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Structure of the trypanosome transferrin receptor reveals mechanisms of ligand recognition and immune evasion

机译:锥虫体转移素受体的结构揭示了配体识别和免疫逃避的机制

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To maintain prolonged infection of mammals, African trypano-somes have evolved remarkable surface coats and a system of antigenic variation1. Within these coats are receptors for macromolecular nutrients such as transferrin2,3. These must be accessible to their ligands but must not confer susceptibility to immunoglobulin-mediated attack. Trypanosomes have a wide host range and their receptors must also bind ligands from diverse species. To understand how these requirements are achieved, in the context of transferrin uptake, we determined the structure of a Trypanosoma brucei transferrin receptor in complex with human transferrin, showing how this heterodimeric receptor presents a large asymmetric ligand-binding platform. The trypanosome genome contains a family of around 14 transferrin receptors4, which has been proposed to allow binding to transferrin from different mammalian hosts5,6. However, we find that a single receptor can bind trans-ferrin from a broad range of mammals, indicating that receptor variation is unlikely to be necessary for promiscuity of host infection. In contrast, polymorphic sites and N-linked glycans are preferentially found in exposed positions on the receptor surface, not contacting transferrin, suggesting that transfer-rin receptor diversification is driven by a need for antigenic variation in the receptor to prolong survival in a host.
机译:为了维持哺乳动物的长时间感染,非洲耳蛋白酶有一些题为出现显着的表面涂层和抗原变异系统。在这些涂层内是用于大分子营养素如转铁蛋白2,3的受体。它们的配体必须可以访问这些,但不能赋予免疫球蛋白介导的攻击易感性。锥虫具有宽的宿主范围,其受体还必须从不同的物种中结合配体。为了了解如何实现这些要求,在转铁蛋白摄取的背景下,我们确定了与人转移素复合物的脑蛋白酶瘤的结构的结构,呈现该异二聚体受体如何呈现大的不对称配体结合平台。锥虫组基因组含有约14个转移素受体4的家族,这已经提出允许从不同哺乳动物Hosts5,6中结合转移素。然而,我们发现单个受体可以从宽范围的哺乳动物中结合转铁素,表明受体变化不太可能对宿主感染的滥交是必要的。相反,多晶态位点和N-连接的聚糖优先在受体表面上的暴露位置中发现,不接触转移素,表明转移rin受体多样化是通过对受体中​​的抗原变异来延长宿主中存活的需求。

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