Microarray-based detection and expression analysis of drug resistance in an animal model of peritoneal metastasis from colon cancer

IF 4.2 3区 医学 Q2 ONCOLOGY Clinical & Experimental Metastasis Pub Date : 2024-04-12 DOI:10.1007/s10585-024-10283-5
Vugar Yagublu, Bayram Bayramov, Christoph Reissfelder, Javahir Hajibabazade, Shalala Abdulrahimli, Michael Keese
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Abstract

Chemotherapy drugs efficiently eradicate rapidly dividing differentiated cells by inducing cell death, but poorly target slowly dividing cells, including cancer stem cells and dormant cancer cells, in the later course of treatment. Prolonged exposure to chemotherapy results in a decrease in the proportion of apoptotic cells in the tumour mass. To investigate and characterize the molecular basis of this phenomenon, microarray-based expression analysis was performed to compare tHcred2-DEVD-EGFP-caspase 3-sensor transfected C-26 tumour cells that were harvested after engraftment into mice treated with or without 5-FU. Peritoneal metastasis was induced by intraperitoneal injection of C-26 cells, which were subsequently reisolated from omental metastatic tumours after the mice were sacrificed by the end of the 10th day after tumour injection. The purity of reisolated tHcred2-DEVD-EGFP-caspase 3-sensor-expressing C-26 cells was confirmed using FLIM, and total RNA was extracted for gene expression profiling. The validation of relative transcript levels was carried out via real-time semiquantitative RT‒PCR assays. Our results demonstrated that chemotherapy induced the differential expression of mediators of cancer cell dormancy and cell survival-related genes and downregulation of both intrinsic and extrinsic apoptotic signalling pathways. Despite the fact that some differentially expressed genes, such as BMP7 and Prss11, have not been thoroughly studied in the context of chemoresistance thus far, they might be potential candidates for future studies on overcoming drug resistance.

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基于芯片的结肠癌腹膜转移动物模型耐药性检测和表达分析
化疗药物通过诱导细胞死亡有效地消灭了快速分裂分化的细胞,但在后期治疗过程中,对缓慢分裂的细胞,包括癌症干细胞和休眠癌细胞的靶向作用较差。长期接受化疗会导致肿瘤组织中凋亡细胞比例下降。为了研究和描述这一现象的分子基础,研究人员进行了基于芯片的表达分析,比较了tHcred2-DEVD-EGFP-caspase 3传感器转染的C-26肿瘤细胞,这些细胞在移植到接受或不接受5-FU治疗的小鼠体内后被收获。通过腹腔注射 C-26 细胞诱导腹膜转移,在肿瘤注射后第 10 天小鼠被处死后,从网膜转移瘤中重新分离出 C-26 细胞。利用 FLIM 确认了重新分离的 tHcred2-DEVD-EGFP-caspase 3 传感器表达的 C-26 细胞的纯度,并提取总 RNA 进行基因表达谱分析。通过实时半定量 RT-PCR 检测验证了相对转录水平。我们的研究结果表明,化疗诱导了癌细胞休眠介质和细胞存活相关基因的差异表达,并下调了内在和外在凋亡信号通路。尽管一些差异表达基因(如 BMP7 和 Prss11)迄今为止尚未在化疗耐药性方面得到深入研究,但它们可能是未来克服耐药性研究的潜在候选基因。
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来源期刊
CiteScore
7.80
自引率
5.00%
发文量
55
审稿时长
12 months
期刊介绍: The Journal''s scope encompasses all aspects of metastasis research, whether laboratory-based, experimental or clinical and therapeutic. It covers such areas as molecular biology, pharmacology, tumor biology, and clinical cancer treatment (with all its subdivisions of surgery, chemotherapy and radio-therapy as well as pathology and epidemiology) insofar as these disciplines are concerned with the Journal''s core subject of metastasis formation, prevention and treatment.
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