Exploring Non-orthosteric Interactions with a Series of Potent and Selective A3 Antagonists

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dc.contributor.affiliationUniversidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicasgl
dc.contributor.affiliationUniversidade de Santiago de Compostela. Centro de Investigación en Química Biolóxica e Materiais Molecularesgl
dc.contributor.affiliationUniversidade de Santiago de Compostela. Departamento de Química Orgánicagl
dc.contributor.authorMiranda Pastoriza, Darío
dc.contributor.authorBernárdez Alfaya, Rodrigo
dc.contributor.authorAzuaje Guerrero, Jhonny Alberto
dc.contributor.authorPrieto Díaz, Rubén
dc.contributor.authorMajellaro, Maria
dc.contributor.authorTamhankar, Ashish V.
dc.contributor.authorKoenekoop, Lucien
dc.contributor.authorGonzález García, Alejandro
dc.contributor.authorGioé Gallo, Claudia
dc.contributor.authorMallo-Abreu, Ana
dc.contributor.authorBrea Floriani, José Manuel
dc.contributor.authorLoza García, María Isabel
dc.contributor.authorGarcía Rey, Aitor
dc.contributor.authorGarcía Mera, Xerardo
dc.contributor.authorGutiérrez de Terán, Hugo
dc.contributor.authorSotelo Pérez, Eddy
dc.date.accessioned2022-09-16T11:34:54Z
dc.date.available2022-09-16T11:34:54Z
dc.date.issued2022
dc.description.abstractA library of potent and highly A3AR selective pyrimidine-based compounds was designed to explore non-orthosteric interactions within this receptor. Starting from a prototypical orthosteric A3AR antagonist (ISVY130), the structure-based design explored functionalized residues at the exocyclic amide L1 region and aimed to provide additional interactions outside the A3AR orthosteric site. The novel ligands were assembled through an efficient and succinct synthetic approach, resulting in compounds that retain the A3AR potent and selective profile while improving the solubility of the original scaffold. The experimentally demonstrated tolerability of the L1 region to structural functionalization was further assessed by molecular dynamics simulations, giving hints of the non-orthosteric interactions explored by these series. The results pave the way to explore newly functionalized A3AR ligands, including covalent drugs and molecular probes for diagnostic and delivery purposesgl
dc.description.peerreviewedSIgl
dc.description.sponsorshipThis work has received financial support from the Consellería de Cultura, Educación e Ordenación Universitaria [Galician Government (grant: ED431B 2020/43)], the Xunta de Galicia (Centro singular de investigación de Galicia accreditation 2019-2022, ED431G 2019/03), the European Union (European Regional Development Fund - ERDF), the Swedish Research Council (grant: 521-2014-2118), and the Swedish strategic research program eSSENCE. The computational studies were conducted with the resources available from the Swedish National Infrastructure for Computing (SNIC). The project was carried out within the framework of the collaborative EU COST action ERNEST (CA18133)gl
dc.identifier.citationACS Med. Chem. Lett. 2022, 13, 2, 243–249gl
dc.identifier.doi10.1021/acsmedchemlett.1c00598
dc.identifier.issn1948-5875
dc.identifier.urihttp://hdl.handle.net/10347/29225
dc.language.isoenggl
dc.publisherACS Publicationsgl
dc.relation.publisherversionhttps://doi.org/10.1021/acsmedchemlett.1c00598gl
dc.rights© 2022 The Authors. Published by American Chemical Society. This work is under a CC Attribution 4.0 International (CC BY 4.0)gl
dc.rightsAtribución 4.0 Internacional
dc.rights.accessRightsopen accessgl
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectA3 Adenosine receptorsgl
dc.subjectAdenosine antagonistsgl
dc.subjectPyrimidinesgl
dc.subjectUgi reactiongl
dc.subjectMulticomponent reactionsgl
dc.titleExploring Non-orthosteric Interactions with a Series of Potent and Selective A3 Antagonistsgl
dc.typejournal articlegl
dc.type.hasVersionVoRgl
dspace.entity.typePublication
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relation.isAuthorOfPublication.latestForDiscoveryc59a1715-e9fc-490d-abb4-0d691f3ff34c

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