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鉴定表达非溶血性肺炎球菌溶血素的侵袭性1型肺炎球菌分离株。

Identification of invasive serotype 1 pneumococcal isolates that express nonhemolytic pneumolysin.

作者信息

Kirkham Lea-Ann S, Jefferies Johanna M C, Kerr Alison R, Jing Yu, Clarke Stuart C, Smith Andrew, Mitchell Tim J

机构信息

Division of Infection and Immunity, Institute of Biomedical and Life Sciences, University of Glasgow, Scotland.

出版信息

J Clin Microbiol. 2006 Jan;44(1):151-9. doi: 10.1128/JCM.44.1.151-159.2006.

Abstract

Recently, there has been an increase in invasive pneumococcal disease (IPD) caused by serotype 1 Streptococcus pneumoniae throughout Europe. Serotype 1 IPD is associated with bacteremia and pneumonia in Europe and North America, especially in neonates, and is ranked among the top five most prevalent pneumococcal serotypes in at least 10 countries. The currently licensed pediatric pneumococcal vaccine does not afford protection to this serotype. Upon screening of 252 clinical isolates of S. pneumoniae, we discovered mutations in the pneumolysin gene of two out of the four serotype 1 strains present in the study group. Analysis of an additional 28 serotype 1 isolates from patients with IPD from various Scottish Health Boards, revealed that >50% had mutations in their pneumolysin genes. This resulted in the expression of nonhemolytic forms of pneumolysin. All of the strains producing nonhemolytic pneumolysin were sequence type 306 (ST306), whereas those producing "wild-type" pneumolysin were ST227. The mutations were in a region of pneumolysin involved in pore formation. These mutations can be made in vitro to give the nonhemolytic phenotype. Pneumolysin is generally conserved throughout all serotypes of S. pneumoniae and is essential for full invasive disease; however, it appears that serotype 1 ST306 does not require hemolytically active pneumolysin to cause IPD.

摘要

最近,在欧洲,由1型肺炎链球菌引起的侵袭性肺炎球菌病(IPD)有所增加。在欧洲和北美,1型IPD与菌血症和肺炎相关,尤其是在新生儿中,并且在至少10个国家中位列最常见的五种肺炎球菌血清型之一。目前已获许可的儿科肺炎球菌疫苗对该血清型没有保护作用。在对252株肺炎链球菌临床分离株进行筛查时,我们在研究组中存在的4株1型菌株中的2株的肺炎溶血素基因中发现了突变。对来自苏格兰各个卫生委员会的另外28株IPD患者的1型分离株进行分析后发现,超过50%的菌株其肺炎溶血素基因存在突变。这导致了非溶血型肺炎溶血素的表达。所有产生非溶血型肺炎溶血素的菌株均为序列型306(ST306),而产生“野生型”肺炎溶血素的菌株为ST227。这些突变发生在肺炎溶血素中参与孔形成的区域。这些突变可以在体外产生非溶血表型。肺炎溶血素在所有肺炎链球菌血清型中通常是保守的,并且对于完全侵袭性疾病至关重要;然而,似乎1型ST306血清型在引起IPD时并不需要具有溶血活性的肺炎溶血素。

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