Synthesis and evaluation of new Reissert analogs as HIV-1 RT inhibitors. 2. Benzo[f]quinoline and pyridine derivatives.

Drug design and discovery Pub Date : 1997-04-01
A Monge, E Alvarez, C San Martín, E Nadal, I Ruiz, M Font, J J Martínez-Irujo, E Santiago, I Prieto, J J Lasarte, P Sarobe, F Borrás
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Abstract

The synthesis and preliminary evaluation of new benzo[f]quinoline and pyridine derivatives, obtained by application of the Reissert method and its modifications, as HIV-1 RT inhibitors and anti-infectives are presented. The most active products against HIV-1 RT wild type are the ethyl 2-cyano-1,2-dihydrobenzo[f]quinoline-1-carboxylate 2b, propyl 2-cyano-1,2-dihydrobenzo[f]quinoline-1-carboxylate 2c, and 2-cyano-1-(2'-furoyl)-1,2-dihydrobenzo[f]quinoline 2n, which maintain their activity against the mutant type P236L, resulting inactive against the Y181C type. Using the data previously obtained by our research team for analogous series derived from quinoline as reference, the compounds which have now been obtained present an increase in the cytotoxic character attributable to the introduction of a benzene ring fused with the quinoline base nucleus, as well as a decrease of the activity as HIV-1 RT inhibitors when the quinoline benzenic ring is eliminated.

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新的Reissert类似物作为HIV-1 RT抑制剂的合成和评价。2. 苯并喹啉和吡啶衍生物。
介绍了利用Reissert方法及其修饰获得的新型苯并[f]喹啉和吡啶衍生物的合成和初步评价,这些衍生物可作为HIV-1 RT抑制剂和抗感染药物。对HIV-1 RT野生型最有效的产物是乙基2-氰基1,2-二氢苯并[f]喹啉-1-羧酸2b,丙基2-氰基1,2-二氢苯并[f]喹啉-1-羧酸2c和2-氰基1-(2′-呋喃基)1,2-二氢苯并[f]喹啉2n,它们对突变型P236L保持活性,对Y181C型无效。利用我们的研究团队之前从喹啉衍生的类似系列中获得的数据作为参考,现在获得的化合物由于引入与喹啉碱基核融合的苯环而呈现出细胞毒性增加的特征,并且当喹啉苯环被消除时,作为HIV-1 RT抑制剂的活性降低。
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