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Extending the Isotopically Resolved Mass Range of Orbitrap Mass Spectrometers

机译:扩展Orbitrap质谱仪的同位素分辨质量范围

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摘要

The routine analysis of large biomolecules (greater than 30 kDa) has been a challenge for Orbitrap mass spectrometers due to the relatively high kinetic energy of ions entering and within the Orbitrap mass analyzer. This characteristic results in rapid signal decay for large biomolecules due to energetic collisions with background gas molecules. Here, we report a method to significantly enhance the analysis of large biomolecules in an Orbitrap mass spectrometer. The combination of reduced C-trap and higher energy collisional dissociation (HCD) cell bath gas pressures, using helium as the bath gas and trapping ions in the HCD cell prior to mass analysis, greatly increased sensitivity and reduced signal decay for large protein ions. As a result, isotopic resolution of monoclonal immunoglobulin G was achieved, and we have established a new high-mass record for which accurate mass measurement and isotopic resolution have been achieved.
机译:大型生物分子(大于30 kDa)的常规分析对于Orbitrap质谱仪来说是一个挑战,因为进入和进入Orbitrap质量分析仪的离子具有较高的动能。由于与背景气体分子的强烈碰撞,此特征导致大型生物分子的信号迅速衰减。在这里,我们报告了一种显着增强Orbitrap质谱仪中大型生物分子分析的方法。减少的C捕集阱和较高的能量碰撞解离(HCD)细胞浴气体压力相结合,使用氦气作为浴气体并在质量分析之前将离子捕获在HCD细胞中,大大提高了灵敏度,并减少了大蛋白离子的信号衰减。结果,实现了单克隆免疫球蛋白G的同位素分离,并且我们建立了一个新的高质量记录,该记录已实现了精确的质量测量和同位素分离。

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