Structural modeling, energetic analysis and molecular design of a π-stacking system at the complex interface of pediatric respiratory syncytial virus nucleocapsid with the C-terminal peptide of phosphoprotein

Haiyan Liu; Lili Shen; Chunhua Pan; Weihua Huang

doi:10.1016/j.bpc.2022.106916

Structural modeling, energetic analysis and molecular design of a π-stacking system at the complex interface of pediatric respiratory syncytial virus nucleocapsid with the C-terminal peptide of phosphoprotein

Biophys Chem. 2023 Jan:292:106916. doi: 10.1016/j.bpc.2022.106916. Epub 2022 Oct 29.

Authors

Haiyan Liu¹, Lili Shen¹, Chunhua Pan¹, Weihua Huang²

Affiliations

¹ Department of Pediatrics, Suzhou Kowloon Hospital, Shanghai Jiao Tong University School of Medicine, Suzhou 215000, China.
² Department of Pediatrics, Suzhou Kowloon Hospital, Shanghai Jiao Tong University School of Medicine, Suzhou 215000, China. Electronic address: weihuahuang@yeah.net.

PMID: 36343393
DOI: 10.1016/j.bpc.2022.106916

Abstract

Human respiratory syncytial virus (RSV) is a primary cause of lower respiratory tract infections and hospital visits during infancy and childhood. The RSV phosphoprotein (P) is a major polymerase cofactor that interacts with nucleoprotein (N) to promote the recognition of ribonucleoprotein complex (RNP) by viral RNA polymerase. The binding pocket of N protein is chemically diverse, in or around which a number of aromatic and charged amino acid residues are observed. Previously, a nonapeptide segment (P peptide, ²³³DNDLSLEDF²⁴¹) representing the C-terminal tail of P protein was identified to mediate the N-P interaction with a moderate affinity, in which the Phe241 at the end of P's C-terminus plays a critical role in the binding of P peptide to N protein. Here, we found that the side-chain aromatic phenyl moiety of P Phe241 residue can form short- and long-range cation-π interactions with N Arg132 and Arg150 residues, respectively, as well as T-shaped and parallel-displaced π-π stackings with N Tyr135 and His151 residues, respectively, which co-define a geometrically satisfactory π-stacking system at the complex interface of N protein with P peptide, thus largely stabilizing the complex architecture. The stacking effect was further optimized by systematically mutating the P Phe241 residue to other natural and non-natural aromatic amino acids with diverse chemical substitutions at the phenyl moiety to examine their structural and energetic effects on π-stacking system and on protein-peptide binding. The electron-donating mutations at the phenyl moiety of P Phe241 residue can effectively enhance the π-stacking system and then promote peptide binding, whereas the bulky and positively charged mutations would considerably impair the peptide potency by introducing steric hindrance and electrostatic repulsion. The [Tyr]P, [Thp]P and [Fph]P mutants were determined to have an increased affinity relative to wild-type P peptide, which could be used as self-inhibitory peptides to competitively disrupt the native interaction between N and P proteins.

Keywords: Molecular modeling and design; Nucleoprotein; Pediatric pneumonia; Peptide; Phosphoprotein; Respiratory syncytial virus; π-Stacking system.

Publication types

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

MeSH terms

Child
Humans
Nucleocapsid / metabolism
Nucleoproteins
Peptides / chemistry
Phosphoproteins / chemistry
Phosphoproteins / genetics
Phosphoproteins / metabolism
Respiratory Syncytial Virus, Human* / chemistry
Respiratory Syncytial Virus, Human* / genetics
Respiratory Syncytial Virus, Human* / metabolism

Substances

Phosphoproteins
Nucleoproteins
Peptides