Analysis of CD8 T Cell Response During the 2013-2016 Ebola Epidemic in West Africa

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2018 Jul 25

PMID 30038008

Citations 40

Authors

Saori Sakabe

Brian M Sullivan

Jessica N Hartnett

Refugio Robles-Sikisaka

Karthik Gangavarapu

Beatrice Cubitt

Brian C Ware

Dylan Kotliar

Luis M Branco

Augustine Goba

Mambu Momoh

John Demby Sandi

Lansana Kanneh

Donald S Grant

Robert F Garry

Kristian G Andersen

Juan Carlos de la Torre

Pardis C Sabeti

John S Schieffelin

Michael B A Oldstone

Affiliations

Soon will be listed here.

Abstract

The recent Ebola epidemic exemplified the importance of understanding and controlling emerging infections. Despite the importance of T cells in clearing virus during acute infection, little is known about Ebola-specific CD8 T cell responses. We investigated immune responses of individuals infected with Ebola virus (EBOV) during the 2013-2016 West Africa epidemic in Sierra Leone, where the majority of the >28,000 EBOV disease (EVD) cases occurred. We examined T cell memory responses to seven of the eight Ebola proteins (GP, sGP, NP, VP24, VP30, VP35, and VP40) and associated HLA expression in survivors. Of the 30 subjects included in our analysis, CD8 T cells from 26 survivors responded to at least one EBOV antigen. A minority, 10 of 26 responders (38%), made CD8 T cell responses to the viral GP or sGP. In contrast, 25 of the 26 responders (96%) made response to viral NP, 77% to VP24 (20 of 26), 69% to VP40 (18 of 26), 42% (11 of 26) to VP35, with no response to VP30. Individuals making CD8 T cells to EBOV VP24, VP35, and VP40 also made CD8 T cells to NP, but rarely to GP. We identified 34 CD8 T cell epitopes for Ebola. Our data indicate the immunodominance of the EBOV NP-specific T cell response and suggest that its inclusion in a vaccine along with the EBOV GP would best mimic survivor responses and help boost cell-mediated immunity during vaccination.

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