In Silico Insights towards the Identification of NLRP3 Druggable Hot Spots

Mekni, Nedra; Rosa, Maria de Lurdes Pereira; Cipollina, Chiara; Gulotta, Maria Rita; Simone, Giada De; Lombino, Jessica; Padova, Alessandro; Perricone, Ugo

doi:10.3390/ijms20204974

Cited by 20 publications

(21 citation statements)

References 29 publications

(48 reference statements)

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“…A homology model of NLRP3 was prepared from the crystal structure of NLRC4 and the FASTA sequence of human NLRP3 ( ). Perricone and coworkers used this homology model in a Molecular Dynamics (MD) study with MCC950 ( Figure 5 ) and its analogues [ 51 ]. Detection of all potential druggable binding sites close to the Walker B region were detected by docking MCC950 as a probe, using grid-based and geometry-based algorithm approaches.…”

Section: Computational Approaches To Design New Nlrp3 Inhibitorsmentioning

confidence: 99%

Inhibiting the NLRP3 Inflammasome

2020

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Inflammasomes are protein complexes which are important in several inflammatory diseases. Inflammasomes form part of the innate immune system that triggers the activation of inflammatory cytokines interleukin (IL)-1β and IL-18. The inflammasome most studied in sterile inflammation and non-communicable disease is the NLRP3 inflammasome. Upon activation by diverse pathogen or disease associated signals, NLRP3 nucleates the oligomerization of an adaptor protein ASC forming a platform (the inflammasome) for the recruitment and activation of the protease caspase-1. Active caspase-1 catalyzes the processing and release of IL-1β and IL-18, and via cleavage of the pore forming protein gasdermin D can drive pyroptotic cell death. This review focuses on the structural basis and mechanism for NLRP3 inflammasome signaling in the context of drug design, providing chemical structures, activities, and clinical potential of direct inflammasome inhibitors. A cryo-EM structure of NLRP3 bound to NEK7 protein provides structural insight and aids in the discovery of novel NLRP3 inhibitors utilizing ligand-based or structure-based approaches.

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Section: Computational Approaches To Design New Nlrp3 Inhibitorsmentioning

confidence: 99%

Inhibiting the NLRP3 Inflammasome

2020

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“…In this study, the most promising NLRP3 specific inhibitor MCC950 was selected as the control, [ 101 ] was a potential therapeutic for NLRP3‐associated diseases. [ 102 ] Docking study has shown that MCC950 binding with amino acid residues, such as Arg165, Thr167 and Thr379.…”

Section: Molecular Docking Of Quinones With Nlrp3mentioning

confidence: 99%

Quinones as preventive agents in Alzheimer’s diseases: focus on NLRP3 inflammasomes

Chen

Gao

Peng

et al. 2020

Journal of Pharmacy and Pharmacology

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Objectives Alzheimer's disease (AD) is a hidden neurological degenerative disease, which main clinical manifestations are cognitive dysfunction, memory impairment and mental disorders. Neuroinflammation is considered as a basic response of the central nervous system. NLRP3 (Nucleotide-binding domain leucine-rich repeat (NLR) and pyrin domain containing receptor 3) inflammasome is closely related to the occurrence of neuroinflammation. Activation of the NLRP3 inflammasome results in the release of cytokines, pore formation and ultimately pyroptosis, which has demonstrated one of the critical roles in AD pathogenesis. Inhibition of the activity of NLRP3 is one of the focuses of the research. Therefore, NLRP3 represents an attractive pharmacological target, and discovery compounds with good NLRP3 inhibitory activity are particularly important. Key findings Quinones have good neuroprotective effects and prevent AD, which may be related to their regulation of inflammatory response. The molecular docking was used to explore 12 quinones with AD prevention and treatment and NLRP3. Docking results showed that the combination of anthraquinones and NLRP3 were the best, and the top two chemical compounds were Purpurin and Rhein, which are the most promising NLRP3 inhibitors. Summary These quinones may provide the theoretical basis for finding lead compounds for novel neuroprotective agents. Quinones as NLRP3 inflammasomes inhibitors Da-bao Chen et al.

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“…It is noteworthy that this bi‐molecular interaction is not a traditional example of PPI, in which the interaction interfaces are often shallow with lack of deep pockets and it does not bear a canonical active site to target with a synthetic ligand. In general, in PPI, both protein partners establish high affinity contacts through the so‐called hot spot amino acids . These residues are mainly hydrophobic and usually widely dislocated along the whole protein surfaces, and thus sequentially not connected among them within the same protein, creating a discontinuous epitope .…”

Section: Resultsmentioning

confidence: 99%

“…In general, in PPI, both protein partners establish high affinity contacts through the so-called hot spot amino acids. [62] These residues are mainly hydrophobic and usually widely dislocated along the whole protein surfaces, and thus sequentially not connected among them within the same protein, creating a discontinuous epitope. [63][64][65] Notably, from the currently available PDB structures of ACE2-S protein interaction (PDB IDs: 6M17 and 6M0J), the complex shows a one to one interaction pattern, where the contacts between the two proteins are mediated mainly by hydrogen bonds, some salt bridges and few Van der Waals forces.…”

Section: Computational Alanine Scanning On Sars-cov-2 -Ace2 Interactimentioning

confidence: 99%

Targeting SARS‐CoV‐2 RBD Interface: a Supervised Computational Data‐Driven Approach to Identify Potential Modulators

et al. 2020

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Coronavirus disease 2019 (COVID-19) has spread out as a pandemic threat affecting over 2 million people. The infectious process initiates via binding of SARS-CoV-2 Spike (S) glycoprotein to host angiotensin-converting enzyme 2 (ACE2). The interaction is mediated by the receptor-binding domain (RBD) of S glycoprotein, promoting host receptor recognition and binding to ACE2 peptidase domain (PD), thus representing a promising target for therapeutic intervention. Herein, we present a computational study aimed at identifying small molecules potentially able to target RBD. Although targeting PPI remains a challenge in drug discovery, our investigation highlights that interaction between SARS-CoV-2 RBD and ACE2 PD might be prone to small molecule modulation, due to the hydrophilic nature of the bi-molecular recognition process and the presence of druggable hot spots. The fundamental objective is to identify, and provide to the international scientific community, hit molecules potentially suitable to enter the drug discovery process, preclinical validation and development.

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In Silico Insights towards the Identification of NLRP3 Druggable Hot Spots

Cited by 20 publications

References 29 publications

Inhibiting the NLRP3 Inflammasome

Inhibiting the NLRP3 Inflammasome

Quinones as preventive agents in Alzheimer’s diseases: focus on NLRP3 inflammasomes

Targeting SARS‐CoV‐2 RBD Interface: a Supervised Computational Data‐Driven Approach to Identify Potential Modulators

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