4.8 Article

Data-Dependent Acquisition Ladder for Capillary Electrophoresis Mass Spectrometry-Based Ultrasensitive (Neuro)Proteomics

期刊

ANALYTICAL CHEMISTRY
卷 93, 期 48, 页码 15964-15972

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acs.analchem.1c03327

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资金

  1. Arnold and Mabel Beckman Foundation Beckman Young Investigator Award
  2. COSMOS Club Award

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Using micro-analytical capillary electrophoresis electrospray ionization technology for protein measurement allows for a better understanding of the nervous system. This technology can be used to achieve deeper coverage of the neuroproteome with trace amounts of starting materials.
Measurement of broad types of proteins from a small number of cells to single cells would help to better understand the nervous system but requires significant leaps in sensitivity in high-resolution mass spectrometry (HRMS). Micro-analytical capillary electrophoresis electrospray ionization (CE-ESI) offers a path to ultrasensitive proteomics by integrating scalability with sensitivity. Here, we systematically evaluate performance limitations in this technology to develop a data acquisition strategy with deeper coverage of the neuroproteome from trace amounts of starting materials than traditional dynamic exclusion. During standard data-dependent acquisition (DDA), compact migration challenged the duty cycle of second-stage transitions and redundant targeting of abundant peptide signals lowered their identification success rate. DDA was programmed to progressively exclude a static set of high-intensity peptide signals throughout replicate measurements, essentially forming rungs of a DDA ladder. The method was tested for similar to 500 pg portions of a protein digest from cultured hippocampal (primary) neurons (mouse), which estimated the total amount of protein from a single neuron. The analysis of similar to 5 ng of protein digest over all replicates, approximating similar to 10 neurons, identified 428 nonredundant proteins (415 quantified), an similar to 35% increase over traditional DDA. The identified proteins were enriched in neuronal marker genes and molecular pathways of neurobiological importance. The DDA ladder enhances CE-HRMS sensitivity to single-neuron equivalent amounts of proteins, thus expanding the analytical toolbox of neuroscience.

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