Cargando…
In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion
We developed a murine spine metastasis model by screening five metastatic non-small cell lung cancer cell lines (PC-9, A549, NCI-H1299, NCI-H460, H2030). A549 cells displayed the highest tendency towards spine metastases. After three rounds of selection in vivo, we isolated a clone named A549L6, whi...
| Autores principales: | , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Impact Journals LLC
2015
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673208/ https://www.ncbi.nlm.nih.gov/pubmed/26090868 |
| _version_ | 1782404690784288768 |
|---|---|
| author | Cai, Xiaopan Luo, Jian Yang, Xinghai Deng, Huayun Zhang, Jishen Li, Shichang Wei, Haifeng Yang, Cheng Xu, Leqin Jin, Rongrong Li, Zhenxi Zhou, Wang Ding, JianDong Chu, Jianjun Jia, Lianshun Jia, Qi Tan, Chengjun Liu, Mingyao Xiao, Jianru |
| author_facet | Cai, Xiaopan Luo, Jian Yang, Xinghai Deng, Huayun Zhang, Jishen Li, Shichang Wei, Haifeng Yang, Cheng Xu, Leqin Jin, Rongrong Li, Zhenxi Zhou, Wang Ding, JianDong Chu, Jianjun Jia, Lianshun Jia, Qi Tan, Chengjun Liu, Mingyao Xiao, Jianru |
| author_sort | Cai, Xiaopan |
| collection | PubMed |
| description | We developed a murine spine metastasis model by screening five metastatic non-small cell lung cancer cell lines (PC-9, A549, NCI-H1299, NCI-H460, H2030). A549 cells displayed the highest tendency towards spine metastases. After three rounds of selection in vivo, we isolated a clone named A549L6, which induced spine metastasis in 80% of injected mice. The parameters of the A549L6 cell spinal metastatic mouse models were consistent with clinical spine metastasis features. All the spinal metastatic mice developed symptoms of nerve compression after 40 days. A549L6 cells had increased migration, invasiveness and decreased adhesion compared to the original A549L0 cells. In contrast, there was no significant differences in cell proliferation, apoptosis and sensitivity to chemotherapeutic agents such as cisplatin. Comparative transcriptomic analysis and Real-time PCR analysis showed that expression of signaling molecules regulating several tumor properties including migration (MYL9), metastasis (CEACAM6, VEGFC, CX3CL1, CST1, CCL5, S100A9, IGF1, NOTCH3), adhesion (FN1, CEACAM1) and inflammation (TRAF2, NFκB2 and RelB) were altered in A549L6 cells. We suggest that migration, adhesion and inflammation related genes contribute to spine metastatic capacity. |
| format | Online Article Text |
| id | pubmed-4673208 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2015 |
| publisher | Impact Journals LLC |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-46732082015-12-23 In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion Cai, Xiaopan Luo, Jian Yang, Xinghai Deng, Huayun Zhang, Jishen Li, Shichang Wei, Haifeng Yang, Cheng Xu, Leqin Jin, Rongrong Li, Zhenxi Zhou, Wang Ding, JianDong Chu, Jianjun Jia, Lianshun Jia, Qi Tan, Chengjun Liu, Mingyao Xiao, Jianru Oncotarget Research Paper We developed a murine spine metastasis model by screening five metastatic non-small cell lung cancer cell lines (PC-9, A549, NCI-H1299, NCI-H460, H2030). A549 cells displayed the highest tendency towards spine metastases. After three rounds of selection in vivo, we isolated a clone named A549L6, which induced spine metastasis in 80% of injected mice. The parameters of the A549L6 cell spinal metastatic mouse models were consistent with clinical spine metastasis features. All the spinal metastatic mice developed symptoms of nerve compression after 40 days. A549L6 cells had increased migration, invasiveness and decreased adhesion compared to the original A549L0 cells. In contrast, there was no significant differences in cell proliferation, apoptosis and sensitivity to chemotherapeutic agents such as cisplatin. Comparative transcriptomic analysis and Real-time PCR analysis showed that expression of signaling molecules regulating several tumor properties including migration (MYL9), metastasis (CEACAM6, VEGFC, CX3CL1, CST1, CCL5, S100A9, IGF1, NOTCH3), adhesion (FN1, CEACAM1) and inflammation (TRAF2, NFκB2 and RelB) were altered in A549L6 cells. We suggest that migration, adhesion and inflammation related genes contribute to spine metastatic capacity. Impact Journals LLC 2015-06-10 /pmc/articles/PMC4673208/ /pubmed/26090868 Text en Copyright: © 2015 Cai et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Paper Cai, Xiaopan Luo, Jian Yang, Xinghai Deng, Huayun Zhang, Jishen Li, Shichang Wei, Haifeng Yang, Cheng Xu, Leqin Jin, Rongrong Li, Zhenxi Zhou, Wang Ding, JianDong Chu, Jianjun Jia, Lianshun Jia, Qi Tan, Chengjun Liu, Mingyao Xiao, Jianru In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title | In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title_full | In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title_fullStr | In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title_full_unstemmed | In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title_short | In vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| title_sort | in vivo selection for spine-derived highly metastatic lung cancer cells is associated with increased migration, inflammation and decreased adhesion |
| topic | Research Paper |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673208/ https://www.ncbi.nlm.nih.gov/pubmed/26090868 |
| work_keys_str_mv | AT caixiaopan invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT luojian invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT yangxinghai invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT denghuayun invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT zhangjishen invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT lishichang invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT weihaifeng invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT yangcheng invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT xuleqin invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT jinrongrong invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT lizhenxi invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT zhouwang invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT dingjiandong invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT chujianjun invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT jialianshun invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT jiaqi invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT tanchengjun invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT liumingyao invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion AT xiaojianru invivoselectionforspinederivedhighlymetastaticlungcancercellsisassociatedwithincreasedmigrationinflammationanddecreasedadhesion |