Antiinflammatory property of 3-aryl-5-(n-propyl)1,2,4-oxadiazoles and antimicrobial property of 3-aryl-5-(n-propyl)-4,5-dihydro-1,2,4-oxadiazoles:: Their syntheses and spectroscopic studies

被引：79

作者：

Srivastava, RM

Lima, AD

Viana, SS

Silva, MJD

Catanho, MTJA

de Morais, JOF

机构：

[1] Univ Fed Pernambuco, Dept Quim Fundamental, BR-50740540 Recife, PE, Brazil

[2] Univ Fed Pernambuco, Dept Biofis, Recife, PE, Brazil

[3] Univ Fed Pernambuco, Dept Antibiot, BR-50690901 Recife, PE, Brazil

来源：

BIOORGANIC & MEDICINAL CHEMISTRY | 2003年 / 11卷 / 08期

关键词：

D O I：

10.1016/S0968-0896(03)00035-X

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The synthesis of six 3-aryl-5-(n-propyl)-4,5dihydro-1,2,4-oxadiazoles 3a-f has been achieved in a facile manner by the reaction of an appropriate arylamidoxime 1a-f with butyraldehyde 2. Oxidation of 3a-f individually using MnO2 in CH2Cl2 or sodium hypochlorite in THF/H2O furnished 1,2,4-oxadiazoles 4a-f in good to excellent yields. Compounds 4a-f were also evaluated against inflammation. Except 4e, all of them reduced inflammation, however, 4c presented better antiinflammatory activity. A preliminary antimicrobial activity tests of 3a-f showed that these compounds possess activity against some microorganisms. In fact, 3c and 3f have been found to be more effective against Stapkylococcus aureus, Mycobacterium smegmatis, and Candida albicans. (C) 2003 Elsevier Science Ltd. All rights reserved.

引用

页码：1821 / 1827

页数：7

共 22 条

[11] Structural basis for selective inhibition of cyclooxygenase-2 by anti-inflammatory agents [J].

Kurumbail, RG ;

Stevens, AM ;

Gierse, JK ;

McDonald, JJ ;

Stegeman, RA ;

Pak, JY ;

Gildehaus, D ;

Miyashiro, JM ;

Penning, TD ;

Seibert, K ;

Isakson, PC ;

Stallings, WC .

NATURE, 1996, 384 (6610) :644-648

[12] CARRAGEENAN PAW EDEMA IN MOUSE [J].

LEVY, L .

LIFE SCIENCES PART 1 PHYSIOLOGY AND PHARMACOLOGY AND PART 2 BIOCHEMISTRY GENERAL AND MOLECULAR BIOLOGY, 1969, 8 (11P1) :601-&

[13] Novel terphenyls as selective cyclooxygenase-2 inhibitors and orally active anti-inflammatory agents [J].

Li, JJ ;

Norton, MB ;

Reinhard, EJ ;

Anderson, GD ;

Gregory, SA ;

Isakson, PC ;

Koboldt, CM ;

Masferrer, JL ;

Perkins, WE ;

Seibert, K ;

Zhang, Y ;

Zweifel, BS ;

Reitz, DB .

JOURNAL OF MEDICINAL CHEMISTRY, 1996, 39 (09) :1846-1856

[14] Flexibility of the NSAID binding site in the structure of human cyclooxygenase-2 [J].

Luong, C ;

Miller, A ;

Barnett, J ;

Chow, J ;

Ramesha, C ;

Browner, MF .

NATURE STRUCTURAL BIOLOGY, 1996, 3 (11) :927-933

[15]

MALAVAUD C, 1973, B SOC CHIM FR II-CH, P2996

[16]

MPONDO TNG, 1972, CR ACAD SCI C CHIM, V274, P2026

[17] SYNTHESIS, SPECTROSCOPIC STUDIES AND THE MECHANISM OF FORMATION OF 4,5-DIHYDRO-1,2,4-OXADIAZOLES [J].

SRIVASTAVA, RM ;

FREIRE, MVS ;

CHAVES, ASSC ;

BELTRAO, TM ;

CARPENTER, GB .

JOURNAL OF HETEROCYCLIC CHEMISTRY, 1987, 24 (01) :101-105

[18]

Srivastava RM, 2000, HETEROCYCL COMMUN, V6, P41

[19] Synthesis of 3-aryl-5-[thien-3-yl methyl]-1,2,4-oxadiazoles [J].

Srivastava, RM ;

Oliveira, FJS ;

Machado, DS ;

Souto-Maior, RM .

SYNTHETIC COMMUNICATIONS, 1999, 29 (09) :1437-1450

[20] INDUCIBLE ISOFORMS OF CYCLOOXYGENASE AND NITRIC-OXIDE SYNTHASE IN INFLAMMATION [J].

VANE, JR ;

MITCHELL, JA ;

APPLETON, I ;

TOMLINSON, A ;

BISHOPBAILEY, D ;

CROXTALL, J ;

WILLOUGHBY, DA .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (06) :2046-2050

← 1 2 3 →