Cargando…
Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs
Cancer cells can survive chemotherapy-induced stress, but how they recover from it is not known. Using a temporal multiomics approach, we delineate the global mechanisms of proteotoxic stress resolution in multiple myeloma cells recovering from proteasome inhibition. Our observations define layered...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
National Academy of Sciences
2021
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8092411/ https://www.ncbi.nlm.nih.gov/pubmed/33883278 http://dx.doi.org/10.1073/pnas.2018229118 |
| _version_ | 1783687654530875392 |
|---|---|
| author | Saavedra-García, Paula Roman-Trufero, Monica Al-Sadah, Hibah A. Blighe, Kevin López-Jiménez, Elena Christoforou, Marilena Penfold, Lucy Capece, Daria Xiong, Xiaobei Miao, Yirun Parzych, Katarzyna Caputo, Valentina S. Siskos, Alexandros P. Encheva, Vesela Liu, Zijing Thiel, Denise Kaiser, Martin F. Piazza, Paolo Chaidos, Aristeidis Karadimitris, Anastasios Franzoso, Guido Snijders, Ambrosius P. Keun, Hector C. Oyarzún, Diego A. Barahona, Mauricio Auner, Holger W. |
| author_facet | Saavedra-García, Paula Roman-Trufero, Monica Al-Sadah, Hibah A. Blighe, Kevin López-Jiménez, Elena Christoforou, Marilena Penfold, Lucy Capece, Daria Xiong, Xiaobei Miao, Yirun Parzych, Katarzyna Caputo, Valentina S. Siskos, Alexandros P. Encheva, Vesela Liu, Zijing Thiel, Denise Kaiser, Martin F. Piazza, Paolo Chaidos, Aristeidis Karadimitris, Anastasios Franzoso, Guido Snijders, Ambrosius P. Keun, Hector C. Oyarzún, Diego A. Barahona, Mauricio Auner, Holger W. |
| author_sort | Saavedra-García, Paula |
| collection | PubMed |
| description | Cancer cells can survive chemotherapy-induced stress, but how they recover from it is not known. Using a temporal multiomics approach, we delineate the global mechanisms of proteotoxic stress resolution in multiple myeloma cells recovering from proteasome inhibition. Our observations define layered and protracted programs for stress resolution that encompass extensive changes across the transcriptome, proteome, and metabolome. Cellular recovery from proteasome inhibition involved protracted and dynamic changes of glucose and lipid metabolism and suppression of mitochondrial function. We demonstrate that recovering cells are more vulnerable to specific insults than acutely stressed cells and identify the general control nonderepressable 2 (GCN2)-driven cellular response to amino acid scarcity as a key recovery-associated vulnerability. Using a transcriptome analysis pipeline, we further show that GCN2 is also a stress-independent bona fide target in transcriptional signature-defined subsets of solid cancers that share molecular characteristics. Thus, identifying cellular trade-offs tied to the resolution of chemotherapy-induced stress in tumor cells may reveal new therapeutic targets and routes for cancer therapy optimization. |
| format | Online Article Text |
| id | pubmed-8092411 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2021 |
| publisher | National Academy of Sciences |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-80924112021-05-12 Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs Saavedra-García, Paula Roman-Trufero, Monica Al-Sadah, Hibah A. Blighe, Kevin López-Jiménez, Elena Christoforou, Marilena Penfold, Lucy Capece, Daria Xiong, Xiaobei Miao, Yirun Parzych, Katarzyna Caputo, Valentina S. Siskos, Alexandros P. Encheva, Vesela Liu, Zijing Thiel, Denise Kaiser, Martin F. Piazza, Paolo Chaidos, Aristeidis Karadimitris, Anastasios Franzoso, Guido Snijders, Ambrosius P. Keun, Hector C. Oyarzún, Diego A. Barahona, Mauricio Auner, Holger W. Proc Natl Acad Sci U S A Biological Sciences Cancer cells can survive chemotherapy-induced stress, but how they recover from it is not known. Using a temporal multiomics approach, we delineate the global mechanisms of proteotoxic stress resolution in multiple myeloma cells recovering from proteasome inhibition. Our observations define layered and protracted programs for stress resolution that encompass extensive changes across the transcriptome, proteome, and metabolome. Cellular recovery from proteasome inhibition involved protracted and dynamic changes of glucose and lipid metabolism and suppression of mitochondrial function. We demonstrate that recovering cells are more vulnerable to specific insults than acutely stressed cells and identify the general control nonderepressable 2 (GCN2)-driven cellular response to amino acid scarcity as a key recovery-associated vulnerability. Using a transcriptome analysis pipeline, we further show that GCN2 is also a stress-independent bona fide target in transcriptional signature-defined subsets of solid cancers that share molecular characteristics. Thus, identifying cellular trade-offs tied to the resolution of chemotherapy-induced stress in tumor cells may reveal new therapeutic targets and routes for cancer therapy optimization. National Academy of Sciences 2021-04-27 2021-04-21 /pmc/articles/PMC8092411/ /pubmed/33883278 http://dx.doi.org/10.1073/pnas.2018229118 Text en Copyright © 2021 the Author(s). Published by PNAS. https://creativecommons.org/licenses/by/4.0/This open access article is distributed under Creative Commons Attribution License 4.0 (CC BY) (https://creativecommons.org/licenses/by/4.0/) . |
| spellingShingle | Biological Sciences Saavedra-García, Paula Roman-Trufero, Monica Al-Sadah, Hibah A. Blighe, Kevin López-Jiménez, Elena Christoforou, Marilena Penfold, Lucy Capece, Daria Xiong, Xiaobei Miao, Yirun Parzych, Katarzyna Caputo, Valentina S. Siskos, Alexandros P. Encheva, Vesela Liu, Zijing Thiel, Denise Kaiser, Martin F. Piazza, Paolo Chaidos, Aristeidis Karadimitris, Anastasios Franzoso, Guido Snijders, Ambrosius P. Keun, Hector C. Oyarzún, Diego A. Barahona, Mauricio Auner, Holger W. Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title | Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title_full | Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title_fullStr | Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title_full_unstemmed | Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title_short | Systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| title_sort | systems level profiling of chemotherapy-induced stress resolution in cancer cells reveals druggable trade-offs |
| topic | Biological Sciences |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8092411/ https://www.ncbi.nlm.nih.gov/pubmed/33883278 http://dx.doi.org/10.1073/pnas.2018229118 |
| work_keys_str_mv | AT saavedragarciapaula systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT romantruferomonica systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT alsadahhibaha systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT blighekevin systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT lopezjimenezelena systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT christoforoumarilena systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT penfoldlucy systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT capecedaria systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT xiongxiaobei systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT miaoyirun systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT parzychkatarzyna systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT caputovalentinas systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT siskosalexandrosp systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT enchevavesela systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT liuzijing systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT thieldenise systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT kaisermartinf systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT piazzapaolo systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT chaidosaristeidis systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT karadimitrisanastasios systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT franzosoguido systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT snijdersambrosiusp systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT keunhectorc systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT oyarzundiegoa systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT barahonamauricio systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs AT aunerholgerw systemslevelprofilingofchemotherapyinducedstressresolutionincancercellsrevealsdruggabletradeoffs |