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Serum Metabolic Alterations upon Zika Infection

Authors :: Carlos Fernando O. R. Melo
Jeany Delafiori
Diogo N. de Oliveira
Tatiane M. Guerreiro
Cibele Z. Esteves
Estela de O. Lima
Victoria Pando-Robles
Rodrigo R. Catharino
the Zika-Unicamp Network
Guilherme P. Milanez
Gabriela M. do Nascimento
André R. R. Freitas
Rodrigo Angerami
Fábio T. Maranhão Costa
Clarice W. Arns
Mariangela R. Resende
Eliana Amaral
Renato P. Junior
Carolina C. Ribeiro-do-Valle
Helaine Milanez
Maria L. Moretti
Jose L. Proenca-Modena
Glaucia M. Pastore
Kleber Y. Fertrin
Márcia T. Garcia
Roseli Calil
João R. B. Júnior
Giuliane J. Lajos
Maria L. Costa
Marcos T. N. da Silva
Albina Altemani
Ana C. Coan
Maria F. Colella-Santos
Andrea P. B. von Zuben
Marco A. R. Vinolo
Rosemeire F. de O. de Paula
Carla C. Judice
Juliana A. Leite
Leonardo C. Caserta
Ana P. de Moraes
Ana C. S. Barnabé
Ana L. R. da Soledade
Daniel A. T. Teixeira
Évellyn R. de Morais
Felipe R. Santos
Source :: Frontiers in Microbiology, Vol 8 (2017)
Publication Year :: 2017
Publisher :: Frontiers Media S.A., 2017.
Abstract: Zika virus (ZIKV) infection has recently emerged as a major concern worldwide due to its strong association with nervous system malformation (microcephaly) of fetuses in pregnant women infected by the virus. Signs and symptoms of ZIKV infection are often mistaken with other common viral infections. Since transmission may occur through biological fluids exchange and coitus, in addition to mosquito bite, this condition is an important infectious disease. Thus, understanding the mechanism of viral infection has become an important research focus, as well as providing potential targets for assertive clinical diagnosis and quality screening for hemoderivatives. Within this context, the present work analyzed blood plasma from 79 subjects, divided as a control group and a ZIKV-infected group. Samples underwent direct-infusion mass spectrometry and statistical analysis, where eight markers related to the pathophysiological process of ZIKV infection were elected and characterized. Among these, Angiotensin (1-7) and Angiotensin I were upregulated under infection, showing an attempt to induce autophagy of the infected cells. However, this finding is concerning about hypertensive individuals under treatment with inhibitors of the Renin-Angiotensin System (RAS), which could reduce this response against the virus and exacerbate the symptoms of the infection. Moreover, one of the most abundant glycosphingolipids in the nervous tissue, Ganglioside GM2, was also elected in the present study as an infection biomarker. Considered an important pathogen receptor at membrane's outer layer, this finding represents the importance of gangliosides for ZIKV infection and its association with brain tropism. Furthermore, a series of phosphatidylinositols were also identified as biomarkers, implying a significant role of the PI3K-AKT-mTOR Pathway in this mechanism. Finally, these pathways may also be understood as potential targets to be considered in pharmacological intervention studies on ZIKV infection management.