Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.

Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.

A promising strategy for the enhancement of vaccine-mediated immune responses is by directly targeting protein antigens to immune cells. Targeting of antigens to the dendritic cell (DC) molecule Clec9A has been shown to enhance antibody affinity and titers for model antigens, and influenza and enter...

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Main Authors: Hannah A D King, Christopher A Gonelli, Kirsteen M Tullett, Mireille H Lahoud, Damian F J Purcell, Heidi E Drummer, Pantelis Poumbourios, Rob J Center
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0220986
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spelling doaj-d564ce87a08a43f9a3a3f5e3be9de5282021-03-03T21:21:54ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01148e022098610.1371/journal.pone.0220986Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.Hannah A D KingChristopher A GonelliKirsteen M TullettMireille H LahoudDamian F J PurcellHeidi E DrummerPantelis PoumbouriosRob J CenterA promising strategy for the enhancement of vaccine-mediated immune responses is by directly targeting protein antigens to immune cells. Targeting of antigens to the dendritic cell (DC) molecule Clec9A has been shown to enhance antibody affinity and titers for model antigens, and influenza and enterovirus antigens, and may be advantageous for immunogens that otherwise fail to elicit antibodies with sufficient titers and breadth for broad protection, such as the envelope protein (Env) of HIV. Previously employed targeting strategies often utilize receptor-specific antibodies, however it is impractical to conjugate a bivalent IgG antibody to oligomeric antigens, including HIV Env trimers. Here we designed single chain variable fragment (scFv) and single chain Fab (scFab) constructs of a Clec9A-targeting antibody, expressed as genetically fused conjugates with the soluble ectodomain of Env, gp140. This conjugation did not affect the presentation of Env neutralising antibody epitopes. The scFab moiety was shown to be more stable than scFv, and in the context of gp140 fusions, was able to mediate better binding to recombinant and cell surface-expressed Clec9A, although the level of binding to cell-surface Clec9A was lower than that of the anti-Clec9A IgG. However, binding to Clec9A on the surface of DCs was not detected. Mouse immunization experiments suggested that the Clec9A-binding activity of the scFab-gp140 conjugate was insufficient to enhance Env-specific antibody responses. This is an important first proof of principle study demonstrating the conjugation of a scFab to an oligomeric protein antigen, and that an scFab displays better antigen binding than the corresponding scFv. Future developments of this technique that increase the scFab affinity will provide a valuable means to target oligomeric proteins to cell surface antigens of interest, improving vaccine-generated immune responses.https://doi.org/10.1371/journal.pone.0220986
collection DOAJ
language English
format Article
sources DOAJ
author Hannah A D King
Christopher A Gonelli
Kirsteen M Tullett
Mireille H Lahoud
Damian F J Purcell
Heidi E Drummer
Pantelis Poumbourios
Rob J Center
spellingShingle Hannah A D King
Christopher A Gonelli
Kirsteen M Tullett
Mireille H Lahoud
Damian F J Purcell
Heidi E Drummer
Pantelis Poumbourios
Rob J Center
Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
PLoS ONE
author_facet Hannah A D King
Christopher A Gonelli
Kirsteen M Tullett
Mireille H Lahoud
Damian F J Purcell
Heidi E Drummer
Pantelis Poumbourios
Rob J Center
author_sort Hannah A D King
title Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
title_short Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
title_full Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
title_fullStr Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
title_full_unstemmed Conjugation of an scFab domain to the oligomeric HIV envelope protein for use in immune targeting.
title_sort conjugation of an scfab domain to the oligomeric hiv envelope protein for use in immune targeting.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2019-01-01
description A promising strategy for the enhancement of vaccine-mediated immune responses is by directly targeting protein antigens to immune cells. Targeting of antigens to the dendritic cell (DC) molecule Clec9A has been shown to enhance antibody affinity and titers for model antigens, and influenza and enterovirus antigens, and may be advantageous for immunogens that otherwise fail to elicit antibodies with sufficient titers and breadth for broad protection, such as the envelope protein (Env) of HIV. Previously employed targeting strategies often utilize receptor-specific antibodies, however it is impractical to conjugate a bivalent IgG antibody to oligomeric antigens, including HIV Env trimers. Here we designed single chain variable fragment (scFv) and single chain Fab (scFab) constructs of a Clec9A-targeting antibody, expressed as genetically fused conjugates with the soluble ectodomain of Env, gp140. This conjugation did not affect the presentation of Env neutralising antibody epitopes. The scFab moiety was shown to be more stable than scFv, and in the context of gp140 fusions, was able to mediate better binding to recombinant and cell surface-expressed Clec9A, although the level of binding to cell-surface Clec9A was lower than that of the anti-Clec9A IgG. However, binding to Clec9A on the surface of DCs was not detected. Mouse immunization experiments suggested that the Clec9A-binding activity of the scFab-gp140 conjugate was insufficient to enhance Env-specific antibody responses. This is an important first proof of principle study demonstrating the conjugation of a scFab to an oligomeric protein antigen, and that an scFab displays better antigen binding than the corresponding scFv. Future developments of this technique that increase the scFab affinity will provide a valuable means to target oligomeric proteins to cell surface antigens of interest, improving vaccine-generated immune responses.
url https://doi.org/10.1371/journal.pone.0220986
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