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一种针对新型隐球菌葡糖醛酸木甘露聚糖的单克隆抗体对肽和多糖均表现出水解活性。

A Monoclonal Antibody to Cryptococcus neoformans Glucuronoxylomannan Manifests Hydrolytic Activity for Both Peptides and Polysaccharides.

作者信息

Bowen Anthony, Wear Maggie P, Cordero Radames J B, Oscarson Stefan, Casadevall Arturo

机构信息

From the Department of Microbiology and Immunology, Albert Einstein College of Medicine, Bronx, New York 10461.

the Department of Molecular Microbiology and Immunology, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland 21205, and.

出版信息

J Biol Chem. 2017 Jan 13;292(2):417-434. doi: 10.1074/jbc.M116.767582. Epub 2016 Nov 21.

Abstract

Studies in the 1980s first showed that some natural antibodies were "catalytic" and able to hydrolyze peptide or phosphodiester bonds in antigens. Many naturally occurring catalytic antibodies have since been isolated from human sera and associated with positive and negative outcomes in autoimmune disease and infection. The function and prevalence of these antibodies, however, remain unclear. A previous study suggested that the 18B7 monoclonal antibody against glucuronoxylomannan (GXM), the major component of the Cryptococcus neoformans polysaccharide capsule, hydrolyzed a peptide antigen mimetic. Using mass spectrometry and Förster resonance energy transfer techniques, we confirm and characterize the hydrolytic activity of 18B7 against peptide mimetics and show that 18B7 is able to hydrolyze an oligosaccharide substrate, providing the first example of a naturally occurring catalytic antibody for polysaccharides. Additionally, we show that the catalytic 18B7 antibody increases release of capsular polysaccharide from fungal cells. A serine protease inhibitor blocked peptide and oligosaccharide hydrolysis by 18B7, and a putative serine protease-like active site was identified in the light chain variable region of the antibody. An algorithm was developed to detect similar sites present in unique antibody structures in the Protein Data Bank. The putative site was found in 14 of 63 (22.2%) catalytic antibody structures and 119 of 1602 (7.4%) antibodies with no annotation of catalytic activity. The ability of many antibodies to cleave antigen, albeit slowly, supports the notion that this activity is an important immunoglobulin function in host defense. The discovery of GXM hydrolytic activity suggests new therapeutic possibilities for polysaccharide-binding antibodies.

摘要

20世纪80年代的研究首次表明,一些天然抗体具有“催化”作用,能够水解抗原中的肽键或磷酸二酯键。此后,许多天然存在的催化抗体已从人血清中分离出来,并与自身免疫性疾病和感染的阳性和阴性结果相关。然而,这些抗体的功能和普遍性仍不清楚。先前的一项研究表明,针对新型隐球菌多糖荚膜主要成分葡糖醛酸木聚糖(GXM)的18B7单克隆抗体可水解一种肽抗原模拟物。我们使用质谱和荧光共振能量转移技术,证实并表征了18B7对肽模拟物的水解活性,并表明18B7能够水解寡糖底物,这为天然存在的多糖催化抗体提供了首个实例。此外,我们表明催化性的18B7抗体可增加真菌细胞荚膜多糖的释放。一种丝氨酸蛋白酶抑制剂可阻断18B7对肽和寡糖的水解,并且在该抗体的轻链可变区鉴定出一个推定的丝氨酸蛋白酶样活性位点。开发了一种算法来检测蛋白质数据库中独特抗体结构中存在的相似位点。在63个催化抗体结构中的14个(22.2%)以及1602个无催化活性注释的抗体中的119个(7.4%)中发现了推定的位点。许多抗体尽管水解速度缓慢,但仍具有切割抗原的能力,这支持了这种活性是宿主防御中重要的免疫球蛋白功能这一观点。GXM水解活性的发现为多糖结合抗体带来了新的治疗可能性。

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