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Molecular Detection of Targeted Major Histocompatibility Complex I-Bound Peptides Using a Probabilistic Measure and Nanospray MS3 on a Hybrid Quadrupole-Linear Ion Trap

机译:分子检测目标的主要组织相容性复杂的I绑定肽使用概率测度和纳米喷雾MS3在混合四极线性离子阱上。

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摘要

A nanospray MS3 method deployed on a quadrupole linear ion trap hybrid can detect targeted peptides with high dynamic range and high sensitivity from complex mixtures without separations. The method uses a recognition algorithm that is a modification of the relative (Kullback−Leibler, KL) entropy characterization of probabilistic distance to detect if reference MS3 fragmentation patterns are components of acquired MS3 spectra. The recognition reflects the probabilistic structure of physical MS measurements unlike the Euclidean or inner product metrics widely used for comparing spectra. It capably handles spectra with a significant chemical ion background in contrast to the Euclidean metric or the direct relative entropy. The full nanospray MS3 method allows both the detection and quantitation of targets without the need to obtain isotopically labeled standards. By avoiding chromatographic separations and its associated surface losses, the detection can be applied to complex samples on a very limited material scale. The methodology is illustrated by applications to the medically important problem of detecting targeted major histocompatibility complex (MHC) I associated peptides extracted from limited cell numbers.
机译:部署在四极线性离子阱杂交体上的纳米喷雾MS3方法无需分离即可检测复杂混合物中具有高动态范围和高灵敏度的目标肽。该方法使用一种识别算法,该算法是对概率距离的相对(Kullback-Leibler,KL)熵表征的一种修改,以检测参考MS3碎片模式是否是所采集MS3光谱的组成部分。该识别反映了物理MS测量的概率结构,这与广泛用于比较光谱的欧几里德或内积度量不同。与欧几里得度量或直接相对熵相比,它能够处理具有重要化学离子背景的光谱。完整的纳米喷雾MS3方法无需检测同位素标记的标准物即可检测和定量目标。通过避免色谱分离及其相关的表面损失,可以将检测应用于非常有限的材料规模的复杂样品。该方法通过在医学上的重要问题的检测得到说明,该问题对检测从有限细胞数中提取的靶向主要组织相容性复合物(MHC)I相关肽具有重要意义。

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