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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02035696
Other study ID # V58P16
Secondary ID 2013-002081-39
Status Completed
Phase Phase 1/Phase 2
First received
Last updated
Start date December 2013
Est. completion date December 2014

Study information

Verified date June 2018
Source Seqirus
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

To evaluate the safety and immunogenicity of four influenza vaccines in children 6 months to < 48 months of age


Recruitment information / eligibility

Status Completed
Enrollment 671
Est. completion date December 2014
Est. primary completion date June 2014
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 6 Months to 48 Months
Eligibility Inclusion Criteria:

- Healthy subject, male or female, 6 through < 48 months of age at the time of enrollment, who has never previously received an influenza vaccine

- Individual who has a parent or guardian that can give written informed consent after understanding the nature of the study and are available for follow-up

Exclusion Criteria:

- Individuals recently vaccinated against influenza

- Subjects with contraindications to receive influenza vaccine

Study Design


Related Conditions & MeSH terms


Intervention

Biological:
Trivalent influenza vaccine (TIVc)

Trivalent influenza vaccine-licensed
Licensed influenza vaccine

Locations

Country Name City State
Finland Site 502 Kuopio
Finland Site 506 Tampere
Philippines Site 301 Manila
Philippines Site 302 Muntinlupa
Thailand Site 201 Bangkok
Thailand Site 202 Bangkok
United States Site 102 Charleston South Carolina
United States Site 121 Gainesville Georgia
United States Site 115 Houston Texas
United States Site 109 Little Rock Arkansas
United States Site 112 Long Beach California
United States Site 111 Miami Florida
United States Site 108 Miami Beach Florida
United States Site 101 Omaha Nebraska
United States Site 104 Omaha Nebraska
United States Site 105 Omaha Nebraska
United States Site 106 Omaha Nebraska
United States Site 113 Ontario California
United States Site 116 Phoenix Arizona
United States Site 118 Saint George Utah
United States Site 110 Salt Lake City Utah
United States Site 117 San Diego California
United States Site 120 Spokane Washington
United States Site 107 Thornton Colorado
United States Site 119 Tucson Arizona
United States Site 114 West Covina California
United States Site 103 Youngstown Ohio

Sponsors (2)

Lead Sponsor Collaborator
Seqirus Novartis Vaccines

Countries where clinical trial is conducted

United States,  Finland,  Philippines,  Thailand, 

Outcome

Type Measure Description Time frame Safety issue
Primary Ratios of Geometric Mean Titer (GMT) in Subjects (6 to <48 Months Old) After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of ratios of GMTs in subjects (6 to <48 months old), measured by hemagglutination inhibition (HI) assay, day 1 to day 50 after vaccination with two doses of either TIVc or TIVe vaccine Day 50/Day 1
Primary Percentages of Subjects (6 to <48 Months Old) Achieving Seroconversion or Significant Increase After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms number (%) of subjects (6 to <48 months old) achieving seroconversion as measured by HI antibody titer, day 50 after vaccination with two doses of either TIVc or TIVe vaccine Seroconversion was defined as subjects with either a pre-vaccination (baseline) HI titer < 1:10 and post-vaccination HI titer = 1:40 or with a pre-vaccination HI titer = 1:10 and a = 4-fold increase in post-vaccination HI antibody titer Day 50 post vaccination
Primary Desirability Index Score of Subjects (6 to <48 Months Old) Reporting Severe Solicited Local and Systemic Reactions After Vaccination With Either TIVc or TIVe Vaccine Differences in percentages of subjects (6 to <48 months old) with severe local solicited AEs and severe solicited systemic AEs, 3 days after vaccination with either TIVc or TIVe vaccine was assessed in terms of an individual desirability index score (High dose, Full dose, Half dose TIVc vs. TIVe vaccine). An individual desirability index score was assigned to each (non-transformed) safety value based on predefined functions. Each desirability index score is assigned a value between 0 and 1, wherein 0 is an undesirable response and 1 is a highly desirable response. Day 1 to Day 3
Secondary Percentages of Subjects (6 to <48 Months Old) Achieving Seroconversion or Significant Increase After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of number (%) of subjects (6 to <48 months old) achieving seroconversion as measured by HI assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine
Seroconversion was defined as subjects with either a pre-vaccination (baseline) HI titer < 1:10 and post-vaccination HI titer = 1:40 or with a pre-vaccination HI titer = 1:10 and a = 4-fold increase in post-vaccination HI antibody titer
The Center for Biologics Evaluation, Research, and Review (CBER) criterion for pediatric population is that the lower bound of the two-sided 95% confidence interval (CI) for the percentage of subjects achieving seroconversion for HI antibody should meet or exceed 40%
The Committee for Medicinal Products for Human Use (CHMP) criterion for pediatric population is that the percentage of subjects achieving seroconversion or significant increase in HI antibody titers >40%
Day 50 post vaccination
Secondary Percentages of Subjects (6 to <48 Months Old) Achieving HI Titer =1:40 After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of number (%) of subjects (6 to <48 months old) achieving HI titer =1:40 as measured by HI assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine
The CBER criterion for pediatric population is that the lower bound of the two-sided 95% CI for the percentage of subjects achieving an HI antibody titer =1:40 should meet or exceed 70%
The CHMP criterion for pediatric population is that the percentage of subjects achieving HI antibody titers =1:40 should be >70%
Day 1, Day 50 post vaccination
Secondary Geometric Mean Ratios (GMR) in Subjects (6 to <48 Months Old) After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of GMR in subjects (6 to <48 months old) as measured by HI assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine
The CHMP criterion is mean geometric ratio (GMR) >2.5
Day 50 post vaccination over day 1
Secondary Geometric Mean Ratios (GMR) in Subjects (6 to <48 Months Old) After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of GMR in subjects (6 to <48 months old) as measured by MN assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine Day 50 post vaccination over day 1
Secondary Percentages of Subjects (6 to <48 Months Old) With High Post Vaccination HI Titers (i.e. HI Titers =1:110, =1:150, =1:330 and =1:629) After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of number (%) of subjects (6 to <48 months old) achieving post vaccination HI titers (i.e. HI titers =1:110, =1:150, =1:330 and =1:629) as measured by HI assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine Day 1 and Day 50 post vaccination
Secondary Percentages of Subjects (6 to <48 Months Old) Achieving MN Titer =1:20 After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of number (%) of subjects (6 to <48 months old) achieving MN titer =1:20 as measured by MN assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine
Post-vaccination MN titer =1:20 was defined as for subjects with baseline (day 1) MN titer <1:10, or a minimum 2-fold increase in titer on day 50 for subjects with baseline titer =1:10 and corresponding 95% CI
Day 1 and Day 50 post vaccination
Secondary Percentages of Subjects (6 to <48 Months Old) Achieving MN Titer =1:40 After Receiving Two Doses of Either TIVc or TIVe Vaccine Immunogenicity was assessed in terms of number (%) of subjects (6 to <48 months old) achieving MN titer =1:40 as measured by MN assay, day 50 after vaccination with two doses of either TIVc or TIVe vaccine
Post-vaccination MN titer =1:40 was defined as for subjects with baseline (day 1) MN titer <1:10, or a minimum 4-fold increase in titer on day 50 for subjects with baseline titer =1:10 and corresponding 95% CI
Day 1 and Day 50 post vaccination
Secondary Number of Subjects (6 to <48 Months Old) Reporting Solicited Local (Grading Type I) and Systemic Adverse Events (AEs) After Two Doses of Either TIVc or TIVe Vaccine Safety was assessed in terms of number of subjects (6 to <48 months old) reporting solicited local and systemic reactions, day 1 to day 7 after vaccination with two doses of either TIVc or TIVe vaccine (By Any Vaccination) Day 1 to Day 7
Secondary Number of Subjects (6 to <48 Months Old) Reporting Unsolicited Adverse Events (AEs) After Two Doses of Either TIVc or TIVe Vaccine Safety was assessed in terms of number of subjects (6 to <48 months old) reporting unsolicited reactions after Each /any Vaccination from Day 1 [Post Vaccination] to Day 29 [Pre Clinic Visit] and Day 29 [Post Vaccination] to Day 50 [Pre Clinic Visit] , Serious Adverse Events (SAEs), AEs leading to New Onset of Chronic Diseases (NOCD), AEs leading to withdrawal from the study and concomitant medications (day 1 to day 209) after vaccination with two doses of either TIVc or TIVe vaccine (By Any Vaccination) Unsolicited AEs after Each/any Vaccination from Day 1 to Day 29 and Day 29 to Day 50 , Day 1 to Day 209
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