2019
DOI: 10.1038/s41598-019-46484-2
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Human DC-SIGN and CD23 do not interact with human IgG

Abstract: The precise mechanisms underlying anti-inflammatory effects of intravenous immunoglobulin (IVIg) therapies remain elusive. The sialylated IgG fraction within IVIg has been shown to be therapeutically more active in mouse models. Functionally, it has been suggested that IgG undergoes conformational changes upon Fc-sialylation which sterically impede binding to conventional FcγRs, but simultaneously allow binding to human DC-SIGN (SIGN-R1 in mice) and also CD23. These latter C-type lectins have been proposed res… Show more

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Cited by 44 publications
(25 citation statements)
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“…However, other studies have challenged this hypothesis. The evidence of a direct interaction between sialylated IgG and DC-SIGN is not fully supported in the literature (66,67). Moreover, there is conflicting evidence suggesting that the sialylated Fc fragment of IgG is dispensable for the anti-inflammatory mechanisms of high-dose IVIg (68)(69)(70)(71)(72).…”
Section: Upregulation Of the Inhibitory Fcγriib And Increase In The Amentioning
confidence: 99%
See 1 more Smart Citation
“…However, other studies have challenged this hypothesis. The evidence of a direct interaction between sialylated IgG and DC-SIGN is not fully supported in the literature (66,67). Moreover, there is conflicting evidence suggesting that the sialylated Fc fragment of IgG is dispensable for the anti-inflammatory mechanisms of high-dose IVIg (68)(69)(70)(71)(72).…”
Section: Upregulation Of the Inhibitory Fcγriib And Increase In The Amentioning
confidence: 99%
“…It has been proposed that sialylated IgG binds to DC-SIGN in addition to CD23, a C-type lectin which is also a known low-affinity IgE receptor characteristically expressed on B cells, inducing the suppression of B cells (189). However, there has been disagreement as to whether there is a direct interaction between IgG and DC-SIGN/CD23 (67,190). A further proposed mechanism of action of high-dose IVIg is the interaction between the sialylated Fc fragment of IgG and CD22, an I-type lectin expressed on B cells, which results in the activation of the ITIM signaling cascade, subsequently promoting B cell apoptosis (183,191,192).…”
Section: B Lymphocytesmentioning
confidence: 99%
“…All of them belong to the superfamily of CLRs unified by the structural feature of the C-type lectin domain. Nevertheless, it has at least to be noted that the IgG binding capability of DC-SIGN and FcεRII has recently been challenged (125).…”
Section: The Low Affinity Ige Receptor Fcεrii (Cd23)mentioning
confidence: 99%
“…They further differ in their intracellular motifs responsible for receptor internalization, cycling and signaling [summarized in ( 121 )]. Because of this complexity, here we will focus only on the three so far described type II FcRs, DC-SIGN (CD209), Dectin-1 (CLEC7A) and Fcε receptor II (FcεRII; CD23) characterized by the ability to bind immunoglobulins ( Figure 2 ) although this is a current matter of debate ( 119 , 122 125 ).…”
Section: Properties and Expression Of Type II Fc Receptorsmentioning
confidence: 99%
“…Recent reports have thoroughly screened these effects making use of large glycan arrays, evidencing striking affinity changes sometimes arising from remote chemical modifications. [91][92][93] As examples, the presence of terminal sialylation completely abrogates recognition, [92] as well as the elongation of the GlcNAc 2 Man 3 GlcNAc 2 scaffold with Galβ1-4, although the negative effect is asymmetric, given that the presence of one unique Gal moiety at the α1-6 branch still permits a weak binding (Figure 4, left). [91,93] Similarly, bisecting residues and double core fucosylation at the reducing end of the chitobiose disaccharide also produce an affinity loss in general.…”
Section: Relevant Interacting Monosaccharides and Glycansmentioning
confidence: 99%