Defining the challenges and opportunities for using patient-derived models in prostate cancer research

W. Nathaniel Brennen; Clémentine Le Magnen; Sofia Karkampouna; Nicolas Anselmino; Nathalie Bock; Nicholas Choo; Ashlee K. Clark; Ilsa M. Coleman; Robin Dolgos; Alison M. Ferguson; David L. Goode; Marianna Krutihof-de Julio; Nora M. Navone; Peter S. Nelson; Edward O'Neill; Laura H. Porter; Weranja Ranasinghe; Takuro Sunada; Elizabeth D. Williams; Lisa M. Butler; Eva Corey; Wytske M. van Weerden; Renea A. Taylor; Gail P. Risbridger; Mitchell G. Lawrence

doi:10.1002/pros.24682

Defining the challenges and opportunities for using patient-derived models in prostate cancer research

W. Nathaniel Brennen, Clémentine Le Magnen, Sofia Karkampouna, Nicolas Anselmino, Nathalie Bock, Nicholas Choo, Ashlee K. Clark, Ilsa M. Coleman, Robin Dolgos, Alison M. Ferguson, David L. Goode, Marianna Krutihof-de Julio, Nora M. Navone, Peter S. Nelson, Edward O'Neill, Laura H. Porter, Weranja Ranasinghe, Takuro Sunada, Elizabeth D. Williams, Lisa M. ButlerEva Corey, Wytske M. van Weerden, Renea A. Taylor, Gail P. Risbridger, Mitchell G. Lawrence

Genitourinary Medical Oncology

Research output: Contribution to journal › Review article › peer-review

Abstract

Background: There are relatively few widely used models of prostate cancer compared to other common malignancies. This impedes translational prostate cancer research because the range of models does not reflect the diversity of disease seen in clinical practice. In response to this challenge, research laboratories around the world have been developing new patient-derived models of prostate cancer, including xenografts, organoids, and tumor explants. Methods: In May 2023, we held a workshop at the Monash University Prato Campus for researchers with expertise in establishing and using a variety of patient-derived models of prostate cancer. This review summarizes our collective ideas on how patient-derived models are currently being used, the common challenges, and future opportunities for maximizing their usefulness in prostate cancer research. Results: An increasing number of patient-derived models for prostate cancer are being developed. Despite their individual limitations and varying success rates, these models are valuable resources for exploring new concepts in prostate cancer biology and for preclinical testing of potential treatments. Here we focus on the need for larger collections of models that represent the changing treatment landscape of prostate cancer, robust readouts for preclinical testing, improved in vitro culture conditions, and integration of the tumor microenvironment. Additional priorities include ensuring model reproducibility, standardization, and replication, and streamlining the exchange of models and data sets among research groups. Conclusions: There are several opportunities to maximize the impact of patient-derived models on prostate cancer research. We must develop large, diverse and accessible cohorts of models and more sophisticated methods for emulating the intricacy of patient tumors. In this way, we can use the samples that are generously donated by patients to advance the outcomes of patients in the future.

Original language	English (US)
Pages (from-to)	623-635
Number of pages	13
Journal	Prostate
Volume	84
Issue number	7
DOIs	https://doi.org/10.1002/pros.24682
State	Accepted/In press - 2024

Keywords

explants
models
organoids
tumor microenvironment
xenografts

ASJC Scopus subject areas

Oncology
Urology

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10.1002/pros.24682

Cite this

Brennen, W. N., Le Magnen, C., Karkampouna, S., Anselmino, N., Bock, N., Choo, N., Clark, A. K., Coleman, I. M., Dolgos, R., Ferguson, A. M., Goode, D. L., Krutihof-de Julio, M., Navone, N. M., Nelson, P. S., O'Neill, E., Porter, L. H., Ranasinghe, W., Sunada, T., Williams, E. D., ... Lawrence, M. G. (Accepted/In press). Defining the challenges and opportunities for using patient-derived models in prostate cancer research. Prostate, 84(7), 623-635. https://doi.org/10.1002/pros.24682

Brennen, WN, Le Magnen, C, Karkampouna, S, Anselmino, N, Bock, N, Choo, N, Clark, AK, Coleman, IM, Dolgos, R, Ferguson, AM, Goode, DL, Krutihof-de Julio, M, Navone, NM, Nelson, PS, O'Neill, E, Porter, LH, Ranasinghe, W, Sunada, T, Williams, ED, Butler, LM, Corey, E, van Weerden, WM, Taylor, RA, Risbridger, GP & Lawrence, MG 2024, 'Defining the challenges and opportunities for using patient-derived models in prostate cancer research', Prostate, vol. 84, no. 7, pp. 623-635. https://doi.org/10.1002/pros.24682

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title = "Defining the challenges and opportunities for using patient-derived models in prostate cancer research",

abstract = "Background: There are relatively few widely used models of prostate cancer compared to other common malignancies. This impedes translational prostate cancer research because the range of models does not reflect the diversity of disease seen in clinical practice. In response to this challenge, research laboratories around the world have been developing new patient-derived models of prostate cancer, including xenografts, organoids, and tumor explants. Methods: In May 2023, we held a workshop at the Monash University Prato Campus for researchers with expertise in establishing and using a variety of patient-derived models of prostate cancer. This review summarizes our collective ideas on how patient-derived models are currently being used, the common challenges, and future opportunities for maximizing their usefulness in prostate cancer research. Results: An increasing number of patient-derived models for prostate cancer are being developed. Despite their individual limitations and varying success rates, these models are valuable resources for exploring new concepts in prostate cancer biology and for preclinical testing of potential treatments. Here we focus on the need for larger collections of models that represent the changing treatment landscape of prostate cancer, robust readouts for preclinical testing, improved in vitro culture conditions, and integration of the tumor microenvironment. Additional priorities include ensuring model reproducibility, standardization, and replication, and streamlining the exchange of models and data sets among research groups. Conclusions: There are several opportunities to maximize the impact of patient-derived models on prostate cancer research. We must develop large, diverse and accessible cohorts of models and more sophisticated methods for emulating the intricacy of patient tumors. In this way, we can use the samples that are generously donated by patients to advance the outcomes of patients in the future.",

keywords = "explants, models, organoids, tumor microenvironment, xenografts",

author = "Brennen, {W. Nathaniel} and {Le Magnen}, Cl{\'e}mentine and Sofia Karkampouna and Nicolas Anselmino and Nathalie Bock and Nicholas Choo and Clark, {Ashlee K.} and Coleman, {Ilsa M.} and Robin Dolgos and Ferguson, {Alison M.} and Goode, {David L.} and {Krutihof-de Julio}, Marianna and Navone, {Nora M.} and Nelson, {Peter S.} and Edward O'Neill and Porter, {Laura H.} and Weranja Ranasinghe and Takuro Sunada and Williams, {Elizabeth D.} and Butler, {Lisa M.} and Eva Corey and {van Weerden}, {Wytske M.} and Taylor, {Renea A.} and Risbridger, {Gail P.} and Lawrence, {Mitchell G.}",

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year = "2024",

doi = "10.1002/pros.24682",

language = "English (US)",

volume = "84",

pages = "623--635",

journal = "Prostate",

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T1 - Defining the challenges and opportunities for using patient-derived models in prostate cancer research

AU - Brennen, W. Nathaniel

AU - Le Magnen, Clémentine

AU - Karkampouna, Sofia

AU - Anselmino, Nicolas

AU - Bock, Nathalie

AU - Choo, Nicholas

AU - Clark, Ashlee K.

AU - Coleman, Ilsa M.

AU - Dolgos, Robin

AU - Ferguson, Alison M.

AU - Goode, David L.

AU - Krutihof-de Julio, Marianna

AU - Navone, Nora M.

AU - Nelson, Peter S.

AU - O'Neill, Edward

AU - Porter, Laura H.

AU - Ranasinghe, Weranja

AU - Sunada, Takuro

AU - Williams, Elizabeth D.

AU - Butler, Lisa M.

AU - Corey, Eva

AU - van Weerden, Wytske M.

AU - Taylor, Renea A.

AU - Risbridger, Gail P.

AU - Lawrence, Mitchell G.

PY - 2024

Y1 - 2024

N2 - Background: There are relatively few widely used models of prostate cancer compared to other common malignancies. This impedes translational prostate cancer research because the range of models does not reflect the diversity of disease seen in clinical practice. In response to this challenge, research laboratories around the world have been developing new patient-derived models of prostate cancer, including xenografts, organoids, and tumor explants. Methods: In May 2023, we held a workshop at the Monash University Prato Campus for researchers with expertise in establishing and using a variety of patient-derived models of prostate cancer. This review summarizes our collective ideas on how patient-derived models are currently being used, the common challenges, and future opportunities for maximizing their usefulness in prostate cancer research. Results: An increasing number of patient-derived models for prostate cancer are being developed. Despite their individual limitations and varying success rates, these models are valuable resources for exploring new concepts in prostate cancer biology and for preclinical testing of potential treatments. Here we focus on the need for larger collections of models that represent the changing treatment landscape of prostate cancer, robust readouts for preclinical testing, improved in vitro culture conditions, and integration of the tumor microenvironment. Additional priorities include ensuring model reproducibility, standardization, and replication, and streamlining the exchange of models and data sets among research groups. Conclusions: There are several opportunities to maximize the impact of patient-derived models on prostate cancer research. We must develop large, diverse and accessible cohorts of models and more sophisticated methods for emulating the intricacy of patient tumors. In this way, we can use the samples that are generously donated by patients to advance the outcomes of patients in the future.

AB - Background: There are relatively few widely used models of prostate cancer compared to other common malignancies. This impedes translational prostate cancer research because the range of models does not reflect the diversity of disease seen in clinical practice. In response to this challenge, research laboratories around the world have been developing new patient-derived models of prostate cancer, including xenografts, organoids, and tumor explants. Methods: In May 2023, we held a workshop at the Monash University Prato Campus for researchers with expertise in establishing and using a variety of patient-derived models of prostate cancer. This review summarizes our collective ideas on how patient-derived models are currently being used, the common challenges, and future opportunities for maximizing their usefulness in prostate cancer research. Results: An increasing number of patient-derived models for prostate cancer are being developed. Despite their individual limitations and varying success rates, these models are valuable resources for exploring new concepts in prostate cancer biology and for preclinical testing of potential treatments. Here we focus on the need for larger collections of models that represent the changing treatment landscape of prostate cancer, robust readouts for preclinical testing, improved in vitro culture conditions, and integration of the tumor microenvironment. Additional priorities include ensuring model reproducibility, standardization, and replication, and streamlining the exchange of models and data sets among research groups. Conclusions: There are several opportunities to maximize the impact of patient-derived models on prostate cancer research. We must develop large, diverse and accessible cohorts of models and more sophisticated methods for emulating the intricacy of patient tumors. In this way, we can use the samples that are generously donated by patients to advance the outcomes of patients in the future.

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KW - models

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Defining the challenges and opportunities for using patient-derived models in prostate cancer research

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Keywords

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