * Suspect/verified diagnosis of hypersensibility to any ingredient of the vaccine. * One of the parents or legal guardians of the minor does not agree with the study. * Any other circumstances that may potentially damage the minor or prevent procedures from being carried out according to evaluation of the research team. * Child shows signs or symptoms of an active intercurrent disease (e.g. fever, rash, etc.) that may interfere with the evaluation of adverse events after immunization at the research team's discretion. In this case, the participant may be reevaluated within the following three months in order to verify eligibility.

Design outcomes

Primary

Measure	Time frame
Immunogenicity: General seroconversion rate 45 days following immunization. Safety: General rate of local and systemic adverse events after immunization according to definition established by Brighton Collaboration Group	45 days after immunization

Secondary

Measure	Time frame
Degree and duration of local and systemic adverse events after immunization according to the Brighton Collaboration Group recommendations.	45 days after immunization
Seroconversion rates and number of local and systemic adverse events after immunization according to delivery system (needle-free injector or syringe with needle) for each dose tested	45 days after immunization
Actual volume administered intradermally according to the delivery system (needle-free injector or syringe with needle) for each fractional dose tested	At immunization
Participants' parents or legal guardians acceptability according to the delivery system (needle-free injector or syringe with needle) for each dose tested	45 days after immunization
Distribution of vaccine jet evaluated through ultrasound for the needle-free injector group	5 minutes after immunization

Countries

Brazil

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026