儿科患者泰比培南细菌分离株药敏的年度变化调查——儿科泰比培南透视酯颗粒上市后的监测。

The Japanese journal of antibiotics Pub Date : 2016-08-01
Toshie Sugano, Toshihiko Takata, Nami Senju, Yoshihiro Takayama, Takashi Ida
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引用次数: 0

摘要

我们对口服碳青霉烯类抗菌剂泰比培南pivoxil (10% orapene fine granules for pediatric)进行了上市后监测,以研究细菌对泰比培南(TBPM)的敏感性变化。本次监测中使用的菌株是2010年4月至2015年3月期间从日本15家医疗机构的儿科患者中分离到的甲氧西林敏感金黄色葡萄球菌(MSSA: 303株)、肺炎链球菌(554株)、其他链球菌(242株:包括化脓性链球菌133株)、卡他莫拉菌(306株)和流感嗜血杆菌(506株)。调查共进行了3次(2010年4月- 2011年3月、2012年4月- 2013年3月和2014年4月- 2015年3月),在这些调查期间,按年龄分类的分离株频次来看,均存在大量婴幼儿分离株。TBPM对msa、肺炎链球菌、其他链球菌、卡塔林分枝杆菌和流感嗜血杆菌的MIC90值分别为0.015 ~ 0.03、0.06、0.008 ~ 0.015(化脓性链球菌为0.002)、0.03和0.5 ~ 1 μg/mL,均小于2倍,MIC90值未见显著升高。另一方面,包括TBPM和青霉素在内的碳青霉烯类药物对肺炎链球菌的mic50值在调查期间降至1/4 ~ 1/8,gPRSP*¹(48.7% ~ 26.1%)降低和gPISP (2x)*²(24.1% ~ + 46.8%)升高参与了这些敏感性变化。在肺炎链球菌中,mefA*⁴引起的大环内酯类耐药菌株减少(38.5% ~ 18.8%),而ermB*⁴引起的大环内酯类耐药菌株增加(41.7% ~ 62.4%)。在流感嗜血杆菌中,产生gBLNAR* 35和β-内酰胺酶的菌株的频率分别约为60-70%和7-9%,在易感性方面没有明显变化。对从儿科患者中收集的临床分离株进行上市后监测的易感性调查结果显示,TBPM的易感性没有下降。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Investigations on yearly changes in tebipenem susceptibility of bacterial isolates from pediatric patients -A post-marketing surveillance of tebipenem pivoxil granules for pediatric.

We conducted the post-marketing surveillance of tebipenem pivoxil (Orapeneme fine granules 10% for pediatric), an oral carbapenem antibacterial agent, to investigate changes in bacterial susceptibility against tebipenem (TBPM). Bacterial strains used in this surveillance were methicillin-susceptible Staphylococcus aureus (MSSA: 303 strains), Streptococcus pneumoniae (554 strains), other Streptococcus spp. (242 strains: including Streptococcus pyogenes 133 strains), Moraxella catarrhalis (306 strains) and Haemophilus influenzae (506 strains) isolated from pediatric patients in 15 medical facilities in Japan between April 2010 and March 2015. Investigation was conducted three times (April 2010-March 2011, April 2012-March 2013 and April 2014-March 2015), and in any of these investigation periods, there were a large number of isolates from infants in terms of the frequency of isolates by age. The MIC90s of TBPM against MSSA, S. pneumoniae, other Streptococcus spp., M. catarrhalis and H. influenzae in these investigations were 0.015-0.03, 0.06, 0.008-0.015 (0.002 for S. pyogenes), 0.03 and 0.5-1 μg/mL, respectively, which were less than 2-fold, and a remarkable increase in MIC90 was not shown. On the other hand, the MIC50s of carbapenems including TBPM and penicillins against S. pneumoniae decreased to 1/4-1/8 during the investigation periods, and decreased gPRSP*¹ (48.7% - 26.1%) and increased gPISP (2x)*² (24.1% -+ 46.8%) were suggested to be involved in these changes in susceptibility. In S. pneumoniae, a decrease of macrolides-resistant strains due to mefA*³ (38.5% - 18.8%) and an increase of macrolides-resistant strains due to ermB*⁴ (41.7% - 62.4%) were noted. In H. influenzae, the frequencies of gBLNAR*⁵ and β-lactamase-producing strains were about 60-70% and 7-9%, respectively, and a remarkable change in susceptibility was not shown. As a result of investigations in the susceptibility of clinical isolates collected from pediatric patients as post-marketing surveillance, there was no decrease in TBPM susceptibility noted.

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