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Modeling the Interaction between Quinolinate and the Receptor for Advanced Glycation End Products (RAGE): Relevance for Early Neuropathological Processes

机译:建模喹啉酸酯与高级糖基化终产物(RAGE)受体之间的相互作用:与早期神经病理学过程的相关性

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摘要

The receptor for advanced glycation end products (RAGE) is a pattern-recognition receptor involved in neurodegenerative and inflammatory disorders. RAGE induces cellular signaling upon binding to a variety of ligands. Evidence suggests that RAGE up-regulation is involved in quinolinate (QUIN)-induced toxicity. We investigated the QUIN-induced toxic events associated with early noxious responses, which might be linked to signaling cascades leading to cell death. The extent of early cellular damage caused by this receptor in the rat striatum was characterized by image processing methods. To document the direct interaction between QUIN and RAGE, we determined the binding constant (Kb) of RAGE (VC1 domain) with QUIN through a fluorescence assay. We modeled possible binding sites of QUIN to the VC1 domain for both rat and human RAGE. QUIN was found to bind at multiple sites to the VC1 dimer, each leading to particular mechanistic scenarios for the signaling evoked by QUIN binding, some of which directly alter RAGE oligomerization. This work contributes to the understanding of the phenomenon of RAGE-QUIN recognition, leading to the modulation of RAGE function.
机译:晚期糖基化终末产物的受体(RAGE)是一种模式识别受体,参与神经变性和炎症性疾病。 RAGE在与各种配体结合后诱导细胞信号转导。有证据表明,RAGE的上调与喹啉酸(QUIN)诱导的毒性有关。我们调查了QUIN诱导的与早期有害反应有关的毒性事件,这可能与导致细胞死亡的信号级联有关。通过图像处理方法表征了该受体在大鼠纹状体中引起的早期细胞损伤的程度。为了记录QUIN和RAGE之间的直接相互作用,我们通过荧光测定法确定了QUAGE与RAGE(VC1结构域)的结合常数(Kb)。我们为大鼠和人类的RAGE建模了QUIN与VC1域的可能结合位点。 QUIN被发现在多个位点上与VC1二聚体结合,每个都导致QUIN结合引起的信号传导的特殊机制,其中一些直接改变RAGE寡聚化。这项工作有助于理解RAGE-QUIN现象,从而调节RAGE功能。

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