LINCS PCCSE P100 2020

LINCS PCCSE P100 2020
Phospho-proteomic Profiling Dataset of Chemical Perturbations in Multiple Biological Backgrounds
Data License: CC BY 4.0 | ProteomeXchange: PXD017458 | doi: https://doi.org/10.6069/7fyh-be63
  • Organism: Homo sapiens
  • Instrument: Q Exactive HF
  • SpikeIn: Yes
  • Keywords: Data-Independent Acquisition, mass spectrometry, proteomics, phospho-signaling, phosphoproteomics
  • Lab head: Malvina Papanastasiou Submitter: Karen Christianson
Abstract
The Library of Integrated Network-based Cellular Signatures (LINCS) Program aims to create a network-based understanding of biology by cataloging changes in gene expression and other cellular processes that occur when cells are exposed to a variety of perturbing agents. The goal of this project is to test the hypothesis that modulation of phosphorylation-mediated signaling events in response to perturbations can establish new cellular states by altering their epigenetic landscape. We have performed mass spectrometry (MS)-based proteomic assays that target quantitative readouts of phospho-signaling and chromatin modifications in cellular models, following perturbation by compounds with varying mechanisms of action. We have employed 128 compounds and treated 5 cancer and 2 neuronal cell lines. The resulting data collected and tools created have been contributed to the LINCS program for the purpose of making connections among disparate perturbations through phosphoproteomics and chromatin modification signatures in concert with other available data types. The data is publicly available on PanoramaPublic and can be queried using Clue (Broad Institute). Analysis of our data will inform novel therapeutic opportunities and synergies, as dysregulation of phospho-signaling and epigenetic systems are two of the most common molecular etiologies identified in a growing number of diseases.
Experiment Description
Detailed P100 protocols can be found in Abelin et al., 2016, MCP and online at https://panoramaweb.org/wiki/LINCS/Overview%20Information/page.view?name=sops. Briefly, cells were lysed after drug treatment with a urea-based buffer that includes phosphatase inhibitors. Proteins (300-500 μg, depending on the cell type) extracted from the cell lysates underwent trypsin digestion followed by desalting using reversed solid phase extraction. Peptides were mixed with a quality-control set of synthetic isotope-labeled peptide standards to monitor the performance of subsequent steps. Phosphopeptide enrichment occurred on an AssayMAP Bravo automated liquid handling platform (Agilent, Santa Clara, CA) using IMAC chemistry. Samples were processed in a 96-well plate format. Prior to mass spectrometry analysis, a second set of synthetic isotope-labelled internal standards for targeted phosphopeptides were spiked into samples to ensure accurate quantification. Data were acquired using a DIA method as described in Abelin et al., 2016, MCP and ion chromatograms were extracted using Skyline (MacLean et al., 2014).
Sample Description
Drug signatures were profiled in various cancer cell lines (A375, YAPC, A549, MCF7, and PC3) and neuronal cell models (Astrocytes & NPCs). Drugs were grouped into four tranches: epigenetically active, neuroactive, kinase inhibitors and cardiotoxic compounds. A detailed description of their mechanism of action can be found online at https://panoramaweb.org/wiki/LINCS/Overview%20Information/page.view?name=LINCS%20PCCSE%20Overview and https://clue.io/touchstone. Drug stocks were dissolved in DMSO for treatment in cell line media and cells were treated in 6 well plates for 3 hours. For cell harvesting, cells from 2-4 wells of a 6 well plate were scraped in lysis buffer and combined per sample. All drug perturbations occurred in triplicates.
Created on 3/19/21, 11:26 PM
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Config
Plate67Cardiotoxic DrugsAstrocyte Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate66Kinase InhibitorsAstrocyte Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate65Neuroactive DrugsAstrocyte Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate64Epigenetic DrugsAstrocyte Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate63aCardiotoxic DrugsNPC Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate62Cardiotoxic DrugsYAPC Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate61Cardiotoxic DrugsPC3 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate60Cardiotoxic DrugsMCF7 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate59aCardiotoxic DrugsA375 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate58Cardiotoxic DrugsA549 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate34Kinase InhibitorsPC3 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate33Kinase InhibitorsA549 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
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Plate31Neuroactive Drugs (PRM)YAPC Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate30Epigenetic DrugsYAPC Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate29_03HKinase Inhibitors (PRM)MCF7 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate28Kinase Inhibitors (PRM)A375 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate27Kinase InhibitorsNPC Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate25Neuroactive Drugs (PRM)A549 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate24Neuroactive DrugsPC3 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate23Neuroactive DrugsMCF7 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
Plate22Neuroactive DrugsA375 Skyline  GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   GCT  [ View in Morpheus  ]   CFG 
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ZipChip_HR_Metabolomics_2024Protocol_2024-02-05_17-24-05.sky.zip2024-02-05 14:24:2810082159478
22AminoAcids_Fully13CLabeled_2024-01-29_14-30-52.sky.zip2024-01-29 11:32:141044493622
RBD_M_Glyco_2024-01-25_15-29-41.sky.zip2024-01-26 17:23:2672923972,38290
20240104_Neg_FMT_MCBAs_isoRemove_Cleaned_Final_2024-01-25_21-40-19.sky.zip2024-01-26 16:43:4710100300560
20231220_Neg_FMT_BA_Full_reduce_Res50_High_final_2024-01-04_15-44-59.sky.zip2024-01-26 16:43:474051121760
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New_iRBD2024-01-15 23:30:52334747942920
Paired_CSF_Plasma_Serum2024-01-15 23:30:5233474794600
Initial_Targeted_Proteomics2024-01-15 23:30:52334747944410
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173_peptides_iRTs_chromatogram_library_2023-12-22_00-47-19.sky.zip2023-12-22 01:06:36311833561,08220
Figure_8B_Freiburg_ALG1-CDG-Patients_Comparison_2023-12-22_02-34-55.sky.zip2023-12-22 01:06:20226912840060
Figures_4_5_6_7_8A_Heidelberg_CDG-Patients_2023-12-22_02-32-43.sky.zip2023-12-22 01:06:202067124390140
The previous version of this data can be found at https://panoramaweb.org/lincs_pccse_p100_2020_v1.url