PMID- 30770221
OWN - NLM
STAT- MEDLINE
DCOM- 20200629
LR  - 20200629
IS  - 1873-2518 (Electronic)
IS  - 0264-410X (Linking)
VI  - 37
IP  - 12
DP  - 2019 Mar 14
TI  - Persistence and 4-year boosting of the bactericidal response elicited by two- and 
      three-dose schedules of MenB-FHbp: A phase 3 extension study in adolescents.
PG  - 1710-1719
LID - S0264-410X(18)31636-0 [pii]
LID - 10.1016/j.vaccine.2018.11.073 [doi]
AB  - BACKGROUND: The period of heightened risk of invasive meningococcal disease in 
      adolescence extends for >10 years. This study aimed to evaluate persistence of 
      the immune response to the serogroup B meningococcal (MenB) vaccine MenB-FHbp 
      (Trumenba((R)), Bivalent rLP2086) under two- and three-dose primary vaccination 
      schedules, both of which are approved in the United States and the European 
      Union, and to assess safety and immunogenicity of a booster dose. METHODS: This 
      was an open-label extension study of a phase 2 randomized MenB-FHbp study 
      (primary study). This interim analysis includes data through 1 month after 
      booster vaccination. In the primary study, adolescents 11-18 years of age were 
      randomized using an interactive voice or web-based response system to receive 
      120 mug MenB-FHbp under 0-, 1-, 6-month; 0-, 2-, 6-month; 0-, 6-month; 0-, 
      2-month; or 0-, 4-month schedules (termed study groups for the current analysis). 
      For the primary study, participants were blinded to their vaccine study group 
      allocation, but investigators and the study sponsor were unblinded. Immune 
      responses in subjects from the primary study were evaluated through 48 months 
      after primary vaccination (persistence stage; 17 sites in Czech Republic, 
      Denmark, Germany, and Sweden). Safety and immunogenicity of a booster dose given 
      at 48 months after primary vaccination (booster stage; 14 sites in Czech 
      Republic, Denmark, and Sweden) were also assessed. Immune responses were 
      evaluated in serum bactericidal assays with human complement (hSBAs) using four 
      MenB test strains representative of disease-causing MenB strains in the United 
      States and Europe and expressing factor H binding proteins (FHbps) heterologous 
      to the vaccine antigens. The primary immunogenicity endpoints were the 
      proportions of subjects with hSBA titers greater than or equal to the assays' 
      lower limit of quantitation (LLOQ; 1:8 or 1:16 depending on strain) at 12, 18, 
      24, 36, and 48 months after primary vaccination (persistence stage) and 1 and 
      48 months after the primary vaccination series and 1 month after receipt of the 
      booster dose (booster stage). Safety evaluations during the booster stage 
      included local reactions and systemic events by severity, antipyretic use, 
      adverse events (AEs), immediate AEs, serious AEs (SAEs), medically attended AEs 
      (MAEs), newly diagnosed chronic medical conditions (NDCMCs), and missed days of 
      school and work because of AEs. The modified intent-to-treat (mITT) population 
      was used for immunogenicity evaluations in the persistence stage. The booster 
      stage immunogenicity evaluations used the evaluable immunogenicity population; 
      analyses were also performed in the mITT population. For the persistence stage, 
      safety evaluations included subjects with at least one blood draw, whereas for 
      the booster stage, they included subjects who received the booster dose and had 
      available safety data. This trial is registered at ClinicalTrials.gov number 
      NCT01543087. FINDINGS: A total of 465 subjects were enrolled in the persistence 
      stage, and 271 subjects were enrolled in the booster stage. Sera for the 
      extension phase of this interim analysis were collected from September 7, 2012 to 
      December 7, 2015. One month after primary vaccination, 73.8-100.0% of subjects 
      depending on study group responded with hSBA titers >/=LLOQ. Response rates 
      declined during the 12 months after last primary vaccination and then remained 
      stable through 48 months, with 18.0-61.3% of subjects depending on study group 
      having hSBA titers >/=LLOQ at this time point. One month after receipt of the 
      booster dose, 91.9-100.0% of subjects depending on study group had hSBA titers 
      >/=LLOQ against the four primary strains individually and 91.8-98.2% had hSBA 
      titers >/=LLOQ against all four strains combined (composite response). Geometric 
      mean titers were higher after booster vaccination than at 1 month after primary 
      vaccination. Immune responses were generally similar across study groups, 
      regardless of whether a two- or three-dose primary series was received. None of 
      the AEs (2.2-6.9% of subjects depending on study group) or NDCMCs (1.8-5.0%) that 
      were reported during the persistence stage were considered related to the 
      investigational product. Local reactions and systemic events were reported by 
      84.4-93.8% and 68.8-76.6% of subjects depending on study group, respectively, in 
      the booster stage; these were generally similar across study groups, transient, 
      and less frequent than after any primary vaccination. Additionally, there was no 
      general progressive worsening in severity of reactogenicity events (ie, 
      potentiation; </=3 subjects per group), and reactogenicity events did not lead to 
      any study withdrawals. No NDCMCs or immediate AEs were reported during the 
      booster stage. AEs were reported by 3.7-12.5% of subjects depending on study 
      group during the booster stage. The two possibly related AEs included a mild 
      worsening of psoriasis and a severe influenza-like illness that resolved in 
      10 days. INTERPRETATION: Immune responses declined after the primary vaccination 
      series; however, a substantially greater number of subjects retained protective 
      responses at 48 months after primary vaccination compared with subjects having 
      protective responses before vaccination. Persistence trends were similar across 
      all 5 study groups regardless of whether a two- or three-dose primary schedule 
      was received. Furthermore, a booster dose given 48 months after primary 
      vaccination was safe, well-tolerated, and elicited robust immune responses 
      indicative of immunologic memory; these responses were similar between two- and 
      three-dose primary schedule study groups. Use of a booster dose may help further 
      extend protection against MenB disease in adolescents. FUNDING: Pfizer Inc.
CI  - Copyright (c) 2019 Elsevier Ltd. All rights reserved.
FAU - Vesikari, Timo
AU  - Vesikari T
AD  - Vaccine Research Center, University of Tampere Medical School, Biokatu 10, 33520 
      Tampere, Finland.
FAU - Ostergaard, Lars
AU  - Ostergaard L
AD  - Department of Infectious Diseases, Aarhus University Hospital, Skejby, Palle 
      Juul-Jensens Blvd 99, 8200 Aarhus N, Denmark.
FAU - Beeslaar, Johannes
AU  - Beeslaar J
AD  - Pfizer UK Vaccine Research and Development, Horizon Building, Honey Lane, Hurley 
      SL6 6RJ, UK. Electronic address: Johannes.Beeslaar@pfizer.com.
FAU - Absalon, Judith
AU  - Absalon J
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - Eiden, Joseph J
AU  - Eiden JJ
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - Jansen, Kathrin U
AU  - Jansen KU
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - Jones, Thomas R
AU  - Jones TR
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - Harris, Shannon L
AU  - Harris SL
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - Maansson, Roger
AU  - Maansson R
AD  - Pfizer Vaccine Research and Development, 500 Arcola Road, Collegeville, PA 19426, 
      USA.
FAU - Munson, Samantha
AU  - Munson S
AD  - Pfizer Vaccine Research and Development, 500 Arcola Road, Collegeville, PA 19426, 
      USA.
FAU - O'Neill, Robert E
AU  - O'Neill RE
AD  - Pfizer Vaccine Research and Development, 401 North Middletown Road, Pearl River, 
      NY 10965, USA.
FAU - York, Laura J
AU  - York LJ
AD  - Pfizer Vaccine Medical Development, Scientific & Clinical Affairs, 500 Arcola 
      Road, Collegeville, PA 19426, USA.
FAU - Perez, John L
AU  - Perez JL
AD  - Pfizer Vaccine Research and Development, 500 Arcola Road, Collegeville, PA 19426, 
      USA.
LA  - eng
SI  - ClinicalTrials.gov/NCT01543087
PT  - Clinical Trial, Phase III
PT  - Journal Article
PT  - Research Support, Non-U.S. Gov't
DEP - 20190212
PL  - Netherlands
TA  - Vaccine
JT  - Vaccine
JID - 8406899
RN  - 0 (Meningococcal Vaccines)
SB  - IM
MH  - Adolescent
MH  - Adult
MH  - Child
MH  - Female
MH  - Humans
MH  - *Immunization, Secondary
MH  - Male
MH  - Meningitis, Meningococcal/*prevention & control
MH  - Meningococcal Vaccines/*administration & dosage/*immunology
MH  - Neisseria meningitidis, Serogroup B/*immunology
MH  - *Vaccination
MH  - Young Adult
OTO - NOTNLM
OT  - Adolescents
OT  - Booster
OT  - Meningococcal disease
OT  - Persistence
OT  - Serogroup B
OT  - Vaccine
EDAT- 2019/02/17 06:00
MHDA- 2020/07/01 06:00
CRDT- 2019/02/17 06:00
PHST- 2018/02/16 00:00 [received]
PHST- 2018/07/25 00:00 [revised]
PHST- 2018/11/26 00:00 [accepted]
PHST- 2019/02/17 06:00 [pubmed]
PHST- 2020/07/01 06:00 [medline]
PHST- 2019/02/17 06:00 [entrez]
AID - S0264-410X(18)31636-0 [pii]
AID - 10.1016/j.vaccine.2018.11.073 [doi]
PST - ppublish
SO  - Vaccine. 2019 Mar 14;37(12):1710-1719. doi: 10.1016/j.vaccine.2018.11.073. Epub 
      2019 Feb 12.