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Versatility of Biofilm Matrix Molecules in Staphylococcus epidermidis Clinical Isolates and Importance of Polysaccharide Intercellular Adhesin Expression during High Shear Stress

机译:表皮葡萄球菌临床分离株中生物膜基质分子的多功能性和高剪切应力下多糖细胞间粘附素表达的重要性

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Staphylococcus epidermidis is a leading cause of hospital-associated infections, including those of intravascular catheters, cerebrospinal fluid shunts, and orthopedic implants. Multiple biofilm matrix molecules with heterogeneous characteristics have been identified, including proteinaceous, polysaccharide, and nucleic acid factors. Two of the best-studied components in S.?epidermidis include accumulation-associated protein (Aap) and polysaccharide intercellular adhesin (PIA), produced by the enzymatic products of the icaADBC operon. Biofilm composition varies by strain as well as environmental conditions, and strains producing PIA-mediated biofilms are more robust. Clinically, biofilm-mediated infections occur in a variety of anatomical sites with diverse physiological properties. To test the hypothesis that matrix composition exhibits niche specificity, biofilm-related genetic and physical properties were compared between S.?epidermidis strains isolated from high-shear and low-shear environments. Among a collection of 105 clinical strains, significantly more isolates from high-shear environments carried the icaADBC operon than did those from low-shear settings (43.9% versus 22.9%, P 0.05). Additionally, a significantly greater number of high-shear isolates were capable of forming biofilm in vitro in a microtiter assay (82.5% versus 45.8%, P < 0.0001). However, even among high-shear clinical isolates, less than half contained the icaADBC locus; therefore, we selected for ica -negative variants with increased attachment to abiotic surfaces to examine PIA-independent biofilm mechanisms. Sequencing of selected variants identified substitutions capable of enhancing biofilm formation in multiple genes, further highlighting the heterogeneity of S.?epidermidis biofilm molecules and mechanisms. IMPORTANCE Staphylococcus epidermidis is a leading cause of infections related to biomaterials, mostly due to their ability to form biofilm. Biofilm accumulation mechanisms vary, including those that are dependent on specific proteins, environmental DNA (eDNA), or polysaccharide intercellular adhesin (PIA). We found that those isolates obtained from high-shear environments, such as the lumen of a catheter, are more likely to produce PIA-mediated biofilms than those isolates obtained from a low-shear biomaterial-related infection. This suggests that PIA functions as a mechanism that is protective against shear flow. Finally, we performed selection experiments documenting the heterogeneity of biofilm accumulation molecules that function in the absence of PIA, further documenting the biofilm-forming potential of S.?epidermidis .
机译:表皮葡萄球菌是医院相关感染的主要原因,包括血管内导管,脑脊液分流管和整形外科植入物。已经鉴定出具有异质特性的多个生物膜基质分子,包括蛋白质,多糖和核酸因子。在表皮葡萄球菌中研究得最好的两个成分包括由icaADBC操纵子的酶促产物产生的积累相关蛋白(Aap)和多糖细胞间粘附素(PIA)。生物膜的组成因菌株以及环境条件而异,并且产生PIA介导的生物膜的菌株更为牢固。临床上,生物膜介导的感染发生在具有不同生理特性的各种解剖部位。为了检验假说基质组成表现出利基特异性的假说,比较了从高剪切和低剪切环境分离的表皮葡萄球菌菌株与生物膜相关的遗传和物理特性。在105种临床菌株中,来自高剪切环境的分离株携带icaADBC操纵子的比例要比来自低剪切环境的分离株高(43.9%比22.9%,P 0.05)。另外,在微量滴定分析中,大量的高剪切分离物能够在体外形成生物膜(82.5%对45.8%,P <0.0001)。但是,即使在高剪切力临床分离株中,也只有不到一半包含icaADBC基因座。因此,我们选择了与非生物表面具有更高附着力的ica阴性变体,以检查独立于PIA的生物膜机制。所选变体的测序鉴定出能够增强多个基因中生物膜形成的取代,进一步突出了表皮葡萄球菌生物膜分子和机制的异质性。重要表皮葡萄球菌是与生物材料有关的感染的主要原因,主要是由于它们形成生物膜的能力。生物膜的积累机制各不相同,包括那些依赖于特定蛋白质,环境DNA(eDNA)或多糖细胞间粘附素(PIA)的机制。我们发现,从高剪切环境(如导管内腔)获得的分离株比从低剪切生物材料相关感染获得的分离株更有可能产生PIA介导的生物膜。这表明PIA起到防止剪切流的作用。最后,我们进行了选择实验,证明了在没有PIA的情况下起作用的生物膜积累分子的异质性,进一步证明了表皮葡萄球菌的生物膜形成潜力。

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