Respiratory Tract Infections Clinical Trial
Official title:
A Phase 1, Randomized, Observer-Blind, Multi-Center, Dose Ranging Study to Evaluate the Immunogenicity, Safety and Tolerability of Different Formulations of an Adjuvanted or Non-Adjuvanted Cell Culture-derived A/H2N3 Subunit Influenza Virus Vaccine in Healthy Subjects 18 Years and Above
This Phase 1, randomized, observer-blind, dose-ranging clinical study is evaluating 6 different formulations of MF59-adjuvanted and non-adjuvanted H2N3 influenza vaccine. Approximately 600 healthy adult subjects are to be randomized into 1 of 6 possible treatment groups with 100 subjects per group, stratified by age group (born after or before 1968). Each subject will receive an influenza vaccine injection on Day 1 and Day 22. Subjects will be followed up for approximately 12 months after the second vaccine injection. The primary immunogenicity analysis is based on the Day 1, Day 8, Day 22, Day 29, and Day 43 serology data. The primary safety analysis is based on solicited local and systemic adverse events (AEs) reported within 10 days after each vaccination, unsolicited AEs reported within 3 weeks after each vaccination, and serious AEs (SAEs), medically attended AEs (MAAEs), AEs leading to withdrawal from the study, and AEs of special interest (AESIs) reported throughout the study.
Status | Recruiting |
Enrollment | 600 |
Est. completion date | November 2024 |
Est. primary completion date | November 2024 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: - Individuals of 18 years of age and older on the day of informed consent who were not born in 1968. - Individuals who have voluntarily given written informed consent after the nature of the study has been explained according to local regulatory requirements, prior to study entry. - Individuals who can comply with study procedures including follow-up. - Males, females of non-childbearing potential or females of childbearing potential who are using an effective birth control method, at least 30 days prior to informed consent, which they intend to use for at least 2 months after the last study vaccination. Exclusion Criteria: - Females of childbearing potential who are pregnant, lactating, or who have not adhered to a specified set of contraceptive methods from at least 30 days prior to study entry and who do not plan to do so until 2 months after the last study vaccination. - A body mass index (BMI) =35 kg/m2. - Progressive, unstable, or uncontrolled clinical conditions as per investigator's assessment. Subjects must be stable and unchanged for a minimum of 3 months. - Hypersensitivity, including allergy, to any component of vaccines, medicinal products or medical equipment whose use is foreseen in this study. - Clinical conditions representing a contraindication to intramuscular vaccination and blood draws. - Abnormal function of the immune system resulting from: 1. Clinical conditions. 2. Systemic administration of corticosteroids at a dose of =20 mg/day of prednisone or equivalent for more than 14 consecutive days within 90 days prior to informed consent. Topical, inhaled and intranasal corticosteroids are permitted. Intermittent use (one dose in 30 days) of intra-articular corticosteroids are also permitted. 3. Administration of antineoplastic and immunomodulating agents or radiotherapy within 90 days prior to informed consent. - History of any medical condition considered an adverse event of special interest (AESI). - Received immunoglobulins with immunomodulating effects or any blood products within 180 days prior to informed consent. - Received an investigational or non-registered medicinal product within 30 days prior to informed consent. - Study personnel or immediate family or household member of study personnel. - Any other clinical condition that, in the opinion of the investigator, might interfere with the results of the study or pose additional risk to the subject due to participation in the study. - Individuals who received any other vaccines (with the exception of COVID-19 vaccines) within 14 days (for inactivated vaccines) or 28 days (for live vaccines) prior to enrolment in this study or who are planning to receive any vaccine within 28 days from the study vaccines. - Receipt of any (investigational or licensed) COVID-19 vaccine within 14 days (non-replicating vaccines) or 28 days (replicating vaccines) prior to enrollment or plan to receive any COVID-19 vaccine within 14 days from study vaccination. - A known history of Guillain-Barre Syndrome or other demyelinating diseases such as encephalomyelitis and transverse myelitis. |
Country | Name | City | State |
---|---|---|---|
Philippines | De La Salle Medical and Health Sciences Institute | Dasmariñas | Cavite |
Philippines | West Visayas State University Medical Center | Iloilo City | |
Philippines | Manila Doctors Hospital | Manila | |
Philippines | Quirino Memorial Medical Center | Quezon City | |
Philippines | Silang Specialists Medical Center | Silang | |
United States | Meridian Clinical Research | Lincoln | Nebraska |
United States | Meridian Clinical Research | Omaha | Nebraska |
United States | Meridian Clinical Research | Rockville | Maryland |
Lead Sponsor | Collaborator |
---|---|
Seqirus | Department of Health and Human Services |
United States, Philippines,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Geometric mean titer (GMT) of hemagglutination inhibition (HI) antibodies against homologous H2N3 strain - Day 1 | GMT (HI) prevaccination | Day 1 | |
Primary | GMT of HI antibodies against homologous H2N3 strain - Day 8 | GMT (HI) 1 week postvaccination 1 | Day 8 | |
Primary | GMT of HI antibodies against homologous H2N3 strain Day 22 | GMT (HI) 3 weeks postvaccination 1 | Day 22 | |
Primary | GMT of HI antibodies against homologous H2N3 strain - Day 29 | GMT (HI) 1 week postvaccination 2 | Day 29 | |
Primary | GMT of HI antibodies against homologous H2N3 strain - Day 43 | GMT (HI) 3 weeks postvaccination 2 | Day 43 | |
Primary | GMT of microneutralization (MN) antibodies against homologous H2N3 strain - Day 1 | GMT (MN) prevaccination | Day 1 | |
Primary | GMT of MN antibodies against homologous H2N3 strain - Day 8 | GMT (MN) 1 week postvaccination 1 | Day 8 | |
Primary | GMT of MN antibodies against homologous H2N3 strain - Day 22 | GMT (MN) 3 weeks postvaccination 1 | Day 22 | |
Primary | GMT of MN antibodies against homologous H2N3 strain - Day 29 | GMT (MN) 1 week postvaccination 2 | Day 29 | |
Primary | GMT of MN antibodies against homologous H2N3 strain - Day 43 | GMT (MN) 3 weeks postvaccination 2 | Day 43 | |
Primary | Geometric mean fold increase (GMFI) of HI antibodies against homologous H2N3 strain - Day 8 | GMFI (HI) 1 week postvaccination 1 compared to prevaccination | Day 8 | |
Primary | GMFI of HI antibodies against homologous H2N3 strain - Day 22 | GMFI (HI) 3 weeks postvaccination 1 compared to prevaccination | Day 22 | |
Primary | GMFI of HI antibodies against homologous H2N3 strain - Day 29 | GMFI (HI) 1 week postvaccination 2 compared to prevaccination | Day 29 | |
Primary | GMFI of HI antibodies against homologous H2N3 strain - Day 43 | GMFI (HI) 3 weeks postvaccination 2 compared to prevaccination | Day 43 | |
Primary | GMFI of MN antibodies against homologous H2N3 strain - Day 8 | GMFI (MN) 1 week postvaccination 1 compared to prevaccination | Day 8 | |
Primary | GMFI of MN antibodies against homologous H2N3 strain - Day 22 | GMFI (MN) 3 weeks postvaccination 1 compared to prevaccination | Day 22 | |
Primary | GMFI of MN antibodies against homologous H2N3 strain - Day 29 | GMFI (MN) 1 week postvaccination 2 compared to prevaccination | Day 29 | |
Primary | GMFI of MN antibodies against homologous H2N3 strain - Day 43 | GMFI (MN) 3 weeks postvaccination 2 compared to prevaccination | Day 43 | |
Primary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Day 1 | % =1:40 (HI) prevaccination | Day 1 | |
Primary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Day 8 | % =1:40 (HI) 1 week postvaccination 1 | Day 8 | |
Primary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Day 22 | % =1:40 (HI) 3 weeks postvaccination 1 | Day 22 | |
Primary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Day 29 | % =1:40 (HI) 1 week postvaccination 2 | Day 29 | |
Primary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Day 43 | % =1:40 (HI) 3 weeks postvaccination 2 | Day 43 | |
Primary | Percentages of subjects with MN titers =1:40 against homologous H2N3 strain - Day 1 | % =1:40 (MN) prevaccination | Day 1 | |
Primary | Percentages of subjects with MN titers =1:40 against homologous H2N3 strain - Day 8 | % =1:40 (MN) 1 week postvaccination 1 | Day 8 | |
Primary | Percentages of subjects with MN titers =1:40 against homologous H2N3 strain - Day 22 | % =1:40 (MN) 3 weeks postvaccination 1 | Day 22 | |
Primary | Percentages of subjects with MN titers =1:40 against homologous H2N3 strain - Day 29 | % =1:40 (MN) 1 week postvaccination 2 | Day 29 | |
Primary | Percentages of subjects with MN titers =1:40 against homologous H2N3 strain - Day 43 | % =1:40 (MN) 3 weeks postvaccination 2 | Day 43 | |
Primary | Percentages of subjects with seroconversion by HI against homologous H2N3 strain - Day 8 | % seroconversion (HI) 1 week postvaccination 1, defined as a =4-fold increase in HI titer postvaccination in those with prevaccination titer =1:10, or a postvaccination HI titer =1:40 for subjects with baseline titer <1:10 | Day 8 | |
Primary | Percentages of subjects with seroconversion by HI against homologous H2N3 strain - Day 22 | % seroconversion (HI) 3 weeks postvaccination 1, defined as a =4-fold increase in HI titer postvaccination in those with prevaccination titer =1:10, or a postvaccination HI titer =1:40 for subjects with baseline titer <1:10 | Day 22 | |
Primary | Percentages of subjects with seroconversion by HI against homologous H2N3 strain - Day 29 | % seroconversion (HI) 1 week postvaccination 2, defined as a =4-fold increase in HI titer postvaccination in those with prevaccination titer =1:10, or a postvaccination HI titer =1:40 for subjects with baseline titer <1:10 | Day 29 | |
Primary | Percentages of subjects with seroconversion by HI against homologous H2N3 strain - Day 43 | % seroconversion (HI) 3 weeks postvaccination 2, defined as a =4-fold increase in HI titer postvaccination in those with prevaccination titer =1:10, or a postvaccination HI titer =1:40 for subjects with baseline titer <1:10 | Day 43 | |
Primary | Percentages of subjects with seroconversion by MN against homologous H2N3 strain - Day 8 | % seroconversion (MN) 1 week postvaccination 1, defined as a =4-fold increase in MN titer postvaccination in those with prevaccination titer =lower limit of quantification (LLOQ), or a postvaccination MN titer =4×LLOQ for subjects with baseline titer Day 8 |
| |
Primary | Percentages of subjects with seroconversion by MN against homologous H2N3 strain - Day 22 | % seroconversion (MN) 3 weeks postvaccination 1, defined as a =4-fold increase in MN titer postvaccination in those with prevaccination titer =lower limit of quantification (LLOQ), or a postvaccination MN titer =4×LLOQ for subjects with baseline titer Day 22 |
| |
Primary | Percentages of subjects with seroconversion by MN against homologous H2N3 strain - Day 29 | % seroconversion (MN) 1 week postvaccination 2, defined as a =4-fold increase in MN titer postvaccination in those with prevaccination titer =lower limit of quantification (LLOQ), or a postvaccination MN titer =4×LLOQ for subjects with baseline titer Day 29 |
| |
Primary | Percentages of subjects with seroconversion by MN against homologous H2N3 strain - Day 43 | % seroconversion (MN) 3 weeks postvaccination 2, defined as a =4-fold increase in MN titer postvaccination in those with prevaccination titer =lower limit of quantification (LLOQ), or a postvaccination MN titer =4×LLOQ for subjects with baseline titer Day 43 |
| |
Primary | Number and percentages of subjects reporting solicited local and systemic adverse events (AEs) - Day 1 through Day 10 | 10 consecutive days postvaccination 1 | Day 1 through Day 10 | |
Primary | Number and percentages of subjects reporting solicited local and systemic AEs - Day 22 through Day 31 | 10 consecutive days postvaccination 2 | Day 22 through Day 31 | |
Primary | Number and percentage of subjects reporting any unsolicited AEs | For 3 weeks following each vaccination | Day 1 through Day 43 | |
Primary | Number and percentage of subjects reporting serious AEs (SAEs), AEs leading to withdrawal, AEs of special interest (AESI) and medically attended AEs (MAAEs) | From vaccination until study completion | Day 1 through Day 387 | |
Secondary | GMT of ELLA titers as a measure of anti-neuraminidase (NA) immunogenicity | GMT (ELLA) prevaccination, 1 and 3 weeks postvaccination | Day 1, Day 8, Day 22, Day 29, Day 43 | |
Secondary | GMFI of ELLA titers as a measure of anti-NA immunogenicity | GMFI (ELLA) 1 and 3 weeks postvaccination compared to prevaccination | Day 8, Day 22, Day 29, Day 43 | |
Secondary | Percentage of subjects with =4-fold increase in ELLA titer as a measure of anti-NA immunogenicity | % =4-fold increase (ELLA) 1 and 3 weeks postvaccination compared to prevaccination | Day 8, Day 22, Day 29, Day 43 | |
Secondary | GMT of HI antibodies against homologous H2N3 strain - Persistence | GMT (HI) 6 and 12 months postvaccination 2 | Day 202, Day 387 | |
Secondary | GMT of MN antibodies against homologous H2N3 strain - Persistence | GMT (MN) 6 and 12 months postvaccination 2 | Day 202, Day 387 | |
Secondary | GMT of ELLA titer as a measure of anti-NA immunogenicity- Persistence | GMT (ELLA) 6 and 12 months postvaccination 2 | Day 202, Day 387 | |
Secondary | GMFI of HI antibodies against homologous H2N3 strain - Persistence | GMFI (HI) 6 and 12 months postvaccination 2 compared to prevaccination | Day 202, Day 387 | |
Secondary | GMFI of MN antibodies against homologous H2N3 strain - Persistence | GMFI (MN) 6 and 12 months postvaccination 2 compared to prevaccination | Day 202, Day 387 | |
Secondary | GMFI of ELLA titer as a measure of anti-NA immunogenicity- Persistence | GMFI (ELLA) 6 and 12 months postvaccination 2 compared to prevaccination | Day 202, Day 387 | |
Secondary | Percentages of subjects with HI titers =1:40 against homologous H2N3 strain - Persistence | % =1:40 (HI) 6 and 12 months postvaccination 2 | Day 202, Day 387 | |
Secondary | Percentages of subjects with MN titers =1:40, =1:80 and =1:160 against homologous H2N3 strain - Persistence | % =1:40, =1:80 and =1:160 (MN) 6 and 12 months postvaccination 2 | Day 202, Day 387 | |
Secondary | Percentages of subjects with seroconversion by HI against homologous H2N3 strain - Persistence | % seroconversion (HI) 6 and 12 months postvaccination 2, defined as a =4-fold increase in HI titer postvaccination in those with prevaccination titer =1:10, or a postvaccination HI titer =1:40 for subjects with baseline titer <1:10 | Day 202, Day 387 | |
Secondary | Percentages of subjects with seroconversion by MN against homologous H2N3 strain - Persistence | % seroconversion (MN) 6 and 12 months postvaccination 2, defined as a =4-fold increase in MN titer postvaccination in those with prevaccination titer =LLOQ, or a postvaccination MN titer =4×LLOQ for subjects with baseline titer Day 202, Day 387 |
| |
Secondary | Percentage of subjects with =4-fold increase in ELLA titer as a measure of anti-NA immunogenicity - Persistence | % =4-fold increase (ELLA) 6 and 12 months postvaccination 2 compared to prevaccination | Day 202, Day 387 |
Status | Clinical Trial | Phase | |
---|---|---|---|
Completed |
NCT05525494 -
Patient Portal Flu Vaccine Reminders (5)
|
N/A | |
Completed |
NCT04537663 -
Prevention Of Respiratory Tract Infection And Covid-19 Through BCG Vaccination In Vulnerable Older Adults
|
Phase 4 | |
Terminated |
NCT04583280 -
A Study of Rilematovir in Infants and Children and Subsequently in Neonates Hospitalized With Acute Respiratory Tract Infection Due to Respiratory Syncytial Virus (RSV)
|
Phase 3 | |
Completed |
NCT03321968 -
Lot-to-lot Consistency of a Plant-Derived Quadrivalent Virus-Like Particles Influenza Vaccine in Healthy Adults
|
Phase 3 | |
Active, not recruiting |
NCT03251196 -
TB Sequel: Pathogenesis and Risk Factors of Long-term Sequelae of Pulmonary TB
|
||
Completed |
NCT02561871 -
A Study to Evaluate the Safety, Tolerability and Immunogenicity of Ad26.RSV.FA2 Followed by Ad35.RSV.FA2 in Healthy Adult Volunteers
|
Phase 1 | |
Terminated |
NCT02032056 -
Effect of Probiotics in Reducing Infections and Allergies in Young Children During the Complementary Feeding Period
|
N/A | |
Completed |
NCT01911143 -
A Retrospective, Blinded Validation of a Host-response Based Diagnostics
|
N/A | |
Completed |
NCT01419262 -
DO IT Trial: Vitamin D Outcomes and Interventions In Toddlers
|
Phase 3 | |
Terminated |
NCT01432080 -
Steroids, Azithromycin, Montelukast, and Symbicort (SAMS) for Viral Respiratory Tract Infection Post Allotransplant
|
Phase 2 | |
Completed |
NCT00984945 -
Safety Study of a Plant-based H5 Virus-Like Particles (VLP) Vaccine in Healthy Adults
|
Phase 1 | |
Completed |
NCT00127686 -
Effect of Honey and Dextromethorphan on Nocturnal Cough and Sleep
|
Phase 1 | |
Active, not recruiting |
NCT01107223 -
Long Term Effect of General Practitioner Education on Antibiotic Prescribing
|
N/A | |
Completed |
NCT03739112 -
Efficacy of a Plant-derived Quadrivalent Virus-like Particle (VLP) Vaccine in the Elderly
|
Phase 3 | |
Completed |
NCT04144491 -
Effect of L. Rhamnosus Yoba on RTI and Other Health Outcomes Among Children (3-6 Years) in Uganda
|
N/A | |
Completed |
NCT05318235 -
Virus Interactions in the Respiratory Tract; a Cohort Study With Children
|
||
Active, not recruiting |
NCT04170348 -
Daily Vitamin D for Sickle-cell Respiratory Complications
|
Phase 2 | |
Completed |
NCT04525040 -
ProbioKid as Prevention Among Kids With Frequent URTI
|
N/A | |
Completed |
NCT05535777 -
Patient Portal Flu Vaccine Reminders_RCT 5 (LADHS)
|
N/A | |
Not yet recruiting |
NCT05914324 -
Outpatient Pediatric Pulse Oximeters in Africa
|
N/A |