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小鼠和人类抗神经节苷脂抗体的硫脂结合特性

Sulfatide binding properties of murine and human antiganglioside antibodies.

作者信息

Townson Kate, Greenshields Kay N, Veitch Jean, Nicholl Dawn, Eckhardt Matthias, Galanina Oxana, Bovin Nicolai, Samain Eric, Antoine Tatiana, Bundle David, Zhang Ping, Ling Chang Chun, Willison Hugh J

机构信息

Division of Clinical Neurosciences, Glasgow Biomedical Research Centre, University of Glasgow, G12 8TA Scotland.

出版信息

Glycobiology. 2007 Nov;17(11):1156-66. doi: 10.1093/glycob/cwm095. Epub 2007 Sep 13.

Abstract

Antiganglioside antibodies form an important component of the innate and adaptive B cell repertoire, where they provide antimicrobial activity through binding encapsulated bacterial glycans. In an aberrant role, they target peripheral nerve gangliosides to induce autoimmune nerve injury. An important characteristic of antiganglioside antibodies is their ability to selectively recognize highly defined glycan structures. Since sialylated and sulfated glycans often share lectin recognition patterns, we here explored the possibility that certain antiganglioside antibodies might also bind 3-O-sulfo-beta-D-galactosylceramide (sulfatide), an abundant constituent of plasma and peripheral nerve myelin, that could thereby influence any immunoregulatory or autoimmune properties. Out of 25 antiganglioside antibodies screened in solid phase assays, 20 also bound sulfatide (10(-5) to 10(-6) M range) in addition to their favored ganglioside glycan epitope ( approximately 10(-7) M range). Solution inhibition studies demonstrated competition between ganglioside and sulfatide, indicating close proximity or sharing of the antigen binding variable region domain. Sulfatide and 3-O-sulfo-beta-D-galactose were unique in having this property amongst a wide range of sulfated glycans screened, including 4- and 6-O-sulfo-beta-D-galactose analogues. Antiganglioside antibody binding to 3-O-sulfo-beta-D-galactose was highly dependent upon the spatial presentation of the ligand, being completely inhibited by conjugation to protein or polyacrylamide (PAA) matrices. Binding was also absent when sulfatide was incorporated into plasma membranes, including myelin, under conditions in which antibody binding to ganglioside was retained. These data demonstrate that sulfatide binding is a common property of antiganglioside antibodies that may provide functional insights into, and consequences for this component of the innate immune repertoire.

摘要

抗神经节苷脂抗体是先天性和适应性B细胞库的重要组成部分,它们通过结合被包裹的细菌聚糖发挥抗菌活性。在异常情况下,它们会靶向周围神经节苷脂,引发自身免疫性神经损伤。抗神经节苷脂抗体的一个重要特征是其能够选择性识别高度明确的聚糖结构。由于唾液酸化和硫酸化聚糖通常具有共同的凝集素识别模式,我们在此探讨了某些抗神经节苷脂抗体也可能结合3 - O - 磺基 - β - D - 半乳糖神经酰胺(硫苷脂)的可能性,硫苷脂是血浆和周围神经髓鞘的丰富成分,可能会影响任何免疫调节或自身免疫特性。在固相分析中筛选的25种抗神经节苷脂抗体中,除了它们偏爱的神经节苷脂聚糖表位(约10⁻⁷ M范围)外,有20种还结合硫苷脂(10⁻⁵至10⁻⁶ M范围)。溶液抑制研究表明神经节苷脂和硫苷脂之间存在竞争,这表明抗原结合可变区结构域紧密相邻或共享。在广泛筛选的硫酸化聚糖(包括4 - 和6 - O - 磺基 - β - D - 半乳糖类似物)中,硫苷脂和3 - O - 磺基 - β - D - 半乳糖具有这种特性。抗神经节苷脂抗体与3 - O - 磺基 - β - D - 半乳糖的结合高度依赖于配体的空间呈现,与蛋白质或聚丙烯酰胺(PAA)基质结合会完全抑制这种结合。在抗体与神经节苷脂结合得以保留的条件下,当硫苷脂掺入包括髓鞘在内的质膜中时,结合也不存在。这些数据表明,硫苷脂结合是抗神经节苷脂抗体的共同特性,这可能为先天性免疫库的这一组成部分提供功能方面的见解及其后果。

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