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» Articles » PMID: 32402284

A Non-structural 1 Protein G53D Substitution Attenuates a Clinically Tested Live Dengue Vaccine

Overview
Journal Cell Rep
Publisher Cell Press
Specialties Biology
Cell Biology
Molecular Biology
Date 2020 May 14
PMID 32402284
Citations 10
Authors
Milly M Choy
Dorothy H L Ng
Tanamas Siriphanitchakorn
Wy Ching Ng
Karin B Sundstrom
Hwee Cheng Tan
Summer L Zhang
Kitti W K Chan
Menchie Manuel
R Manjunatha Kini
Kuan Rong Chan
Subhash G Vasudevan
Eng Eong Ooi
Affiliations
Soon will be listed here.
Abstract

The molecular basis of dengue virus (DENV) attenuation remains ambiguous and hampers a targeted approach to derive safe but nonetheless immunogenic live vaccine candidates. Here, we take advantage of DENV serotype 2 PDK53 vaccine strain, which recently and successfully completed a phase-3 clinical trial, to identify how this virus is attenuated compared to its wild-type parent, DENV2 16681. Site-directed mutagenesis on a 16681 infectious clone identifies a single G53D substitution in the non-structural 1 (NS1) protein that reduces 16681 infection and dissemination in both Aedes aegypti, as well as in mammalian cells to produce the characteristic phenotypes of PDK53. Mechanistically, NS1 G53D impairs the function of a known host factor, the endoplasmic reticulum (ER)-resident ribophorin 1 protein, to properly glycosylate NS1 and thus induce a host antiviral gene through ER stress responses. Our findings provide molecular insights on DENV attenuation on a clinically tested strain.

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