Synthesis and antiinflammatory activity of 2H-tetrazol-2-acetic acids, esters and amides.

Drug design and delivery Pub Date : 1990-09-01
P Kumar, E E Knaus
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Abstract

A series of 5-(pyridyl)-2H-tetrazol-2-acetic acids (16-21), esters (10-15), and amides (22-27) was synthesized in order to investigate the effect of 5-substituents (R1 = 2-, 3- or 4-pyridyl) and alpha-substituents (R2 = H, Me) on anti-inflammatory activity. The point of attachment of the R1-pyridyl substituent influenced potency. The relative potencies in the acetic acid ester, acetic acid and acetamide classes of compounds were 2- and 4- greater than 3-pyr, 2- and 3- greater than 4-pyr, and 4- greater than 2- and 3-pyr, respectively. In the acetic acid ester and acetamide classes, compounds having a R2 hydrogen substituent were generally more potent than corresponding methyl substituted compounds, whereas, in the acetic acid class the reverse applied. The relative order of anti-inflammatory potency was generally amide greater than ester greater than acid. 2-[5-(4-Pyridyl)-2H-tetrazol-2-yl]acetamide (26) was the most effective antiinflammatory agent in the series, reducing inflammation by 53% at 3 and 5 hr after a 25 mg/kg po dose.

2h -四氮唑-2-乙酸、酯和酰胺的合成及其抗炎活性。
合成了一系列5-(吡啶基)- 2h -四唑-2-乙酸(16-21)、酯(10-15)和酰胺(22-27),研究了5-取代基(R1 = 2-、3-或4-吡啶基)和α -取代基(R2 = H, Me)对抗炎活性的影响。r1 -吡啶取代基的附着点影响其效价。乙酸酯类、乙酸类和乙酰胺类化合物的相对效价分别为2-和4-大于3-pyr, 2-和3-大于4-pyr, 4-大于2-和3-pyr。在乙酸酯类和乙酰胺类中,具有R2氢取代基的化合物通常比相应的甲基取代化合物更有效,而在乙酸类中则相反。抗炎效力的相对顺序一般为酰胺>酯>酸。2-[5-(4-吡啶基)- 2h -四唑-2-基]乙酰胺(26)是该系列中最有效的抗炎药,在25 mg/kg po剂量后3和5小时炎症减轻53%。
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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