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Merck
  • Maternal Anti-Dengue IgG Fucosylation Predicts Susceptibility to Dengue Disease in Infants.

Maternal Anti-Dengue IgG Fucosylation Predicts Susceptibility to Dengue Disease in Infants.

Cell reports (2020-05-14)
Natalie K Thulin, R Camille Brewer, Robert Sherwood, Stylianos Bournazos, Karlie G Edwards, Nitya S Ramadoss, Jeffery K Taubenberger, Matthew Memoli, Andrew J Gentles, Prasanna Jagannathan, Sheng Zhang, Daniel H Libraty, Taia T Wang
摘要

Infant mortality from dengue disease is a devastating global health burden that could be minimized with the ability to identify susceptibility for severe disease prior to infection. Although most primary infant dengue infections are asymptomatic, maternally derived anti-dengue immunoglobulin G (IgGs) present during infection can trigger progression to severe disease through antibody-dependent enhancement mechanisms. Importantly, specific characteristics of maternal IgGs that herald progression to severe infant dengue are unknown. Here, we define ≥10% afucosylation of maternal anti-dengue IgGs as a risk factor for susceptibility of infants to symptomatic dengue infections. Mechanistic experiments show that afucosylation of anti-dengue IgGs promotes FcγRIIIa signaling during infection, in turn enhancing dengue virus replication in FcγRIIIa+ monocytes. These studies identify a post-translational modification of anti-dengue IgGs that correlates with risk for symptomatic infant dengue infections and define a mechanism by which afucosylated antibodies and FcγRIIIa enhance dengue infections.

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Sigma-Aldrich
ELISA 用 3,3′,5,5′-四甲基联苯胺 (TMB) 液体底物系统, peroxidase substrate
Sigma-Aldrich
用于ELISA的碱性磷酸酶黄色(pNPP)液体底物系统, ready to use solution
Sigma-Aldrich
岩藻糖基转移酶抑制剂,2F-过乙酰基-岩藻糖, 2F-Peracetyl-Fucose is a cell-permeable fluorinated fucose derivative that acts as an inhibitor of fucosyltransferases following its uptake and metabolic transformation into a GDP-fucose mimetic.