In silico studies of interactions of peptide-conjugated cholesterol metabolites and betulinic acid with EGFR, LDR, and N-terminal fragment of CCKA receptors

Madeline M Bashant; Saige M Mitchell; Lucy R Hart; Charlotta G Lebedenko; Ipsita A Banerjee

doi:10.1007/s00894-021-05007-5

In silico studies of interactions of peptide-conjugated cholesterol metabolites and betulinic acid with EGFR, LDR, and N-terminal fragment of CCKA receptors

J Mol Model. 2021 Dec 28;28(1):16. doi: 10.1007/s00894-021-05007-5.

Authors

Madeline M Bashant¹, Saige M Mitchell¹, Lucy R Hart¹, Charlotta G Lebedenko¹, Ipsita A Banerjee²

Affiliations

¹ Department of Chemistry, Fordham University, 441 East Fordham Road, Bronx, NY, 10458, USA.
² Department of Chemistry, Fordham University, 441 East Fordham Road, Bronx, NY, 10458, USA. banerjee@fordham.edu.

PMID: 34961887
DOI: 10.1007/s00894-021-05007-5

Abstract

In this work, we designed three new ligands by conjugating cholesterol metabolites 3-hydroxy-5-cholestenoic acid (3-HC) and 3-oxo-4-cholestenoic acid (3-OC) and the natural tri-terpenoid betulinic acid with the tumor-targeting peptide YHWYGYTPQNVI. Molecular interactions with the unconjugated peptide and the conjugates were examined with three receptors that are commonly overexpressed in pancreatic adenocarcinoma cells using ligand docking and molecular dynamics. This study demonstrated the utility of the designed conjugates as a valuable scaffold for potentially targeting EGFR and LDLR receptors. Our results indicate that the conjugates showed strong binding affinities and formation of stable complexes with EGFR, while the unconjugated peptide, BT-peptide conjugate, an 3-HC-peptide conjugate showed the formation of fairly stable complexes with LDLR receptor. For EGFR, two receptor kinase domains were explored. Interactions with the N-terminal domain of CCKA-R were relatively weaker. For LDLR, binding occurred in the beta-propeller region. For the N-terminal fragment of CCKA-R, the conjugates induced significant conformational changes in the receptor. The molecular dynamic simulations for 100 ns demonstrate that BT-peptide conjugates and the unconjugated peptide had the highest binding and formed the most stable complexes with EGFR. RMSD and trajectory analyses indicate that these molecules transit to a dynamically stable configuration in most cases within 60 ns. NMA analysis indicated that amongst the conjugates that showed relatively higher interactions with the respective receptors, the highest potential for deformability was seen for the N-terminal-47 amino acid region of the CCKA-R receptor with and the lowest for the LDLR-receptor. Thus, the newly designed compounds may be evaluated in the future toward developing drug delivery materials for targeting tumor cells overexpressing LDLR or EGFR.

Keywords: Cholesterol derivatives; EGFR; LDLR; Over-expressed; Receptor targeting; Tumor-targeted peptides.

MeSH terms

Amino Acid Sequence
Betulinic Acid
Cholesterol / chemistry*
ErbB Receptors / chemistry
Humans
Ligands
Models, Molecular*
Molecular Docking Simulation
Molecular Dynamics Simulation
Molecular Structure
Pentacyclic Triterpenes / chemistry*
Peptides / chemistry*
Protein Binding
Receptor, Cholecystokinin A / chemistry*
Receptors, LDL / chemistry*
Structure-Activity Relationship

Substances

LDLR protein, human
Ligands
Pentacyclic Triterpenes
Peptides
Receptor, Cholecystokinin A
Receptors, LDL
Cholesterol
EGFR protein, human
ErbB Receptors
Betulinic Acid