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Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition

To identify therapeutic targets for KRAS mutant pancreatic cancer, we conduct a druggable genome small interfering RNA (siRNA) screen and determine that suppression of BCAR1 sensitizes pancreatic cancer cells to ERK inhibition. Integrative analysis of genome-scale CRISPR-Cas9 screens also identify B...

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Autores principales: Waters, Andrew M., Khatib, Tala O., Papke, Bjoern, Goodwin, Craig M., Hobbs, G. Aaron, Diehl, J. Nathaniel, Yang, Runying, Edwards, A. Cole, Walsh, Katherine H., Sulahian, Rita, McFarland, James M., Kapner, Kevin S., Gilbert, Thomas S.K., Stalnecker, Clint A., Javaid, Sehrish, Barkovskaya, Anna, Grover, Kajal R., Hibshman, Priya S., Blake, Devon R., Schaefer, Antje, Nowak, Katherine M., Klomp, Jennifer E., Hayes, Tikvah K., Kassner, Michelle, Tang, Nanyun, Tanaseichuk, Olga, Chen, Kaisheng, Zhou, Yingyao, Kalkat, Manpreet, Herring, Laura E., Graves, Lee M., Penn, Linda Z., Yin, Hongwei H., Aguirre, Andrew J., Hahn, William C., Cox, Adrienne D., Der, Channing J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8340308/
https://www.ncbi.nlm.nih.gov/pubmed/34192548
http://dx.doi.org/10.1016/j.celrep.2021.109291
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author Waters, Andrew M.
Khatib, Tala O.
Papke, Bjoern
Goodwin, Craig M.
Hobbs, G. Aaron
Diehl, J. Nathaniel
Yang, Runying
Edwards, A. Cole
Walsh, Katherine H.
Sulahian, Rita
McFarland, James M.
Kapner, Kevin S.
Gilbert, Thomas S.K.
Stalnecker, Clint A.
Javaid, Sehrish
Barkovskaya, Anna
Grover, Kajal R.
Hibshman, Priya S.
Blake, Devon R.
Schaefer, Antje
Nowak, Katherine M.
Klomp, Jennifer E.
Hayes, Tikvah K.
Kassner, Michelle
Tang, Nanyun
Tanaseichuk, Olga
Chen, Kaisheng
Zhou, Yingyao
Kalkat, Manpreet
Herring, Laura E.
Graves, Lee M.
Penn, Linda Z.
Yin, Hongwei H.
Aguirre, Andrew J.
Hahn, William C.
Cox, Adrienne D.
Der, Channing J.
author_facet Waters, Andrew M.
Khatib, Tala O.
Papke, Bjoern
Goodwin, Craig M.
Hobbs, G. Aaron
Diehl, J. Nathaniel
Yang, Runying
Edwards, A. Cole
Walsh, Katherine H.
Sulahian, Rita
McFarland, James M.
Kapner, Kevin S.
Gilbert, Thomas S.K.
Stalnecker, Clint A.
Javaid, Sehrish
Barkovskaya, Anna
Grover, Kajal R.
Hibshman, Priya S.
Blake, Devon R.
Schaefer, Antje
Nowak, Katherine M.
Klomp, Jennifer E.
Hayes, Tikvah K.
Kassner, Michelle
Tang, Nanyun
Tanaseichuk, Olga
Chen, Kaisheng
Zhou, Yingyao
Kalkat, Manpreet
Herring, Laura E.
Graves, Lee M.
Penn, Linda Z.
Yin, Hongwei H.
Aguirre, Andrew J.
Hahn, William C.
Cox, Adrienne D.
Der, Channing J.
author_sort Waters, Andrew M.
collection PubMed
description To identify therapeutic targets for KRAS mutant pancreatic cancer, we conduct a druggable genome small interfering RNA (siRNA) screen and determine that suppression of BCAR1 sensitizes pancreatic cancer cells to ERK inhibition. Integrative analysis of genome-scale CRISPR-Cas9 screens also identify BCAR1 as a top synthetic lethal interactor with mutant KRAS. BCAR1 encodes the SRC substrate p130Cas. We determine that SRC-inhibitor-mediated suppression of p130Cas phosphorylation impairs MYC transcription through a DOCK1-RAC1-β-catenin-dependent mechanism. Additionally, genetic suppression of TUBB3, encoding the βIII-tubulin subunit of microtubules, or pharmacological inhibition of microtubule function decreases levels of MYC protein in a calpain-dependent manner and potently sensitizes pancreatic cancer cells to ERK inhibition. Accordingly, the combination of a dual SRC/tubulin inhibitor with an ERK inhibitor cooperates to reduce MYC protein and synergistically suppress the growth of KRAS mutant pancreatic cancer. Thus, we demonstrate that mechanistically diverse combinations with ERK inhibition suppress MYC to impair pancreatic cancer proliferation.
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spelling pubmed-83403082021-08-05 Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition Waters, Andrew M. Khatib, Tala O. Papke, Bjoern Goodwin, Craig M. Hobbs, G. Aaron Diehl, J. Nathaniel Yang, Runying Edwards, A. Cole Walsh, Katherine H. Sulahian, Rita McFarland, James M. Kapner, Kevin S. Gilbert, Thomas S.K. Stalnecker, Clint A. Javaid, Sehrish Barkovskaya, Anna Grover, Kajal R. Hibshman, Priya S. Blake, Devon R. Schaefer, Antje Nowak, Katherine M. Klomp, Jennifer E. Hayes, Tikvah K. Kassner, Michelle Tang, Nanyun Tanaseichuk, Olga Chen, Kaisheng Zhou, Yingyao Kalkat, Manpreet Herring, Laura E. Graves, Lee M. Penn, Linda Z. Yin, Hongwei H. Aguirre, Andrew J. Hahn, William C. Cox, Adrienne D. Der, Channing J. Cell Rep Article To identify therapeutic targets for KRAS mutant pancreatic cancer, we conduct a druggable genome small interfering RNA (siRNA) screen and determine that suppression of BCAR1 sensitizes pancreatic cancer cells to ERK inhibition. Integrative analysis of genome-scale CRISPR-Cas9 screens also identify BCAR1 as a top synthetic lethal interactor with mutant KRAS. BCAR1 encodes the SRC substrate p130Cas. We determine that SRC-inhibitor-mediated suppression of p130Cas phosphorylation impairs MYC transcription through a DOCK1-RAC1-β-catenin-dependent mechanism. Additionally, genetic suppression of TUBB3, encoding the βIII-tubulin subunit of microtubules, or pharmacological inhibition of microtubule function decreases levels of MYC protein in a calpain-dependent manner and potently sensitizes pancreatic cancer cells to ERK inhibition. Accordingly, the combination of a dual SRC/tubulin inhibitor with an ERK inhibitor cooperates to reduce MYC protein and synergistically suppress the growth of KRAS mutant pancreatic cancer. Thus, we demonstrate that mechanistically diverse combinations with ERK inhibition suppress MYC to impair pancreatic cancer proliferation. 2021-06-29 /pmc/articles/PMC8340308/ /pubmed/34192548 http://dx.doi.org/10.1016/j.celrep.2021.109291 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) ).
spellingShingle Article
Waters, Andrew M.
Khatib, Tala O.
Papke, Bjoern
Goodwin, Craig M.
Hobbs, G. Aaron
Diehl, J. Nathaniel
Yang, Runying
Edwards, A. Cole
Walsh, Katherine H.
Sulahian, Rita
McFarland, James M.
Kapner, Kevin S.
Gilbert, Thomas S.K.
Stalnecker, Clint A.
Javaid, Sehrish
Barkovskaya, Anna
Grover, Kajal R.
Hibshman, Priya S.
Blake, Devon R.
Schaefer, Antje
Nowak, Katherine M.
Klomp, Jennifer E.
Hayes, Tikvah K.
Kassner, Michelle
Tang, Nanyun
Tanaseichuk, Olga
Chen, Kaisheng
Zhou, Yingyao
Kalkat, Manpreet
Herring, Laura E.
Graves, Lee M.
Penn, Linda Z.
Yin, Hongwei H.
Aguirre, Andrew J.
Hahn, William C.
Cox, Adrienne D.
Der, Channing J.
Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title_full Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title_fullStr Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title_full_unstemmed Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title_short Targeting p130Cas- and microtubule-dependent MYC regulation sensitizes pancreatic cancer to ERK MAPK inhibition
title_sort targeting p130cas- and microtubule-dependent myc regulation sensitizes pancreatic cancer to erk mapk inhibition
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8340308/
https://www.ncbi.nlm.nih.gov/pubmed/34192548
http://dx.doi.org/10.1016/j.celrep.2021.109291
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