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朗格汉斯蛋白与伯贝克颗粒的结构研究:一种大分子组织模型。

Structural studies of langerin and Birbeck granule: a macromolecular organization model.

作者信息

Thépaut Michel, Valladeau Jenny, Nurisso Alessandra, Kahn Richard, Arnou Bertrand, Vivès Corinne, Saeland Sem, Ebel Christine, Monnier Carine, Dezutter-Dambuyant Colette, Imberty Anne, Fieschi Franck

机构信息

Laboratoire des Proteines Membranaires, CEA, DSV, Institut de Biologie Structurale (IBS), Grenoble, France.

出版信息

Biochemistry. 2009 Mar 31;48(12):2684-98. doi: 10.1021/bi802151w.

Abstract

Dendritic cells, a sentinel immunity cell lineage, include different cell subsets that express various C-type lectins. For example, epidermal Langerhans cells express langerin, and some dermal dendritic cells express DC-SIGN. Langerin is a crucial component of Birbeck granules, the Langerhans cell hallmark organelle, and may have a preventive role toward HIV, by its internalization into Birbeck granules. Since langerin carbohydrate recognition domain (CRD) is crucial for HIV interaction and Birbeck granule formation, we produced the CRD of human langerin and solved its structure at 1.5 A resolution. On this basis gp120 high-mannose oligosaccharide binding has been evaluated by molecular modeling. Hydrodynamic studies reveal a very elongated shape of recombinant langerin extracellular domain (ECD). A molecular model of the langerin ECD, integrating the CRD structure, has been generated and validated by comparison with hydrodynamic parameters. In parallel, Langerhans cells were isolated from human skin. From their analysis by electron microscopy and the langerin ECD model, an ultrastructural organization is proposed for Birbeck granules. To delineate the role of the different langerin domains in Birbeck granule formation, we generated truncated and mutated langerin constructs. After transfection into a fibroblastic cell line, we highlighted, in accordance with our model, the role of the CRD in the membrane zipping occurring in BG formation as well as some contribution of the cytoplasmic domain. Finally, we have shown that langerin ECD triggering with a specific mAb promotes global rearrangements of LC morphology. Our results open the way to the definition of a new membrane deformation mechanism.

摘要

树突状细胞是一种哨兵免疫细胞谱系,包括表达各种C型凝集素的不同细胞亚群。例如,表皮朗格汉斯细胞表达朗格素,一些真皮树突状细胞表达DC-SIGN。朗格素是伯贝克颗粒(朗格汉斯细胞标志性细胞器)的关键组成部分,通过内化进入伯贝克颗粒,可能对HIV具有预防作用。由于朗格素碳水化合物识别结构域(CRD)对于HIV相互作用和伯贝克颗粒形成至关重要,我们制备了人朗格素的CRD并以1.5埃分辨率解析了其结构。在此基础上,通过分子模拟评估了gp120高甘露糖寡糖结合情况。流体动力学研究揭示了重组朗格素胞外域(ECD)非常细长的形状。通过与流体动力学参数比较,生成并验证了整合CRD结构的朗格素ECD分子模型。同时,从人皮肤中分离出朗格汉斯细胞。通过电子显微镜分析和朗格素ECD模型,提出了伯贝克颗粒的超微结构组织。为了阐明朗格素不同结构域在伯贝克颗粒形成中的作用,我们构建了截短和突变的朗格素构建体。转染到成纤维细胞系后,我们根据模型突出了CRD在伯贝克颗粒形成中发生的膜拉链作用以及胞质结构域的一些贡献。最后,我们表明用特异性单克隆抗体触发朗格素ECD可促进朗格汉斯细胞形态的整体重排。我们的结果为定义一种新的膜变形机制开辟了道路。

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