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用于评估卵巢患者来源肿瘤类器官中RAD51介导的同源重组的自动评分

Automated Scoring to Assess RAD51-Mediated Homologous Recombination in Ovarian Patient-Derived Tumor Organoids.

作者信息

Thorel Lucie, Elie Nicolas, Morice Pierre-Marie, Weiswald Louis-Bastien, Florent Romane, Perréard Marion, Giffard Florence, Ricou Agathe, Leman Raphaël, Babin Guillaume, Lebrun Jean-François, Martin Sandrine, Briand Mélanie, Lambert Bernard, Joly Florence, Blanc-Fournier Cécile, Vaur Dominique, Dolivet Enora, Plancoulaine Benoit, Poulain Laurent

机构信息

INSERM U1086 ANTICIPE, Université de Caen Normandie, Caen, France; Comprehensive Cancer Center François Baclesse, UNICANCER, Caen, France.

US PLATON-VIRTUAL'HIS Platform, Université de Caen Normandie, Caen, France.

出版信息

Lab Invest. 2025 Apr;105(4):104097. doi: 10.1016/j.labinv.2025.104097. Epub 2025 Jan 23.

Abstract

Poly(ADP-ribose) polymerase inhibitors (PARPi) have been shown to improve progression-free survival, particularly in homologous recombination-deficient ovarian cancers. Identifying patients eligible for PARPi is currently based on next-generation sequencing, but the persistence of genomic scars in tumors after restoration of homologous recombination (HR) or epigenetic changes can be a limitation. Functional assays could thus be used to improve this profiling and faithfully identify homologous recombination-deficient tumors. The repair capacity (RECAP) test assesses the formation of RAD51 foci in proliferating cells after irradiation and can be used on tumors as well as on patient-derived tumor organoids (PDTO). However, RAD51 foci scoring is often performed manually without standardization. The purpose of this translational study was to develop an automated tool for scoring RAD51-mediated HR based on whole slide imaging of ovarian PDTO. To that end, we quantified Cyclin A2 and RAD51 immunofluorescence on 9 PDTO models derived from 8 ovarian cancer patients, and next, we compared the RECAP test results to genome instability score and to the patient clinical response. We therefore developed a standardized and automatized quantitative histoimaging tool allowing a comparative RAD51 foci evaluation and thus to define the HR status in PDTO. Our RECAP-based classification was correlated to the genome instability score, offering a new opportunity for standardization of HR assessment in PDTO. This new automated tool to score HR status, which remains to be validated on a large cohort of patients, may thus be used as a complement to next-generation sequencing-based tests in order to improve the identification of the number of patients eligible for PARPi.

摘要

聚(ADP - 核糖)聚合酶抑制剂(PARPi)已被证明可改善无进展生存期,尤其是在同源重组缺陷的卵巢癌中。目前,基于下一代测序来识别适合PARPi治疗的患者,但在同源重组(HR)恢复或发生表观遗传变化后,肿瘤中基因组疤痕的持续存在可能是一个限制因素。因此,功能检测可用于改进这种分析,并准确识别同源重组缺陷的肿瘤。修复能力(RECAP)检测评估照射后增殖细胞中RAD51灶的形成,可用于肿瘤以及患者来源的肿瘤类器官(PDTO)。然而,RAD51灶评分通常是手动进行的,缺乏标准化。这项转化研究的目的是基于卵巢PDTO的全玻片成像开发一种自动评分RAD51介导的HR的工具。为此,我们对来自8例卵巢癌患者的9个PDTO模型上的细胞周期蛋白A2和RAD51免疫荧光进行了定量,接下来,我们将RECAP检测结果与基因组不稳定性评分以及患者的临床反应进行了比较。因此,我们开发了一种标准化和自动化的定量组织成像工具,可进行RAD51灶的比较评估,从而确定PDTO中的HR状态。我们基于RECAP的分类与基因组不稳定性评分相关,为PDTO中HR评估的标准化提供了新机会。这种用于评分HR状态的新型自动化工具,仍有待在大量患者队列中进行验证,因此可作为基于下一代测序检测的补充,以改进对适合PARPi治疗患者数量的识别。

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