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Escape from adamantane: scaffold optimization of novel P2X7 antagonists featuring complex polycycles

Autor/a

Barniol-Xicota, Marta

Kwak, Seung-Hwa

Lee, So-Deok

Caseley, Emily

Valverde Murillo, Elena

Jiang, Lin-Hua

Kim, Yong-Chul

Vázquez Cruz, Santiago

Fecha de publicación

2019-03-06T14:39:43Z

2019-03-06T14:39:43Z

2017-01-16

2019-03-06T14:39:43Z

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Resumen

The adamantane scaffold, despite being widely used in medicinal chemistry, is not devoid of problems. In recent years we have developed new polycyclic scaffolds as surrogates of the adamantane group with encouraging results in multiple targets. As an adamantane scaffold is a common structural feature in several P2X7 receptor antagonists, herein we report the synthesis and pharmacological evaluation of multiple replacement options of adamantane that maintain a good activity profile. Molecular modeling studies support the binding of the compounds to a site close to the central pore, rather than to the ATP-binding site and shed light on the structural requirements for novel P2X7 antagonists.

Tipo de documento

Artículo

Versión aceptada

Lengua

Inglés

Materias y palabras clave

Receptors cel·lulars; Medicaments; Cell receptors; Drugs

Publicado por

Elsevier Ltd

Documentos relacionados

Versió postprint del document publicat a: https://doi.org/10.1016/j.bmcl.2017.01.039

Bioorganic & Medicinal Chemistry Letters, 2017, vol. 27, p. 759-763

https://doi.org/10.1016/j.bmcl.2017.01.039

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Derechos

cc-by-nc-nd (c) Elsevier Ltd, 2017

http://creativecommons.org/licenses/by-nc-nd/3.0/es

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Farmacologia, Toxicologia i Química Terapèutica [675]

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