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作为解读致病机制的模型和工具的抗体:关于一种与免疫调节粘附素反应的独特单克隆抗体的综述

Antibodies as Models and Tools to Decipher Pathogenic Development: Review about a Unique Monoclonal Antibody Reacting with Immunomodulatory Adhesins.

作者信息

Leroy Jordan, Lecointe Karine, Coulon Pauline, Sendid Boualem, Robert Raymond, Poulain Daniel

机构信息

CNRS, UMR 8576, UGSF-Unité de Glycobiologie Structurale et Fonctionnelle, University of Lille, F-59000 Lille, France.

INSERM U1285, University of Lille, F-59000 Lille, France.

出版信息

J Fungi (Basel). 2023 May 31;9(6):636. doi: 10.3390/jof9060636.

Abstract

Candidiasis, caused mainly by , a natural commensal of the human digestive tract and vagina, is the most common opportunistic fungal infection at the mucosal and systemic levels. Its high morbi-mortality rates have led to considerable research to identify the molecular mechanisms associated with the switch to pathogenic development and to diagnose this process as accurately as possible. Since the 1980s, the advent of monoclonal antibody (mAb) technology has led to significant progress in both interrelated fields. This linear review, intended to be didactic, was prompted by considering how, over several decades, a single mAb designated 5B2 contributed to the elucidation of the molecular mechanisms of pathogenesis based on β-1,2-linked oligomannoside expression in species. These contributions starting from the structural identification of the minimal epitope as a di-mannoside from the β-1,2 series consisted then in the demonstration that it was shared by a large number of cell wall proteins differently anchored in the cell wall and the discovery of a cell wall glycoplipid shed by the yeast in contact of host cells, the phospholipomannan. Cytological analysis revealed an overall highly complex epitope expression at the cell surface concerning all growth phases and a patchy distribution resulting from the merging of cytoplasmic vesicles to plasmalema and further secretion through cell wall channels. On the host side, the mAb 5B2 led to identification of Galectin-3 as the human receptor dedicated to β-mannosides and signal transduction pathways leading to cytokine secretion directing host immune responses. Clinical applications concerned in vivo imaging of infectious foci, direct examination of clinical samples and detection of circulating serum antigens that complement the Platelia Ag test for an increased sensitivity of diagnosis. Finally, the most interesting character of mAb 5B2 is probably its ability to reveal pathogenic behaviour in reacting specifically with vaginal secretions from women infected versus colonized by this species as well as to display higher reactivity with strains isolated in pathogenic circumstances or even linked to an unfavourable prognosis for systemic candidiasis. Together with a detailed referenced description of these studies, the review provides a complementary reading frame by listing the wide range of technologies involving mAb 5B2 over time, evidencing a practical robustness and versatility unique so far in the Candida field. Finally, the basic and clinical perspectives opened up by these studies are briefly discussed with regard to prospects for future applications of mAb 5B2 in current research challenges.

摘要

念珠菌病主要由白色念珠菌引起,它是人类消化道和阴道的一种天然共生菌,是黏膜和全身层面最常见的机会性真菌感染。其高发病率和死亡率促使人们进行大量研究,以确定与致病发展转变相关的分子机制,并尽可能准确地诊断这一过程。自20世纪80年代以来,单克隆抗体(mAb)技术的出现使得这两个相关领域都取得了重大进展。这篇旨在具有教学意义的线性综述,是在思考几十年来一种名为5B2的单克隆抗体如何基于白色念珠菌中β-1,2-连接的寡甘露糖苷表达来阐明致病分子机制的过程中产生的。这些贡献始于将最小表位结构鉴定为β-1,2系列的二甘露糖苷,接着证明它由大量以不同方式锚定在细胞壁中的细胞壁蛋白共享,并发现酵母在与宿主细胞接触时释放的一种细胞壁糖脂——磷脂甘露聚糖。细胞学分析揭示了在细胞表面所有生长阶段的整体高度复杂的表位表达,以及由于细胞质囊泡与质膜融合并通过细胞壁通道进一步分泌而导致的斑驳分布。在宿主方面,单克隆抗体5B2导致鉴定出半乳糖凝集素-3作为专门针对β-甘露糖苷的人类受体以及导致细胞因子分泌从而指导宿主免疫反应的信号转导途径。临床应用涉及念珠菌感染灶的体内成像、临床样本的直接检查以及循环血清抗原的检测,这些补充了普瑞泰利念珠菌抗原检测以提高诊断的敏感性。最后,单克隆抗体5B2最有趣的特性可能是它能够通过与感染该菌种而非定植该菌种的女性阴道分泌物特异性反应来揭示念珠菌的致病行为,以及与在致病情况下分离的菌株甚至与系统性念珠菌病不良预后相关的菌株表现出更高的反应性。除了对这些研究进行详细的参考文献描述外,该综述还通过列出随着时间推移涉及单克隆抗体5B2的广泛技术提供了一个补充阅读框架,证明了在念珠菌领域迄今为止独特的实际稳健性和多功能性。最后,就单克隆抗体5B2在当前研究挑战中的未来应用前景简要讨论了这些研究开辟的基础和临床前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a834/10302264/8d9ae3e6d04a/jof-09-00636-g001.jpg

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