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首页> 外文期刊>Antimicrobial agents and chemotherapy. >gyrA and gyrB Mutations Are Implicated in Cross-Resistance to Ciprofloxacin and Moxifloxacin in Clostridium difficile.
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gyrA and gyrB Mutations Are Implicated in Cross-Resistance to Ciprofloxacin and Moxifloxacin in Clostridium difficile.

机译:gyrA和gyrB突变涉及艰难梭菌中对环丙沙星和莫西沙星的交叉耐药性。

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摘要

A total of 198 nonrepetitive clinical strains of Clostridium difficile isolated from different French hospitals in 1991 (n = 100) and 1997 (n = 98) were screened for decreased susceptibility to fluoroquinolones by plating onto Wilkins-Chalgren agar containing 16 micro g of ciprofloxacin per ml. The frequency of decreased susceptibility was 7% (14 of 198) and was identical for the years 1991 and 1997. Serogroups C, H, D, A9, and K accounted for five, four, two, one, and one of the resistant strains, respectively, one strain being nontypeable. Arbitrarily primed PCR typing showed that all resistant strains had unique patterns except two serotype C strains, which could not be clearly distinguished. All isolates with decreased susceptibility carried a mutation either in gyrA (eight mutations, amino acid changes Asp71-->Val in one, Thr82-->Ile in six, and Ala118-->Thr in one) or in gyrB (six mutations, amino acid changes Asp426-->Asn in five and Arg447-->Leu in one). These changes are similar to those already described in other species except for Asp71-->Val, which is novel, and Ala118-->Thr, which is exceptional. Attempts to detect the topoisomerase IV parC gene by PCR amplification with universal parC primers or DNA-DNA hybridization under low-stringency conditions were unsuccessful. The susceptibilities of all resistant strains to ciprofloxacin and ethidium bromide were not affected by the addition of reserpine at 20 micro g/ml. In conclusion, decreased susceptibility to fluoroquinolones in C. difficile is rare in France and is associated with the occurrence of a gyrA or gyrB mutation.
机译:分别于1991年(n = 100)和1997年(n = 98)从法国不同医院分离出的198株难辨梭状芽胞杆菌临床菌株,通过将其平板接种到每毫升含16微克环丙沙星的Wilkins-Chalgren琼脂上,筛选出对氟喹诺酮类药物敏感性降低的方法。毫升易感性降低的频率为7%(198个中的14个),并且在1991年和1997年相同。血清群C,H,D,A9和K占抗药性菌株的5、4、2、1和1个。分别是一种菌株是不可分型的。任意引发的PCR分型显示,除两个血清型C菌株外,所有抗性菌株均具有独特的模式,无法清楚地区分。所有敏感性降低的分离株都在gyrA中突变(八个突变,一个氨基酸突变Asp71-> Val,一个在Thr82-> Ile中,六个在Ala118-> Thr中,在一个gyrB中突变(六个突变,氨基酸变化Asp426-> Asn变为5,而Arg447-> Leu变为1)。这些变化与其他物种中已描述的变化相似,除了新颖的Asp71-> Val和例外的Ala118-> Thr。通过通用parC引物进行PCR扩增或在低严格条件下进行DNA-DNA杂交检测拓扑异构酶IV parC基因的尝试均未成功。加入20μg / ml的利血平不会影响所有对环丙沙星和溴化乙锭具有抗性的菌株的敏感性。总之,在法国难辨梭状芽胞杆菌对氟喹诺酮类药物的敏感性降低在法国很少见,并且与gyrA或gyrB突变的发生有关。

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