Synthesis, biological studies and molecular modeling investigation of 1,3-dimethyl-2,4-dioxo-6-methyl-8-(substituted) 1,2,3,4-tetrahydro [1,2,4]-triazolo [3,4-f]-purines as potential adenosine receptor antagonists

Farmaco (Societa chimica italiana : 1989) Pub Date : 2005-04-01 DOI:10.1016/j.farmac.2005.01.008

Giorgia Pastorin , Chiara Bolcato , Barbara Cacciari , Sonja Kachler , Karl-Norbert Klotz , Christian Montopoli , Stefano Moro , Giampiero Spalluto

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引用次数: 9

Abstract

A new series of potential adenosine receptor antagonists with a [1,2,4]-triazolo-[3,4-f]-purine structure have been synthesized, and their affinities at the four adenosine receptor subtypes (A₁, A_2A, A_2B and A₃) have been evaluated. The design was based on the demonstrated approach to novel A₃ adenosine receptor antagonists of adding a third ring to the xanthine structure. Unfortunately, all the synthesized compounds were completely inactive at all four adenosine receptor subtypes independently of their substitutions. Preliminary molecular modeling investigation has demonstrated that only a low degree of steric and electrostatic complementarity has been observed for all the new synthesized triazolo-purines with respect to other structurally related A₃ receptor antagonists. This analysis yielded valuable information about structure–activity relationships and further design of potential adenosine receptor antagonists.

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潜在腺苷受体拮抗剂1,3-二甲基-2,4-二氧基-6-甲基-8-(取代)1,2,3,4-四氢[1,2,4]-三唑[3,4-f]-嘌呤的合成、生物学研究和分子模型研究

合成了一系列具有[1,2,4]-三唑-[3,4-f]-嘌呤结构的潜在腺苷受体拮抗剂，并对其在4种腺苷受体亚型(A1, A2A, A2B和A3)上的亲和力进行了评价。该设计基于在黄嘌呤结构上添加第三环的新型A3腺苷受体拮抗剂的演示方法。不幸的是，所有合成的化合物在所有四种腺苷受体亚型上都完全失活，独立于它们的取代。初步的分子模拟研究表明，所有新合成的三唑嘌呤相对于其他结构相关的A3受体拮抗剂只有低程度的空间和静电互补性。该分析提供了有关结构-活性关系和进一步设计潜在腺苷受体拮抗剂的有价值的信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Farmaco (Societa chimica italiana : 1989)

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