Enhanced Expression of lmb Gene Encoding Laminin-Binding Protein in Streptococcus agalactiae Strains Harboring IS1548 in scpB-lmb Intergenic Region

被引:47
作者
Al Safadi, Rim [1 ]
Amor, Souheila [1 ]
Hery-Arnaud, Genevieve [1 ]
Spellerberg, Barbara [2 ]
Lanotte, Philippe [1 ]
Mereghetti, Laurent [1 ]
Gannier, Francois [3 ]
Quentin, Roland [1 ,4 ]
Rosenau, Agnes [1 ]
机构
[1] Univ Tours, UFR Med, Equipe Accueil Bacteries & Risque Maternofoetal 3, Inst Federatif Rech Agents Transmissibles & Infec, Tours, France
[2] Univ Ulm Klinikum, Inst Med Mikrobiol & Hyg, Ulm, Germany
[3] Univ Tours, UFR Sci, UMR CNRS FRE Physiol Cellules Cardiaques & Vasc 3, Tours, France
[4] CHRU Tours, Hop Trousseau, Serv Bacteriol & Hyg Hosp, Tours, France
关键词
GROUP-B-STREPTOCOCCUS; INVASIVE NEONATAL DISEASE; MICROVASCULAR ENDOTHELIAL-CELLS; GROUP-II INTRON; C5A PEPTIDASE; MOLECULAR CHARACTERIZATION; INSERTIONAL ACTIVATION; POPULATION-STRUCTURE; BIOFILM FORMATION; EPITHELIAL-CELLS;
D O I
10.1371/journal.pone.0010794
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Group B streptococcus (GBS) is the main cause of neonatal sepsis and meningitis. Bacterial surface proteins play a major role in GBS binding to and invasion of different host surfaces. The scpB and lmb genes, coding for fibronectin-binding and laminin-binding surface proteins, are present in almost all human GBS isolates. The scpB-lmb intergenic region is a hot spot for integration of two mobile genetic elements (MGEs): the insertion element IS1548 or the group II intron GBSi1. We studied the structure of scpB-lmb intergenic region in 111 GBS isolates belonging to the intraspecies major clonal complexes (CCs). IS1548 was mostly found (72.2%) in CC19 serotype III strains recovered more specifically (92.3%) from neonatal meningitis. GBSi1 was principally found (70.6%) in CC17 strains, mostly (94.4%) of serotype III, but also (15.7%) in CC19 strains, mostly (87.5%) of serotype II. No MGE was found in most strains of the other CCs (76.0%), notably CC23, CC10 and CC1. Twenty-six strains representing these three genetic configurations were selected to investigate the transcription and expression levels of scpB and lmb genes. Quantitative RT-PCR showed that lmb transcripts were 5.0- to 9.6-fold higher in the group of strains with IS1548 than in the other two groups of strains (P<0.001). Accordingly, the binding ability to laminin was 3.8- to 6.6-fold higher in these strains (P <= 0.001). Moreover, Lmb amount expressed on the cell surface was 2.4- to 2.7-fold greater in these strains (P<0.001). By contrast, scpB transcript levels and fibronectin binding ability were similar in the three groups of strains. Deletion of the IS1548 sequence between scpB and lmb genes in a CC19 serotype III GBS strain substantially reduced the transcription of lmb gene (13.5-fold), the binding ability to laminin (6.2-fold), and the expression of Lmb protein (5.0-fold). These data highlight the importance of MGEs in bacterial virulence and demonstrate the up-regulation of lmb gene by IS1548; the increased lmb gene expression observed in CC19 serotype III strains with IS1548 may play a role in their ability to cause neonatal meningitis and endocarditis.
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