Probing IgG1 FC-Multimodal Nanoparticle Interactions: A Combined Nuclear Magnetic Resonance and Molecular Dynamics Simulations Approach

Ronak B Gudhka; Mayank Vats; Camille L Bilodeau; Scott A McCallum; Mark A McCoy; David J Roush; Mark A Snyder; Steven M Cramer

doi:10.1021/acs.langmuir.1c02114

Probing IgG1 F_C-Multimodal Nanoparticle Interactions: A Combined Nuclear Magnetic Resonance and Molecular Dynamics Simulations Approach

Langmuir. 2021 Oct 19;37(41):12188-12203. doi: 10.1021/acs.langmuir.1c02114. Epub 2021 Oct 11.

Authors

Ronak B Gudhka, Mayank Vats, Camille L Bilodeau, Scott A McCallum, Mark A McCoy¹, David J Roush², Mark A Snyder³, Steven M Cramer

Affiliations

¹ Mass Spectrometry & Biophysics, Merck & Co., Inc., 2000 Galloping Hill Road, Kenilworth, New Jersey 07033, United States.
² Biologics Process R&D, Downstream Purification Development and Engineering, Merck & Co., Inc., 2000 Galloping Hill Road, Kenilworth, New Jersey 07033, United States.
³ Process Chemistry Division, Bio-Rad Laboratories, Hercules, California 94547, United States.

PMID: 34633195
DOI: 10.1021/acs.langmuir.1c02114

Abstract

In this study, NMR and molecular dynamics simulations were employed to study IgG1 F_C binding to multimodal surfaces. Gold nanoparticles functionalized with two multimodal cation-exchange ligands (Capto and Nuvia) were synthesized and employed to carry out solution-phase NMR experiments with the F_C. Experiments with perdeuterated ¹⁵N-labeled F_C and the multimodal surfaces revealed micromolar residue-level binding affinities as compared to millimolar binding affinities with these ligands in free solution, likely due to cooperativity and avidity effects. The binding of F_C with the Capto ligand nanoparticles was concentrated near an aliphatic cluster in the C_H2/C_H3 interface, which corresponded to a focused hydrophobic region. In contrast, binding with the Nuvia ligand nanoparticles was more diffuse and corresponded to a large contiguous positive electrostatic potential region on the side face of the F_C. Results with lower-ligand-density nanoparticles indicated a decrease in binding affinity for both systems. For the Capto ligand system, several aliphatic residues on the F_C that were important for binding to the higher-density surface did not interact with the lower-density nanoparticles. In contrast, no significant difference was observed in the interacting residues on the F_C to the high- and low-ligand density Nuvia surfaces. The binding affinities of F_C to both multimodal-functionalized nanoparticles decreased in the presence of salt due to the screening of multiple weak interactions of polar and positively charged residues. For the Capto ligand nanoparticle system, this resulted in an even more focused hydrophobic binding region in the interface of the C_H2 and C_H3 domains. Interestingly, for the Nuvia ligand nanoparticles, the presence of salt resulted in a large transition from a diffuse binding region to the same focused binding region determined for Capto nanoparticles at 150 mM salt. Molecular dynamics simulations corroborated the NMR results and provided important insights into the molecular basis of F_C binding to these different multimodal systems containing clustered (observed at high-ligand densities) and nonclustered ligand surfaces. This combined biophysical and simulation approach provided significant insights into the interactions of F_C with multimodal surfaces and sets the stage for future analyses with even more complex biotherapeutics.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Gold
Immunoglobulin G
Ligands
Magnetic Resonance Spectroscopy
Metal Nanoparticles*
Molecular Dynamics Simulation*

Substances

Immunoglobulin G
Ligands
Gold