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O-聚糖对于诱导针对携带鞭毛A的致死性感染产生保护性抗体至关重要。

The O-glycan is essential for the induction of protective antibodies against lethal infection by flagella A-bearing .

作者信息

Choi Myeongjin, Shridhar Surekha, Fox Heather, Luo Kun, Amin Mohammed N, Tennant Sharon M, Simon Raphael, Cross Alan S

机构信息

Center for Vaccine Development and Global Health, University of Maryland School of Medicine, Baltimore, Maryland, USA.

Korea Institute of Toxicology, Daejeon, Republic of Korea.

出版信息

Infect Immun. 2024 Mar 12;92(3):e0042723. doi: 10.1128/iai.00427-23. Epub 2024 Feb 23.

Abstract

To address the problem of increased antimicrobial resistance, we developed a glycoconjugate vaccine comprised of O-polysaccharides (OPS) of the four most prevalent serotypes of (KP) linked to recombinant flagellin types A and B (rFlaA and rFlaB) of (PA). Flagellin is the major subunit of the flagellar filament. Flagella A and B, essential virulence factors for PA, are glycosylated with different glycans. We previously reported that while both rFlaA and rFlaB were highly immunogenic, only the rFlaB antisera reduced PA motility and protected mice from lethal PA infection in a mouse model of thermal injury. Since recombinant flagellin is not glycosylated, we examined the possibility that the glycan on native FlaA (nFlaA) might be critical to functional immune responses. We compared the ability of nFlaA to that of native, deglycosylated FlaA (dnFlaA) to induce functionally active antisera. O glycan was removed from nFlaA with trifluoromethanesulfonic acid. Despite the similar high-titered anti-FlaA antibody levels elicited by nFlaA, rFlaA, and dnFlaA, only the nFlaA antisera inhibited PA motility and protected mice following lethal intraperitoneal bacterial challenge. Both the protective efficacy and carrier protein function of nFlaA were retained when conjugated to KP O1 OPS. We conclude that unlike the case with FlaB O glycan, the FlaA glycan is an important epitope for the induction of functionally active anti-FlaA antibodies.

摘要

为解决抗菌药物耐药性增加的问题,我们研发了一种糖缀合物疫苗,该疫苗由肺炎克雷伯菌(KP)四种最常见血清型的O-多糖(OPS)与铜绿假单胞菌(PA)的重组鞭毛蛋白A和B型(rFlaA和rFlaB)连接而成。鞭毛蛋白是鞭毛丝的主要亚基。鞭毛A和B是PA的重要毒力因子,它们被不同的聚糖糖基化。我们之前报道过,虽然rFlaA和rFlaB都具有高度免疫原性,但在热损伤小鼠模型中,只有rFlaB抗血清能降低PA的运动性并保护小鼠免受致死性PA感染。由于重组鞭毛蛋白未被糖基化,我们研究了天然FlaA(nFlaA)上的聚糖可能对功能性免疫反应至关重要的可能性。我们比较了nFlaA与天然去糖基化FlaA(dnFlaA)诱导功能活性抗血清的能力。用三氟甲磺酸从nFlaA上去除O聚糖。尽管nFlaA、rFlaA和dnFlaA引发的抗FlaA抗体水平相似,但只有nFlaA抗血清在致死性腹腔细菌攻击后能抑制PA的运动性并保护小鼠。当与KP O1 OPS偶联时,nFlaA的保护效力和载体蛋白功能均得以保留。我们得出结论,与FlaB O聚糖的情况不同,FlaA聚糖是诱导功能活性抗FlaA抗体的重要表位。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6fb/10929410/0f9ccee680d4/iai.00427-23.f001.jpg

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