4.8 Article

A draft map of the mouse pluripotent stem cell spatial proteome

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NATURE COMMUNICATIONS
卷 7, 期 -, 页码 -

出版社

NATURE RESEARCH
DOI: 10.1038/ncomms9992

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资金

  1. ERASMUS Placement scholarship
  2. Wellcome Trust [099135/Z/12/Z]
  3. BBSRC grant [BB/D526088/1]
  4. European Union 7th Framework Program (PRIMEXS project) [262067]
  5. BBSRC Tools and Resources Development Fund [BB/K00137X/1]
  6. ERC Advanced Investigator grant
  7. Alexander S. Onassis Public Benefit Foundation
  8. Foundation for Education and European Culture (IPEP)
  9. Embiricos Trust Scholarship of Jesus College Cambridge
  10. Commonwealth Split Site PhD Scholarship
  11. BBSRC [BB/H024247/1, BB/K00137X/1] Funding Source: UKRI
  12. Biotechnology and Biological Sciences Research Council [BB/K00137X/1, BB/H024247/1] Funding Source: researchfish

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Knowledge of the subcellular distribution of proteins is vital for understanding cellular mechanisms. Capturing the subcellular proteome in a single experiment has proven challenging, with studies focusing on specific compartments or assigning proteins to subcellular niches with low resolution and/or accuracy. Here we introduce hyperLOPIT, a method that couples extensive fractionation, quantitative high-resolution accurate mass spectrometry with multivariate data analysis. We apply hyperLOPIT to a pluripotent stem cell population whose subcellular proteome has not been extensively studied. We provide localization data on over 5,000 proteins with unprecedented spatial resolution to reveal the organization of organelles, sub-organellar compartments, protein complexes, functional networks and steady-state dynamics of proteins and unexpected subcellular locations. The method paves the way for characterizing the impact of post-transcriptional and post-translational modification on protein location and studies involving proteome-level locational changes on cellular perturbation. An interactive open-source resource is presented that enables exploration of these data.

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