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Prostate organoids: emerging experimental tools for translational research
Michael Beshiri, … , Juan Juan Yin, Kathleen Kelly
Michael Beshiri, … , Juan Juan Yin, Kathleen Kelly
Published May 15, 2023
Citation Information: J Clin Invest. 2023;133(10):e169616. https://doi.org/10.1172/JCI169616.
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Review

Prostate organoids: emerging experimental tools for translational research

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Abstract

Organoid technology has provided new translational research opportunities in oncology, in part by enabling the development of patient-representative living biobanks. Prostate cancer research historically has been constrained to a small number of in vitro models, limiting the ability to translate experimental conclusions for contemporary, heterogeneous patient populations. The facility of organoid culture methods to maintain luminal prostate epithelia, the common lineage of prostate cancers, has greatly expanded the phenotypic and genotypic diversity of available tractable models, including luminal stem/progenitor cells and progressive patient-derived cancers. Biobanks of patient prostate cancer organoids enable increased accuracy in predicting therapeutic efficacy and informative clinical trial designs. Here, we discuss how prostate organoid technology is currently being used, the promising areas of future therapeutic applications, and the current obstacles to be overcome.

Authors

Michael Beshiri, Supreet Agarwal, Juan Juan Yin, Kathleen Kelly

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Figure 1

From CRPC organoid to clinical trial.

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From CRPC organoid to clinical trial.
Patient biopsy and PDX tissues are...
Patient biopsy and PDX tissues are used to establish prostate cancer organoids that recapitulate subclasses of patients with CRPC. Patient-representative organoid banks can be used for high-throughput drug screening and comprehensive biomarker detection. Following marker determinations, integrated data can be used to elucidate the most promising patient populations to consider. neg, negative.

Copyright © 2023 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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