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Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()

Patient-derived xenograft (PDX) tumor models have emerged as a new approach to evaluate the effects of cancer drugs on patients’ personalized tumor grafts enabling to select the best treatment for the cancer patient and providing a new tool for oncology drug developers. Here, we report that human tu...

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Autores principales: Bondarenko, Gennadiy, Ugolkov, Andrey, Rohan, Stephen, Kulesza, Piotr, Dubrovskyi, Oleksii, Gursel, Demirkan, Mathews, Jeremy, O’Halloran, Thomas V., Wei, Jian J., Mazar, Andrew P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Neoplasia Press 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4611072/
https://www.ncbi.nlm.nih.gov/pubmed/26476081
http://dx.doi.org/10.1016/j.neo.2015.09.004
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author Bondarenko, Gennadiy
Ugolkov, Andrey
Rohan, Stephen
Kulesza, Piotr
Dubrovskyi, Oleksii
Gursel, Demirkan
Mathews, Jeremy
O’Halloran, Thomas V.
Wei, Jian J.
Mazar, Andrew P.
author_facet Bondarenko, Gennadiy
Ugolkov, Andrey
Rohan, Stephen
Kulesza, Piotr
Dubrovskyi, Oleksii
Gursel, Demirkan
Mathews, Jeremy
O’Halloran, Thomas V.
Wei, Jian J.
Mazar, Andrew P.
author_sort Bondarenko, Gennadiy
collection PubMed
description Patient-derived xenograft (PDX) tumor models have emerged as a new approach to evaluate the effects of cancer drugs on patients’ personalized tumor grafts enabling to select the best treatment for the cancer patient and providing a new tool for oncology drug developers. Here, we report that human tumors engrafted in immunodeficient mice are susceptible to formation of B-and T-cell PDX tumors. We xenografted human primary and metastatic tumor samples into immunodeficient mice and found that a fraction of PDX tumors generated from patients’ samples of breast, colon, pancreatic, bladder and renal cancer were histologically similar to lymphocytic neoplasms. Moreover, we found that the first passage of breast and pancreatic cancer PDX tumors after initial transplantation of the tumor pieces from the same human tumor graft could grow as a lymphocytic tumor in one mouse and as an adenocarcinoma in another mouse. Whereas subcutaneous PDX tumors resembling human adenocarcinoma histology were slow growing and non-metastatic, we found that subcutaneous PDX lymphocytic tumors were fast growing and formed large metastatic lesions in mouse lymph nodes, liver, lungs, and spleen. PDX lymphocytic tumors were comprised of B-cells which were Epstein-Barr virus positive and expressed CD45 and CD20. Because B-cells are typically present in malignant solid tumors, formation of B-cell tumor may evolve in a wide range of PDX tumor models. Although PDX tumor models show great promise in the development of personalized therapy for cancer patients, our results suggest that confidence in any given PDX tumor model requires careful screening of lymphocytic markers.
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spelling pubmed-46110722015-11-10 Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors() Bondarenko, Gennadiy Ugolkov, Andrey Rohan, Stephen Kulesza, Piotr Dubrovskyi, Oleksii Gursel, Demirkan Mathews, Jeremy O’Halloran, Thomas V. Wei, Jian J. Mazar, Andrew P. Neoplasia Article Patient-derived xenograft (PDX) tumor models have emerged as a new approach to evaluate the effects of cancer drugs on patients’ personalized tumor grafts enabling to select the best treatment for the cancer patient and providing a new tool for oncology drug developers. Here, we report that human tumors engrafted in immunodeficient mice are susceptible to formation of B-and T-cell PDX tumors. We xenografted human primary and metastatic tumor samples into immunodeficient mice and found that a fraction of PDX tumors generated from patients’ samples of breast, colon, pancreatic, bladder and renal cancer were histologically similar to lymphocytic neoplasms. Moreover, we found that the first passage of breast and pancreatic cancer PDX tumors after initial transplantation of the tumor pieces from the same human tumor graft could grow as a lymphocytic tumor in one mouse and as an adenocarcinoma in another mouse. Whereas subcutaneous PDX tumors resembling human adenocarcinoma histology were slow growing and non-metastatic, we found that subcutaneous PDX lymphocytic tumors were fast growing and formed large metastatic lesions in mouse lymph nodes, liver, lungs, and spleen. PDX lymphocytic tumors were comprised of B-cells which were Epstein-Barr virus positive and expressed CD45 and CD20. Because B-cells are typically present in malignant solid tumors, formation of B-cell tumor may evolve in a wide range of PDX tumor models. Although PDX tumor models show great promise in the development of personalized therapy for cancer patients, our results suggest that confidence in any given PDX tumor model requires careful screening of lymphocytic markers. Neoplasia Press 2015-10-19 /pmc/articles/PMC4611072/ /pubmed/26476081 http://dx.doi.org/10.1016/j.neo.2015.09.004 Text en © 2015 The Authors http://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/).
spellingShingle Article
Bondarenko, Gennadiy
Ugolkov, Andrey
Rohan, Stephen
Kulesza, Piotr
Dubrovskyi, Oleksii
Gursel, Demirkan
Mathews, Jeremy
O’Halloran, Thomas V.
Wei, Jian J.
Mazar, Andrew P.
Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title_full Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title_fullStr Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title_full_unstemmed Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title_short Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors()
title_sort patient-derived tumor xenografts are susceptible to formation of human lymphocytic tumors()
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4611072/
https://www.ncbi.nlm.nih.gov/pubmed/26476081
http://dx.doi.org/10.1016/j.neo.2015.09.004
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