Issue 18, 2023
From the journal:

Physical Chemistry Chemical Physics

Dissecting the species-specific recognition of Neoseptin 3 by TLR4/MD2 via molecular dynamics simulations

Siru Wu,ab   Cong Zhang,ab   Yibo Wang,a   Penghui Li,c   Xiubo Duc  and  Xiaohui Wang ORCID logo *abd  

* Corresponding authors

a Laboratory of Chemical Biology, Changchun Institute of Applied Chemistry, Chinese Academy of Sciences, Changchun, Jilin, China
E-mail: xiaohui.wang@ciac.ac.cn

b School of Applied Chemistry and Engineering, University of Science and Technology of China, Hefei, Anhui, China

c Shenzhen Key Laboratory of Marine Biotechnology and Ecology, College of Life Sciences and Oceanography, Shenzhen University, Shenzhen, Guangdong, China

d Beijing National Laboratory for Molecular Sciences, Beijing, China

Abstract

Toll-like receptor 4 (TLR4) is crucial in the innate immune response with species-specific recognition. As a novel small-molecule agonist for mouse TLR4/MD2, Neoseptin 3 fails to activate human TLR4/MD2, while the underlying mechanism is unclear. Herein, molecular dynamics simulations were performed to investigate the species-specific molecular recognition of Neoseptin 3. Lipid A, a classic TLR4 agonist showing no apparent species-specific sensing by TLR4/MD2, was also investigated for comparison. Neoseptin 3 and lipid A showed similar binding patterns with mouse TLR4/MD2. Although the binding free energies of Neoseptin 3 interacting with TLR4/MD2 from mouse and human species were similar, protein–ligand interactions and the details of the dimerization interface were substantially different between Neoseptin 3-bound mouse and human heterotetramers at the atomic level. Neoseptin 3 binding made human (TLR4/MD2)2 more flexible than human (TLR4/MD2/Lipid A)2, especially at the TLR4 C-terminus and MD2, which drives human (TLR4/MD2)2 fluctuating away from the active conformation. In contrast to mouse (TLR4/MD2/2*Neoseptin 3)2 and mouse/human (TLR4/MD2/Lipid A)2 systems, Neoseptin 3 binding to human TLR4/MD2 led to the separating trend of the C-terminus of TLR4. Furthermore, the protein–protein interactions at the dimerization interface between TLR4 and the neighboring MD2 in the human (TLR4/MD2/2*Neoseptin 3)2 system were much weaker than those of the lipid A-bound human TLR4/MD2 heterotetramer. These results explained the inability of Neoseptin 3 to activate human TLR4 signaling and accounted for the species-specific activation of TLR4/MD2, which provides insight for transforming Neoseptin 3 as a human TLR4 agonist.

Graphical abstract: Dissecting the species-specific recognition of Neoseptin 3 by TLR4/MD2 via molecular dynamics simulations

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Article information

DOI
https://doi.org/10.1039/D3CP00949A
Article type
Paper
Submitted
01 Mar 2023
Accepted
20 Apr 2023
First published
21 Apr 2023

Phys. Chem. Chem. Phys., 2023,25, 13012-13018

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Dissecting the species-specific recognition of Neoseptin 3 by TLR4/MD2 via molecular dynamics simulations

S. Wu, C. Zhang, Y. Wang, P. Li, X. Du and X. Wang, Phys. Chem. Chem. Phys., 2023, 25, 13012 DOI: 10.1039/D3CP00949A

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