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血清对11种广谱抗生素体外活性的影响。

Effect of serum on the in vitro activities of 11 broad-spectrum antibiotics.

作者信息

Perl T M, Pfaller M A, Houston A, Wenzel R P

机构信息

Department of Medicine, University of Iowa College of Medicine, Iowa City.

出版信息

Antimicrob Agents Chemother. 1990 Nov;34(11):2234-9. doi: 10.1128/AAC.34.11.2234.

Abstract

We evaluated the effect of serum on the in vitro activities of 11 antimicrobial agents against gram-negative isolates obtained from 100 patients with nosocomial bacteremia. The test organisms included 25 stains of Pseudomonas aeruginosa and 75 strains of the family Enterobacteriaceae. MICs were determined by broth microdilution with Mueller-Hinton broth alone or supplemented with 25 or 50% pooled, heat-inactivated human serum (25S or 50S, respectively). Among the antibiotics evaluated, the protein binding ranged from 9 to 95%. The antibiotics tested and their MICs for 90% of the strains tested in 50S included ciprofloxacin (0.12 micrograms/ml), ceftazidime (1 micrograms/ml), imipenem (1 micrograms/ml), aztreonam (4 micrograms/ml), cefpirome (4 micrograms/ml), cefotaxime (16 micrograms/ml), cefoperazone (16 micrograms/ml), desacetylcefotaxime plus cefotaxime (32 micrograms/ml), ceftriaxone (greater than 32 micrograms/ml), ticarcillin (128 micrograms/ml), and desacetylcefotaxime (greater than 128 micrograms/ml). MICs for 90% of the strains tested were calculated with 95% confidence intervals to show the precision of the MICs for these strains. With the exceptions of ceftriaxone (greater than 95% protein bound) and cefoperazone (90% protein bound), serum had no significant effect on the in vitro activities of various agents. A fourfold-or-greater increase in the MIC of ceftriaxone was observed in 45 of 100 isolates with 50S and in 30 of 100 isolates with 25S. With cefoperazone, 17 of 100 isolates demonstrated more than 2 twofold dilution increases in 50S. Testing of antibiotics which were less protein bound illustrated minor effects primarily with members of the Enterobacteriaceae. The presence of serum did not adversely affect the in vitro activities of broad-spectrum agents against these nosocomial isolates.

摘要

我们评估了血清对11种抗菌药物针对从100例医院获得性菌血症患者中分离出的革兰氏阴性菌的体外活性的影响。测试菌株包括25株铜绿假单胞菌和75株肠杆菌科细菌。采用肉汤微量稀释法,分别用单独的 Mueller-Hinton肉汤或添加25%或50%混合的热灭活人血清(分别为25S或50S)来测定最低抑菌浓度(MIC)。在所评估的抗生素中,蛋白结合率范围为9%至95%。在50S中测试的抗生素及其对90%测试菌株的MIC包括环丙沙星(0.12微克/毫升)、头孢他啶(1微克/毫升)、亚胺培南(1微克/毫升)、氨曲南(4微克/毫升)、头孢匹罗(4微克/毫升)、头孢噻肟(16微克/毫升)、头孢哌酮(16微克/毫升)、去乙酰头孢噻肟加头孢噻肟(32微克/毫升)、头孢曲松(大于32微克/毫升)、替卡西林(128微克/毫升)和去乙酰头孢噻肟(大于128微克/毫升)。计算90%测试菌株的MIC,并给出95%置信区间以显示这些菌株MIC的精确性。除头孢曲松(蛋白结合率大于95%)和头孢哌酮(蛋白结合率90%)外,血清对各种药物的体外活性无显著影响。在100株分离菌中,45株在50S血清存在时以及30株在25S血清存在时,头孢曲松的MIC增加了四倍或更多。对于头孢哌酮,100株分离菌中有17株在50S血清存在时显示出超过两倍的稀释度增加。对蛋白结合较少的抗生素进行测试表明,主要对肠杆菌科细菌成员有轻微影响。血清的存在并未对这些广谱药物针对这些医院分离菌的体外活性产生不利影响。

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