Deciphering genetic and nongenetic factors underlying tumour dormancy: insights from multiomics analysis of two syngeneic MRD models of melanoma and leukemia.

IF 4.3 2区 生物学 Q1 BIOLOGY Biological Research Pub Date : 2024-09-03 DOI:10.1186/s40659-024-00540-y
Marie-Océane Laguillaumie, Sofia Titah, Aurélie Guillemette, Bernadette Neve, Frederic Leprêtre, Pascaline Ségard, Faruk Azam Shaik, Dominique Collard, Jean-Claude Gerbedoen, Léa Fléchon, Lama Hasan Bou Issa, Audrey Vincent, Martin Figeac, Shéhérazade Sebda, Céline Villenet, Jérôme Kluza, William Laine, Isabelle Fournier, Jean-Pascal Gimeno, Maxence Wisztorski, Salomon Manier, Mehmet Cagatay Tarhan, Bruno Quesnel, Thierry Idziorek, Yasmine Touil
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引用次数: 0

Abstract

Background: Tumour dormancy, a resistance mechanism employed by cancer cells, is a significant challenge in cancer treatment, contributing to minimal residual disease (MRD) and potential relapse. Despite its clinical importance, the mechanisms underlying tumour dormancy and MRD remain unclear. In this study, we employed two syngeneic murine models of myeloid leukemia and melanoma to investigate the genetic, epigenetic, transcriptomic and protein signatures associated with tumour dormancy. We used a multiomics approach to elucidate the molecular mechanisms driving MRD and identify potential therapeutic targets.

Results: We conducted an in-depth omics analysis encompassing whole-exome sequencing (WES), copy number variation (CNV) analysis, chromatin immunoprecipitation followed by sequencing (ChIP-seq), transcriptome and proteome investigations. WES analysis revealed a modest overlap of gene mutations between melanoma and leukemia dormancy models, with a significant number of mutated genes found exclusively in dormant cells. These exclusive genetic signatures suggest selective pressure during MRD, potentially conferring resistance to the microenvironment or therapies. CNV, histone marks and transcriptomic gene expression signatures combined with Gene Ontology (GO) enrichment analysis highlighted the potential functional roles of the mutated genes, providing insights into the pathways associated with MRD. In addition, we compared "murine MRD genes" profiles to the corresponding human disease through public datasets and highlighted common features according to disease progression. Proteomic analysis combined with multi-omics genetic investigations, revealed a dysregulated proteins signature in dormant cells with minimal genetic mechanism involvement. Pathway enrichment analysis revealed the metabolic, differentiation and cytoskeletal remodeling processes involved in MRD. Finally, we identified 11 common proteins differentially expressed in dormant cells from both pathologies.

Conclusions: Our study underscores the complexity of tumour dormancy, implicating both genetic and nongenetic factors. By comparing genomic, transcriptomic, proteomic, and epigenomic datasets, our study provides a comprehensive understanding of the molecular landscape of minimal residual disease. These results provide a robust foundation for forthcoming investigations and offer potential avenues for the advancement of targeted MRD therapies in leukemia and melanoma patients, emphasizing the importance of considering both genetic and nongenetic factors in treatment strategies.

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解密肿瘤休眠的遗传和非遗传因素:对黑色素瘤和白血病两种共生 MRD 模型进行多组学分析的启示。
背景:肿瘤休眠是癌细胞采用的一种抵抗机制,是癌症治疗中的一个重大挑战,会导致最小残留病(MRD)和潜在复发。尽管肿瘤休眠具有重要的临床意义,但肿瘤休眠和 MRD 的机制仍不清楚。在这项研究中,我们采用了骨髓性白血病和黑色素瘤的两种合成小鼠模型来研究与肿瘤休眠相关的遗传学、表观遗传学、转录组学和蛋白质特征。我们采用多组学方法阐明了驱动MRD的分子机制,并确定了潜在的治疗靶点:我们进行了深入的全组学分析,包括全外显子组测序(WES)、拷贝数变异(CNV)分析、染色质免疫沉淀测序(ChIP-seq)、转录组和蛋白质组研究。WES分析显示,黑色素瘤和白血病休眠模型的基因突变略有重叠,大量突变基因只存在于休眠细胞中。这些独有的基因特征表明,在MRD期间存在选择性压力,有可能使细胞对微环境或疗法产生抗药性。CNV、组蛋白标记和转录组基因表达特征与基因本体(GO)富集分析相结合,突显了突变基因的潜在功能作用,为了解与MRD相关的通路提供了线索。此外,我们还通过公共数据集将 "小鼠 MRD 基因 "特征与相应的人类疾病进行了比较,并根据疾病的进展突出了共同特征。蛋白质组分析与多组学遗传学研究相结合,揭示了休眠细胞中蛋白质失调的特征,其中遗传机制的参与度极低。通路富集分析揭示了 MRD 所涉及的代谢、分化和细胞骨架重塑过程。最后,我们确定了两种病理休眠细胞中差异表达的11种常见蛋白质:结论:我们的研究强调了肿瘤休眠的复杂性,涉及遗传和非遗传因素。通过比较基因组、转录组、蛋白质组和表观基因组数据集,我们的研究提供了对极小残留病分子图谱的全面了解。这些结果为今后的研究奠定了坚实的基础,并为推进白血病和黑色素瘤患者的 MRD 靶向治疗提供了潜在的途径,强调了在治疗策略中考虑遗传和非遗传因素的重要性。
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来源期刊
Biological Research
Biological Research 生物-生物学
CiteScore
10.10
自引率
0.00%
发文量
33
审稿时长
>12 weeks
期刊介绍: Biological Research is an open access, peer-reviewed journal that encompasses diverse fields of experimental biology, such as biochemistry, bioinformatics, biotechnology, cell biology, cancer, chemical biology, developmental biology, evolutionary biology, genetics, genomics, immunology, marine biology, microbiology, molecular biology, neuroscience, plant biology, physiology, stem cell research, structural biology and systems biology.
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