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从百日咳博德特氏菌脂多糖五糖末端合成寡糖,并确定抗百日咳抗体识别的最小表位。

Synthesis of oligosaccharides from terminal B. pertussis LPS pentasaccharide and definition of the minimal epitope recognized by anti-pertussis antibodies.

机构信息

Chengdu Olisynn Biotech. Co., Ltd., Building 3, Tianfu Life science Park. No 88, South Keyuan Rd., Chengdu, Sichuan, 610041, People's Republic of China.

State Key Laboratory of Biotherapy and Cancer Center, West China Hospital, Sichuan University, Chengdu, 610041, People's Republic of China.

出版信息

Glycoconj J. 2024 Oct;41(4-5):241-254. doi: 10.1007/s10719-024-10160-z. Epub 2024 Jul 24.

Abstract

Pertussis vaccines have been very effective in controlling whooping-cough epidemics but are ineffective in controlling circulation in older children and adults, thus facilitating the onset of future outbreaks. Antibodies against the lipopolysaccharide could reduce the carriage of the bacteria, its circulation, and transmission. The oligosaccharide fragments from the lipopolysaccharide may become a potential complement to existing vaccines in the form of protein glycoconjugates. An important step in the development of this type of vaccine is defining the minimal oligosaccharide epitope recognized by B. pertussis anti-lipopolysaccharide antibodies. This paper describes the complete synthesis of oligosaccharides containing two to five monosaccharide units corresponding to the pentasaccharide at the nonreducing end of the lipooligosaccharide and their recognition by mice and rabbit antibodies elicited against whole-cell B. pertussis. For the first time, we report that the terminal disaccharide, α-D-GlcNAcp-(1 → 4)-(2,3-di-NAc)-D-ManAp acid is the minimal structure recognized by antibodies induced by B. pertussis.

摘要

百日咳疫苗在控制百日咳流行方面非常有效,但对控制年长儿童和成人的传播无效,从而促进了未来疫情的爆发。针对脂多糖的抗体可以减少细菌的携带、传播和传播。脂多糖的寡糖片段可能成为现有疫苗的潜在补充形式,即蛋白糖缀合物。这种疫苗开发的重要步骤是确定 B 型百日咳抗脂多糖抗体识别的最小寡糖表位。本文描述了含有两个到五个单糖单元的寡糖的完全合成,这些寡糖对应于脂寡糖非还原端的五糖,以及它们对针对全细胞 B 型百日咳的小鼠和兔抗体的识别。我们首次报道,末端二糖,α-D-GlcNAcp-(1→4)-(2,3-二乙酰基)-D-ManAp 酸是由 B 型百日咳诱导的抗体识别的最小结构。

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