A single birth dose of Hepatitis B vaccine induces polyfunctional CD4+ T helper cells

Author:

Strandmark Julia,Darboe Alansana,Diray-Arce Joann,Ben-Othman Rym,Vignolo Sofia M.,Rao Shun,Smolen Kinga K.,Leroux-Roels Geert,Idoko Olubukola T.,Sanchez-Schmitz Guzmán,Ozonoff Al,Levy Ofer,Kollmann Tobias R.,Marchant Arnaud,Kampmann Beate

Abstract

A single birth-dose of Hepatitis B vaccine (HepB) can protect newborns from acquiring Hepatitis B infection through vertical transmission, though several follow-up doses are required to induce long-lived protection. In addition to stimulating antibodies, a birth-dose of HepB might also induce polyfunctional CD4+T-cells, which may contribute to initial protection. We investigated whether vaccination with HepB in the first week of life induced detectable antigen-specific CD4+T-cells after only a single dose and following completion of the entire HepB vaccine schedule (3 doses). Using HBsAg- stimulated peripheral blood mononuclear cells from 344 infants, we detected increased populations of antigen-specific polyfunctional CD154+IL-2+TNFα+CD4+T-cells following a single birth-dose of HepB in a proportion of infants. Frequencies of polyfunctional T-cells increased following the completion of the HepB schedule but increases in the proportion of responders as compared to following only one dose was marginal. Polyfunctional T-cells correlated positively with serum antibody titres following the birth dose (day30) and completion of the 3-dose primary HepB vaccine series (day 128). These data indicate that a single birth dose of HepB provides immune priming for both antigen-specific B- and T cells

Funder

National Institutes of Health

Publisher

Frontiers Media SA

Subject

Immunology,Immunology and Allergy

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