Translation of triple-negative breast cancer behavior from the xenograft model to human model
Background: For xenograft models of triple-negative breast cancer (TNBC) to be valuable in development of molecularly-targeted drugs, careful characterization is essential to their validation. The present study aimed to validate the TNBC xenograft model with a specific focus on angiogenesis. Met...
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Tehran University of Medical Sciences
2016-11-01
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| Series: | Basic & Clinical Cancer Research |
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| Online Access: | https://bccr.tums.ac.ir/index.php/bccrj/article/view/199 |
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doaj-272d8798ad7047b8b8fb9c37f9787ba32021-04-04T07:07:01ZengTehran University of Medical SciencesBasic & Clinical Cancer Research2228-65272228-54662016-11-0183Translation of triple-negative breast cancer behavior from the xenograft model to human modelSanaz Rismanchi0Ahad Muhammadnejad1Elahe Keyhani2Samad Muhammadnejad3Saeid Amanpour4Cancer Biology Research Center, Cancer Institute, Tehran University of Medical Sciences, Tehran, IranCancer Research Center, Cancer Institute, Tehran University of Medical Sciences, Tehran, IranGenetics Research Center, University of Social Welfare & Rehabilitation Sciences, Tehran, IranResearch Center for Molecular and Cellular Imaging, Tehran University of Medical Sciences, Tehran, IranCancer Biology Research Center, Cancer Institute, Tehran University of Medical Sciences, Tehran, Iran Background: For xenograft models of triple-negative breast cancer (TNBC) to be valuable in development of molecularly-targeted drugs, careful characterization is essential to their validation. The present study aimed to validate the TNBC xenograft model with a specific focus on angiogenesis. Methods: Twelve TNBC xenograft tumors and 12 human breast cancer tumors (HTNBC) were included in this study. Both groups were grade III and p53 positive. Nuclear pleomorphism and mitotic count were analyzed by hematoxylin and eosin (H&E) stains respectively. Basal cytokeratin (CK5/6), vimentin, cathepsin-D, Ki-67 (for proliferation), and MVD-CD34 (for angiogenesis) markers were examined by immunohistochemistry (IHC). The association of Microvesseles density (MVD) with Ki-67, nuclear pleomorphism, and mitotic count was assessed in each group separately, and HTNBCs were compared with the xenograft group. Results: The xenograft models showed a significant correlation between angiogenesis (MVD) and cell proliferation (Ki-67), nuclear pleomorphism, and mitotic count (p= 0.0398; p= 0.020; p=0.001, respectively). The HTNBC group also showed a similar trend, except nuclear pleomorphism (p=0.193), which did not correlate with angiogenesis. Comparison between the two groups showed significant changes in cell proliferation (Ki-67 and vimentin). The difference in proliferation rate and vimentin expression between the two groups can be due to biological diversity between human and mice and epithelial-mesenchymal transition (EMT), respectively. Conclusion: Our results, re-emphasize the significance of angiogenic treatment therapy in patients with TNBC, and further validate the TNBC xenograft model as a valid model for drug discovery and development. https://bccr.tums.ac.ir/index.php/bccrj/article/view/199Triple-negative breast cancerXenograft modelsAngiogenesisTranslational researchValidity |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Sanaz Rismanchi Ahad Muhammadnejad Elahe Keyhani Samad Muhammadnejad Saeid Amanpour |
| spellingShingle |
Sanaz Rismanchi Ahad Muhammadnejad Elahe Keyhani Samad Muhammadnejad Saeid Amanpour Translation of triple-negative breast cancer behavior from the xenograft model to human model Basic & Clinical Cancer Research Triple-negative breast cancer Xenograft models Angiogenesis Translational research Validity |
| author_facet |
Sanaz Rismanchi Ahad Muhammadnejad Elahe Keyhani Samad Muhammadnejad Saeid Amanpour |
| author_sort |
Sanaz Rismanchi |
| title |
Translation of triple-negative breast cancer behavior from the xenograft model to human model |
| title_short |
Translation of triple-negative breast cancer behavior from the xenograft model to human model |
| title_full |
Translation of triple-negative breast cancer behavior from the xenograft model to human model |
| title_fullStr |
Translation of triple-negative breast cancer behavior from the xenograft model to human model |
| title_full_unstemmed |
Translation of triple-negative breast cancer behavior from the xenograft model to human model |
| title_sort |
translation of triple-negative breast cancer behavior from the xenograft model to human model |
| publisher |
Tehran University of Medical Sciences |
| series |
Basic & Clinical Cancer Research |
| issn |
2228-6527 2228-5466 |
| publishDate |
2016-11-01 |
| description |
Background: For xenograft models of triple-negative breast cancer (TNBC) to be valuable in development of molecularly-targeted drugs, careful characterization is essential to their validation. The present study aimed to validate the TNBC xenograft model with a specific focus on angiogenesis.
Methods: Twelve TNBC xenograft tumors and 12 human breast cancer tumors (HTNBC) were included in this study. Both groups were grade III and p53 positive. Nuclear pleomorphism and mitotic count were analyzed by hematoxylin and eosin (H&E) stains respectively. Basal cytokeratin (CK5/6), vimentin, cathepsin-D, Ki-67 (for proliferation), and MVD-CD34 (for angiogenesis) markers were examined by immunohistochemistry (IHC). The association of Microvesseles density (MVD) with Ki-67, nuclear pleomorphism, and mitotic count was assessed in each group separately, and HTNBCs were compared with the xenograft group.
Results: The xenograft models showed a significant correlation between angiogenesis (MVD) and cell proliferation (Ki-67), nuclear pleomorphism, and mitotic count (p= 0.0398; p= 0.020; p=0.001, respectively). The HTNBC group also showed a similar trend, except nuclear pleomorphism (p=0.193), which did not correlate with angiogenesis. Comparison between the two groups showed significant changes in cell proliferation (Ki-67 and vimentin). The difference in proliferation rate and vimentin expression between the two groups can be due to biological diversity between human and mice and epithelial-mesenchymal transition (EMT), respectively.
Conclusion: Our results, re-emphasize the significance of angiogenic treatment therapy in patients with TNBC, and further validate the TNBC xenograft model as a valid model for drug discovery and development.
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| topic |
Triple-negative breast cancer Xenograft models Angiogenesis Translational research Validity |
| url |
https://bccr.tums.ac.ir/index.php/bccrj/article/view/199 |
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