Molecular Simulation of Oncostatin M and Receptor (OSM–OSMR) Interaction as a Potential Therapeutic Target for Inflammatory Bowel Disease

Du, Qingqing; Yan, Qian; Xue, Weiwei

doi:10.3389/fmolb.2020.00029

Cited by 23 publications

(18 citation statements)

References 43 publications

(61 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We use the MM/GBSA method (Kollman et al., 2000), which has been widely employed to characterize the thermodynamics properties of different types of protein–protein interactions (PPIs; Du et al., 2020; Tu et al., 2018; Wang et al., 2019), to estimate the binding affinities between Nbs and RBD. Table 1 lists the total binding free energy (Δ G tol ) as well as their compositing terms including the electrostatic interaction energy (Δ E ele ), van der Waals interaction energy (Δ E vdW ), non‐polar solvent energy (Δ G nonpol ), and polar solvent energy (Δ G pol ).…”

Section: Resultsmentioning

confidence: 99%

Computational design and modeling of nanobodies toward SARS‐CoV‐2 receptor binding domain

et al. 2021

Self Cite

View full text Add to dashboard Cite

The ongoing pandemic of coronavirus disease 2019 (COVID‐19) caused by severe acute respiratory syndrome coronavirus 2 (SARS‐CoV‐2) has become a global health concern and pose a serious threat to humanity. There is an urgent need for developing therapeutic drugs and (or) biologics to prevent the spread of the virus. The life cycle of SARS‐CoV‐2 shows that the virus enters host cells by first binding to angiotensin‐converting enzyme 2 (ACE2) through its spike protein receptor‐binding domain (RBD). Therefore, blocking the binding between of ACE2 and SARS‐CoV‐2 RBD can inhibit the virus infection in the host cells. In this study, by grafting the complementarity‐determining regions (CDRs) of developed SARS‐CoV, MERS‐CoVs specific neutralizing antibodies (nAbs) include monoclonal antibodies (mAbs) as well as SARS‐CoV‐2 mAbs onto a known stable nanobody (Nb) scaffold, and a total of 16 Nbs sequences were designed. Five Nbs, namely CS01, CS02, CS03, CS10, and CS16, were selected based on the free energy landscape of protein docking verified by the recently reported Nb‐RBD cocrystal structures. CS01, CS02, and CS03 occupied the ACE2 binding site of RBD, while CS10 and CS16 were proposed to inhibit the interaction between RBD and ACE2 through an allosteric mechanism. Based on the structures of the five Nbs in complex with RBD, seven brand‐new Nbs with enhanced binding affinities (CS02_RD01, CS03_RD01, CS03_RD02, CS03_RD03, CS03_RD04, CS16_RD01, and CS16_RD02) were generated by redesign of residues on the interface of the five Nbs contact with SARS‐CoV‐2 RBD. In addition, the identified “hot spots” on the interface of each complex provide useful information to understand the binding mechanism of designed Nbs to SARS‐CoV‐2 RBD. In sum, the predicted stabilities and high binding affinities of the 11 (re)designed Nbs indicating the potential of the developed computational framework in this work to design effective agents to block the infection of SARS‐CoV‐2.

show abstract

Section: Resultsmentioning

confidence: 99%

Computational design and modeling of nanobodies toward SARS‐CoV‐2 receptor binding domain

et al. 2021

Self Cite

View full text Add to dashboard Cite

show abstract

“…Arg398 of C-Raf and Lys80 of RKIP could be regarded as "hot spot" residues along with the above previously identified interface residues and deemed to be druggable sites for future development of novel inhibitors. Using one of the identified "hot spots" as an example, a long-time scale 300 ns MD simulation was performed for the Arg398Ala mutation according to the similar strategy adopted in previous PPI study (Du et al, 2020). A noteworthy difference was noticed near the mutation site when the representative trajectory extracted at 180 ns (RMSD of 0.9 nm) was compared with the representative WT snapshot (Figure 5).…”

Section: Discussionmentioning

confidence: 99%

“…The AMBER99SB-ILDN forcefield was applied to generate the topology parameters of the structural complexes (Lindorff-Larsen et al, 2010;Venkatesan et al, 2015;Zarei, et al, 2017;Galeazzi et al, 2018). The binary complexes were then surrounded by dodecahedron periodic box of SPCE water molecules (Selent et al, 2013;Venkatesan et al, 2015;Galeazzi et al, 2018;Du et al, 2020). Cl − ions were added to the systems to neutralize it prior to minimization (Supplementary Table S1).…”

Section: Analysis Of Interaction Dynamicsmentioning

confidence: 99%

Exploring the Binding Interaction of Raf Kinase Inhibitory Protein With the N-Terminal of C-Raf Through Molecular Docking and Molecular Dynamics Simulation

Parate

Rampogu

Lee

et al. 2021

Front. Mol. Biosci.

View full text Add to dashboard Cite

Protein-protein interactions are indispensable physiological processes regulating several biological functions. Despite the availability of structural information on protein-protein complexes, deciphering their complex topology remains an outstanding challenge. Raf kinase inhibitory protein (RKIP) has gained substantial attention as a favorable molecular target for numerous pathologies including cancer and Alzheimer’s disease. RKIP interferes with the RAF/MEK/ERK signaling cascade by endogenously binding with C-Raf (Raf-1 kinase) and preventing its activation. In the current investigation, the binding of RKIP with C-Raf was explored by knowledge-based protein-protein docking web-servers including HADDOCK and ZDOCK and a consensus binding mode of C-Raf/RKIP structural complex was obtained. Molecular dynamics (MD) simulations were further performed in an explicit solvent to sample the conformations for when RKIP binds to C-Raf. Some of the conserved interface residues were mutated to alanine, phenylalanine and leucine and the impact of mutations was estimated by additional MD simulations and MM/PBSA analysis for the wild-type (WT) and constructed mutant complexes. Substantial decrease in binding free energy was observed for the mutant complexes as compared to the binding free energy of WT C-Raf/RKIP structural complex. Furthermore, a considerable increase in average backbone root mean square deviation and fluctuation was perceived for the mutant complexes. Moreover, per-residue energy contribution analysis of the equilibrated simulation trajectory by HawkDock and ANCHOR web-servers was conducted to characterize the key residues for the complex formation. One residue each from C-Raf (Arg398) and RKIP (Lys80) were identified as the druggable “hot spots” constituting the core of the binding interface and corroborated by additional long-time scale (300 ns) MD simulation of Arg398Ala mutant complex. A notable conformational change in Arg398Ala mutant occurred near the mutation site as compared to the equilibrated C-Raf/RKIP native state conformation and an essential hydrogen bonding interaction was lost. The thirteen binding sites assimilated from the overall analysis were mapped onto the complex as surface and divided into active and allosteric binding sites, depending on their location at the interface. The acquired information on the predicted 3D structural complex and the detected sites aid as promising targets in designing novel inhibitors to block the C-Raf/RKIP interaction.

show abstract

“…The H187 residue is located in the region linking three hot spot sites of the OSM-OSMR binding task [19]. The change from basic histidine to polar glutamine, although not directly affecting a binding hot spot, could alter the conformation of the sites active in OSM-OSMR interaction.…”

Section: Discussionmentioning

confidence: 99%

“…The whole protein model is shown on the left, while the region around H187 is enlarged in the right, distinguishing between the wt (above) and the p.H187Q variant sequence (below). The region is further zoomed in to show the three hotspots sites around H187 reported by Du et al [19] in yellow, blue, and red, respectively, with the Tyr214 residue being the hot spot binding residue in common between the three.…”

Section: In Silico Analysis Of the Effects Of Rs34675408 On The Osmr Structurementioning

confidence: 99%

The OSMR Gene Is Involved in Hirschsprung Associated Enterocolitis Susceptibility through an Altered Downstream Signaling

Bachetti

Rosamilia

Bartolucci

et al. 2021

IJMS

View full text Add to dashboard Cite

Hirschsprung (HSCR) Associated Enterocolitis (HAEC) is a common life-threatening complication in HSCR. HAEC is suggested to be due to a loss of gut homeostasis caused by impairment of immune system, barrier defense, and microbiome, likely related to genetic causes. No gene has been claimed to contribute to HAEC occurrence, yet. Genetic investigation of HAEC by Whole-Exome Sequencing (WES) on 24 HSCR patients affected (HAEC) or not affected (HSCR-only) by enterocolitis and replication of results on a larger panel of patients allowed the identification of the HAEC susceptibility variant p.H187Q in the Oncostatin-M receptor (OSMR) gene (14.6% in HAEC and 5.1% in HSCR-only, p = 0.0024). Proteomic analysis on the lymphoblastoid cell lines from one HAEC patient homozygote for this variant and one HAEC patient not carrying the variant revealed two well distinct clusters of proteins significantly up or downregulated upon OSM stimulation. A marked enrichment in immune response pathways (q < 0.0001) was shown in the HAEC H187 cell line, while proteins upregulated in the HAEC Q187 lymphoblasts sustained pathways likely involved in pathogen infection and inflammation. In conclusion, OSMR p.H187Q is an HAEC susceptibility variant and perturbates the downstream signaling cascade necessary for the gut immune response and homeostasis maintenance.

show abstract

Molecular Simulation of Oncostatin M and Receptor (OSM–OSMR) Interaction as a Potential Therapeutic Target for Inflammatory Bowel Disease

Cited by 23 publications

References 43 publications

Computational design and modeling of nanobodies toward SARS‐CoV‐2 receptor binding domain

Computational design and modeling of nanobodies toward SARS‐CoV‐2 receptor binding domain

Exploring the Binding Interaction of Raf Kinase Inhibitory Protein With the N-Terminal of C-Raf Through Molecular Docking and Molecular Dynamics Simulation

The OSMR Gene Is Involved in Hirschsprung Associated Enterocolitis Susceptibility through an Altered Downstream Signaling

Contact Info

Product

Resources

About