A new pancreatic adenocarcinoma-derived organoid model of acquired chemoresistance to FOLFIRINOX: First insight of the underlying mechanisms

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2021-09-24 DOI:10.1111/boc.202100003
Elsa Hadj Bachir, Charles Poiraud, Sonia Paget, Nicolas Stoup, Soumaya El Moghrabi, Belinda Duchêne, Nathalie Jouy, Antonino Bongiovanni, Meryem Tardivel, Louis-Bastien Weiswald, Marie Vandepeutte, César Beugniez, Fabienne Escande, Emmanuelle Leteurtre, OrgaRES consortium, Laurent Poulain, Chann Lagadec, Pascal Pigny, Nicolas Jonckheere, Florence Renaud, Stephanie Truant, Isabelle Van Seuningen, Audrey Vincent
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引用次数: 8

Abstract

Background Information

Although improvements have been made in the management of pancreatic adenocarcinoma (PDAC) during the past 20 years, the prognosis of this deadly disease remains poor with an overall 5-year survival under 10%. Treatment with FOLFIRINOX, a combined regimen of 5-fluorouracil, irinotecan (SN-38) and oxaliplatin, is nonetheless associated with an excellent initial tumour response and its use has allowed numerous patients to go through surgery while their tumour was initially considered unresectable. These discrepancies between initial tumour response and very low long-term survival are the consequences of rapidly acquired chemoresistance and represent a major therapeutic frontier. To our knowledge, a model of resistance to the combined three drugs has never been described due to the difficulty of modelling the FOLFIRINOX protocol both in vitro and in vivo. Patient-derived tumour organoids (PDO) are the missing link that has long been lacking in the wide range of epithelial cancer models between 2D adherent cultures and in vivo xenografts. In this work we sought to set up a model of PDO with resistance to FOLFIRINOX regimen that we could compare to the paired naive PDO.

Results

We first extrapolated physiological concentrations of the three drugs using previous pharmacodynamics studies and bi-compartmental elimination models of oxaliplatin and SN-38. We then treated PaTa-1818x naive PDAC organoids with six cycles of 72 h-FOLFIRINOX treatment followed by 96 h interruption. Thereafter, we systematically compared treated organoids to PaTa-1818x naive organoids in terms of growth, proliferation, viability and expression of genes involved in cancer stemness and aggressiveness.

Conclusions

We reproductively obtained resistant organoids FoxR that significantly showed less sensitivity to FOLFORINOX treatment than the PaTa-1818x naive organoids from which they were derived. Our resistant model is representative of the sequential steps of chemoresistance observed in patients in terms of growth arrest (proliferation blockade), residual disease (cell quiescence/dormancy) and relapse.

Significance

To our knowledge, this is the first genuine in vitro model of resistance to the three drugs in combined therapy. This new PDO model will be a great asset for the discovery of acquired chemoresistance mechanisms, knowledge that is mandatory before offering new therapeutic strategies for pancreatic cancer.

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一种新的胰腺腺癌衍生的对FOLFIRINOX获得性化疗耐药的类器官模型:首次了解其潜在机制
虽然在过去的20年里,胰腺腺癌(PDAC)的治疗已经取得了进展,但这种致命疾病的预后仍然很差,总5年生存率低于10%。FOLFIRINOX是一种5-氟尿嘧啶、伊立替康(n -38)和奥沙利铂的联合治疗方案,尽管如此,它的治疗与良好的初始肿瘤反应有关,并且它的使用允许许多患者在最初被认为无法切除的肿瘤时进行手术。这些最初的肿瘤反应和非常低的长期生存之间的差异是快速获得的化疗耐药的后果,代表了一个主要的治疗前沿。据我们所知,由于FOLFIRINOX方案在体外和体内建模的困难,从未描述过对三种药物联合耐药的模型。患者源性肿瘤类器官(PDO)是2D贴壁培养和体内异种移植之间广泛的上皮癌模型中长期缺乏的缺失环节。在这项工作中,我们试图建立一个对FOLFIRINOX方案耐药的PDO模型,我们可以将其与配对的幼稚PDO进行比较。我们首先利用先前的药理学研究和奥沙利铂和SN-38的双室消除模型推断出三种药物的生理浓度。然后,我们对PaTa-1818x初始PDAC类器官进行了6个周期的72 h- folfirinox治疗,随后中断96 h。随后,我们系统地比较了经过处理的类器官与未经PaTa-1818x处理的类器官在生长、增殖、活力以及与癌症干性和侵袭性相关的基因表达方面的差异。结论:我们获得了耐药类器官FoxR,其对FOLFORINOX治疗的敏感性明显低于其衍生的PaTa-1818x原始类器官。我们的耐药模型代表了在生长停止(增殖阻断)、残留疾病(细胞静止/休眠)和复发方面观察到的患者化疗耐药的顺序步骤。据我们所知,这是第一个真正的三种药物联合治疗的体外耐药模型。这种新的PDO模型将成为发现获得性化疗耐药机制的重要资产,这是在提供胰腺癌新治疗策略之前必须了解的知识。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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