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Preserved genetic diversity in organoids cultured from biopsies of human colorectal cancer metastases

机译:从人类大肠癌转移灶活检组织培养的类器官中的遗传多样性得到保留

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摘要

Tumor organoids are 3D cultures of cancer cells. They can be derived from the tumor of each individual patient, thereby providing an attractive ex vivo assay to tailor treatment. Using patient-derived tumor organoids for this purpose requires that organoids derived from biopsies maintain the genetic diversity of the in vivo tumor. In this study tumor biopsies were obtained from 14 patients with metastatic colorectal cancer (i) to test the feasibility of organoid culture from metastatic biopsy specimens and (ii) to compare the genetic diversity of patient-derived tumor organoids and the original tumor biopsy. Genetic analysis was performed using SOLiD sequencing for 1,977 cancer-relevant genes. Copy number profiles were generated from sequencing data using CopywriteR. Here we demonstrate that organoid cultures can be established from tumor biopsies of patients with metastatic colorectal cancer with a success rate of 71%. Genetic analysis showed that organoids reflect the metastasis from which they were derived. Ninety percent of somatic mutations were shared between organoids and biopsies from the same patient, and the DNA copy number profiles of organoids and the corresponding original tumor show a correlation of 0.89. Most importantly, none of the mutations that were found exclusively in either the tumor or organoid culture are in driver genes or genes amenable for drug targeting. These findings support further exploration of patient-derived organoids as an ex vivo platform to personalize anticancer treatment.
机译:肿瘤类器官是癌细胞的3D培养物。它们可以源自每个个体患者的肿瘤,从而提供了有吸引力的离体测定以调整治疗。为此目的使用患者来源的肿瘤类器官需要从活检组织衍生的类器官保持体内肿瘤的遗传多样性。在这项研究中,从14例转移性结直肠癌患者中进行了肿瘤活检(i)从转移性活检标本中测试类器官培养的可行性,以及(ii)比较患者源性肿瘤类器官与原始肿瘤活检的遗传多样性。使用SOLiD测序对1,977个与癌症相关的基因进行了遗传分析。副本编号配置文件是使用CopywriteR从测序数据生成的。在这里,我们证明可以从转移性结直肠癌患者的肿瘤活检中建立类器官培养物,成功率为71%。遗传分析表明类器官反映了其起源的转移。来自同一患者的类器官和活组织检查之间共有90%的体细胞突变,类器官和相应的原始肿瘤的DNA拷贝数分布显示出0.89的相关性。最重要的是,仅在肿瘤或类器官培养物中发现的突变均不在驱动基因或适合药物靶向的基因中。这些发现支持进一步探索患者来源的类器官作为个体化抗癌治疗的离体平台。

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