Sir William Dunn School of Pathology, University of Oxford, South Parks Road, Oxford OX1 3RE, UK.
Structure. 2013 May 7;21(5):820-32. doi: 10.1016/j.str.2013.03.008. Epub 2013 Apr 18.
CD200 is a widely distributed membrane glycoprotein that regulates myeloid cell activity through its interaction with an inhibitory receptor (CD200R). The interaction is of interest as a target for treating excessive inflammation and for treating leukemia. There are closely related proteins to CD200R that give activating signals making this a "paired receptor." We report X-ray crystallography structures for the inhibitory CD200R, the activating receptor CD200RLa, and a complex between CD200R and CD200. Both CD200 and CD200R contain two Ig-like domains and interact through their NH₂ terminal domains compatible with immunological synapse-like interactions occurring between myeloid cells and other CD200-expressing cells. The failure of the activating receptor to bind CD200 resides in subtle changes around the interface. CD200 has been acquired by herpes viruses to mimic the host interaction. CD200R has evolved rapidly presumably driven by pathogen pressure but it may also be important in homeostasis through interactions with commensal bacteria.
CD200 是一种广泛分布的膜糖蛋白,通过与其抑制性受体(CD200R)相互作用来调节髓样细胞活性。这种相互作用作为治疗过度炎症和治疗白血病的靶点引起了人们的兴趣。还有与 CD200R 密切相关的蛋白,它们提供激活信号,使其成为“配对受体”。我们报告了抑制性 CD200R、激活性受体 CD200RLa 以及 CD200R 和 CD200 之间复合物的 X 射线晶体结构。CD200 和 CD200R 都包含两个 Ig 样结构域,并通过其 NH₂ 末端结构域相互作用,与髓样细胞与其他表达 CD200 的细胞之间发生的免疫突触样相互作用相兼容。激活受体不能与 CD200 结合的原因在于界面周围的细微变化。疱疹病毒获得了 CD200,以模拟宿主相互作用。CD200R 迅速进化,可能是病原体压力驱动的,但它也可能通过与共生细菌的相互作用在体内平衡中很重要。
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