通过工程化癌症类器官的原位移植对结直肠癌进展进行遗传剖析。
Genetic dissection of colorectal cancer progression by orthotopic transplantation of engineered cancer organoids.
机构信息
Hubrecht Institute, Royal Netherlands Academy of Arts and Sciences and University Medical Center (UMC) Utrecht, 3584 CT Utrecht, The Netherlands.
Cancer Genomics Netherlands, UMC Utrecht, 3584 CG, Utrecht, The Netherlands.
出版信息
Proc Natl Acad Sci U S A. 2017 Mar 21;114(12):E2357-E2364. doi: 10.1073/pnas.1701219114. Epub 2017 Mar 7.
Abstract
In the adenoma-carcinoma sequence, it is proposed that intestinal polyps evolve through a set of defined mutations toward metastatic colorectal cancer (CRC). Here, we dissect this adenoma-carcinoma sequence in vivo by using an orthotopic organoid transplantation model of human colon organoids engineered to harbor different CRC mutation combinations. We demonstrate that sequential accumulation of oncogenic mutations in Wnt, EGFR, P53, and TGF-β signaling pathways facilitates efficient tumor growth, migration, and metastatic colonization. We show that reconstitution of specific niche signals can restore metastatic growth potential of tumor cells lacking one of the oncogenic mutations. Our findings imply that the ability to metastasize-i.e., to colonize distant sites-is the direct consequence of the loss of dependency on specific niche signals.
摘要
在腺瘤-癌序列中,有人提出肠道息肉通过一系列明确的突变向转移性结直肠癌(CRC)进化。在这里,我们通过使用一种原位类器官移植模型来在体内剖析这个腺瘤-癌序列,该模型中,人类结肠类器官被设计成携带不同的 CRC 突变组合。我们证明,Wnt、EGFR、P53 和 TGF-β 信号通路中的致癌突变的顺序积累促进了肿瘤的有效生长、迁移和转移性定植。我们表明,特定龛位信号的重建可以恢复缺乏一种致癌突变的肿瘤细胞的转移生长潜力。我们的研究结果表明,转移能力——即定植于远处部位的能力——是对特定龛位信号的依赖性丧失的直接后果。
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