Computational Characterization of the Binding Properties of the HIV1-Neutralizing Antibody PG16 and Design of PG16-Derived CDRH3 Peptides

Deubler M, Weißenborn L, Leukel S, Horn A, Eichler J, Sticht H (2023)

Publication Type: Journal article

Publication year: 2023

Journal

Biology MDPI

Book Volume: 12

Article Number: 824

Journal Issue: 6

DOI: 10.3390/biology12060824

Abstract

PG16 is a broadly neutralizing antibody that binds to the gp120 subunit of the HIV-1 Env protein. The major interaction site is formed by the unusually long complementarity determining region (CDR) H3. The CDRH3 residue Tyr100H is known to represent a tyrosine sulfation site; however, this modification is not present in the experimental complex structure of PG16 with full-length HIV-1 Env. To investigate the role of sulfation for this complex, we modeled the sulfation of Tyr100H and compared the dynamics and energetics of the modified and unmodified complex by molecular dynamics simulations at the atomic level. Our results show that sulfation does not affect the overall conformation of CDRH3, but still enhances gp120 interactions both at the site of modification and for the neighboring residues. This stabilization affects not only protein–protein contacts, but also the interactions between PG16 and the gp120 glycan shield. Furthermore, we also investigated whether PG16-CDRH3 is a suitable template for the development of peptide mimetics. For a peptide spanning residues 93-105 of PG16, we obtained an experimental EC50 value of 3 (Formula presented.) (Formula presented.) for the binding of gp120 to the peptide. This affinity can be enhanced by almost one order of magnitude by artificial disulfide bonding between residues 99 and 100F. In contrast, any truncation results in significantly lower affinity, suggesting that the entire peptide segment is involved in gp120 recognition. Given their high affinity, it should be possible to further optimize the PG16-derived peptides as potential inhibitors of HIV invasion.

Authors with CRIS profile

Manuel Deubler Professur für Bioinformatik Lucas Weißenborn Lehrstuhl für Pharmazeutische Chemie Simon Leukel Lehrstuhl für Pharmazeutische Chemie Anselm Horn Professur für Bioinformatik Jutta Eichler Professur für Pharmazeutische Chemie Heinrich Sticht Professur für Bioinformatik

Additional Organisation(s)

Erlangen National High Performance Computing Center (NHR@FAU) FAU Forschungszentrum Neue Wirkstoffe (FAU NeW)

How to cite

APA:

Deubler, M., Weißenborn, L., Leukel, S., Horn, A., Eichler, J., & Sticht, H. (2023). Computational Characterization of the Binding Properties of the HIV1-Neutralizing Antibody PG16 and Design of PG16-Derived CDRH3 Peptides. Biology, 12(6). https://doi.org/10.3390/biology12060824

MLA:

Deubler, Manuel, et al. "Computational Characterization of the Binding Properties of the HIV1-Neutralizing Antibody PG16 and Design of PG16-Derived CDRH3 Peptides." Biology 12.6 (2023).

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