mRNA vaccine boosting enhances antibody responses against SARS-CoV-2 Omicron variant in patients with antibody deficiency syndromes

Ofer Zimmerman
Alexa Michelle Altman Doss
Paulina Kaplonek
Laura A. VanBlargan
Chieh-Yu Liang
Rita E. Chen
Jennifer Marie Monroy
H. James Wedner
Anthony Kulczycki
Tarisa L. Mantia
Caitlin C. O’Shaughnessy
Hannah G. Davis-Adams
Harry L. Bertera
Lucas J. Adams
Saravanan Raju
Fang R. Zhao
Christopher J. Rigell
Tiffany Biason Dy
Andrew L. Kau
Zhen Ren
Jackson Turner
Jane A. O’Halloran
Rachel M. Presti
Daved H Fremont
Peggy L. Kendall
Ali H. Ellebedy
Galit Alter
Michael S. Diamond

1 evaluations Published on Jan 28, 2022

This article on Sciety

Abstract

Patients with primary antibody deficiency syndromes (PAD) have poor humoral immune responses requiring immunoglobulin replacement therapy. We followed PAD patients after SARS-CoV-2 vaccination by evaluating their immunoglobulin replacement products and serum for anti-spike binding, FcγR binding, and neutralizing activities. Immunoglobulin replacement products had low anti-spike and receptor binding domain (RBD) titers and neutralizing activity. In COVID-19-naive PAD patients, anti-spike and RBD titers increased after mRNA vaccination but decreased to pre-immunization levels by 90 days. Patients vaccinated after SARS-CoV-2 infection developed higher responses comparable to healthy donors. Most vaccinated PAD patients had serum neutralizing antibody titers above an estimated correlate of protection against ancestral SARS-CoV-2 and Delta virus but not against Omicron virus, although this was improved by boosting. Thus, currently used immunoglobulin replacement products likely have limited protective activity, and immunization and boosting of PAD patients with mRNA vaccines should confer at least short-term immunity against SARS-CoV-2 variants, including Omicron.

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