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首页> 外文期刊>Journal of mass spectrometry: JMS >A biuret-derived, MS-cleavable cross-linking reagent for protein structural analysis: A proof-of-principle study
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A biuret-derived, MS-cleavable cross-linking reagent for protein structural analysis: A proof-of-principle study

机译:用于蛋白质结构分析的基础脲衍生的MS可切割的交联试剂:验证原则研究

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摘要

Chemical cross-linking combined with mass spectrometry (XL-MS) and computational modeling has evolved as an alternative method to derive protein 3D structures and to map protein interaction networks. Special focus has been laid recently on the development and application of cross-linkers that are cleavable by collisional activation as they yield distinct signatures in tandem mass spectra. Building on our experiences with cross-linkers containing an MS-labile urea group, we now present the biuret-based, CID-MS/MS-cleavable cross-linker imidodicarbonyl diimidazole (IDDI) and demonstrate its applicability for protein cross-linking studies based on the four model peptides angiotensin II, MRFA, substance P, and thymopentin.
机译:化学交联与质谱(XL-MS)和计算建模结合,作为衍生蛋白质3D结构和映射蛋白质相互作用网络的替代方法。 最近对特殊重点进行了奠定了关于通过碰撞激活可释放的交联剂的开发和应用,因为它们在串联质谱中产生明显的签名。 建立我们对含有MS稳定尿素组的交联剂的经验,我们现在出现了基于Biurec的CID-MS / MS可切换的交联剂酰亚胺酰亚胺羰基二咪唑(IDDI),并证明了其基于蛋白质交联研究的适用性 在四种模型肽血管紧张素II,MRFA,物质P和胸腺前素。

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