Immunogenicity of standard and extended dosing intervals of BNT162b2 mRNA vaccine

Abuelgasim, H; Adele, S; Adland, E; Adlou, S; Akther, HD; Al-Taei, S; Alhussni, A; Ali, M; Altmann, T; Amini, A; Angyal, A; Ansari, MA; Arancibia-Cárcamo, CV; Austin, JA; Barnes, E; Bayley, M; Bridges-Webb, A; Brown, A; Brown, H; Brown, R; Carroll, M; Chalk, J; Chand, M; Chawla, A; Chinnakannan, S; Conlon, CP; Cross, A; Cutteridge, J; de Lara, C; de Silva, TI; Deeks, AS; Dejnirattisai, W; Denly, L; Diffey, B; Dimitriadis, S; Dobson, SL; Dold, C; Donnison, T; Drake, TM; Dunachie, S; Duncan, CJA; Dupont, M; Eyre, D; Fairman, A; Faustini, S; Foulkes, S; Frater, J; Gardiner, S; Gilbert-Jarmillo, J; Gillson, N; Goulder, P; Hackstein, C-P; Hall, V; Hambleton, S; Haniffa, M; Hargreaves, A; Haworth, J; Hering, LM; Holmes, J; Hopkins, S; Horner, E; Hornsby, H; Jeffery, K; Johnson, S; Johnson, S; Jones, C; Jämsén, A; Kasanyinga, M; Kelly, S; Kilby, JA; Kirk, R; Klenerman, P; Knight, ML; Lawrie, A; Lee, L; Lett, L; Lillie, K; Lim, N; Linder, A; Longet, S; Malone, T; Matthews, PC; Meardon, N; Mehta, H; Mentzer, AJ; Mongkolsapaya, J; Moore, SC; Nicols, AR; Ogbe, A; O’Donnell, D; Pace, M; Payne, BAI; Payne, RP; Phillips, E; Platt, G; Pollard, AJ; Poolan, S; Provine, N; Ramamurthy, N; Reyes, LS; Richter, A; Robinson, N; Romaniuk, L; Rongkard, P; Rowland-Jones, SL; Saei, A; Sampson, OL; Sandhar, G; Screaton, G; Shields, A; Simmons, B; Skelly, DT; Spegarova, JS; Stafford, L; Stephenson, E; Subramaniam, K; Supasa, P; Thaventhiran, J; Thomas, S; Tipton, T; Travis, S; Tucker, S; Turtle, L; Turton, H; Tyerman, JK; Watson, A; Watson, L; Weeks, E; Whitham, R; Wilson, R; Wood, S; Wootton, DG; Wright, R; Xiao, H; Zawia, AAT

Immunogenicity of standard and extended dosing intervals of BNT162b2 mRNA vaccine

Authors: H Abuelgasim
S Adele
E Adland
S Adlou
HD Akther
S Al-Taei
A Alhussni
M Ali
T Altmann
A Amini
A Angyal
MA Ansari
CV Arancibia-Cárcamo
JA Austin
E Barnes
M Bayley
A Bridges-Webb
A Brown
H Brown
R Brown
M Carroll
J Chalk
M Chand
A Chawla
S Chinnakannan
CP Conlon
A Cross
J Cutteridge
C de Lara
TI de Silva
AS Deeks
W Dejnirattisai
L Denly
B Diffey
S Dimitriadis
SL Dobson
C Dold
T Donnison
TM Drake
S Dunachie
CJA Duncan
M Dupont
D Eyre
A Fairman
S Faustini
S Foulkes
J Frater
S Gardiner
J Gilbert-Jarmillo
N Gillson
P Goulder
C-P Hackstein
V Hall
S Hambleton
M Haniffa
A Hargreaves
J Haworth
LM Hering
J Holmes
S Hopkins
E Horner
H Hornsby
K Jeffery
S Johnson
S Johnson
C Jones
A Jämsén
M Kasanyinga
S Kelly
JA Kilby
R Kirk
P Klenerman
ML Knight
A Lawrie
L Lee
L Lett
K Lillie
N Lim
A Linder
S Longet
T Malone
PC Matthews
N Meardon
H Mehta
AJ Mentzer
J Mongkolsapaya
SC Moore
AR Nicols
A Ogbe
D O’Donnell
M Pace
BAI Payne
RP Payne
E Phillips
G Platt
AJ Pollard
S Poolan
N Provine
N Ramamurthy
LS Reyes
A Richter
N Robinson
L Romaniuk
P Rongkard
SL Rowland-Jones
A Saei
OL Sampson
G Sandhar
G Screaton
A Shields
B Simmons
DT Skelly
JS Spegarova
L Stafford
E Stephenson
K Subramaniam
P Supasa
J Thaventhiran
S Thomas
T Tipton
S Travis
S Tucker
L Turtle
H Turton
JK Tyerman
A Watson
L Watson
E Weeks
R Whitham
R Wilson
S Wood
DG Wootton
R Wright
H Xiao
AAT Zawia
Publication date: 1 January 2021
Publisher: 'Elsevier BV'
Doi

Abstract

Extension of the interval between vaccine doses for the BNT162b2 mRNA vaccine was introduced in the United Kingdom to accelerate population coverage with a single dose. At this time, trial data were lacking, and we addressed this in a study of United Kingdom healthcare workers. The first vaccine dose induced protection from infection from the circulating alpha (B.1.1.7) variant over several weeks. In a substudy of 589 individuals, we show that this single dose induces severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) neutralizing antibody (NAb) responses and a sustained B and T cell response to the spike protein. NAb levels were higher after the extended dosing interval (6–14 weeks) compared with the conventional 3- to 4-week regimen, accompanied by enrichment of CD4+ T cells expressing interleukin-2 (IL-2). Prior SARS-CoV-2 infection amplified and accelerated the response. These data on dynamic cellular and humoral responses indicate that extension of the dosing interval is an effective immunogenic protocol