A Bivalent Omicron-BA.4/BA.5-Adapted BNT162b2 Booster in ≥12-Year-Olds

被引：7

作者：

Usdan, Lisa ^{[1
]}

Patel, Sohil ^{[2
]}

Rodriguez, Hector ^{[3
]}

Xu, Xia ^{[4
]}

Lee, Dung-Yang

Finn, Daniel ^{[5
]}

Wyper, Hayley ^{[2
]}

Lowry, Francine S. ^{[4
]}

Mensa, Federico J. ^{[6
]}

Lu, Claire ^{[7
]}

Cooper, David ^{[7
]}

Koury, Kenneth ^{[7
]}

Anderson, Annaliesa S. ^{[7
]}

Tureci, Ozlem

Sahin, Ugur ^{[6
]}

Swanson, Kena A. ^{[7
]}

Gruber, William C. ^{[7
]}

Kitchin, Nicholas ^{[2
]}

机构：

[1] CNS Healthcare, Memphis, TN USA

[2] Pfizer, Vaccine Res & Dev, Honey Lane, Hurley SL6 6RJ, England

[3] Acevedo Clin Res Associates, Miami, FL USA

[4] Pfizer, Vaccine Res & Dev, Collegeville, PA USA

[5] Kentucky Pediat Adult Res, Bardstown, KY USA

[6] BioNTech, Mainz, Germany

[7] Pfizer, Vaccine Res & Dev, Pearl River, NY USA

来源：

CLINICAL INFECTIOUS DISEASES | 2024年 / 78卷 / 05期

关键词：

BNT162b2; vaccine; SARS-CoV-2; Omicron variant; booster; immunogenicity; UNITED-STATES; VACCINE;

D O I：

10.1093/cid/ciad718

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Background Protection against contemporary severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants requires sequence-adapted vaccines.Methods In this ongoing phase 2/3 trial, 12-17-year-olds (n = 108), 18-55-year-olds (n = 313), and >55-year-olds (n = 306) who previously received 3 original BNT162b2 30-mu g doses, received a fourth dose (second booster) of 30-mu g bivalent original/Omicron-BA.4/BA.5-adapted BNT162b2 (BNT162b2-Omi.BA.4/BA.5). For comparisons with original BNT162b2, participants were selected from another phase 3 trial. Immunologic superiority 1 month after vaccination, with respect to 50% neutralizing titers (lower bound [LB] of 2-sided 95% confidence interval [CI] for geometric mean ratio [GMR], >1), and noninferiority with respect to seroresponse rates (LB of 2-sided 95% CI for rate difference, greater than -5%), for Omicron BA.4/BA.5 were assessed in >55-year-olds versus original BNT162b2 as a second booster. Noninferiority with respect to neutralizing titer level (LB of 2-sided 95% CI for GMR, > 0.67) and seroresponse rate (LB of 2-sided 95% CI for rate difference, greater than -10%) of Omicron BA.4/BA.5 immune response for BNT162b2-Omi.BA.4/BA.5 in 18-55 versus >55-year-olds was assessed.Results One month after vaccination in >55-year-olds, the model-adjusted GMR of Omicron BA.4/BA.5 neutralizing titers for the BNT162b2-Omi.BA.4/BA.5 versus BNT162b2 groups (2.91 [95% CI, 2.45-3.44]) demonstrated the superiority of BNT162b2-Omi.BA.4/BA.5. Adjusted difference in the percentages of >55-year-olds with seroresponse (26.77% [95% CI, 19.59-33.95]) showed noninferiority of BNT162b2-Omi.BA.4/BA.5 to BNT162b2. Noninferiority of BNT162b2-Omi.BA.4/BA.5 in 18-55-year-olds compared with >55-year-olds was met for model-adjusted GMR and seroresponse. Geometric mean titers in 12-17-year-olds increased from baseline to 1 month after vaccination. The BNT162b2-Omi.BA.4/BA.5 safety profile was similar to the profiles for booster doses of bivalent Omicron BA.1-modified BNT162b2 and original BNT162b2 reported in previous studies.Conclusions Based on immunogenicity and safety data up to 1 month after vaccination in participants who previously received 3 original BNT162b2 doses, a BNT162b2-Omi.BA.4/BA.5 30-mu g booster has a favorable benefit-risk profile.Clinical Trials Registration NCT05472038

引用

页码：1194 / 1203

页数：10

共 50 条

[1] Bivalent Omicron BA.4/BA.5 BNT162b2 Vaccine in 6-Month- to <12-Year-Olds
Sher, Lawrence D.
Boakye-Appiah, Justice K.
Hill, Sungeen
Wasserman, Emily
Xu, Xia
Maldonado, Yvonne
Walter, Emmanuel B.
Munoz, Flor M.
Paulsen, Grant C.
Englund, Janet A.
Talaat, Kawsar R.
Barnett, Elizabeth D.
Kamidani, Satoshi
Senders, Shelly
Simoes, Eric A. F.
Belanger, Kelly
Parikh, Vrunda
Ma, Hua
Wang, Xingbin
Lu, Claire
Cooper, David
Koury, Kenneth
Anderson, Annaliesa S.
Tuereci, Oezlem
Sahin, Ugur
Swanson, Kena A.
Gruber, William C.
Gurtman, Alejandra
Kitchin, Nicholas
Sabharwal, Charu
JOURNAL OF THE PEDIATRIC INFECTIOUS DISEASES SOCIETY, 2024, 13 (08) : 421 - 429
[2] Bivalent Omicron BA.1-Adapted BNT162b2 Booster in Adults Older than 55 Years
Winokur, P.
Gayed, J.
Fitz-Patrick, D.
Thomas, S. J. J.
Diya, O.
Lockhart, S.
Xu, X.
Zhang, Y.
Bangad, V
Schwartz, H. I. I.
Denham, D.
Cardona, J. F. F.
Usdan, L.
Ginis, J.
Mensa, F. J. J.
Zou, J.
Xie, X.
Shi, P. -Y
Lu, C.
Buitrago, S.
Scully, I. L. L.
Cooper, D.
Koury, K.
Jansen, K. U. U.
Tureci, O.
Sahin, U.
Swanson, K. A. A.
Gruber, W. C. C.
Kitchin, N.
NEW ENGLAND JOURNAL OF MEDICINE, 2023, 388 (03) : 214 - 227
[3] Antibody Response to Omicron BA.4-BA.5 Bivalent Booster
Wang, Qian
Bowen, Anthony
Valdez, Riccardo
Gherasim, Carmen
Gordon, Aubree
Liu, Lihong
Ho, David D. D.
NEW ENGLAND JOURNAL OF MEDICINE, 2023, 388 (06) : 567 - 569
[4] Cytokine and Chemokine Production in Mice Inoculated with NVX-CoV2373 (Nuvaxovid®) in Comparison with Omicron BA.4/5 Bivalent BNT162b2 (Comirnaty®)
Nakayama, Tetsuo
Ito, Takashi
Ishiyama, Ryoka
Katayama, Kazuhiko
VACCINES, 2023, 11 (11)
[5] Comparative Effectiveness of the Bivalent (Original/Omicron BA.4/BA.5) mRNA COVID-19 Vaccines mRNA-1273.222 and BNT162b2 Bivalent in Adults with Underlying Medical Conditions in the United States
Kopel, Hagit
Nguyen, Van Hung
Bogdanov, Alina
Winer, Isabelle
Boileau, Catherine
Ducruet, Thierry
Zeng, Ni
Winer-Jones, Jessamine P.
Esposito, Daina B.
Bausch-Jurken, Mary
Beck, Ekkehard
Bonafede, Machaon
Mansi, James A.
VACCINES, 2024, 12 (10)
[6] Humoral Immune Responses after an Omicron-Adapted Booster BNT162b2 Vaccination in Patients with Lymphoid Malignancies
Heftdal, Line Dam
Hansen, Cecilie Bo
Hamm, Sebastian Rask
Perez-Alos, Laura
Fogh, Kamille
Pries-Heje, Mia
Hasselbalch, Rasmus Bo
Moller, Dina Leth
Gang, Anne Ortved
Ostrowski, Sisse Rye
Frikke-Schmidt, Ruth
Sorensen, Erik
Hilsted, Linda
Bundgaard, Henning
Garred, Peter
Iversen, Kasper
Sabin, Caroline
Nielsen, Susanne Dam
Gronbaek, Kirsten
VIRUSES-BASEL, 2024, 16 (01):
[7] Immunogenicity of Omicron BA.1-adapted BNT162b2 vaccines: randomized trial, 3-month follow-up
Barda, Noam
Lustig, Yaniv
Indenbaum, Victoria
Zibly, Daniel
Joseph, Gili
Asraf, Keren
Weiss-Ottolenghi, Yael
Amit, Sharon
Kliker, Limor
Abd Elkader, Bayan
Ben-Ami, Eytan
Canetti, Michal
Koren, Ravit
Katz-Likvornik, Shiri
Halpern, Osnat
Mendelson, Ella
Doolman, Ram
Harats, Dror
Kreiss, Yitshak
Mandelboim, Michal
Regev-Yochay, Gili
CLINICAL MICROBIOLOGY AND INFECTION, 2023, 29 (07) : 918 - 923
[8] Effects of a booster dose of BNT162b2 on spike-binding antibodies to SARS-CoV-2 Omicron BA.2, BA.3, BA.4 and BA.5 subvariants in infection-na?ve and previously-infected individuals
Kuzel, Timothy G.
Fu, Jia
Anderson, Mark
Stec, Michael
Boler, Michael
Behun, Dylan
Gosha, Amy
Cloherty, Gavin
Landay, Alan
Moy, James
VACCINE, 2023, 41 (04) : 879 - 882
[9] Omicron BA.1 neutralizing antibody response following Delta breakthrough infection compared with booster vaccination of BNT162b2
Shohei Yamamoto
Kouki Matsuda
Kenji Maeda
Yusuke Oshiro
Natsumi Inamura
Tetsuya Mizoue
Maki Konishi
Junko S. Takeuchi
Kumi Horii
Mitsuru Ozeki
Haruhito Sugiyama
Hiroaki Mitsuya
Wataru Sugiura
Norio Ohmagari
BMC Infectious Diseases, 23
[10] Second booster dose improves antibody neutralization against BA.1, BA.5 and BQ.1.1 in individuals previously immunized with CoronaVac plus BNT162B2 booster protocol
Campos, Guilherme R. F.
Almeida, Nathalie Bonatti Franco
Filgueiras, Priscilla Soares
Corsini, Camila Amormino
Gomes, Sarah Vieira Contin
de Miranda, Daniel Alvim Pena
de Assis, Jessica Vieira
Silva, Thais Barbara de Souza
Alves, Pedro Augusto
Fernandes, Gabriel da Rocha
de Oliveira, Jaquelline Germano
Rahal, Paula
Grenfell, Rafaella Fortini Queiroz
Nogueira, Mauricio L.
FRONTIERS IN CELLULAR AND INFECTION MICROBIOLOGY, 2024, 14

← 1 2 3 4 5 →