Unraveling Extremely Damaging IRAK4 Variants and Their Potential Implications for IRAK4 Inhibitor Efficacy

Mohammed Y Behairy; Refaat A Eid; Hassan M Otifi; Heitham M Mohammed; Mohammed A Alshehri; Ashwag Asiri; Majed Aldehri; Mohamed Samir A Zaki; Khaled M Darwish; Sameh S Elhady; Nahla H El-Shaer; Muhammad Alaa Eldeen

doi:10.3390/jpm13121648

Unraveling Extremely Damaging IRAK4 Variants and Their Potential Implications for IRAK4 Inhibitor Efficacy

J Pers Med. 2023 Nov 26;13(12):1648. doi: 10.3390/jpm13121648.

Affiliations

¹ Department of Microbiology and Immunology, Faculty of Pharmacy, University of Sadat City, Sadat City 32897, Egypt.
² Department of Pathology, College of Medicine, King Khalid University, Abha P.O. Box 61421, Saudi Arabia.
³ Department of Anatomy, College of Medicine, King Khalid University, Abha P.O. Box 61421, Saudi Arabia.
⁴ Department of Child Health, College of Medicine, King Khalid University, Abha P.O. Box 62529, Saudi Arabia.
⁵ Department of Medicinal Chemistry, Faculty of Pharmacy, Suez Canal University, Ismailia 41522, Egypt.
⁶ Department of Natural Products, Faculty of Pharmacy, King Abdulaziz University, Jeddah 21589, Saudi Arabia.
⁷ Department of Zoology, Faculty of Science, Zagazig University, Zagazig 44511, Egypt.

Abstract

Interleukin-1-receptor-associated kinase 4 (IRAK4) possesses a crucial function in the toll-like receptor (TLR) signaling pathway, and the dysfunction of this molecule could lead to various infectious and immune-related diseases in addition to cancers. IRAK4 genetic variants have been linked to various types of diseases. Therefore, we conducted a comprehensive analysis to recognize the missense variants with the most damaging impacts on IRAK4 with the employment of diverse bioinformatics tools to study single-nucleotide polymorphisms' effects on function, stability, secondary structures, and 3D structure. The residues' location on the protein domain and their conservation status were investigated as well. Moreover, docking tools along with structural biology were engaged in analyzing the SNPs' effects on one of the developed IRAK4 inhibitors. By analyzing IRAK4 gene SNPs, the analysis distinguished ten variants as the most detrimental missense variants. All variants were situated in highly conserved positions on an important protein domain. L318S and L318F mutations were linked to changes in IRAK4 secondary structures. Eight SNPs were revealed to have a decreasing effect on the stability of IRAK4 via both I-Mutant 2.0 and Mu-Pro tools, while Mu-Pro tool identified a decreasing effect for the G198E SNP. In addition, detrimental effects on the 3D structure of IRAK4 were also discovered for the selected variants. Molecular modeling studies highlighted the detrimental impact of these identified SNP mutant residues on the druggability of the IRAK4 ATP-binding site towards the known target inhibitor, HG-12-6, as compared to the native protein. The loss of important ligand residue-wise contacts, altered protein global flexibility, increased steric clashes, and even electronic penalties at the ligand-binding site interfaces were all suggested to be associated with SNP models for hampering the HG-12-6 affinity towards IRAK4 target protein. This given model lays the foundation for the better prediction of various disorders relevant to IRAK4 malfunction and sheds light on the impact of deleterious IRAK4 variants on IRAK4 inhibitor efficacy.

Keywords: SNPs; TLR signaling; bioinformatics; innate immunity; molecular dynamics.

Grants and funding

RGP2/17/44/King Khalid University