Decoding chromosomal instability insights in CRC by integrating omics and patient-derived organoids.

IF 11.4 1区医学 Q1 ONCOLOGY

Journal of Experimental & Clinical Cancer Research Pub Date : 2025-02-28 DOI:10.1186/s13046-025-03308-8

Federica Papaccio, Manuel Cabeza-Segura, Blanca García-Micó, Francisco Gimeno-Valiente, Sheila Zúñiga-Trejos, Valentina Gambardella, María Fernanda Gutiérrez-Bravo, Carolina Martinez-Ciarpaglini, Pilar Rentero-Garrido, Tania Fleitas, Susana Roselló, Juan Antonio Carbonell-Asins, Marisol Huerta, David Moro-Valdezate, Desamparados Roda, Noelia Tarazona, Manuel M Sánchez Del Pino, Andrés Cervantes, Josefa Castillo

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引用次数: 0

Abstract

Background: Chromosomal instability (CIN) is involved in about 70% of colorectal cancers (CRCs) and is associated with poor prognosis and drug resistance. From a clinical perspective, a better knowledge of these tumour's biology will help to guide therapeutic strategies more effectively.

Methods: We used high-density chromosomal microarray analysis to evaluate CIN level of patient-derived organoids (PDOs) and their original mCRC tissues. We integrated the RNA-seq and mass spectrometry-based proteomics data from PDOs in a functional interaction network to identify the significantly dysregulated processes in CIN. This was followed by a proteome-wGII Pearson correlation analysis and an in silico validation of main findings using functional genomic databases and patient-tissues datasets to prioritize the high-confidence CIN features.

Results: By applying the weighted Genome Instability Index (wGII) to identify CIN, we classified PDOs and demonstrated a good correlation with tissues. Multi-omics analysis showed that our organoids recapitulated genomic, transcriptomic and proteomic CIN features of independent tissues cohorts. Thanks to proteotranscriptomics, we uncovered significant associations between mitochondrial metabolism and epithelial-mesenchymal transition in CIN CRC PDOs. Correlating PDOs wGII with protein abundance, we identified a subset of proteins significantly correlated with CIN. Co-localisation analysis in PDOs strengthened the putative role of IPO7 and YAP, and, through in silico analysis, we found that some of the targets give significant dependencies in cell lines with CIN compatible status.

Conclusions: We first demonstrated that PDO models are a faithful reflection of CIN tissues at the genetic and phenotypic level. Our new findings prioritize a subset of genes and molecular processes putatively required to cope with the burden on cellular fitness imposed by CIN and associated with disease aggressiveness.

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通过整合组学和患者来源的类器官来解码CRC的染色体不稳定性见解。

背景：染色体不稳定性（CIN）涉及约70%的结直肠癌（crc），并与预后不良和耐药相关。从临床角度来看，更好地了解这些肿瘤的生物学将有助于更有效地指导治疗策略。方法：采用高密度染色体微阵列分析方法评价患者源性类器官（PDOs）及其原mCRC组织的CIN水平。我们将来自PDOs的基于RNA-seq和质谱的蛋白质组学数据整合到一个功能相互作用网络中，以确定CIN中显著失调的过程。随后进行蛋白质组- wgii Pearson相关性分析，并使用功能基因组数据库和患者组织数据集对主要发现进行计算机验证，以优先考虑高置信度的CIN特征。结果：通过加权基因组不稳定性指数（wGII）来鉴定CIN，我们对pdo进行了分类，并证明了与组织的良好相关性。多组学分析表明，我们的类器官重现了独立组织队列的基因组学、转录组学和蛋白质组学CIN特征。由于蛋白质转录组学，我们发现了CIN CRC PDOs中线粒体代谢和上皮-间质转化之间的显著关联。将PDOs wGII与蛋白质丰度相关联，我们确定了与CIN显着相关的蛋白质子集。pdo的共定位分析加强了IPO7和YAP的假设作用，并且通过计算机分析，我们发现一些靶点在具有CIN兼容状态的细胞系中具有显着依赖性。结论：我们首先证明了PDO模型在遗传和表型水平上是CIN组织的忠实反映。我们的新发现优先考虑了一组基因和分子过程，这些基因和分子过程被认为是应对CIN施加的细胞适应性负担和与疾病侵袭性相关的负担所必需的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Experimental & Clinical Cancer Research 医学-肿瘤学

CiteScore

18.20

自引率

1.80%

发文量

333

审稿时长

1 months

期刊介绍： The Journal of Experimental & Clinical Cancer Research is an esteemed peer-reviewed publication that focuses on cancer research, encompassing everything from fundamental discoveries to practical applications. We welcome submissions that showcase groundbreaking advancements in the field of cancer research, especially those that bridge the gap between laboratory findings and clinical implementation. Our goal is to foster a deeper understanding of cancer, improve prevention and detection strategies, facilitate accurate diagnosis, and enhance treatment options. We are particularly interested in manuscripts that shed light on the mechanisms behind the development and progression of cancer, including metastasis. Additionally, we encourage submissions that explore molecular alterations or biomarkers that can help predict the efficacy of different treatments or identify drug resistance. Translational research related to targeted therapies, personalized medicine, tumor immunotherapy, and innovative approaches applicable to clinical investigations are also of great interest to us. We provide a platform for the dissemination of large-scale molecular characterizations of human tumors and encourage researchers to share their insights, discoveries, and methodologies with the wider scientific community. By publishing high-quality research articles, reviews, and commentaries, the Journal of Experimental & Clinical Cancer Research strives to contribute to the continuous improvement of cancer care and make a meaningful impact on patients' lives.