Influenza Clinical Trial
Official title:
Evaluation of The Safety and Immunogenicity of an Influenza A/H1N1 Vaccine (IVACFLU), Produced by IVAC, in Healthy Adults in Vietnam
Verified date | February 2019 |
Source | PATH |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The study hypothesis is that two 0.5 ml doses of non-adjuvanted whole virion monovalent A/H1N1 influenza vaccine (IVACFLU)-—each dose with an HA content of 15 mcg from A/California/07/2009 (H1N1)-like virus-—will be safe and immunogenic in healthy adults.
Status | Completed |
Enrollment | 48 |
Est. completion date | December 2012 |
Est. primary completion date | November 2012 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 49 Years |
Eligibility |
Inclusion Criteria: - Male or female adult 18 (age of legal consent in Vietnam) through 40 years of age at the enrollment visit. - Literate and willing to provide written informed consent. - Free of obvious health problems, as established by the medical history and screening evaluations, including physical examination. - Capable and willing to complete diary cards and willing to return for all follow-up visits - For females, willing to utilize reliable birth control measures (intrauterine device, birth control pills, condoms) through the Day 42 visit. Exclusion Criteria: - Participation in another clinical trial involving any therapy within the previous three months or planned enrollment in such a trial during the period of this study. - Receipt of any non-study vaccine within four weeks prior to enrollment or refusal to postpone receipt of such vaccines until after the Day 42 visit. - Current or recent (within two weeks of enrollment) acute illness with or without fever. - Receipt of immune globulin or other blood products within three months prior to study enrollment or planned receipt of such products prior to the Day 42 visit. - Chronic administration (defined as more than 14 consecutively-prescribed days) of immunosuppressants or other immune-modulating therapy within six months prior to study enrollment. (For corticosteroids, this means prednisone or equivalent, >=0.5 mg per kg per day; topical steroids are allowed.) - History of asthma. - Hypersensitivity after previous administration of any vaccine. - Other AE following immunization, at least possibly related to previous receipt of any vaccine. - Suspected or known hypersensitivity to any of the study vaccine components, including chicken or egg protein. - Known hypersensitivities (allergies) to food or the natural environment. - Acute or chronic clinically significant pulmonary, cardiovascular, hepatic, metabolic, neurologic, psychiatric or renal functional abnormality, as determined by medical history, physical examination or clinical laboratory screening tests, which in the opinion of the investigator, might interfere with the study objectives.. - History of leukemia or any other blood or solid organ cancer. - History of thrombocytopenic purpura or known bleeding disorder. - History of seizures. - Known or suspected immunosuppressed or immunodeficient condition of any kind, including HIV infection. - Known chronic HBV or HCV infection. - Known active tuberculosis or symptoms of active tuberculosis, regardless of cause. - History of chronic alcohol abuse and/or illegal drug use. - Pregnancy or lactation. (A negative pregnancy test will be required before administration of study vaccine or placebo for all women of childbearing potential.) - History of Guillain-Barre' Syndrome - Any condition that, in the opinion of the investigator, would increase the health risk to the subject if he/she participates in the study or would interfere with the evaluation of the study objectives. |
Country | Name | City | State |
---|---|---|---|
Vietnam | Ben Luc Health Center | Ben Luc | Long An |
Lead Sponsor | Collaborator |
---|---|
PATH | Institute of Vaccines and Medical Biologicals, Vietnam, Pasteur Institute, Ho Chi Minh City |
Vietnam,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Number of Participants With Maximum Systemic Reaction After Vaccination 1 | Systemic and local reactogenicity data were collected on Study Days 0, 7, 21 and 28, prevaccination, and within 60 minutes post-vaccination by clinic staff. Subjects completed diary cards for 7 days after each vaccination and received visits from the investigator's clinical team at Days 1 and 5 following each vaccination. Solicited systemic reactogenicity events included body temperature, feverishness, chills, cough, difficulty breathing, runny nose, nasal congestion, sore throat, hoarseness of voice, headache, confusion, convulsions/seizures, fatigue/malaise, muscle aches, joint pain, pink or red eyes, sore eyes, itchy eyes, drainage from eyes, ear pain or discharge, rash, abdominal pain, diarrhea, vomiting and jaundice. Solicited local reactogenicity included size of redness, size of swelling, size of induration, pain, and tenderness. | 7 days | |
Primary | Number of Participants With Maximum Systemic Reaction After Vaccination 2 | Systemic and local reactogenicity data were collected on Study Days 0, 7, 21 and 28, prevaccination, and within 60 minutes post-vaccination by clinic staff. Subjects completed diary cards for 7 days after each vaccination and received visits from the investigator's clinical team at Days 1 and 5 following each vaccination. Solicited systemic reactogenicity events included body temperature, feverishness, chills, cough, difficulty breathing, runny nose, nasal congestion, sore throat, hoarseness of voice, headache, confusion, convulsions/seizures, fatigue/malaise, muscle aches, joint pain, pink or red eyes, sore eyes, itchy eyes, drainage from eyes, ear pain or discharge, rash, abdominal pain, diarrhea, vomiting and jaundice. Solicited local reactogenicity included size of redness, size of swelling, size of induration, pain, and tenderness. | 7 days | |
Primary | Number of Participants With Maximum Local Reaction After Vaccination 1 | Systemic and local reactogenicity data were collected on Study Days 0, 7, 21 and 28, prevaccination, and within 60 minutes post-vaccination by clinic staff. Subjects completed diary cards for 7 days after each vaccination and received visits from the investigator's clinical team at Days 1 and 5 following each vaccination. Solicited local reactogenicity included size of redness, size of swelling, size of induration, pain, and tenderness. | 7 days | |
Primary | Number of Participants With Maximum Local Reaction After Vaccination 2 | Systemic and local reactogenicity data were collected on Study Days 0, 7, 21 and 28, prevaccination, and within 60 minutes post-vaccination by clinic staff. Subjects completed diary cards for 7 days after each vaccination and received visits from the investigator's clinical team at Days 1 and 5 following each vaccination. Solicited local reactogenicity included size of redness, size of swelling, size of induration, pain, and tenderness. | 7 days | |
Primary | Unsolicited, Non-serious Adverse Events | Subjects completed diary cards for 7 days after each vaccination and received visits from the investigator's clinical team at Days 1 and 5 following each vaccination. Adverse events were collected throughout the study period, and were graded for severity; however unsolicited adverse events were assessed only for relationship to vaccine if the events were immediate reactions or considered to be serious adverse events. | 7 days after each dose (Day 7 and Day 28) | |
Secondary | Geometric Mean Titer of Hemagglutination-inhibition Antibodies (HAI) | Day 0, 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 0, Day 21 and Day 42 | |
Secondary | Ratio of Geometric Mean Titer of Hemagglutination-inhibition Antibodies (HAI) | Day 0, 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 0, Day 21 and Day 42 | |
Secondary | Number and Percentage of All Subjects Achieving a Four-fold Rise in Hemagglutination-inhibition Antibodies (HAI) | Day 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Achieving a Four-fold Rise in Hemagglutination-inhibition Antibodies (HAI) Among Subjects With Baseline Titer Less Than 40 | Day 21 and Day 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Achieving a Four-fold Rise in Hemagglutination-inhibition Antibodies (HAI) Among Subjects With Baseline Titer Greater Than 40 | Day 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Developing a Seroprotective Hemagglutination-inhibition (HAI) Antibody Titer | Seroprotection defined as an HAI titer =1:40. Day 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 21 and Day 42 | |
Secondary | Geometric Mean Titer of Microneutralizing (MN) Antibodies | Day 0, 21 and 42 specimens were tested in the microneutralization (MN) assay. The microneutralization assay determines the titer of neutralizing antibodies against influenza A/H1N1. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The 50% neutralizing antibody titer is the reciprocal of the corresponding serum dilution. The geometric mean titers (GMT) and corresponding confidence intervals were based on a log 10 scale. | Day 0, Day 21 and Day 42 | |
Secondary | Ratio of Geometric Mean Titer of Microneutralization (MN) Antibodies | Day 0, 21 and 42 specimens were tested in the microneutralization (MN) assay. The microneutralization assay determines the titer of neutralizing antibodies against influenza A/H1N1. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The 50% neutralizing antibody titer is the reciprocal of the corresponding serum dilution. The geometric mean titers (GMT) and corresponding confidence intervals were based on a log 10 scale. | Day 0, Day 21 and Day 42 | |
Secondary | Number and Percentage of All Subjects Achieving a Four-fold Rise in Microneutralization (MN) Antibodies | Day 21 and 42 specimens were tested in the microneutralization (MN) assay. The microneutralization assay determines the titer of neutralizing antibodies against influenza A/H1N1. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The 50% neutralizing antibody titer is the reciprocal of the corresponding serum dilution. The geometric mean titers (GMT) and corresponding confidence intervals were based on a log 10 scale. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Achieving a Four-fold Rise in Microneutralizing (MN) Antibodies Among Subjects With Baseline Titer Less Than 40 | Day 21 and 42 blood samples from study subjects (n=48) were tested. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The hemagglutination titer was reported as the reciprocal of the highest dilution that caused hemagglutination and was expressed in HA units (HAU)/50µL, calculated as the average of results of duplicate wells. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Achieving a Four-fold Rise in Microneutralizing (MN) Antibodies Among Subjects With Baseline Titer Greater Than 40 | Day 21 and 42 specimens were tested in the microneutralization (MN) assay. The microneutralization assay determines the titer of neutralizing antibodies against influenza A/H1N1. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The 50% neutralizing antibody titer is the reciprocal of the corresponding serum dilution. The geometric mean titers (GMT) and corresponding confidence intervals were based on a log 10 scale. | Day 21 and Day 42 | |
Secondary | Number and Percentage of Subjects Developing a Seroprotective Microneutralizing (MN) Antibody Titer | Seroprotection defined as an antibody titer of 1:40 or greater. Day 21 and 42 specimens were tested in the microneutralization (MN) assay. The microneutralization assay determines the titer of neutralizing antibodies against influenza A/H1N1. The assay is performed in duplicate wells of 2-fold serial dilutions of serum. The 50% neutralizing antibody titer is the reciprocal of the corresponding serum dilution. The geometric mean titers (GMT) and corresponding confidence intervals were based on a log 10 scale. | Day 21 and Day 42 |
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