Haemophilus Influenzae Type b Clinical Trial
Official title:
A Phase III, Randomized, Multinational Study, Double-blinded for the Immunogenicity and Consistency Evaluation of 3 Hib-MenCY-TT Vaccine Lots and Single-blinded and Controlled for the Evaluation of Safety and Immunogenicity of GSK Biologicals' Haemophilus Influenzae Type b and Neisseria Meningitidis Serogroups C and Y-tetanus Toxoid Conjugate Vaccine Combined (Hib-MenCY-TT) Compared to Monovalent Hib Vaccine in Healthy Infants at 2, 4, 6, and 12 to 15 Months of Age.
| Verified date | November 2016 |
| Source | GlaxoSmithKline |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This study evaluates the immunogenicity and consistency of 3 Hib-MenCY-TT vaccine lots and the safety and immunogenicity of Hib-MenCY-TT vaccine compared to a control group receiving licensed Hib conjugate vaccine, when each are co-administered with Pediarix® to healthy infants at 2, 4, and 6 months of age. The study will also evaluate the safety and immunogenicity of Hib-MenCY-TT vaccine compared to a control group receiving licensed Hib conjugate vaccine, when each are co-administered with M-M-R® II and Varivax® at 12 to 15 months of age.
| Status | Completed |
| Enrollment | 4441 |
| Est. completion date | February 26, 2008 |
| Est. primary completion date | August 27, 2007 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 6 Weeks to 15 Months |
| Eligibility |
Inclusion Criteria: - Subjects for whom the investigator believes that parents/guardians can and will comply with the requirements of the protocol - A male or female between, and including, 6 and 12 weeks of age at the time of the first vaccination. - Written informed consent obtained from the parent or guardian of the subject. - Healthy subjects as established by medical history and clinical examination before entering into the study. - Born after 36 weeks gestation. - Infants who have not received a previous dose of hepatitis B vaccine or those who have received only 1 dose of hepatitis B vaccine administered at least 30 days prior to enrollment. - Infants may have received a birth dose of Bacillus Calmette-Guérin (BCG) vaccine. Exclusion Criteria: - Use of any investigational or non-registered product (drug or vaccine) other than the study vaccine(s) within 30 days preceding the first dose of study vaccine, or planned use during the study period. - Chronic administration (defined as more than 14 days) of immunosuppressants or other immune-modifying drugs since birth. - Planned administration/ administration of a vaccine not foreseen by the study protocol within 30 days of the first dose of study vaccine(s). (Synagis® [palivizumab, MedImmune], Prevnar (Prevenar), rotavirus vaccine, and influenza vaccine are allowed. - Previous vaccination against Neisseria meningitidis, Haemophilus influenzae type b, diphtheria, tetanus, pertussis, and/or poliovirus; more than one previous dose of hepatitis B vaccine. - History of Neisseria meningitidis, Haemophilus influenzae type b, diphtheria, tetanus, pertussis, hepatitis B, and/or poliovirus disease. - Any confirmed or suspected immunosuppressive or immunodeficient condition based on medical history and physical examination (no laboratory testing is required). - History of allergic disease or reactions likely to be exacerbated by any component of the vaccines, including dry natural latex rubber. - Major congenital defects or serious chronic illness. - History of any neurologic disorders or seizures. - Acute disease at time of enrollment. - Administration of immunoglobulins and/or any blood products since birth or planned administration during the study period. - Concurrent participation in another clinical study, at any time during the study period, in which the subject has been or will be exposed to an investigational or a non-investigational product (pharmaceutical product or device). Additional specific criteria for the US subjects in Cohort 1. In addition, for Cohorts 2 and 3, subjects should not be administered M-M-R II and Varivax if any of these criteria apply: - History of measles, mumps, rubella or varicella. - Previous vaccination against measles, mumps, rubella or varicella. - Hypersensitivity to any component of the vaccines, including gelatin or neomycin. - Patients receiving immunosuppressive therapy. - Individuals with blood dyscrasias, leukemia, lymphomas of any type, or other malignant neoplasms affecting the bone marrow or lymphatic systems. - Individuals with primary and acquired immunodeficiency states. - Individuals with a family history of congenital or hereditary immunodeficiency, until the immune competence of the potential vaccine recipient is demonstrated. - Individuals with active tuberculosis. - Acute disease at time of booster vaccination. |
| Country | Name | City | State |
|---|---|---|---|
| Australia | GSK Investigational Site | Carlton | Victoria |
| Australia | GSK Investigational Site | Herston | Queensland |
| Australia | GSK Investigational Site | Randwick | New South Wales |
| Australia | GSK Investigational Site | South Brisbane | Queensland |
| Mexico | GSK Investigational Site | Mexico, D.F. | |
| United States | GSK Investigational Site | Amarillo | Texas |
| United States | GSK Investigational Site | Arkansas City | Kansas |
| United States | GSK Investigational Site | Baltimore | Maryland |
| United States | GSK Investigational Site | Bardstown | Kentucky |
| United States | GSK Investigational Site | Beaver Falls | Pennsylvania |
| United States | GSK Investigational Site | Birmingham | Alabama |
| United States | GSK Investigational Site | Birmingham | Alabama |
| United States | GSK Investigational Site | Boardman | Ohio |
| United States | GSK Investigational Site | Bossier City | Louisiana |
| United States | GSK Investigational Site | Boston | Massachusetts |
| United States | GSK Investigational Site | Brainerd | Minnesota |
| United States | GSK Investigational Site | Bronx | New York |
| United States | GSK Investigational Site | Bryant | Arkansas |
| United States | GSK Investigational Site | Canton | Ohio |
| United States | GSK Investigational Site | Charleston | South Carolina |
| United States | GSK Investigational Site | Cleveland | Ohio |
| United States | GSK Investigational Site | Cocoa Beach | Florida |
| United States | GSK Investigational Site | Columbus | Ohio |
| United States | GSK Investigational Site | Des Moines | Iowa |
| United States | GSK Investigational Site | Des Moines | Iowa |
| United States | GSK Investigational Site | Durham | North Carolina |
| United States | GSK Investigational Site | Durham | North Carolina |
| United States | GSK Investigational Site | East Artesia | California |
| United States | GSK Investigational Site | Erie | Pennsylvania |
| United States | GSK Investigational Site | Fall River | Massachusetts |
| United States | GSK Investigational Site | Fayetteville | Arkansas |
| United States | GSK Investigational Site | Fort Worth | Texas |
| United States | GSK Investigational Site | Fountain Valley | California |
| United States | GSK Investigational Site | Fresno | California |
| United States | GSK Investigational Site | Fresno | California |
| United States | GSK Investigational Site | Fresno | California |
| United States | GSK Investigational Site | Galveston | Texas |
| United States | GSK Investigational Site | Greenville | Pennsylvania |
| United States | GSK Investigational Site | Gresham | Oregon |
| United States | GSK Investigational Site | Hershey | Pennsylvania |
| United States | GSK Investigational Site | Huber Heights | Ohio |
| United States | GSK Investigational Site | Ithaca | New York |
| United States | GSK Investigational Site | Jamaica Plain | Massachusetts |
| United States | GSK Investigational Site | Kalamazoo | Michigan |
| United States | GSK Investigational Site | Kansas City | Kansas |
| United States | GSK Investigational Site | La Crosse | Wisconsin |
| United States | GSK Investigational Site | La Jolla | California |
| United States | GSK Investigational Site | Layton | Utah |
| United States | GSK Investigational Site | Lexington | Kentucky |
| United States | GSK Investigational Site | Lexington | South Carolina |
| United States | GSK Investigational Site | Little Rock | Arkansas |
| United States | GSK Investigational Site | Little Rock | Arkansas |
| United States | GSK Investigational Site | Longmont | Colorado |
| United States | GSK Investigational Site | Louisville | Kentucky |
| United States | GSK Investigational Site | Mechanicsville | Virginia |
| United States | GSK Investigational Site | Melbourne | Florida |
| United States | GSK Investigational Site | Nampa | Idaho |
| United States | GSK Investigational Site | New Hartford | New York |
| United States | GSK Investigational Site | Norfolk | Virginia |
| United States | GSK Investigational Site | North Las Vegas | Nevada |
| United States | GSK Investigational Site | Norwich | Connecticut |
| United States | GSK Investigational Site | Oakland | California |
| United States | GSK Investigational Site | Omaha | Nebraska |
| United States | GSK Investigational Site | Paramount | California |
| United States | GSK Investigational Site | Pembroke Pines | Florida |
| United States | GSK Investigational Site | Philadelphia | Pennsylvania |
| United States | GSK Investigational Site | Phoenix | Arizona |
| United States | GSK Investigational Site | Pittsburgh | Pennsylvania |
| United States | GSK Investigational Site | Pittsburgh | Pennsylvania |
| United States | GSK Investigational Site | Pittsburgh | Pennsylvania |
| United States | GSK Investigational Site | Pittsburgh | Pennsylvania |
| United States | GSK Investigational Site | Pleasant Grove | Utah |
| United States | GSK Investigational Site | Portage | Michigan |
| United States | GSK Investigational Site | Providence | Rhode Island |
| United States | GSK Investigational Site | Raleigh | North Carolina |
| United States | GSK Investigational Site | Rochester | New York |
| United States | GSK Investigational Site | Rockledge | Florida |
| United States | GSK Investigational Site | Rolling Hills Estates | California |
| United States | GSK Investigational Site | Sacramento | California |
| United States | GSK Investigational Site | Saint George | Utah |
| United States | GSK Investigational Site | Saint Paul | Minnesota |
| United States | GSK Investigational Site | San Antonio | Texas |
| United States | GSK Investigational Site | Sellersville | Pennsylvania |
| United States | GSK Investigational Site | South Euclid | Ohio |
| United States | GSK Investigational Site | South Jordan | Utah |
| United States | GSK Investigational Site | Stevensville | Michigan |
| United States | GSK Investigational Site | Stony Brook | New York |
| United States | GSK Investigational Site | Sylva | North Carolina |
| United States | GSK Investigational Site | Syracuse | New York |
| United States | GSK Investigational Site | Temple | Texas |
| United States | GSK Investigational Site | Tulsa | Oklahoma |
| United States | GSK Investigational Site | Vancouver | Washington |
| United States | GSK Investigational Site | West Covina | California |
| Lead Sponsor | Collaborator |
|---|---|
| GlaxoSmithKline |
United States, Australia, Mexico,
Bryant K, McVernon J, Marchant C, Nolan T, Marshall G, Richmond P, Marshall H, Nissen M, Lambert S, Aris E, Mesaros N, Miller J. Immunogenicity and safety of measles-mumps-rubella and varicella vaccines coadministered with a fourth dose of Haemophilus influenzae type b and Neisseria meningitidis serogroups C and Y-tetanus toxoid conjugate vaccine in toddlers: a pooled analysis of randomized trials. Hum Vaccin Immunother. 2012 Aug;8(8):1036-41. doi: 10.4161/hv.20357. Epub 2012 Aug 1. — View Citation
Bryant KA et al. Immune response to measles, mumps, rubella (MMR) and varicella (V) vaccine coadministered with a fourth dose of Haemophilus influenzae type b - Neisseria meningitidis serogroups C and Y - tetanus toxoid conjugate (HibMenCY) vaccine in toddlers. Abstract presented at the Annual meeting of Pediatric Academic Societies (PAS). Vancouver, Canada, 1-4 May 2010.
Bryant KA, Marshall GS, Marchant CD, Pavia-Ruiz N, Nolan T, Rinderknecht S, Blatter M, Aris E, Lestrate P, Boutriau D, Friedland LR, Miller JM. Immunogenicity and safety of H influenzae type b-N meningitidis C/Y conjugate vaccine in infants. Pediatrics. 2011 Jun;127(6):e1375-85. doi: 10.1542/peds.2009-2992. Epub 2011 May 29. — View Citation
Bryant KA, Marshall GS. Haemophilus influenzae type b-Neisseria meningitidis serogroups C and Y tetanus toxoid conjugate vaccine for infants and toddlers. Expert Rev Vaccines. 2011 Jul;10(7):941-50. doi: 10.1586/erv.11.90. Review. — View Citation
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Anti-Polyribosyl Ribitol Phosphate (PRP) Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Primary | Neisseria Meningitidis Serogroup C (MenC) Serum Bactericidal Assay Using Human Complement (hSBA) Antibody Titers | Titers were expressed as Geometric Mean Titers (GMTs) This analysis occured on the cohort 1 : Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Primary | Neisseria Meningitidis Serogroup Y (MenY) Serum Bactericidal Assay Using Human Complement (hSBA) Antibody Titers | Titers are expressen as Geometric Mean Titers (GMTs) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Primary | hSBA-MenC Antibody Titers | Titers are expressed as Geometric Mean Titers (GMTs) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and 42 days after the fourth dose | |
| Primary | hSBA-MenY Antibody Titers | Titers are expressed as Geometric Mean Titers (GMTs) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and 42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-PRP Antibody Concentration Equal to or Above 1.0 Microgram Per Milliliter (µg/mL) | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | One month after primary vaccination | |
| Primary | Number of Subjects With hSBA-MenC Titer Equal to or Above 1:8 | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | 42 days after the fourth dose | |
| Primary | Number of Subjects With hSBA-MenY Titer Equal to or Above 1:8 | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | 42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-measles Antibody Concentrations Equal to or Above 150 Milli-international Units Per Milli-liter (mIU/ML) | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody concentrations below 150 mIU/mL. Co-administration with MMR-II vaccine |
42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-PRP Antibody Concentration Equal to or Above 1.0 Microgram Per Milliliter | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | 42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-mumps Titer Equal to or Above 28 Estimated Dose 50 (ED50) | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-mumps antibody titers below 28 ED50 Co-administration with MMR-II vaccine. |
42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-rubella Antibody Concentrations Equal to or Above 10 International Units Per Milli-litre (IU/mL) | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody concentrations below 4 IU/mL. Co-administration with MMR-II vaccine. |
42 days after the fourth dose | |
| Primary | Number of Subjects With Anti-varicella Titer Equal to or Above 1:5 | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody titer below 1:5. Co-administration with Varivax vaccine. |
42 days after the fourth dose | |
| Secondary | Number of Subjects With Anti-tetanus (Anti-T) and Anti-diphtheria Toxoid (Anti-D) Antibody Concentrations Equal to or Above 0.1 International Units Per Millilitre (IU/mL) | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | One month after primary vaccination | |
| Secondary | Anti-D and Anti-T Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in international units per milliliter (IU/mL). This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Number of Subjects With Anti Hepatitis B Surface Antigen (Anti-HBs) Antibody Concentrations Equal to or Above 10.0 Milli-international Units Per Millilitre (mIU/mL) | Results are stratified by the presence or absence of a birth dose of hepatitis B vaccine. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Anti-HBS Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in milli-International units per milliliter (mIU/mL) Results are stratified by the presence or absence of a birth dose of hepatitis B vaccine. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Number of Subjects With Anti-pertussis Toxoid (Anti-PT), Anti-filamentous Hemagglutinin (Anti-FHA) and Anti-pertactin (Anti-PRN) Antibody Concentrations Equal to or Above 5 ELISA Units Per Millilitre (EL.U/mL) | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | One month after primary vaccination | |
| Secondary | Anti-PT, Anti-FHA and Anti-PRN Antibody Concentrations | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | One month after primary vaccination | |
| Secondary | Number of Subjects With Anti-poliovirus Types 1, 2 and 3 Equal to or Above 8 Estimated Dose 50 (ED50) | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | One month after primary vaccination | |
| Secondary | Anti-poliovirus Types 1, 2 and 3 Titers | Titers are expressed as Geometric Mean Titers (GMTs) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Number of Subjects With Antibodies to Neisseria Meningitidis Serogroup C and Y Polysaccharide Capsule (Anti-PSC and Anti-PSY) Concentrations Equal to or Above the Cut-off Values | Anti-PSC and anti-PSY antibody cut-off values assessed were >=0.3 microgram per milliliter (µg/mL) and >=2.0 µg/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Anti-PSC and Anti-PSY Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per milliliter (µg/mL) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after primary vaccination | |
| Secondary | Number of Subjects With Anti-PRP Antibody Concentrations Equal to or Above the Cut-off Values | Anti-PRP antibody cut-off values assessed were >=0.15 microgram per milliliter (µg/mL) and >=1.0 µg/mL. The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Number of Subjects With Anti-PRP Antibody Concentrations Equal to or Above the Cut-off Values | Anti-PRP antibody cut-off values assessed were >=0.15 microgram per milliliter (µg/mL) and >=1.0 µg/mL. The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | Anti-PRP Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL) The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Anti-PRP Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL) The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | Number of Subjects With hSBA-MenC and hSBA-MenY Titers Equal to or Above the Cut-off Values | hSBA-MenC/Y antibody cut-off values assessed were >=1:4 and >=1:8 The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Number of Subjects With hSBA-MenC and hSBA-MenY Titers Equal to or Above the Cut-off Values | hSBA-MenC/Y antibody cut-off values assessed were >=1:4 and >=1:8. The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | hSBA-MenC and hSBA-MenY Antibody Titers | Titres are expressed as Geometric Mean Titers (GMTs). The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | hSBA-MenC and hSBA-MenY Antibody Titers | Titers are expressed as Geometric Mean Titers (GMTs) The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | Number of Subjects With Anti-PSC and Anti-PSY Antibody Concentrations Equal to or Above the Cut-off Values | Anti-PSC and anti-PSY antibody cut-off values assessed were >=0.3 microgram per milliliter (µg/mL) and >=2.0 µg/mL. The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Number of Subjects With Anti-PSC and Anti-PSY Antibody Concentrations Equal to or Above the Cut-off Values | Anti-PSC and anti-PSY antibody cut-off values assessed were >=0.3 µg/mL and >=2.0 µg/mL. The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | Anti-PSC and Anti-PSY Antibodies Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per milliliter (µg/mL). The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Anti-PSC and Anti-PSY Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL). The analysis was performed on the cohort 3 (Non-US Safety and Immunogenicity): Cohort 3 was to include the subjects enrolled at 1 center in Mexico. Only descriptive immunogenicity results were reported for this cohort. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and one month after fourth dose vaccination | |
| Secondary | Number of Subjects With Anti-PRP Antibody Concentrations Equal to or Above the Cut-off Value | Anti-PRP antibody cut-off values assessed were >=0.15 µg/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Anti-PRP Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL). This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course and prior to the fourth dose vaccination | |
| Secondary | Number of Subjects With hSBA-MenC and hSBA-MenY Antibody Titers Equal to or Above the Cut-off Values | hSBA-MenC and hSBA-MenY antibody cut-off values assessed were >=1:4 and >=1:8. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
One month after the primary vaccination course | |
| Secondary | Number of Subjects With Anti-PSC and Anti-PSY Antibody Concentrations Equal to or Above the Cut-off Values | Anti-PSC and anti-PSY antibody cut-off values assessed were >=0.3 µg/mL and >=2.0 µg/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and 42 days after fourth dose vaccination | |
| Secondary | Anti-PSC and Anti-PSY Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL). This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
Prior to the fourth dose vaccination and 42 days after fourth dose vaccination | |
| Secondary | Number of Subjects With Anti-PRP Antibody Concentrations Equal to or Above 0.15 Microgram Per Milliliter (µg/mL) | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | Prior to the fourth dose vaccination and 42 days after fourth vaccination | |
| Secondary | Anti-PRP Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in microgram per millilitre (µg/mL) This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
Prior to the fourth vaccination and 42 days after fourth vaccination | |
| Secondary | Number of Subjects With hSBA-MenC and hSBA-MenY Antibody Concentrations Equal to or Above 1:4 | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | Prior to the fourth dose vaccination and 42 days after fourth vaccination | |
| Secondary | Number of Subjects With Anti-measles Antibody Concentrations Equal to or Above 200 Milli-international Units Per Millilitre (mIU/mL) | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody concentrations below 150 mIU/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Anti-measles Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in milli-international units per milliliter (mIU/mL). The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody concentrations below 150 mIU/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Number of Subjects With Anti-mumps Titer Equal to or Above the Cut-off Values | Anti-mumps antibody cut-off values assessed were >=28 estimated dose 50 (ED50) and >=51 ED50. The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-mumps antibody titers below 24 ED50. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Anti-mumps Antibody Titers | Titers are expressed as Geometric Mean Titers (GMTs). The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-measles antibody titers below 24 ED50. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Number of Subjects With Anti-rubella Antibody Concentrations Equal to or Above 4 International Units Per Millilitre (IU/mL) | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-rubella antibody concentrations below 4 IU/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Anti-rubella Antibody Concentrations | Concentrations are given as Geometric Mean Concentrations (GMCs) and are expressed in international units per milliliter (IU/mL). The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-rubella antibody concentrations below 4 IU/mL. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Number of Subjects With Anti-varicella Titer Equal to or Above 1:40 | The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-rubella antibody concentrations below 1:5 This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Anti-varicella Antibody Titers | Titers are expressed as Geometric Mean Titers (GMTs) The analysis was performed on initially seronegative subjects. Seronegative subjects are subjects with anti-varicella antibody titers below 1:5 This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. |
42 days after fourth vaccination | |
| Secondary | Number of Subjects With Anti-H1N1, Anti-H3N2 and Anti-influenza-B (Anti B) Antibody Titers Equal to or Above 1:40 | anti-H1N1, anti-H3N2 and anti-influenza-B (anti B) antibody were measured by hemagglutination inhibition assay (HIA), in subjects who received 2 doses of influenza vaccine within the same influenza season of which at least one dose is concomitant with the study vaccine. For the purposes of this study, concomitant administration of influenza vaccine was defined as administration within 28 days before to 7 days after administration of study vaccines. This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. |
Prior to the fourth dose vaccination and one month after the fourth dose vaccination | |
| Secondary | Number of Subjects Reporting Fever Above 39.5 Degrees Celsius/103.1 Degrees Fahrenheit | Fever is defined as temperature (rectal or axillary/tympanic) above 39.5 degrees Celsius (°C) or 103.1 degrees Fahrenheit (°F). | In the 4-day (Day 0-3) follow-up period after primary vaccination course | |
| Secondary | Number of Subjects Reporting Fever Above 39.5 Degrees Celsius/103.1 Degrees Fahrenheit | Fever is defined as temperature (rectal or axillary/tympanic) above 39.5 degrees Celsius (°C) or 103.1 degrees Fahrenheit (°F). | In the 4-day (Day0-3) follow-up period after the fourth dose | |
| Secondary | Number of Subjects Reporting Solicited Local and General Symptoms | Solicited local symptoms assessed were pain, redness and swelling. Solicited genral symptoms assessed were fever, irritability/fussiness, drowsiness and loss of appetite. Fever is defined as temperature (rectal or axillary/tympanic) equal to or above 38.0°C. | Within the 4 days (Day 0-3) following each dose of the primary vaccination course | |
| Secondary | Number of Subjects Reporting Solicited Local and General Symptoms | Solicited local symptoms assessed were pain, redness, swelling and an increase in limb circumference. Solicited general symptoms assessed were fever, irritability/fussiness, drowsiness and lost of appetite. Fever is defined as temperature (rectal or axillary/tympanic) equal to or above 38.0°C | Within the 4 days (Day 0-3) post-vaccination period following the fourth dose | |
| Secondary | Number of Subjects Reporting Unsolicited Adverse Events (AEs) | Unsolicited AE covers any AE reported in addition to those solicited during the clinical study and any solicited symptom with onset outside the specified period of follow-up for solicited symptoms. | Within 31 days (Day 0-30) following the primary vaccination course | |
| Secondary | Number of Subjects Reporting Unsolicited Adverse Events (AEs) | Unsolicited AE covers any AE reported in addition to those solicited during the clinical study and any solicited symptom with onset outside the specified period of follow-up for solicited symptoms. | Within 31 days (Day 0-30) following the fourth dose | |
| Secondary | Number of Subjects Reporting Increased Circumferential Swelling at the Injection Limb(s) | Increased circumferential swelling defined as either swelling with a diameter of >50 mm or a >50 mm increase in the circumference of the mid-limb when compared to the baseline (pre-vaccination) measurement, or any diffuse swelling that interferes with or prevents everyday activities (for example, active playing, eating, sleeping). | Within 4 days (Day 0 to Day 3) after fourth dose vaccination | |
| Secondary | Number of Subjects Reporting General Symptoms Specific to Measles, Mumps, Rubella and Varicella Vaccination | Symptoms assessed were fever, rash/exanthem, parotid/salivary gland swelling, and any suspected signs of meningism including febrile convulsions. Fever is defined as temperature (rectal or axillary/tympanic) equal to or above 38.0°C. | Within 43 days (Day 0 through Day 42) after vaccination | |
| Secondary | Number of Subjects Reporting Serious Adverse Events (SAEs) | SAEs assessed include medical occurrences that results in death, are life threatening, require hospitalization or prolongation of hospitalization, results in disability/incapacity or are a congenital anomaly/birth defect in the offspring of a study subjects. | From Dose 0 through 6 months after the last primary dose or untill administration of the fourth dose | |
| Secondary | Number of Subjects Reporting Serious Adverse Events (SAEs) | SAEs assessed include medical occurrences that results in death, are life threatening, require hospitalization or prolongation of hospitalization, results in disability/incapacity or are a congenital anomaly/birth defect in the offspring of a study subjects. | From the fourth dose through the end of the 6-month safety follow-up | |
| Secondary | Number of Subjects Reporting New Onset of Chronic Illness(es) (NOCDs) | NOCDs include autoimmune disorders, asthma, type I diabetes, allergies. | From Dose 0 through 6 months after the last primary dose or until administration of the fourth dose | |
| Secondary | Number of Subjects Reporting New Onset of Chronic Illness(es) (NOCDs) | NOCDs include autoimmune disorders, asthma, type I diabetes, allergies. | From the fourth dose through the end of the 6-month safety follow-up | |
| Secondary | Number of Subjects Reporting Rash | Rash assessed was hives, idiopathic thrombocytopenic purpura, petechiae. | From Dose 0 through 6 months after the last primary dose or until administration of the fourth dose | |
| Secondary | Number of Subjects Reporting Rash | Rash assessed was hives, idiopathic thrombocytopenic purpura, petechiae. | From the fourth dose through the end of the 6-month safety follow-up | |
| Secondary | Number of Subjects Reporting Adverse Events Resulting in Emergency Room (ER) Visits | Emergency room (ER) visits were not related to well-child care, vaccination, injury or common acute illness such as upper respiratory tract infections; otitis media, pharyngitis, gastroenteritis. | From Dose 0 through 6 months after the last primary dose or until administration of the fourth dose | |
| Secondary | Number of Subjects Reporting Adverse Events Resulting in Physicians (MD) Office Visits. | Physicians (MD) office visits were not related to well-child care, vaccination, injury or common acute illness such as upper respiratory tract infections; otitis media, pharyngitis, gastroenteritis. | From Dose 0 through 6 months after the last primary dose or until administration of the fourth dose | |
| Secondary | Number of Subjects Reporting Adverse Events Resulting in Emergency Room (ER) Visits | Emergency room (ER) visits were not related to well-child care, vaccination, injury or common acute illness such as upper respiratory tract infections; otitis media, pharyngitis, gastroenteritis. | From the fourth dose through the end of the 6-month safety follow-up | |
| Secondary | Number of Subjects Reporting Adverse Events Resulting in Physicians (MD) Office Visits | Physicians (MD) office visits were not related to well-child care, vaccination, injury or common acute illness such as upper respiratory tract infections; otitis media, pharyngitis, gastroenteritis. | From the fourth dose through the end of the 6-month safety follow-up | |
| Secondary | Number of Subjects With Anti-PRP Antibody Concentration Equal to or Above 1.0 Microgram Per Milliliter (µg/mL). | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | Prior to the fourth dose vaccination | |
| Secondary | Number of Subjects With hSBA-MenC and hSBA-MenY Antibody Titer Equal to or Above 1:8. | This analysis occurred on the cohort 1: Cohort 1 was to include subjects in the US on which all immunogenicity analyses were to be based. These subjects also contributed to the safety analysis. | Prior to the fourth dose vaccination |
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT00753649 -
Immunogenicity and Safety of GSK Biologicals' Infanrix Hexa in Infants
|
Phase 4 | |
| Completed |
NCT01214889 -
Study of PENTAXIM™ Vaccine Versus TETRAXIM™ Vaccine Given With ACTHIB™ Vaccine in South Korean Infants.
|
Phase 3 | |
| Completed |
NCT00534833 -
Immunogenicity Study of Antibody Persistence and Booster Effect of DTaP-HB-PRP~T Combined Vaccine or Tritanrix-HepB/Hib™
|
Phase 3 | |
| Completed |
NCT00379977 -
Study to Assess the Safety & Reactogenicity of GSK Biologicals' DTPa/Hib Vaccine When Given at 3, 4 and 5 Months of Age
|
Phase 3 | |
| Completed |
NCT00153556 -
Study to Eliminate Hib Carriage in Rural Alaska Native Villages
|
Phase 4 | |
| Completed |
NCT02853929 -
Evaluation of Immunogenicity and Safety of a Booster Dose of Infanrix Hexa™ in Healthy Infants Born to Mothers Vaccinated With Boostrix™ During Pregnancy or Immediately Post-delivery
|
Phase 4 | |
| Completed |
NCT02858440 -
A Study to Assess the Immunogenicity and Safety of GSK Biologicals' Infanrix-IPV/Hib Vaccine Administered as a Three-dose Vaccination Course at 3, 4.5 and 6 Months of Age and a Booster Dose at 18 Months of Age in Healthy Infants in Russia
|
Phase 3 | |
| Completed |
NCT01983540 -
Antibody Persistence at Age 3.5 and 4.5 Years After Primary and Booster DTaP-IPV-Hep B-PRP~T or Infanrix Hexa Vaccination
|
Phase 3 | |
| Completed |
NCT01878435 -
Randomized Controlled Trial of the Impact of Mobile Phone Delivered Reminders and Travel Subsidies to Improve Childhood Immunization Coverage Rates and Timeliness in Western Kenya
|
N/A | |
| Completed |
NCT00401531 -
Comparison of a DTaP-IPV-HB-PRP~T Combined Vaccine to Infanrix™-Hexa, When Administered With Prevnar® in Thai Infants
|
Phase 3 | |
| Completed |
NCT00376779 -
Immunogenicity and Safety of a DTPa-HBV-IPV/Hib Vaccine Given at 2, 3 and 4 Months of Age
|
Phase 2 | |
| Completed |
NCT00831311 -
Study of DTaP-IPV-Hep B-PRP~T Combined Vaccine Compared With PENTAXIM™ and ENGERIX B® PEDIATRICO in Argentinean Infants
|
Phase 2 | |
| Completed |
NCT00254917 -
Assessment of the Immunogenicity and Safety of PENTAXIM™ in Philippines
|
Phase 4 | |
| Completed |
NCT01457547 -
Comparison of Immunogenicity and Reactogenicity of INFANRIX™ HEXA and HEXAVAC™ Vaccines as a Primary Vaccination Course
|
Phase 4 | |
| Completed |
NCT01453998 -
Safety and Immunogenicity of a Booster Dose of New Formulations of GlaxoSmithKline Biologicals' DTPa-HBV-IPV/Hib Vaccine (GSK217744)
|
Phase 2 | |
| Completed |
NCT01449812 -
Immunogenicity and Safety Study of Booster Dose of GSK Biologicals' IPV (Poliorix™) and DTPa/Hib (Infanrix+Hib™) Vaccine
|
Phase 3 | |
| Completed |
NCT00808392 -
Safety and Immunogenicity of a Monovalent Conjugated Vaccine Against Haemophilus Influenzae Type b
|
Phase 3 | |
| Completed |
NCT00307567 -
Multicentre Booster & Immune Memory Study of a Booster Dose of GSK Biologicals' 10-valent Pneumococcal Conjugate Vaccine or a Single Dose of 23-valent Plain Polysaccharide Vaccine in Healthy Children Aged 11-18 Mths, Previously Vaccinated in Study 103488
|
Phase 2 | |
| Completed |
NCT00323050 -
Study of a Booster Dose of Hib-MenC Conjugate Vaccine vs Infanrix Hexa When Given to 14 Month Old Subjects
|
Phase 3 | |
| Completed |
NCT00325156 -
Assess the Safety & Reactogenicity of DTPa-IPV/Hib Vaccine Administered at 3, 4, 5 & 18 Mths of Age, in Healthy Infants
|
Phase 4 |