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针对葡萄球菌多聚-N-乙酰-β-(1-6)-葡萄糖胺低乙酰化形式的抗体优先保护效力的分子基础。

Molecular basis for preferential protective efficacy of antibodies directed to the poorly acetylated form of staphylococcal poly-N-acetyl-beta-(1-6)-glucosamine.

作者信息

Cerca Nuno, Jefferson Kimberly K, Maira-Litrán Tomas, Pier Danielle B, Kelly-Quintos Casie, Goldmann Donald A, Azeredo Joana, Pier Gerald B

机构信息

Channing Laboratory, Brigham and Women's Hospital, Harvard Medical School, 181 Longwood Avenue, Boston, MA 02115, USA.

出版信息

Infect Immun. 2007 Jul;75(7):3406-13. doi: 10.1128/IAI.00078-07. Epub 2007 Apr 30.

Abstract

Poly-N-acetyl-glucosamine (PNAG) is a staphylococcal surface polysaccharide influencing biofilm formation that is also under investigation for its vaccine potential. Antibodies that bind to PNAG with either low (<15%) or high (>90%) levels of acetate are superior at opsonic and protective activity compared with antibodies that bind to PNAG with only high levels (>70%) of acetate. PNAG is synthesized by four proteins encoded within the intercellular adhesin (ica) locus icaADBC. In Staphylococcus epidermidis, icaB encodes a deacetylase needed for the surface retention of PNAG and optimal biofilm formation. In this study, we confirmed that icaB plays a similar role in Staphylococcus aureus and found that an icaB mutant of S. aureus expressed significantly less surface-associated PNAG, was highly susceptible to antibody-independent opsonic killing that could not be enhanced with antibody raised against deacetylated PNAG (dPNAG), and had reduced survival capacity in a murine model of bacteremia. In contrast, an icaB-overexpressing strain produced primarily surface-associated PNAG, was more susceptible to opsonophagocytosis with antibody to dPNAG, and had increased survival in a murine bacteremia model. The highly acetylated secreted PNAG was more effective at blocking opsonic killing mediated by a human monoclonal antibody (mAb) to native PNAG than it was at blocking killing mediated by a human mAb to dPNAG, which by itself was a more effective opsonin. Retention of dPNAG on the surface of S. aureus is key to increased survival during bacteremia and also provides a molecular mechanism explaining the superior opsonic and protective activity of antibody to dPNAG.

摘要

聚 - N - 乙酰葡糖胺(PNAG)是一种影响生物膜形成的葡萄球菌表面多糖,其疫苗潜力也在研究中。与仅结合高乙酸盐水平(>70%)的PNAG的抗体相比,结合低乙酸盐水平(<15%)或高乙酸盐水平(>90%)的PNAG的抗体在调理和保护活性方面更具优势。PNAG由细胞间黏附素(ica)基因座icaADBC内编码的四种蛋白质合成。在表皮葡萄球菌中,icaB编码一种PNAG表面保留和最佳生物膜形成所需的脱乙酰酶。在本研究中,我们证实icaB在金黄色葡萄球菌中起类似作用,并发现金黄色葡萄球菌的icaB突变体表达的表面相关PNAG显著减少,对抗体非依赖性调理杀伤高度敏感,这种杀伤不能通过针对脱乙酰化PNAG(dPNAG)产生的抗体增强,并且在菌血症小鼠模型中的生存能力降低。相比之下,icaB过表达菌株主要产生表面相关的PNAG,对dPNAG抗体的调理吞噬作用更敏感,并且在小鼠菌血症模型中的生存率增加。高度乙酰化的分泌型PNAG在阻断由针对天然PNAG的人单克隆抗体(mAb)介导的调理杀伤方面比阻断由针对dPNAG的人mAb介导的杀伤更有效,而后者本身是一种更有效的调理素。dPNAG在金黄色葡萄球菌表面的保留是菌血症期间生存增加的关键,并且还提供了一种分子机制来解释针对dPNAG的抗体的优越调理和保护活性。

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