Orally active cephalosporins. Part 4: synthesis, structure--activity relationships and oral absorption of novel 3-(4-pyrazolylmethylthio)cephalosporins with various C-7 side chains.

Yamamoto H; Eikyu Y; Okuda S; Kawabata K; Takasugi H; Tanaka H; Matsumoto S; Matsumoto Y; Tawara S

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Orally active cephalosporins. Part 4: synthesis, structure--activity relationships and oral absorption of novel 3-(4-pyrazolylmethylthio)cephalosporins with various C-7 side chains.

机译：口服活性头孢菌素。第4部分：具有各种C-7侧链的新型3-（4-吡唑基甲硫基）头孢菌素的合成，结构-活性关系和口服吸收。

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A series of 3-(4-pyrazolylmethylthio)cephalosporins with various C-7 side chains was designed, synthesized and evaluated for antibacterial activity and oral absorption in rats. Antibacterial activity against Haemophilus influenzae was markedly increased by the C-7 oxime moiety. Deamination at the 2 position of, or introduction of a substituent such as halogen or methyl to, the 5 position of the (Z)-2-(2-aminothiazol-4-yl)-2-(hydroxyimino) moiety improved oral absorption. Among these compounds, FR192752 having a (Z)-2-(2-amino-5-chlorothiazol-4-yl)-2-hydroxyiminoacetamido moiety, showed potent antibacterial activity against both Gram-positive and Gram-negative bacteria including H.influenzae and penicillin G-resistant Streptococcus pneumoniae (PRSP). Further, it showed higher oral absorption than CFDN and FK041.

机译：设计，合成了一系列具有各种C-7侧链的3-（4-吡唑基甲硫基）头孢菌素，并评估了其在大鼠中的抗菌活性和口服吸收。 C-7肟部分显着提高了对流感嗜血杆菌的抗菌活性。在（Z）-2-（2-氨基噻唑-4-基）-2-（羟基亚氨基）部分的5位的2位脱氨基或向其引入卤素或甲基等取代基改善了口服吸收。在这些化合物中，具有（Z）-2-（2-氨基-5-氯噻唑-4-基）-2-羟基亚氨基乙酰胺基的FR192752对革兰氏阳性和革兰氏阴性细菌（包括流感嗜血杆菌）均显示出强大的抗菌活性。和耐青霉素G的肺炎链球菌（PRSP）。此外，它显示出比CFDN和FK041更高的口服吸收。

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《Bioorganic and medicinal chemistry 》 |2002年第5期| 共11页
作者
Yamamoto H; Eikyu Y; Okuda S; Kawabata K; Takasugi H; Tanaka H; Matsumoto S; Matsumoto Y; Tawara S;
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Cephalosporins; 头孢菌素类;

机译：Cephalosporins;头孢菌素类;

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1. Orally active cephalosporins. Part 4: synthesis, structure--activity relationships and oral absorption of novel 3-(4-pyrazolylmethylthio)cephalosporins with various C-7 side chains. [J] . Yamamoto H, Eikyu Y, Okuda S, Bioorganic and medicinal chemistry . 2002 ,第5期

机译：口服活性头孢菌素。第4部分：具有各种C-7侧链的新型3-（4-吡唑基甲硫基）头孢菌素的合成，结构-活性关系和口服吸收。
2. Orally active cephalosporins. Part 3: synthesis, structure-activity relationships and oral absorption of novel C-3 heteroarylmethylthio cephalosporins. [J] . Yamamoto H, Terasawa T, Nakamura A, Bioorganic and medicinal chemistry . 2001 ,第2期

机译：口服活性头孢菌素。第3部分：新型C-3杂芳基甲硫基头孢菌素的合成，构效关系和口服吸收。
3. Orally active cephalosporins. Part 2: synthesis, structure-activity relationships and oral absorption of cephalosporins having a C-3 pyridyl side chain. [J] . Yamamoto H, Terasawa T, Nakamura A, Bioorganic and medicinal chemistry . 2000 ,第5期

机译：口服活性头孢菌素。第2部分：具有C-3吡啶基侧链的头孢菌素的合成，构效关系和口服吸收。
4. ENAHNCED ORAL ABSORPTION OF CELECOXIB IN HUMAN SUBJECTS FROM SELF-EMULSIFYING ORAL DELIVERY SYSTEM [C] . Mamdouh M.Ghorab Proceedings of the 29th Annual Meeting of the Controlled Release Society . 2002

机译：自乳化口腔输送系统增强塞来昔布在人体中的口腔吸收
5. Solid state moisture interaction studies with some oral cephalosporins. [D] . Wadgaonkar, Dilip Bhanudas. 1992

机译：与某些口服头孢菌素的固态水分相互作用研究。
6. In vitro susceptibilities of Bordetella pertussis and Bordetella parapertussis to six new oral cephalosporins. [O] . J E Hoppe, J Müller 1990

机译：百日咳博德特氏菌和副百日咳博德特氏菌对六种新的口服头孢菌素的体外敏感性。
7. Orally Active Cephalosporins. IV. Synthesis, Antibacterial Activity and Oral Absorption of 3-(1H-1,2,3-Triazol-4-yl)thiomethylthio-cephalosporins. [O] . Masaharu KUME, Tadatoshi KUBOTA, Yasuo KIMURA, 1993

机译：口服活跃的头孢菌素。 IV。合成，抗菌活性和3-（1H-1,2,3-三唑-4-基）硫代甲基孢子的口服吸收。
8. Design and Synthesis of Orally Active Inhibitors of Botulinum ToxinMetalloproteases [R] . Zdanovsky, A. G. 1997

机译：肉毒毒素蛋白酶口服活性抑制剂的设计与合成

Orally active cephalosporins. Part 4: synthesis, structure--activity relationships and oral absorption of novel 3-(4-pyrazolylmethylthio)cephalosporins with various C-7 side chains.

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