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Mutational Replacement of Leu-293 in the Class C Enterobacter cloacae P99 β-Lactamase Confers Increased MIC of Cefepime

机译:C类阴沟肠杆菌P99β-内酰胺酶中Leu-293的突变替换可提高头孢吡肟的MIC

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摘要

The class C β-lactamase from Enterobacter cloacae P99 confers resistance to a wide range of broad-spectrum β-lactams but not to the newer cephalosporin cefepime. Using PCR mutagenesis of the E. cloacae P99 ampC gene, we obtained a Leu-293-Pro mutant of the P99 β-lactamase conferring a higher MIC of cefepime (MIC, 8 μg/ml, compared with 0.5 μg/ml conferred by the wild-type enzyme). In addition, the mutant enzyme produced higher resistance to ceftazidime but not to the other β-lactams tested. Mutants with 15 other replacements of Leu-293 were prepared by site-directed random mutagenesis. None of these mutant enzymes conferred MICs of cefepime higher than that conferred by Leu-293-Pro. We determined the kinetic parameters of the purified E. cloacae P99 β-lactamase and the Leu-293-Pro mutant enzyme. The catalytic efficiencies (kcat/Km) of the Leu-293-Pro mutant β-lactamase for cefepime and ceftazidime were increased relative to the respective catalytic efficiencies of the wild-type P99 β-lactamase. These differences likely contribute to the higher MICs of cefepime and ceftazidime conferred by this mutant β-lactamase.
机译:阴沟肠杆菌P99的C类β-内酰胺酶可抵抗多种广谱β-内酰胺,但对较新的头孢菌素头孢吡肟则无抵抗力。使用阴沟肠杆菌P99 ampC基因的PCR诱变,我们获得了P99β-内酰胺酶的Leu-293-Pro突变体,赋予头孢吡肟的MIC较高(MIC为8μg/ ml,而头孢吡肟的MIC为0.5μg/ ml。野生型酶)。另外,突变酶对头孢他啶产生更高的抗性,但对其他测试的β-内酰胺则没有。通过定点随机诱变制备具有15个其他Leu-293替代物的突变体。这些突变酶均不能使头孢吡肟的MIC高于Leu-293-Pro所赋予的MIC。我们确定了纯化的阴沟肠杆菌P99β-内酰胺酶和Leu-293-Pro突变酶的动力学参数。相对于野生型P99β-内酰胺酶的各自催化效率,Leu-293-Pro突变体β-内酰胺酶对头孢吡肟和头孢他啶的催化效率(kcat / Km)增加。这些差异可能有助于该突变的β-内酰胺酶赋予头孢吡肟和头孢他啶的更高的MIC。

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