Title
Whole-exome sequencing reveals insights into genetic susceptibility to congenital zika syndrome
Date Issued
01 June 2021
Access level
open access
Resource Type
journal article
Author(s)
Junior R.d.S.F.
Carvalho J.B.
Morais G.L.
Rossi Á.D.
Pezzuto P.
Azevedo G.S.
Schamber-Reis B.L.
Portari E.A.
Melo A.
Moreira M.E.L.
Guida L.C.
Cunha D.P.
Gomes L.
Vasconcelos Z.F.M.
Faucz F.R.
Tanuri A.
Stratakis C.A.
Aguiar R.S.
Cardoso C.C.
de Vasconcelos A.T.R.
Laboratório Nacional de Computação Científica LNCC/MCTIC Petrópolis
Publisher(s)
Public Library of Science
Abstract
Congenital Zika Syndrome (CZS) is a critical illness with a wide range of severity caused by Zika virus (ZIKV) infection during pregnancy. Life-threatening neurodevelopmental dysfunctions are among the most common phenotypes observed in affected newborns. Risk factors that contribute to susceptibility and response to ZIKV infection may be related to the virus itself, the environment, and maternal genetic background. Nevertheless, the newborn’s genetic contribution to the critical illness is still not elucidated. Here, we aimed to identify possible genetic variants as well as relevant biological pathways that might be associated with CZS phenotypes. For this purpose, we performed a whole-exome sequencing in 40 children born to women with confirmed exposure to ZIKV during pregnancy. We investigated the occurrence of rare harmful single-nucleotide variants (SNVs) possibly associated with inborn errors in genes ontologically related to CZS phenotypes. Moreover, an exome-wide association analysis was also performed using a case-control design (29 CZS cases and 11 controls), for both common and rare variants. Five out of the 29 CZS patients harbored known pathogenic variants likely to contribute to mild to severe manifestations observed. Approximately, 30% of affected individuals carried at least one pathogenic or likely pathogenic SNV in genes candidates to play a role in CZS. Our common variant association analysis detected a suggestive protective effect of the rs2076469 in DISP3 gene (p-value: 1.39 x 10−5). The IL12RB2 gene (p-value: 2.18x10-11) also showed an unusual distribution of non-synonymous rare SNVs in control samples. Finally, genes harboring harmful variants are involved in processes related to CZS phenotypes such as neurological development and immunity. Therefore, both rare and common variations may be likely to contribute as the underlying genetic cause of CZS susceptibility. The variations and pathways identified in this study may also have implications for the development of therapeutic strategies in the future.
Volume
15
Issue
6
Language
English
OCDE Knowledge area
Medicina tropical
Scopus EID
2-s2.0-85110251309
PubMed ID
Source
PLoS Neglected Tropical Diseases
ISSN of the container
19352727
Sponsor(s)
This research was supported by FINEP (grant no. 01.16.0078.00), partially supported by the European Union’s Horizon 2020 Research and Innovation Programme under ZIKAlliance Grant Agreement no. 734548. A.T.R.V. is supported by Conselho Nacional de Desenvolvimento Científico e Tecnológico-CNPq (303170/2017-4), and FAPERJ (26/202.903/20). R.S.A is supported by CNPq (439119/2018-9, 312688/2017-2) and FAPERJ (239765). C.C.C is supported by FAPERJ (E-26/ 202.791/2019 and E-26/010.002278/2019). Z.F.M. V is supported by “Research Incentive Program II (PIP II)”-approved by the research coordination of the Fernandes Figueira Institute (IFF / FIOCRUZ). C. A.S is supported by the intramural program of the Eunice Kennedy Shriver National Institute of Child Health & Human Development. V.B. is supported by RABICO/CAPES Project 88887.333817/2019-00. R.S.F.J is a recipient of a graduate fellowship from CNPq. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Sources of information:
Directorio de Producción Científica
Scopus