Reference Database

YearReference
2020
IgG Subclasses Shape Cytokine Responses by Human Myeloid Immune Cells through Differential Metabolic Reprogramming.
Hoepel, Willianne
Allahverdiyeva, Sona
Harbiye, Haneen
de Taeye, Steven W
van der Ham, Alwin J
de Boer, Leonie
Zaat, Sebastiaan A J
van Weeghel, Michel
Baeten, Dominique L P
Houtkooper, Riekelt H
Everts, Bart
Vidarsson, Gestur
den Dunnen, Jeroen
J Immunol 2020 Dec 15;205 (12): 3400-3407
Abstract

IgG Abs are crucial for various immune functions, including neutralization, phagocytosis, and Ab-dependent cellular cytotoxicity. In this study, we identified another function of IgG by showing that IgG immune complexes elicit distinct cytokine profiles by human myeloid immune cells, which are dependent on FcγR activation by the different IgG subclasses. Using monoclonal IgG subclasses with identical Ag specificity, our data demonstrate that the production of Th17-inducing cytokines, such as TNF, IL-1β, and IL-23, is particularly dependent on IgG2, whereas type I IFN responses are controlled by IgG3, and IgG1 is able to regulate both. In addition, we identified that subclass-specific cytokine production is orchestrated at the posttranscriptional level through distinct glycolytic reprogramming of human myeloid immune cells. Combined, these data identify that IgG subclasses provide pathogen- and cell type-specific immunity through differential metabolic reprogramming by FcγRs. These findings may be relevant for future design of Ab-related therapies in the context of infectious diseases, chronic inflammation, and cancer.

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