Identification of a Zika NS2B epitope as a biomarker for severe clinical phenotypes

Felix F. Loeffler; Isabelle F. T. Viana; Nico Fischer; Danilo F. Coêlho; Carolina S. Silva; Antônio F. Purificação; Catarina M. C. S. Araújo; Bruno H. S. Leite; Ricardo Durães-Carvalho; Tereza Magalhães; Clarice N. L. Morais; Marli T. Cordeiro; Roberto D. Lins; Ernesto T. A. Marques; Thomas Jaenisch

doi:10.1039/D1MD00124H

Identification of a Zika NS2B epitope as a biomarker for severe clinical phenotypes†

Felix F. Loeffler,

‡^a Isabelle F. T. Viana,

‡^b Nico Fischer,^c Danilo F. Coêlho,

^bd Carolina S. Silva,

^e Antônio F. Purificação, Jr.,^b Catarina M. C. S. Araújo,^b Bruno H. S. Leite,^b Ricardo Durães-Carvalho,

^f Tereza Magalhães,^b Clarice N. L. Morais,^b Marli T. Cordeiro,^b Roberto D. Lins,

§^b Ernesto T. A. Marques

§^bg and Thomas Jaenisch §*^ch

Author affiliations

* Corresponding authors

^a Max Planck Institute of Colloids and Interfaces, Department of Biomolecular Systems, Potsdam, Germany

^b Department of Virology, Aggeu Magalhães Institute, Oswaldo Cruz Foundation, Recife, PE, Brazil

^c Section Clinical Tropical Medicine, Department of Infectious Diseases, Heidelberg University Hospital, Germany
E-mail: thomas.jaenisch@urz.uni-heidelberg.de

^d Department of Fundamental Chemistry, Federal University of Pernambuco, Recife, PE, Brazil

^e Department of Chemical Engineering, Federal University of Pernambuco, Recife, PE, Brazil

^f Laboratory of Virology, University of Campinas, Campinas, SP, Brazil

^g Department of Infectious Diseases and Microbiology, University of Pittsburgh, Pittsburgh, PA, USA

^h German Centre for Infection Research (DZIF), Heidelberg Site, Heidelberg, Germany

Abstract

The identification of specific biomarkers for Zika infection and its clinical complications is fundamental to mitigate the infection spread, which has been associated with a broad range of neurological sequelae. We present the characterization of antibody responses in serum samples from individuals infected with Zika, presenting non-severe (classical) and severe (neurological disease) phenotypes, with high-density peptide arrays comprising the Zika NS1 and NS2B proteins. The data pinpoints one strongly IgG-targeted NS2B epitope in non-severe infections, which is absent in Zika patients, where infection progressed to the severe phenotype. This differential IgG profile between the studied groups was confirmed by multivariate data analysis. Molecular dynamics simulations and circular dichroism have shown that the peptide in solution presents itself in a sub-optimal conformation for antibody recognition, which led us to computationally engineer an artificial protein able to stabilize the NS2B epitope structure. The engineered protein was used to interrogate paired samples from mothers and their babies presenting Zika-associated microcephaly and confirmed the absence of NS2B IgG response in those samples. These findings suggest that the assessment of antibody responses to the herein identified NS2B epitope is a strong candidate biomarker for the diagnosis and prognosis of Zika-associated neurological disease.

RSC Medicinal Chemistry

Identification of a Zika NS2B epitope as a biomarker for severe clinical phenotypes†

Abstract

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Identification of a Zika NS2B epitope as a biomarker for severe clinical phenotypes

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