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Experimental and computational insights into the structural dynamics of the Fc fragment of IgG1 subtype from biosimilar VEGF-Trap

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Turkut, Engin
Aldeniz, Alper
Kang, Jungmin
Tosha, Takehiko
Yabashi, Makina
Yilmaz, Baris
Can Timucin, Ahmet
Matsuura, Hiroaki
Kawano, Yoshiaki
Cinkaya, Irfan

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Except where otherwised noted, this item's license is described as CC BY (Attribution)

Abstract

The constant fragment (Fc) of the immunoglobulin G1 (IgG1) subtype is increasingly recognized as a crucial scaffold in the development of advanced therapeutics due to its enhanced specificity, efficacy, and extended half-life. A prime example is VEGF-Trap (Aflibercept), a recombinant fusion protein that merges the Fc region of the IgG1 subtype with the binding domains of vascular endothelial growth factor receptors (VEGFR)-1 and VEGFR-2. The Fc region's role in N-glycosylation is particularly important, as it significantly influences protein stability. Herein, the first near-physiological temperature structures of the N-glycan-bound Fc fragment of IgG1 subtype from a biosimilar VEGF-Trap are presented, determined using the SPring-8 Angstrom Compact free electron LAser (SACLA) and the Turkish Light Source (Turkish DeLight). Comparative analysis with cryogenic structures, including existing data, reveals alternate conformations within the glycan-binding pocket. Furthermore, molecular dynamics simulations indicate the presence of a high degree of structural plasticity, explaining how the protein adapts its structure through conformational changes. The observed structural fluctuations/conformational changes demonstrate the effect of N-glycans on protein stability. These findings offer new insights into the molecular basis of Fc-mediated functions and provide valuable information for the design of next-generation therapeutics.

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Wiley

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Chemistry, Science and technology - other topics, Materials science

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