New insights into the stereochemical requirements of the bradykinin B1 receptor antagonists binding

Lupala, Cecylia S.; Gómez-Gutiérrez, Patricia; Pérez, Juan J.

doi:10.1016/j.jmgm.2016.06.010

Cited by 14 publications

(17 citation statements)

References 62 publications

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“…Docking results confirmed that the two compounds share the same region of the binding site, highlighting the importance of specific anchor points that were previously reported to be necessary for allosteric inhibition by our group [ 19 ] and specifically reported for B1 receptor inhibition in a recent paper [ 23 ]. Docking simulation highlighted how the compound DFL20656 interacts with N114 3.29 and W93 2.60 ( Figure 2 ).…”

Section: Resultssupporting

confidence: 77%

“…To overcome the bias of the templates used in the generation of the model, MD simulation was run allowing the homology model to equilibrate long enough to likely adopt what is more likely a biologically relevant structure [ 43 ]. To evaluate the structural stability of the protein-membrane system, 200 ns of molecular dynamics simulation were run [ 23 , 44 ].…”

Section: Methodsmentioning

confidence: 99%

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Binding Mode Exploration of B1 Receptor Antagonists’ by the Use of Molecular Dynamics and Docking Simulation—How Different Target Engagement Can Determine Different Biological Effects

Gemei

Talarico

Brandolini

et al. 2020

IJMS

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The kinin B1 receptor plays a critical role in the chronic phase of pain and inflammation. The development of B1 antagonists peaked in recent years but almost all promising molecules failed in clinical trials. Little is known about these molecules’ mechanisms of action and additional information will be necessary to exploit the potential of the B1 receptor. With the aim of contributing to the available knowledge of the pharmacology of B1 receptors, we designed and characterized a novel class of allosteric non-peptidic inhibitors with peculiar binding characteristics. Here, we report the binding mode analysis and pharmacological characterization of a new allosteric B1 antagonist, DFL20656. We analyzed the binding of DFL20656 by single point mutagenesis and radioligand binding assays and we further characterized its pharmacology in terms of IC50, B1 receptor internalization and in vivo activity in comparison with different known B1 antagonists. We highlighted how different binding modes of DFL20656 and a Merck compound (compound 14) within the same molecular pocket can affect the biological and pharmacological properties of B1 inhibitors. DFL20656, by its peculiar binding mode, involving tight interactions with N114, efficiently induced B1 receptor internalization and evoked a long-lasting effect in an in vivo model of neuropathic pain. The pharmacological characterization of different B1 antagonists highlighted the effects of their binding modes on activity, receptor occupancy and internalization. Our results suggest that part of the failure of most B1 inhibitors could be ascribed to a lack of knowledge about target function and engagement.

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Section: Resultssupporting

confidence: 77%

Section: Methodsmentioning

confidence: 99%

Binding Mode Exploration of B1 Receptor Antagonists’ by the Use of Molecular Dynamics and Docking Simulation—How Different Target Engagement Can Determine Different Biological Effects

Gemei

Talarico

Brandolini

et al. 2020

IJMS

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“…Novel approaches promise to facilitate the design of original kinin receptor ligands in the future, such as the in silico definition of pharmacophores from the analysis of the docking of several non-peptide antagonists; this has been done for 3-dimensional models of both the B 1 R and B 2 R [90,91]. The pro-drug agonist peptides may be further optimized for additional peptidases that will provide targeted actions on a specific tissue of a selective physiological function.…”

Section: Perspectivesmentioning

confidence: 99%

Bifunctional ligands of the bradykinin B 2 and B 1 receptors: An exercise in peptide hormone plasticity

et al. 2018

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Kinins are the small and fragile hydrophilic peptides related to bradykinin (BK) and derived from circulating kininogens via the action of kallikreins. Kinins bind to the preformed and widely distributed B receptor (BR) and to the inducible B receptor (BR). BRs and BRs are related G protein coupled receptors that possess natural agonist ligands of nanomolar affinity (BK and Lys BK for BRs, Lys-des-Arg-BK for BR). Decades of structure-activity exploration have resulted in the production of peptide analogs that are antagonists, one of which is clinically used (the BR antagonist icatibant), and also non-peptide ligands for both receptor subtypes. The modification of kinin receptor ligands has made them resistant to extracellular or endosomal peptidases and/or produced bifunctional ligands, defined as agonist or antagonist peptide ligands conjugated with a chemical fluorophore (emitting in the whole spectrum, from the infrared to the ultraviolet), a drug-like moiety, an epitope, an isotope chelator/carrier, a cleavable sequence (thus forming a pro-drug) and even a fused protein. Dual molecular targets for specific modified peptides may be a source of side effects or of medically exploitable benefits. Biotechnological protein ligands for either receptor subtype have been produced: they are enhanced green fluorescent protein or the engineered peroxidase APEX2 fused to an agonist kinin sequence at their C-terminal terminus. Antibodies endowed with pharmacological actions (agonist, antagonist) at BR have been reported, though not monoclonal antibodies. These findings define classes of alternative ligands of the kinin receptor of potential therapeutic and diagnostic value.

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“…They built an atomistic model of the receptor aiming to provide deeper insight into its structure, and their experiment allowed to define a common pharmacophore. This finding is potentially useful for the discovery of new compounds [22]. …”

Section: Severe Infection and Contact Activationmentioning

confidence: 99%

The role of contact system in septic shock: the next target? An overview of the current evidence

Nicola

2017

j intensive care

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BackgroundSeptic shock remains challenging to intensive care units worldwide, despite recent documented improvement in mortality over the years. Multiple new therapies have been attempted without success in large clinical trials. Evidence concerning the role of the contact system and bradykinin on septic shock physiological manifestations is shown by this article.ObjectivesThe objective of the study is to review the current evidence linking contact system activation and septic shock, as well as efficacy of available therapies targeting this pathophysiological pathway and to evaluate the potential of further researching the matter.ResultsMultiple animal studies are already available and suggestive of a meaningful role of contact system activation on septic shock. However, human trials are still scarce, and the ones available are not enough to establish such a strong connection. Furthermore, attempted therapies have been successful across multiple species, but not as much in humans. Therefore, contact system and septic shock relationship remains plentiful in questions to be answered in the coming years or decades.ConclusionsWhether the contact system is not as relevant in humans as it is in animals or there is only lack of evidence remains to be explained. The subject is an attractive open field for further research aiming to aid in tackling such a burdensome condition.

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New insights into the stereochemical requirements of the bradykinin B1 receptor antagonists binding

Cited by 14 publications

References 62 publications

Binding Mode Exploration of B1 Receptor Antagonists’ by the Use of Molecular Dynamics and Docking Simulation—How Different Target Engagement Can Determine Different Biological Effects

Binding Mode Exploration of B1 Receptor Antagonists’ by the Use of Molecular Dynamics and Docking Simulation—How Different Target Engagement Can Determine Different Biological Effects

Bifunctional ligands of the bradykinin B 2 and B 1 receptors: An exercise in peptide hormone plasticity

The role of contact system in septic shock: the next target? An overview of the current evidence

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