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B族链球菌血清型III临床分离株携带162kb和183kb毒力标记物对人非极化呼吸道上皮16HBE 14o-细胞的细胞内生存能力。

Intracellular viability in human non-polarized respiratory epithelial 16 HBE 14o- cells by group B Streptococcus serotype III clinical isolates presenting 162-kb and 183-kb virulence markers.

作者信息

Sá de São José Adriana, Miyazaki Neide Hirome T, Hirata Raphael, Mattos-Guaraldi Ana Luiza, Nagao Prescilla Emy

机构信息

Departamento de Biologia Celular e Genética, Instituto de Biologia Roberto Alcântara Gomes, Universidade do Estado do Rio de Janeiro, Maracanã, Brazil.

出版信息

Int J Mol Med. 2006 Mar;17(3):533-8.

PMID:16465404
Abstract

Group B streptococci (GBS), mainly serotype III, are the major cause of neonatal pneumonia, sepsis and meningitis. Virulence potential of GBS strains may determine the outcome of host colonization or infection. Because the lung constitutes a first step in GBS systemic invasion processes, we investigated the adherence and invasion mechanisms of GBS-III clinical isolates to non-polarized human bronchial epithelial 16 HBE 14o- cell line. The presence of genotypic 162-kb and 183-kb virulence markers in all strains was also examined by PFGE. The 162-kb fragment was detected in both liquor (GBS-III 90356) and vagina (GBS-III 39A) isolates, while 183-kb fragment was only observed in strains (GBS-III 39A, 89A, and 80340) isolated from vagina of asymptomatic carriers. The actin-dependent ability to internalize within non-polarized epithelial respiratory cells was demonstrated only by GBS-III clinical isolates presenting the 162-kb virulence marker. GBS-III 39A strain isolated from vagina exhibiting both 183-kb and 162-kb fragments showed a more efficient adherence and invasion properties than GBS-III 90356 isolated from liquor (P<0.001). Our data suggest the expression of additional bacterial virulence factors that may favor adherence and survival to non-polarized respiratory epithelial cells with consequent development of systemic diseases by GBS-III, including some strains isolated from asymptomatic carriers.

摘要

B族链球菌(GBS),主要是血清型III,是新生儿肺炎、败血症和脑膜炎的主要病因。GBS菌株的毒力潜力可能决定宿主定植或感染的结果。由于肺部是GBS全身侵袭过程的第一步,我们研究了GBS-III临床分离株对非极化人支气管上皮16HBE 14o-细胞系的黏附和侵袭机制。还通过脉冲场凝胶电泳(PFGE)检测了所有菌株中162-kb和183-kb基因型毒力标记的存在情况。在脑脊液分离株(GBS-III 90356)和阴道分离株(GBS-III 39A)中均检测到162-kb片段,而仅在无症状携带者阴道分离的菌株(GBS-III 39A、89A和80340)中观察到183-kb片段。仅具有162-kb毒力标记的GBS-III临床分离株表现出在非极化上皮呼吸细胞内内化的肌动蛋白依赖性能力。从阴道分离的同时具有183-kb和162-kb片段的GBS-III 39A菌株比从脑脊液中分离的GBS-III 90356表现出更有效的黏附和侵袭特性(P<0.001)。我们的数据表明,存在其他细菌毒力因子,这些因子可能有利于GBS-III对非极化呼吸道上皮细胞的黏附和存活,从而导致全身性疾病的发生,包括一些从无症状携带者中分离出的菌株。

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