Serogroup C Meningococcal Meningitis Clinical Trial
Official title:
Immunogenicity, Reactogenicity and Safety Assessment of the Meningococcal Serogroup C Vaccine Produced by Bio-Manguinhos / FIOCRUZ in Infants, Children and Adolescents
TYPE / DESIGN STUDY: Clinical trial phase II / III, randomized, double-blind, national
multi-center, with a total of 1,644 research participants stratified into 3 groups according
to age for starting of the primary vaccination schedule (Stratum I - 11 to 19 years, Stratum
II - 1 to 10 years; Stratum III - less than 1 year old).
BACKGROUND / STUDY CASE: Clinical trial phase II / III, which purpose is to evaluate
immunogenicity, safety and reactogenicity of the vaccine against meningococcus C, conjugated
to tetanus toxoid, developed by Bio-Manguinhos / FIOCRUZ (MenCC-Bio). The hypothesis of the
study is that MenCC-BIO vaccine is safe and not inferior in terms of immunogenicity to the
comparator vaccine currently available for the National Immunization Program in the child's
immunization schedule. Thus, MenCC-Bio vaccine may meet the need for expansion of the target
age group of vaccination in routine public health services and will be available to the
National Immunization Program as a strategy to ensure sustainability and self-sufficiency to
vaccination policy.
OBJECTIVES PRIMARY: To assess the immunogenicity of MenCC Bio-vaccine in patients from 3
months to 19 years of age, in relation to the vaccine against meningococcus C currently
provided by the National Immunization Program. To evaluate the safety and reactogenicity of
MenCC Bio-vaccine in patients from 3 months to 19 years old.
SECONDARY OBJECTIVES: Evaluate the cellular immune component to meningococcal C conjugate
vaccine in a subset of survey participants, aged 11 to 19 years.
STUDY POPULATION: Individuals of both sexes, healthy, aged between 3 months and 19 years,
attending the campus of Fiocruz / Rio de Janeiro, or municipal health units in Rio de Janeiro
(living in areas covered by the municipal units health participants) that fit in the study
eligibility criteria.
NUMBER OF CENTRES: Two Clinical sites.
STUDY DURATION: Estimate of 19 months.
INTERVENTION / TREATMENT: Two intervention groups (MenCC-BIO Vaccine and Comparator) in three
age groups, with specific vaccination schedules. For the age groups I and II are applied 2
doses ideal interval of 6 months between them. In stratum III, are recommended 3 doses of the
vaccine, at ages 3, 5 and 12 months of age, according to calendar of the National
Immunization Program.
OUTCOMES PRIMARY:
Immunogenicity:
Proportion of seroconversion defined by the seronegative status change (titles of
bactericidal antibodies in children rabbit complement than 1: 8) to seropositive (titers of
bactericidal antibodies in larger rabbit complement or equal to 1: 8) or increase 4 times of
post vaccinal compared to pre-vacianais after the full vaccination schedule by age stratum.
Geometric mean antibody titers (TGM) pre- and post-vaccination, for each vaccine group, and
the ratio of these securities after the full vaccination schedule by age stratum.
Safety and reactogenicity: Frequency and intensity of adverse events solicited and
unsolicited, which occurred 30 days after vaccination.
SECONDARY OUTCOME : cell detection B (CD19 +) memory phenotype (CD27 + IgD +, CD27 + IgD) in
a subgroup of patients in the age stratum I (11-19 years old). ADDITIONAL INFORMATION age
escalation, with interim analysis of inter-layer security and approval by the Security
Independent Monitoring Committee of progression to the next lower age stratum.
| Status | Recruiting |
| Enrollment | 1644 |
| Est. completion date | April 2020 |
| Est. primary completion date | May 2019 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 3 Months to 19 Years |
| Eligibility |
Inclusion Criteria: - Be current on the national calendar own vaccination for the age group (except for meningitis C vaccine - see exclusion criteria). - Available for monitoring throughout the study period. - Willing to provide name, address, telephone number and other information so that we can contact the person if necessary (eg in case of missing the scheduled visit). - Willing to strictly follow the study protocol. - Legal Responsible and research participants with the ability to understand and sign the free and informed consent and the informed free consent term, according to the particularities of the age groups. - Understand the impossibility to participate in another clinical trial during the time you are participating in the study. - intellectual level or that of his legal guardian (if applicable according to age research participant) for the filling in the forms for registration of signs and symptoms at home. Exclusion Criteria: - Previous vaccination against meningococcus - Personal history of meningitis of any kind. - Personal history of anaphylaxis, asthma, urticaria or other hypersensitivity reaction to previous vaccinations or who have allergies or hypersensitivity to the study vaccine components. - Use of allergy shots with antigens within 14 days or less prior to vaccination. - Immunoglobulin Use in the last 12 months prior to vaccination. - Use of blood products in the 12 months prior to vaccination. - Use of any type of vaccine within 30 days before study vaccination. - The use of injectable vaccines least 30 days after the vaccination study. - Chronic use of any medication, except homeopathic medicines, medication trivial as saline nasal use and vitamins, and birth control. - Prior use of immunosuppressant or cytotoxic medication. individuals are acceptable to have made use of this type of medication not immunosuppressant doses for over 6 months as nasal steroids for allergic rhinitis or topical steroids for uncomplicated dermatitis. - In use of systemic treatment with high doses of steroids (for example, 1 mg / kg / day of prednisone for at least 14 days, or equivalent) or history of chronic use of high power inhaled corticosteroids (e.g., 800 ug per fluticasone day). - Use of any type of medication in clinical trials over a period of one year prior to vaccination. - Personal history of neurological, cardiovascular, respiratory, hepatic, renal, hematologic, rheumatic or autoimmune clinically significant (diseases that have led to hospitalization or prolonged treatment). - Personal history of bleeding disorders diagnosed by a physician or account of capillary fragility (eg. Bruising or bleeding without justifiable cause). - Personal history of seizures. - personal history of psychiatric disease that hinders adherence to protocol, such as psychosis, obsessive-compulsive neuroses, bipolar disorder being treated, diseases that require treatment with lithium and suicidal ideas in the past 5 years prior to enrollment. - Personal history of active malignant disease (eg any type of cancer) or treated you can use during the study. - Personal history of sickle cell anemia. - Asplenia (absence of spleen or removal thereof). - HIV positive or history of any immunosuppressive disease. - Pregnancy or breastfeeding. Additional criteria for female participants of childbearing age: negative pregnancy test prior to application of doses of vaccines. - The presence of any disorder that, in the opinion of the principal investigator, may interfere with the evaluation of the study objectives. - Inability to collect blood for evaluation of pre-vaccine based (baseline). |
| Country | Name | City | State |
|---|---|---|---|
| Brazil | • Unidade de Ensaios Clínicos para Imunobiológicos/Instituto de Tecnologia em Imunobiológicos de Bio-Manguinhos/Fiocruz | Rio de Janeiro |
| Lead Sponsor | Collaborator |
|---|---|
| The Immunobiological Technology Institute (Bio-Manguinhos) / Oswaldo Cruz Foundation (Fiocruz) |
Brazil,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Measure seroconversion proportion | Immediately before administration of the booster dose | ||
| Primary | Measure geometric mean antibody titers (TGM) | Immediately before administration of the booster dose | ||
| Primary | Measure frequency and intensity of adverse events solicited and unsolicited | 30 days after vaccination | ||
| Primary | Measure seroconversion proportion | 30 days after administration of the booster dose | ||
| Primary | Measure the ratio of antibody titers | 30 days after administration of the booster dose | ||
| Primary | Measure the ratio antibody titers | Immediately before administration of the booster dose | ||
| Primary | Measure geometric mean antibody titers (TGM) | 30 days after administration of the booster dose |
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Active, not recruiting |
NCT04061382 -
Sero-epidemiological Survey of England in 2019/2020 - COVID-19
|