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IgLONs 中高度保守的分子特征与其独特的结构和生物学结局形成鲜明对比。

Highly Conserved Molecular Features in IgLONs Contrast Their Distinct Structural and Biological Outcomes.

机构信息

Department of Pharmacology and Toxicology, University of Texas Medical Branch, Galveston, TX 77555, USA; Sealy Center for Structural Biology and Molecular Biophysics, University of Texas Medical Branch, Galveston, TX 77555, USA.

Department of Pharmacology and Toxicology, University of Texas Medical Branch, Galveston, TX 77555, USA; Center for Addiction Research, University of Texas Medical Branch, Galveston, TX 77555, USA.

出版信息

J Mol Biol. 2020 Sep 4;432(19):5287-5303. doi: 10.1016/j.jmb.2020.07.014. Epub 2020 Jul 22.

Abstract

Neuronal growth regulator 1 (NEGR1) and neurotrimin (NTM) are abundant cell-surface proteins found in the brain and form part of the IgLON (Immunoglobulin LSAMP, OBCAM, Neurotrimin) family. In humans, NEGR1 is implicated in obesity and mental disorders, while NTM is linked to intelligence and cognitive function. IgLONs dimerize homophilically and heterophilically, and they are thought to shape synaptic connections and neural circuits by acting in trans (spanning cellular junctions) and/or in cis (at the same side of a junction). Here, we reveal homodimeric structures of NEGR1 and NTM. They assemble into V-shaped complexes via their Ig1 domains, and disruption of the Ig1-Ig1 interface abolishes dimerization in solution. A hydrophobic ridge from one Ig1 domain inserts into a hydrophobic pocket from the opposing Ig1 domain producing an interaction interface that is highly conserved among IgLONs but remarkably plastic structurally. Given the high degree of sequence conservation at the interaction interface, we tested whether different IgLONs could elicit the same biological effect in vivo. In a small-scale study administering different soluble IgLONs directly into the brain and monitoring feeding, only NEGR1 altered food intake significantly. Taking NEGR1 as a prototype, our studies thus indicate that while IgLONs share a conserved mode of interaction and are able to bind each other as homomers and heteromers, they are structurally plastic and can exert unique biological action.

摘要

神经元生长调节因子 1(NEGR1)和神经调节素(NTM)是大脑中丰富的细胞表面蛋白,是免疫球蛋白 LSAMP、OBCAM、神经调节素(IgLON)家族的一部分。在人类中,NEGR1 与肥胖和精神障碍有关,而 NTM 与智力和认知功能有关。IgLONs 同型和异型二聚化,它们被认为通过跨(跨越细胞连接)和/或顺式(在连接的同一侧)作用来塑造突触连接和神经回路。在这里,我们揭示了 NEGR1 和 NTM 的同源二聚体结构。它们通过 Ig1 结构域组装成 V 形复合物,并且 Ig1-Ig1 界面的破坏会在溶液中消除二聚化。一个 Ig1 结构域的疏水性脊插入到相反的 Ig1 结构域的疏水性口袋中,产生一个相互作用界面,该界面在 IgLONs 中高度保守,但结构上非常有弹性。鉴于相互作用界面的高度序列保守性,我们测试了不同的 IgLON 是否可以在体内引起相同的生物学效应。在一项小规模研究中,直接将不同的可溶性 IgLON 注入大脑并监测摄食,只有 NEGR1 显著改变了食物摄入。以 NEGR1 为原型,我们的研究表明,虽然 IgLONs 具有保守的相互作用模式,并且能够作为同型和异型二聚体相互结合,但它们具有结构可塑性,可以发挥独特的生物学作用。

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