首页> 外文期刊>Antimicrobial Resistance and Infection Control >Detection of Pan drug resistance OXA-48 producing Providencia in an ICU patient for the first time in Nepal
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Detection of Pan drug resistance OXA-48 producing Providencia in an ICU patient for the first time in Nepal

机译:尼泊尔首次在ICU患者中检测产生泛耐药性OXA-48的Providencia

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Resistance to antimicrobial agents of pathogenic bacteria has become a major problem in routine medical practices. Carbapenem resistance has long been increasing. The production of carbapenem- hydrolysing β-lactamases (carbapenamases), which include NDM, KPC, OXA-48, IMP-1 and VIM is the most common mechanism. A 56?years old male presented with fever and mental changes with progressively decreasing sensorium for the last 3 days. He was admitted to Intensive care unit (ICU) with a diagnosis of meningoencephalitis. On day seven, he developed ventilator associated pneumonia due Klebsiella pnemoniae and Acinetobacter baumannii. He was on meropenem, but the isolates were susceptible to colistin, tigecyclin and amikacin solely. Hence, amikacin was started with addition of intravenous and nebulized colistin. Subsequently, vital signs improved with resolution of fever. However, on day 18, he developed fever once again with a drop in blood pressure. Inotropic support was maintained, and echinocandins and tigecycline were added to the regimen. Repeat blood and urine culture grew Providencia species, which were resistant to most of the drugs on phenotypic Kirby-Bauer disk diffusion method and are intrinsically resistant to colistin and tigecycline. Phenotypic detection of ESBL (combined disk method), MBL, KPCs, AmpC and co-producer were tested according to updated CLSI guideline and all were negative. But the Modified Hodges test was found to be positive. Consequenty, OXA-48 drug resistance pattern was brought into action by blank disc method according to A Tsakris et al., which revealed indentation of growth toward both EDTA and EDTA/PBA disk indicating production of OXA-48 carbapenamase. To confirm the resistance pattern we processed the isolated colonies for Xpert Carba-R (Cepheid) assay, which detected blaOXA-48 gene and confirmed the OXA-48 drug resistance pattern. Hence, the infecting organism was not susceptible to any of the antibiotics. The patient was kept under isolation and on 31th day of admission, he died of septic shock. Carbapenamase production along with intrinsic colistin resistance in infecting bacterial pathogens can cause fatal outcomes in the resource limited countries like Nepal where new antibiotic combinations ceftazidime+ Avibactam, or aztreonam +avibactam are not available. Drug resistance patterns including OXA 48 producer should be characterized in all cases by standard phenotypic methods or by Xpert Carba-R assay and larger studies are required to know the exact burden of OXA 48 producer in Nepal.
机译:对病原菌的抗菌剂的抗性已成为常规医学实践中的主要问题。长期以来对碳青霉烯的耐药性一直在增加。最常见的机理是产生水解碳青霉烯的β-内酰胺酶(carbapenamases),包括NDM,KPC,OXA-48,IMP-1和VIM。一名56岁的男性在最近3天内表现出发烧和精神变化,感觉觉逐渐下降。他因诊断为脑膜脑炎而被送入重症监护室(ICU)。第七天,他因呼吸道克雷伯菌和鲍曼不动杆菌而患上呼吸机相关性肺炎。他正在服用美罗培南,但分离株仅对大肠杆菌素,替加环素和丁胺卡那霉素敏感。因此,阿米卡星开始于添加静脉内和雾化的粘菌素。随后,随着发烧的消退,生命体征得到改善。但是,在第18天,他又发烧,血压下降。保持正性肌力支持,并在方案中加入棘轮and素和替加环素。重复进行血液和尿液培养,增加了Providencia菌种,它们对表型Kirby-Bauer圆盘扩散法的大多数药物均具有抗性,并且对粘菌素和替加环素具有内在抗性。根据更新的CLSI指南测试了ESBL(组合磁盘方法),MBL,KPC,AmpC和联合生产者的表型检测,所有检测均为阴性。但是发现改良霍奇斯试验是阳性的。因此,根据A Tsakris等人的研究,通过空白圆盘方法使OXA-48耐药性模式起作用,这表明向EDTA和EDTA / PBA圆盘的生长都出现了凹痕,表明产生了OXA-48碳青霉烯酶。为了确认耐药性模式,我们对分离的菌落进行了Xpert Carba-R(造父变星)检测,检测了blaOXA-48基因并确认了OXA-48耐药性模式。因此,感染生物对任何抗生素都不敏感。患者被隔离,入院第31天死于败血性休克。在资源有限的国家(如尼泊尔),碳环戊烷酶的产生以及固有的粘菌素抗性在感染细菌病原体时会导致致命的后果,而尼泊尔则没有新的头孢他啶+阿维巴坦抗生素组合或氨曲南+阿维巴坦抗生素组合。在所有情况下,都应通过标准的表型方法或Xpert Carba-R分析来鉴定包括OXA 48生产者在内的耐药模式,并且需要进行更大的研究才能了解OXA 48生产者在尼泊尔的确切负担。

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