Affinity is an important determinant of the anti-trypanosome activity of nanobodies.

BACKGROUND: The discovery of Nanobodies (Nbs) with a direct toxic activity against African trypanosomes is a recent advancement towards a new strategy against these extracellular parasites. The anti-trypanosomal activity relies on perturbing the highly active recycling of the Variant-specific Surfac...

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Main Authors: Guy Caljon, Benoît Stijlemans, Dirk Saerens, Jan Van Den Abbeele, Serge Muyldermans, Stefan Magez, Patrick De Baetselier
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS Neglected Tropical Diseases
Online Access:http://europepmc.org/articles/PMC3499403?pdf=render
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spelling doaj-3894b70394804fe885feec3f4191e6172020-11-25T02:45:27ZengPublic Library of Science (PLoS)PLoS Neglected Tropical Diseases1935-27271935-27352012-01-01611e190210.1371/journal.pntd.0001902Affinity is an important determinant of the anti-trypanosome activity of nanobodies.Guy CaljonBenoît StijlemansDirk SaerensJan Van Den AbbeeleSerge MuyldermansStefan MagezPatrick De BaetselierBACKGROUND: The discovery of Nanobodies (Nbs) with a direct toxic activity against African trypanosomes is a recent advancement towards a new strategy against these extracellular parasites. The anti-trypanosomal activity relies on perturbing the highly active recycling of the Variant-specific Surface Glycoprotein (VSG) that occurs in the parasite's flagellar pocket. METHODOLOGY/PRINCIPAL FINDINGS: Here we expand the existing panel of Nbs with anti-Trypanosoma brucei potential and identify four categories based on their epitope specificity. We modified the binding properties of previously identified Nanobodies Nb_An05 and Nb_An33 by site-directed mutagenesis in the paratope and found this to strongly affect trypanotoxicity despite retention of antigen-targeting properties. Affinity measurements for all identified anti-trypanosomal Nbs reveal a strong correlation between trypanotoxicity and affinity (K(D)), suggesting that it is a crucial determinant for this activity. Half maximal effective (50%) affinity of 57 nM was calculated from the non-linear dose-response curves. In line with these observations, Nb humanizing mutations only preserved the trypanotoxic activity if the K(D) remained unaffected. CONCLUSIONS/SIGNIFICANCE: This study reveals that the binding properties of Nanobodies need to be compatible with achieving an occupancy of >95% saturation of the parasite surface VSG in order to exert an anti-trypanosomal activity. As such, Nb-based approaches directed against the VSG target would require binding to an accessible, conserved epitope with high affinity.http://europepmc.org/articles/PMC3499403?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Guy Caljon
Benoît Stijlemans
Dirk Saerens
Jan Van Den Abbeele
Serge Muyldermans
Stefan Magez
Patrick De Baetselier
spellingShingle Guy Caljon
Benoît Stijlemans
Dirk Saerens
Jan Van Den Abbeele
Serge Muyldermans
Stefan Magez
Patrick De Baetselier
Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
PLoS Neglected Tropical Diseases
author_facet Guy Caljon
Benoît Stijlemans
Dirk Saerens
Jan Van Den Abbeele
Serge Muyldermans
Stefan Magez
Patrick De Baetselier
author_sort Guy Caljon
title Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
title_short Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
title_full Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
title_fullStr Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
title_full_unstemmed Affinity is an important determinant of the anti-trypanosome activity of nanobodies.
title_sort affinity is an important determinant of the anti-trypanosome activity of nanobodies.
publisher Public Library of Science (PLoS)
series PLoS Neglected Tropical Diseases
issn 1935-2727
1935-2735
publishDate 2012-01-01
description BACKGROUND: The discovery of Nanobodies (Nbs) with a direct toxic activity against African trypanosomes is a recent advancement towards a new strategy against these extracellular parasites. The anti-trypanosomal activity relies on perturbing the highly active recycling of the Variant-specific Surface Glycoprotein (VSG) that occurs in the parasite's flagellar pocket. METHODOLOGY/PRINCIPAL FINDINGS: Here we expand the existing panel of Nbs with anti-Trypanosoma brucei potential and identify four categories based on their epitope specificity. We modified the binding properties of previously identified Nanobodies Nb_An05 and Nb_An33 by site-directed mutagenesis in the paratope and found this to strongly affect trypanotoxicity despite retention of antigen-targeting properties. Affinity measurements for all identified anti-trypanosomal Nbs reveal a strong correlation between trypanotoxicity and affinity (K(D)), suggesting that it is a crucial determinant for this activity. Half maximal effective (50%) affinity of 57 nM was calculated from the non-linear dose-response curves. In line with these observations, Nb humanizing mutations only preserved the trypanotoxic activity if the K(D) remained unaffected. CONCLUSIONS/SIGNIFICANCE: This study reveals that the binding properties of Nanobodies need to be compatible with achieving an occupancy of >95% saturation of the parasite surface VSG in order to exert an anti-trypanosomal activity. As such, Nb-based approaches directed against the VSG target would require binding to an accessible, conserved epitope with high affinity.
url http://europepmc.org/articles/PMC3499403?pdf=render
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