Publication | Open Access
Spatial single-cell mass spectrometry defines zonation of the hepatocyte proteome
21
Citations
26
References
2022
Year
Unknown Venue
EngineeringBiological Mass SpectrometryPathologyMultiomicsSpatial OmicsAbstract Single-cell ProteomicsCellular PhysiologyMultiplexed Ms. ScdvpProteomic TechnologySingle Cell SequencingProteomicsMolecular ImagingBiochemistryLiver PhysiologyComputational PathologyOmicsMulti-omicsMedical Image ComputingSingle-cell AnalysisDeep LearningCell BiologyHepatocyte ProteomeMass SpectrometryComputational BiologyBiomedical ImagingProtein Mass SpectrometryCellular BiochemistrySystems BiologyMedicineCell Detection
Abstract Single-cell proteomics by mass spectrometry (MS) is emerging as a powerful and unbiased method for the characterization of biological heterogeneity. So far, it has been limited to cultured cells, whereas an expansion of the method to complex tissues would greatly enhance biological insights. Here we describe single-cell Deep Visual Proteomics (scDVP), a technology that integrates high-content imaging, laser microdissection and multiplexed MS. scDVP resolves the context-dependent, spatial proteome of murine hepatocytes at a current depth of 1,700 proteins from a slice of a cell. Half of the proteome was differentially regulated in a spatial manner, with protein levels changing dramatically in proximity to the central vein. We applied machine learning to proteome classes and images, which subsequently inferred the spatial proteome from imaging data alone. scDVP is applicable to healthy and diseased tissues and complements other spatial proteomics or spatial omics technologies.
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