Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response

For many years, cell lines and animal models have been essential to improve our understanding of the basis of cell metabolism, signaling, and genetics. They also provided an essential boost to cancer drug discovery. Nevertheless, these model systems failed to reproduce the tumor heterogeneity and th...

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Autores principales: Piro, Geny, Agostini, Antonio, Larghi, Alberto, Quero, Giuseppe, Carbone, Carmine, Esposito, Annachiara, Rizzatti, Gianenrico, Attili, Fabia, Alfieri, Sergio, Costamagna, Guido, Tortora, Giampaolo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8733292/
https://www.ncbi.nlm.nih.gov/pubmed/35004765
http://dx.doi.org/10.3389/fmed.2021.793144
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author Piro, Geny
Agostini, Antonio
Larghi, Alberto
Quero, Giuseppe
Carbone, Carmine
Esposito, Annachiara
Rizzatti, Gianenrico
Attili, Fabia
Alfieri, Sergio
Costamagna, Guido
Tortora, Giampaolo
author_facet Piro, Geny
Agostini, Antonio
Larghi, Alberto
Quero, Giuseppe
Carbone, Carmine
Esposito, Annachiara
Rizzatti, Gianenrico
Attili, Fabia
Alfieri, Sergio
Costamagna, Guido
Tortora, Giampaolo
author_sort Piro, Geny
collection PubMed
description For many years, cell lines and animal models have been essential to improve our understanding of the basis of cell metabolism, signaling, and genetics. They also provided an essential boost to cancer drug discovery. Nevertheless, these model systems failed to reproduce the tumor heterogeneity and the complex biological interactions between cancer cells and human hosts, making a high priority search for alternative methods that are able to export results from model systems to humans, which has become a major bottleneck in the drug development. The emergent human in vitro 3D cell culture technologies have attracted widespread attention because they seem to have the potential to overcome these limitations. Organoids are unique 3D culture models with the ability to self-organize in contained structures. Their versatility has offered an exceptional window of opportunity to approach human cancers. Pancreatic cancers (PCs) patient-derived-organoids (PDOs) preserve histological, genomic, and molecular features of neoplasms they originate from and therefore retain their heterogeneity. Patient-derived organoids can be established with a high success rate from minimal tissue core specimens acquired with endoscopic-ultrasound-guided techniques and assembled into platforms, representing tens to hundreds of cancers each conserving specific features, expanding the types of patient samples that can be propagated and analyzed in the laboratory. Because of their nature, PDO platforms are multipurpose systems that can be easily adapted in co-culture settings to perform a wide spectrum of studies, ranging from drug discovery to immune response evaluation to tumor-stroma interaction. This possibility to increase the complexity of organoids creating a hybrid culture with non-epithelial cells increases the interest in organoid-based platforms giving a pragmatic way to deeply study biological interactions in vitro. In this view, implementing organoid models in co-clinical trials to compare drug responses may represent the next step toward even more personalized medicine. In the present review, we discuss how PDO platforms are shaping modern-day oncology aiding to unravel the most complex aspects of PC.
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spelling pubmed-87332922022-01-07 Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response Piro, Geny Agostini, Antonio Larghi, Alberto Quero, Giuseppe Carbone, Carmine Esposito, Annachiara Rizzatti, Gianenrico Attili, Fabia Alfieri, Sergio Costamagna, Guido Tortora, Giampaolo Front Med (Lausanne) Medicine For many years, cell lines and animal models have been essential to improve our understanding of the basis of cell metabolism, signaling, and genetics. They also provided an essential boost to cancer drug discovery. Nevertheless, these model systems failed to reproduce the tumor heterogeneity and the complex biological interactions between cancer cells and human hosts, making a high priority search for alternative methods that are able to export results from model systems to humans, which has become a major bottleneck in the drug development. The emergent human in vitro 3D cell culture technologies have attracted widespread attention because they seem to have the potential to overcome these limitations. Organoids are unique 3D culture models with the ability to self-organize in contained structures. Their versatility has offered an exceptional window of opportunity to approach human cancers. Pancreatic cancers (PCs) patient-derived-organoids (PDOs) preserve histological, genomic, and molecular features of neoplasms they originate from and therefore retain their heterogeneity. Patient-derived organoids can be established with a high success rate from minimal tissue core specimens acquired with endoscopic-ultrasound-guided techniques and assembled into platforms, representing tens to hundreds of cancers each conserving specific features, expanding the types of patient samples that can be propagated and analyzed in the laboratory. Because of their nature, PDO platforms are multipurpose systems that can be easily adapted in co-culture settings to perform a wide spectrum of studies, ranging from drug discovery to immune response evaluation to tumor-stroma interaction. This possibility to increase the complexity of organoids creating a hybrid culture with non-epithelial cells increases the interest in organoid-based platforms giving a pragmatic way to deeply study biological interactions in vitro. In this view, implementing organoid models in co-clinical trials to compare drug responses may represent the next step toward even more personalized medicine. In the present review, we discuss how PDO platforms are shaping modern-day oncology aiding to unravel the most complex aspects of PC. Frontiers Media S.A. 2021-12-23 /pmc/articles/PMC8733292/ /pubmed/35004765 http://dx.doi.org/10.3389/fmed.2021.793144 Text en Copyright © 2021 Piro, Agostini, Larghi, Quero, Carbone, Esposito, Rizzatti, Attili, Alfieri, Costamagna and Tortora. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Medicine
Piro, Geny
Agostini, Antonio
Larghi, Alberto
Quero, Giuseppe
Carbone, Carmine
Esposito, Annachiara
Rizzatti, Gianenrico
Attili, Fabia
Alfieri, Sergio
Costamagna, Guido
Tortora, Giampaolo
Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title_full Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title_fullStr Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title_full_unstemmed Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title_short Pancreatic Cancer Patient-Derived Organoid Platforms: A Clinical Tool to Study Cell- and Non-Cell-Autonomous Mechanisms of Treatment Response
title_sort pancreatic cancer patient-derived organoid platforms: a clinical tool to study cell- and non-cell-autonomous mechanisms of treatment response
topic Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8733292/
https://www.ncbi.nlm.nih.gov/pubmed/35004765
http://dx.doi.org/10.3389/fmed.2021.793144
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