Influenza, Human Clinical Trial
Official title:
A Phase 3, Randomized, Observer-Blind, Controlled, Multicenter, Clinical Study to Evaluate Immunogenicity and Safety of a MF59-Adjuvanted Quadrivalent Subunit Cell-derived Influenza Vaccine (aQIVc) in Comparison With Quadrivalent Influenza Vaccines, in Adults Aged 50 Years and Older.
Verified date | March 2024 |
Source | Seqirus |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
This is a Phase 3, randomized, parallel-group, comparator-controlled, observer-blind, multicenter study of immunogenicity and safety in approximately 7700 male and female adults aged 50 years and older (approximately equally split between two age groups: 50-64 years; 65 years and older), who are healthy or have stable comorbidities that increase their risk of complications from influenza infection. Three lots of aQIVc will be evaluated for consistency and pooled for the comparison with the 2 control vaccines. Subjects will be randomly assigned to receive 1 of 3 lots of aQIVc, QIV1, or QIV2 in a 1:1:1:2:2 ratio (for a 3:2:2 ratio for aQIVc, QIV1, and QIV2). The study will have a treatment period (Day 1 to Day 29) and a follow-up period (Day 30 up to Day 181); a subset of 770 subjects will be followed up up to Day 365.
Status | Active, not recruiting |
Enrollment | 7741 |
Est. completion date | January 30, 2025 |
Est. primary completion date | March 5, 2024 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 50 Years and older |
Eligibility | Main Inclusion Criteria: - Individuals, aged 50 years and older, who are healthy or have stable comorbidities that increase their risk of complications from influenza infection - Individuals who can comply with all study procedures Main Exclusion Criteria: - Progressive, unstable, or uncontrolled clinical conditions - Known hypersensitivity or allergy to any study vaccine component - Known history of Guillain-Barré syndrome or other demyelinating disease - Condition representing a contraindication to vaccination or blood draw - Abnormal function of immune system due to known disorder or medication. - Influenza vaccination within 180 days prior to informed consent. |
Country | Name | City | State |
---|---|---|---|
Canada | CARe Clinic | Red Deer | Alberta |
Denmark | Amager-Hvidovre Hospital | Hvidovre | |
Denmark | Zealand University Hospital, Roskilde | Roskilde | |
Estonia | Vee Family Doctor's Center OY | Paide | |
Estonia | Merelahe Family Doctors Centre | Tallin | |
Estonia | Al Mare Perearstikeskus OÜ | Tallinn | |
Estonia | Center for Clinical and Basic Research | Tallinn | |
Estonia | OÜ Innomedica | Tallinn | |
Estonia | Clinical Research Centre | Tartu | |
Estonia | Tartu University Hospital | Tartu | |
Germany | emovis GmbH | Berlin | |
Germany | Klinische Forschung Berlin | Berlin | |
Germany | Klinische Forschung Berlin-Mitte GmbH | Berlin | |
Germany | Klinische Forschung Dresden GmbH | Dresden | |
Germany | Klinisches Forschungszentrum Dr. Hagemann am Hausarztzentrum am Germaniaplatz Dr.Hagemann/ Breider | Essen | |
Germany | Studienzentrum Bocholderstrasse | Essen | |
Germany | UHZ Klinische Forschung | Essen | |
Germany | Klinische Forschung Hamburg GmbH | Hamburg | |
Germany | Velocity Clinical Research, Hamburg | Hamburg | |
Germany | Klinische Forschung Hannover-Mitte GmbH | Hannover | |
Germany | Klinische Forschung Karlsruhe GmbH | Karlsruhe | |
Germany | Studienzentrum FMZ Radowsky | Leipzig | |
Germany | Velocity Clinical Research, Leipzig | Leipzig | |
Germany | Research Quist | Mainz | |
Germany | Klinische Forschung Schwerin GmbH | Schwerin | |
Germany | Studienzentrum Leitz Triderm | Stuttgart | |
Pakistan | The Aga Khan University | Karachi | |
Pakistan | Central Park Teaching Hospital | Lahore | |
Philippines | Marilao Saint Michael Family Hospital, Inc | Bulacan | |
Philippines | CARE CT Group Inc. | Cavite | |
Philippines | Health Index Multispecialty and Lying in Clinic | Cavite | |
Philippines | Norzel Medical and Diagnostic Clinic | Cebu City | |
Philippines | Davao Medical School Foundation Inc. Hospital / NEMESIO F. ANLOCOTAN III | Davao City | Davao Del Sur |
Philippines | West Visayas State University Medical Center | Iloilo City | |
Philippines | Las Pinas Doctors Hospital | Las Piñas | Las Pinas City |
Philippines | Ospital ng Makati | Makati City | |
Philippines | Manila Doctors Hospital | Manila | |
Philippines | Mary Johnston Hospital | Manila | |
Philippines | Quirino Memorial Medical Center | Quezon City | |
Philippines | Silang Specialists Medical Center | Silang | Cavite |
United Kingdom | Velocity High Wycombe | High Wycombe | |
United Kingdom | Velocity North London | London | |
United Kingdom | Panthera Biopartners Ltd (Preston) | Preston | |
United Kingdom | Panthera Biopartners Ltd (Manchester) | Rochdale | |
United Kingdom | Panthera Biopartners (Sheffield) | Sheffield | |
United States | Velocity Clinical Research | Baton Rouge | Louisiana |
United States | Velocity Clinical Research | Beachwood | Ohio |
United States | Velocity Clinical Research | Binghamton | New York |
United States | GLCT/Flourish Research | Chicago | Illinois |
United States | CTI Clinical Research Center | Cincinnati | Ohio |
United States | Velocity Clinical Research Cincinnati Blue Ash | Cincinnati | Ohio |
United States | Innovative Research of West Florida | Clearwater | Florida |
United States | Cedar Health Research | Dallas | Texas |
United States | USA and International Research Inc. | Doral | Florida |
United States | Velocity Clinical Research-Providence | East Greenwich | Rhode Island |
United States | Velocity Clinical Research, New Smyrna Beach | Edgewater | Florida |
United States | Centennial Medical Group | Elkridge | Maryland |
United States | Benchmark Research | Fort Worth | Texas |
United States | Velocity Clinical Research, Gaffney | Gaffney | South Carolina |
United States | Velocity Clinical Research | Gulfport | Mississippi |
United States | Great Lakes Clinical Trials, a Flourish Research Site | Gurnee | Illinois |
United States | DM Clinical Research | Houston | Texas |
United States | Marvel Clinical Research | Huntington Beach | California |
United States | Health Awareness, Inc. | Jupiter | Florida |
United States | Alliance for Multispecialty Research-Kansas City | Kansas City | Missouri |
United States | AMR-Knoxville | Knoxville | Tennessee |
United States | Accel Research Sites Network, STP | Largo | Florida |
United States | Alliance for Multispecialty Research LLC, Las Vegas | Las Vegas | Nevada |
United States | Baptist Health Center for Clinical Research | Little Rock | Arkansas |
United States | Velocity Clinical Research - Medford | Medford | Oregon |
United States | Velocity Clinical Research- Boise | Meridian | Idaho |
United States | Benchmark Research | Metairie | Louisiana |
United States | Global Health Research Center, Inc. | Miami Lakes | Florida |
United States | Clinical Research Consulting, LLC | Milford | Connecticut |
United States | JBR Clinical Research | Millcreek | Utah |
United States | IMA Clinical Research | Monroe | Louisiana |
United States | Clinical Research Associates, Inc. | Nashville | Tennessee |
United States | Velocity Clinical Research | New York | New York |
United States | Vestal, Velocity Clinical Research | New York | New York |
United States | Velocity Clinical Research | Norfolk | Nebraska |
United States | Velocity Clinical Research, Omaha | Omaha | Nebraska |
United States | ACRC trials/ Village Health Partners | Plano | Texas |
United States | Velocity Clinical Research | Portsmouth | Virginia |
United States | M3 Wake Research, Inc | Raleigh | North Carolina |
United States | Paradigm Clinical Research Center | Redding | California |
United States | Velocity Clinical Research | Rockville | Maryland |
United States | Sundance Clinical Research, LLC | Saint Louis | Missouri |
United States | Velocity Clinical Research, Sioux City | Sioux City | Iowa |
United States | Velocity Clinical Research, Spartanburg | Spartanburg | South Carolina |
United States | Precision Clinical Research | Sunrise | Florida |
United States | Global Health Research center, Inc. | Tampa | Florida |
United States | Alliance for Multispecialty Research (AMR) Phoenix | Tempe | Arizona |
United States | DM Clinical Research | Tomball | Texas |
United States | Velocity Clinical Research Valparaoso | Valparaiso | Indiana |
United States | Chase Medical Research, LLC | Waterbury | Connecticut |
United States | Velocity Clinical Research | West Jordan | Utah |
Lead Sponsor | Collaborator |
---|---|
Seqirus |
United States, Canada, Denmark, Estonia, Germany, Pakistan, Philippines, United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Immunogenicity Endpoint: Humoral immune responses of 3 lots of aQIVc compared in pairs in terms of Day 29 GMT ratio between each pair among the 3 lots, from antibody titers measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains. | Day 29 | |
Primary | Immunogenicity Endpoint: Humoral immune responses of aQIVc in comparison with QIV1 and QIV2 vaccines in terms of Day 29 GMT and GMT ratio of antibodies measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains.
Noninferiority of aQIVc versus comparator (QIV1 or QIV2) will be demonstrated if the lower limit (LL) of the 2-sided 97.5% CI for the Day 29 GMT ratio (aQIVc/comparator) is =0.67 for each of the 4 vaccine strains. |
Day 29 | |
Primary | Immunogenicity Endpoint: Humoral immune responses of aQIVc in comparison with QIV1 and QIV2 vaccines in terms of Day 1 to Day 29 SCR and SCR difference, from antibody titers measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains.
SCR is the percentage of subjects with seroconversion (defined as either a prevaccination [Day 1] titer <1:10 and a postvaccination [Day 29] titer =1:40, or a prevaccination titer =1:10 and a =4-fold increase in postvaccination titer). Noninferiority of aQIVc versus comparator (QIV1 or QIV2) will be demonstrated if the lower limit (LL) of the 2-sided 97.5% CI for the difference in SCR (aQIVc minus comparator) is =-10% for each of the 4 vaccine strains. |
Day 1 and Day 29 | |
Secondary | Immunogenicity Endpoint: Humoral immune responses of aQIVc in comparison with QIV1 vaccine in terms of Day 29 SCR and SCR difference, GMT and GMT ratio of antibodies measured via HI assay in subjects 65 years and older. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains.
Noninferiority will be demonstrated if the LL of the 2-sided adjusted CI for the Day 29 GMT ratio (aQIVc HD/comparator) is =0.67 for each of the 4 vaccine strains, and the LL of the 2-sided adjusted CI for the difference in SCR (aQIVc HD minus comparator) is =-10% for each of the 4 vaccine strains. |
Day 1 and Day 29 | |
Secondary | Immunogenicity Endpoint: Humoral immune responses of aQIVc in comparison with QIV1 and QIV2 vaccines in terms of Day 29 GMT and GMT ratio of antibodies measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains.
Superiority of aQIVc versus comparator (QIV1 and QIV2) will be demonstrated if the LL of the 2-sided 97.5% CI for the inter-group GMT ratio (aQIVc/comparator) is >1.0 for each of the 4 vaccine strains. |
Day 29 | |
Secondary | Immunogenicity Endpoints: For aQIVc, QIV1, and QIV2 vaccines, Day 29 GMT, Day 1 to Day 29 GMFI, Percentage of subjects with HI titer =1:40 at Day 29, Day 1 to Day 29 SCR, SCR differences and GMT ratio of antibodies measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains, overall and by age subgroup. | Day 1 and Day 29 | |
Secondary | Immunogenicity Endpoints: For aQIVc and QIV1 vaccines, Day 29 GMT, Day 1 to Day 29 GMFI, Percentage of subjects with HI titer =1:40 at Day 29, Day 1 to Day 29 SCR, SCR differences, and GMT ratio of antibodies measured via HI assay. | HI assay will be measured using egg-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains in the HI-egg subset of 2750 subjects, overall and by age subgroup. | Day 1 and Day 29 | |
Secondary | Immunogenicity Endpoints: For aQIVc, QIV1 and QIV2 vaccines, GMT, GMFI, Percentage of subjects with HI titer =1:40, SCR, SCR differences, and GMT ratio of antibodies measured via HI assay. | HI assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains in the long-term subset of 770 subjects, overall and by age subgroup. | Day 1 up to Day 365 | |
Secondary | Immunogenicity Endpoints: For aQIVc, QIV1 and QIV2 vaccines, GMT, GMFI, SCR, SCR difference, and GMT ratio of antibodies measured via MN assay. | MN assay will be measured using cell-derived target viruses for the A/H1N1, A/H3N2, B/Yamagata, and B/Victoria vaccine strains in the long-term subset of 770 subjects, overall and by age subgroup. | Day 1 up to Day 365 | |
Secondary | Safety endpoints: For aQIVc, QIV1 and QIV2 vaccines, the percentages of Subjects with Solicited Local Adverse Events, Solicited Systemic Adverse Events, and Severe Solicited Local and/or Systemic AEs. | Day 1 to Day 7 | ||
Secondary | Safety endpoints: For aQIVc, QIV1 and QIV2 vaccines, the percentage of Subjects with Unsolicited Adverse Events. | Day 1 to Day 29 | ||
Secondary | Safety endpoints: For aQIVc, QIV1 and QIV2 vaccines, the percentages of subjects with Serious Adverse Events (SAEs), AEs Leading to Withdrawal, Adverse Events of Special Interest (AESI) and non-serious Medically Attended Adverse Events (MAAEs). | Day 1 to Day 181 | ||
Secondary | Safety endpoints: For aQIVc, QIV1 and QIV2 vaccines, the percentages of subjects with Serious Adverse Events (SAEs), AEs Leading to Withdrawal, Adverse Events of Special Interest (AESI) and non-serious Medically Attended Adverse Events (MAAEs). | Long-term safety for the long-term subset of 770 subjects | Day 1 to Day 365 |
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