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A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations
Although the value of proteomics has been demonstrated, cost and scale are typically prohibitive, and gene expression profiling remains dominant for characterizing cellular responses to perturbations. However, high-throughput sentinel assays provide an opportunity for proteomics to contribute at a m...
Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
2018
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5951639/ https://www.ncbi.nlm.nih.gov/pubmed/29655704 http://dx.doi.org/10.1016/j.cels.2018.03.012 |
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author | Litichevskiy, Lev Peckner, Ryan Abelin, Jennifer G. Asiedu, Jacob K. Creech, Amanda L. Davis, John F. Davison, Desiree Dunning, Caitlin M. Egertson, Jarrett D. Egri, Shawn Gould, Joshua Ko, Tak Johnson, Sarah A. Lahr, David L. Lam, Daniel Liu, Zihan Lyons, Nicholas J. Lu, Xiaodong MacLean, Brendan X. Mungenast, Alison E. Officer, Adam Natoli, Ted E. Papanastasiou, Malvina Patel, Jinal Sharma, Vagisha Toder, Courtney Tubelli, Andrew A. Young, Jennie Z. Carr, Steven A. Golub, Todd R. Subramanian, Aravind MacCoss, Michael J. Tsai, Li-Huei Jaffe, Jacob D. |
author_facet | Litichevskiy, Lev Peckner, Ryan Abelin, Jennifer G. Asiedu, Jacob K. Creech, Amanda L. Davis, John F. Davison, Desiree Dunning, Caitlin M. Egertson, Jarrett D. Egri, Shawn Gould, Joshua Ko, Tak Johnson, Sarah A. Lahr, David L. Lam, Daniel Liu, Zihan Lyons, Nicholas J. Lu, Xiaodong MacLean, Brendan X. Mungenast, Alison E. Officer, Adam Natoli, Ted E. Papanastasiou, Malvina Patel, Jinal Sharma, Vagisha Toder, Courtney Tubelli, Andrew A. Young, Jennie Z. Carr, Steven A. Golub, Todd R. Subramanian, Aravind MacCoss, Michael J. Tsai, Li-Huei Jaffe, Jacob D. |
author_sort | Litichevskiy, Lev |
collection | PubMed |
description | Although the value of proteomics has been demonstrated, cost and scale are typically prohibitive, and gene expression profiling remains dominant for characterizing cellular responses to perturbations. However, high-throughput sentinel assays provide an opportunity for proteomics to contribute at a meaningful scale. We present a systematic library resource (90 drugs 3 6 cell lines) of proteomic signatures that measure changes in the reduced-representation phosphoproteome (P100) and changes in epigenetic marks on histones (GCP). A majority of these drugs elicited reproducible signatures, but notable cell line- and assay-specific differences were observed. Using the “connectivity” framework, we compared signatures across cell types and integrated data across assays, including a transcriptional assay (L1000). Consistent connectivity among cell types revealed cellular responses that transcended lineage, and consistent connectivity among assays revealed unexpected associations between drugs. We further leveraged the resource against public data to formulate hypotheses for treatment of multiple myeloma and acute lymphocytic leukemia. This resource is publicly available at https://clue.io/proteomics. |
format | Online Article Text |
id | pubmed-5951639 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2018 |
record_format | MEDLINE/PubMed |
spelling | pubmed-59516392018-05-14 A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations Litichevskiy, Lev Peckner, Ryan Abelin, Jennifer G. Asiedu, Jacob K. Creech, Amanda L. Davis, John F. Davison, Desiree Dunning, Caitlin M. Egertson, Jarrett D. Egri, Shawn Gould, Joshua Ko, Tak Johnson, Sarah A. Lahr, David L. Lam, Daniel Liu, Zihan Lyons, Nicholas J. Lu, Xiaodong MacLean, Brendan X. Mungenast, Alison E. Officer, Adam Natoli, Ted E. Papanastasiou, Malvina Patel, Jinal Sharma, Vagisha Toder, Courtney Tubelli, Andrew A. Young, Jennie Z. Carr, Steven A. Golub, Todd R. Subramanian, Aravind MacCoss, Michael J. Tsai, Li-Huei Jaffe, Jacob D. Cell Syst Article Although the value of proteomics has been demonstrated, cost and scale are typically prohibitive, and gene expression profiling remains dominant for characterizing cellular responses to perturbations. However, high-throughput sentinel assays provide an opportunity for proteomics to contribute at a meaningful scale. We present a systematic library resource (90 drugs 3 6 cell lines) of proteomic signatures that measure changes in the reduced-representation phosphoproteome (P100) and changes in epigenetic marks on histones (GCP). A majority of these drugs elicited reproducible signatures, but notable cell line- and assay-specific differences were observed. Using the “connectivity” framework, we compared signatures across cell types and integrated data across assays, including a transcriptional assay (L1000). Consistent connectivity among cell types revealed cellular responses that transcended lineage, and consistent connectivity among assays revealed unexpected associations between drugs. We further leveraged the resource against public data to formulate hypotheses for treatment of multiple myeloma and acute lymphocytic leukemia. This resource is publicly available at https://clue.io/proteomics. 2018-04-11 2018-04-25 /pmc/articles/PMC5951639/ /pubmed/29655704 http://dx.doi.org/10.1016/j.cels.2018.03.012 Text en This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/). |
spellingShingle | Article Litichevskiy, Lev Peckner, Ryan Abelin, Jennifer G. Asiedu, Jacob K. Creech, Amanda L. Davis, John F. Davison, Desiree Dunning, Caitlin M. Egertson, Jarrett D. Egri, Shawn Gould, Joshua Ko, Tak Johnson, Sarah A. Lahr, David L. Lam, Daniel Liu, Zihan Lyons, Nicholas J. Lu, Xiaodong MacLean, Brendan X. Mungenast, Alison E. Officer, Adam Natoli, Ted E. Papanastasiou, Malvina Patel, Jinal Sharma, Vagisha Toder, Courtney Tubelli, Andrew A. Young, Jennie Z. Carr, Steven A. Golub, Todd R. Subramanian, Aravind MacCoss, Michael J. Tsai, Li-Huei Jaffe, Jacob D. A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title | A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title_full | A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title_fullStr | A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title_full_unstemmed | A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title_short | A Library of Phosphoproteomic and Chromatin Signatures for Characterizing Cellular Responses to Drug Perturbations |
title_sort | library of phosphoproteomic and chromatin signatures for characterizing cellular responses to drug perturbations |
topic | Article |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5951639/ https://www.ncbi.nlm.nih.gov/pubmed/29655704 http://dx.doi.org/10.1016/j.cels.2018.03.012 |
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