2014
DOI: 10.1074/jbc.m113.537563
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Structural Insights into Neonatal Fc Receptor-based Recycling Mechanisms

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Cited by 213 publications
(318 citation statements)
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“…Given that amino acid residues involved in FcRn binding, such as M252 and I253, are located on the 250-helix, the observed displacement of the helix is expected to influence the affinity of Fc for FcRn. 20 Furthermore, the difference in the relative orientation of CH2 with respect to CH3 highlights the dynamic nature of the CH2-CH3 domains at different pHs (Supplementary Figure 1). 22 Recently, deuterium exchange studies of human Fc were performed in the absence or presence of FcRn.…”
Section: Resultsmentioning
confidence: 99%
See 1 more Smart Citation
“…Given that amino acid residues involved in FcRn binding, such as M252 and I253, are located on the 250-helix, the observed displacement of the helix is expected to influence the affinity of Fc for FcRn. 20 Furthermore, the difference in the relative orientation of CH2 with respect to CH3 highlights the dynamic nature of the CH2-CH3 domains at different pHs (Supplementary Figure 1). 22 Recently, deuterium exchange studies of human Fc were performed in the absence or presence of FcRn.…”
Section: Resultsmentioning
confidence: 99%
“…Mutation of either of the two histidine residues significantly reduces the binding affinity of Fc with FcRn. 20,21 In addition to His310 and His435, several other Fc residues are involved in making molecular contacts with FcRn (Figure 1).
10.1080/19420862.2018.1490119-F0001Figure 1.( top ) Structural view of human IgG CH2-CH3 domains ( yellow ) in complex with human FcRn α ( green ) and β2M ( cyan ) domains.
…”
Section: Resultsmentioning
confidence: 99%
“…The 1519.g57 Fab’ binding site on human FcRn in solution was determined by HDX and was consistent with that determined by X-ray crystallography (data not shown).
10.1080/19420862.2018.1505464-F0001Figure 1.Crystal structure of complex of human FcRn (deglycosylated extracellular domain) and 1519.g57 Fab’. (A) The binding epitope of 1519.g57 Fab’ on FcRn α-chain is shown in red; (B) PDB 4N0U – human IgG Fc domain interacting with FcRn, demonstrating the overlapping epitope with that of 1519.g57Fab’, 29 (C) FcRn α-chain sequence, showing residues involved in interaction with 1519.g57 Fab’ (in red ). Residues involved in interaction between human FcRn and IgG (Fc domain) or albumin (as described by Oganesyan et al, 2014, highlighted in yellow or in blue, respectively) are also shown.
…”
Section: Resultsmentioning
confidence: 99%
“…Residues involved in interaction between human FcRn and IgG (Fc domain) or albumin (as described by Oganesyan et al, 2014, highlighted in yellow or in blue, respectively) are also shown. The sequence of human FcRn α-chain ECD was taken from Swiss Prot (P55899-1); Residue F44, identified by Oganesyan et al 29 as interacting with albumin, is residue E44 in this sequence and in the sequence of Schmidt et al 30 Dark blue = FcRn α-chain; pale blue = β2 M; magenta = 1519.g57 heavy chain; orange = 1519.g57 light chain; yellow = IgG Fc domain; red = 1519.g57 Fab’ binding epitope on FcRn.…”
Section: Resultsmentioning
confidence: 99%
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