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Expanding the Scope of Cross-Link Identifications by Incorporating Collisional Activated Dissociation and Ultraviolet Photodissociation Methods

机译:通过掺入局部激活的解离和紫外线光切换方法来扩展交联标识的范围

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With the advent of new cross-linking chemistries, analytical technologies, and search algorithms, cross linking has become an increasingly popular strategy for evaluating tertiary and quaternary structures of proteins. Collisional activated dissociation remains the primary MS/MS method for identifications of peptide cross-links in high throughput workflows. Ultraviolet photodissociation (UVPD) at 193 nm has emerged as an alternative ion activation method well-suited for characterization of peptides and has been found in some cases to identify different peptides or provide distinctive sequence information than obtained by collisional activation methods. Complementary high energy collision dissociation (HCD) and UVPD were used in the present study to characterize protein cross-linking for bovine serum albumin, hemoglobin, and E. coli ribosome. Cross-links identified by HCD and UVPD using bis(sulfosuccinimidyl)suberate (BS3), a homobifunctional amine-to-amine cross-linker, and 4-(4,6-dimethoxy-1,3,5-triazin-2-yl)-4-methylmorpholinium chloride (DMTMM), a heterofunctional amine-to-carboxylic acid cross-linker, were evaluated in the present study. While more unique BS3 cross-links were identified by HCD, UVPD, and HCD provided a complementary panel of DMTMM cross-links which extended the degree of structural insight obtained for the proteins.
机译:随着新交联化学的,分析技术和搜索算法的出现,交叉连接已成为评估蛋白质三级和季结构的越来越流行的策略。碰撞活化解离仍然是用于在高吞吐量工作流程中鉴定肽交联的主要MS / MS方法。 193nm的紫外线光积极灭菌(UVPD)作为替代离子活化方法良好地出现了肽的表征,并且已经在某些情况下发现以鉴定不同的肽或提供比通过碰撞活化方法获得的独特序列信息。在本研究中使用互补高能量碰撞解离(HCD)和UVPD,以表征牛血清白蛋白,血红蛋白和大肠杆菌核糖体的蛋白质交联。 HCD和UVPD使用双(磺琥珀酰亚胺酰亚胺)Suberate(BS3),偶氮胺与胺交联剂和4-(4,6-二甲氧基-1,3,5-三嗪-2-基在本研究中评估-4-甲基丙酮氯化铵(DMTMM),异官能胺对羧酸交联剂。虽然通过HCD,UVPD和HCD识别了更独特的BS3交联,但是提供了DMTMM交联的互补面板,其延长了蛋白质获得的结构洞察度。

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