Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway

K-Ras is a well-studied oncogene, and its mutation is frequently found in epithelial cancers like pancreas, lung, and colorectal cancers. Cancer cells harboring K-Ras mutations are difficult to treat due to the drug resistance and metastasis properties. Cancer stem cells (CSCs) are believed the majo...

Descripción completa

Detalles Bibliográficos
Autores principales: Qi, Yan, Zou, Hong, Zhao, XiaoHui, Kapeleris, Joanna, Monteiro, Michael, Li, Feng, Xu, Zhi Ping, Deng, Yizhen, Wu, Yanheng, Tang, Ying, Gu, Wenyi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9650442/
https://www.ncbi.nlm.nih.gov/pubmed/36386200
http://dx.doi.org/10.3389/fphar.2022.996053
_version_ 1784828019725041664
author Qi, Yan
Zou, Hong
Zhao, XiaoHui
Kapeleris, Joanna
Monteiro, Michael
Li, Feng
Xu, Zhi Ping
Deng, Yizhen
Wu, Yanheng
Tang, Ying
Gu, Wenyi
author_facet Qi, Yan
Zou, Hong
Zhao, XiaoHui
Kapeleris, Joanna
Monteiro, Michael
Li, Feng
Xu, Zhi Ping
Deng, Yizhen
Wu, Yanheng
Tang, Ying
Gu, Wenyi
author_sort Qi, Yan
collection PubMed
description K-Ras is a well-studied oncogene, and its mutation is frequently found in epithelial cancers like pancreas, lung, and colorectal cancers. Cancer cells harboring K-Ras mutations are difficult to treat due to the drug resistance and metastasis properties. Cancer stem cells (CSCs) are believed the major cause of chemotherapeutic resistance and responsible for tumor recurrence and metastasis. But how K-Ras mutation affects CSCs and inflammation is not clear. Here, we compared two colon cancer cell lines, HCT-116 and HT-29, with the former being K-Ras(G13D) mutant and the latter being wildtype. We found that HCT-116 cells treated with a K-Ras mutation inhibitor S7333 formed significantly more tumor spheroids than the untreated control, while the wild type of HT-29 cells remained unchanged. However, the size of tumor spheroids was smaller than the untreated controls, indicating their proliferation was suppressed after S7333 treatment. Consistent with this, the expressions of stem genes Lgr5 and CD133 significantly increased and the expression of self-renewal gene TGF-β1 also increased. The flow cytometry analysis indicated that the expression of stem surface marker CD133 increased in the treated HCT-116 cells. To understand the pathway through which the G13D mutation induced the effects, we studied both RAS/ERK and PI3K/Akt pathways using specific inhibitors SCH772984 and BEZ235. The results indicated that RAS/ERK rather than PI3K/Akt pathway was involved. As CSCs play the initial role in cancer development and the inflammation is a vital step during tumor initiation, we analyzed the correlation between increased stemness and inflammation. We found a close correlation of increased Lgr5 and CD133 with proinflammatory factors like IL-17, IL-22, and IL-23. Together, our findings suggest that K-Ras(G13D) mutation promotes cancer cell growth but decreases cancer stemness and inflammation thus tumorigenesis and metastasis potential in colon cancer. Inhibition of this mutation reverses the process. Therefore, care needs be taken when employing targeted therapies to K-Ras(G13D) mutations in clinics.
format Online
Article
Text
id pubmed-9650442
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-96504422022-11-15 Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway Qi, Yan Zou, Hong Zhao, XiaoHui Kapeleris, Joanna Monteiro, Michael Li, Feng Xu, Zhi Ping Deng, Yizhen Wu, Yanheng Tang, Ying Gu, Wenyi Front Pharmacol Pharmacology K-Ras is a well-studied oncogene, and its mutation is frequently found in epithelial cancers like pancreas, lung, and colorectal cancers. Cancer cells harboring K-Ras mutations are difficult to treat due to the drug resistance and metastasis properties. Cancer stem cells (CSCs) are believed the major cause of chemotherapeutic resistance and responsible for tumor recurrence and metastasis. But how K-Ras mutation affects CSCs and inflammation is not clear. Here, we compared two colon cancer cell lines, HCT-116 and HT-29, with the former being K-Ras(G13D) mutant and the latter being wildtype. We found that HCT-116 cells treated with a K-Ras mutation inhibitor S7333 formed significantly more tumor spheroids than the untreated control, while the wild type of HT-29 cells remained unchanged. However, the size of tumor spheroids was smaller than the untreated controls, indicating their proliferation was suppressed after S7333 treatment. Consistent with this, the expressions of stem genes Lgr5 and CD133 significantly increased and the expression of self-renewal gene TGF-β1 also increased. The flow cytometry analysis indicated that the expression of stem surface marker CD133 increased in the treated HCT-116 cells. To understand the pathway through which the G13D mutation induced the effects, we studied both RAS/ERK and PI3K/Akt pathways using specific inhibitors SCH772984 and BEZ235. The results indicated that RAS/ERK rather than PI3K/Akt pathway was involved. As CSCs play the initial role in cancer development and the inflammation is a vital step during tumor initiation, we analyzed the correlation between increased stemness and inflammation. We found a close correlation of increased Lgr5 and CD133 with proinflammatory factors like IL-17, IL-22, and IL-23. Together, our findings suggest that K-Ras(G13D) mutation promotes cancer cell growth but decreases cancer stemness and inflammation thus tumorigenesis and metastasis potential in colon cancer. Inhibition of this mutation reverses the process. Therefore, care needs be taken when employing targeted therapies to K-Ras(G13D) mutations in clinics. Frontiers Media S.A. 2022-10-28 /pmc/articles/PMC9650442/ /pubmed/36386200 http://dx.doi.org/10.3389/fphar.2022.996053 Text en Copyright © 2022 Qi, Zou, Zhao, Kapeleris, Monteiro, Li, Xu, Deng, Wu, Tang and Gu. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Qi, Yan
Zou, Hong
Zhao, XiaoHui
Kapeleris, Joanna
Monteiro, Michael
Li, Feng
Xu, Zhi Ping
Deng, Yizhen
Wu, Yanheng
Tang, Ying
Gu, Wenyi
Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title_full Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title_fullStr Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title_full_unstemmed Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title_short Inhibition of colon cancer K-Ras(G13D) mutation reduces cancer cell proliferation but promotes stemness and inflammation via RAS/ERK pathway
title_sort inhibition of colon cancer k-ras(g13d) mutation reduces cancer cell proliferation but promotes stemness and inflammation via ras/erk pathway
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9650442/
https://www.ncbi.nlm.nih.gov/pubmed/36386200
http://dx.doi.org/10.3389/fphar.2022.996053
work_keys_str_mv AT qiyan inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT zouhong inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT zhaoxiaohui inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT kapelerisjoanna inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT monteiromichael inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT lifeng inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT xuzhiping inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT dengyizhen inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT wuyanheng inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT tangying inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway
AT guwenyi inhibitionofcoloncancerkrasg13dmutationreducescancercellproliferationbutpromotesstemnessandinflammationviaraserkpathway

Ejemplares similares