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通路与选择之间独特的相互作用塑造了结直肠癌腹膜转移的演变过程。

A unique interplay of access and selection shapes peritoneal metastasis evolution in colorectal cancer.

作者信息

Wassenaar Emma Ce, Gorelick Alexander N, Hung Wei-Ting, Cheek David M, Kucukkose Emre, Lee I-Hsiu, Blohmer Martin, Degner Sebastian, Giunta Peter, Wiezer Rene Mj, Raicu Mihaela G, Ubink Inge, Klaasen Sjoerd J, Lansu Nico, Watson Emma V, Corcoran Ryan B, Boland Genevieve, Getz Gad, Kops Geert Jpl, Juric Dejan, Lennerz Jochen K, Boerma Djamila, Kranenburg Onno, Naxerova Kamila

机构信息

Department of Surgery, St. Antonius Hospital, Nieuwegein, the Netherlands.

Department of Surgical Oncology, Laboratory Translational Oncology, University Medical Center Utrecht, Utrecht, the Netherlands.

出版信息

bioRxiv. 2024 Sep 27:2024.09.25.614736. doi: 10.1101/2024.09.25.614736.

Abstract

Whether metastasis in humans can be accomplished by most primary tumor cells or requires the evolution of a specialized trait remains an open question. To evaluate whether metastases are founded by non-random subsets of primary tumor lineages requires extensive, difficult-to-implement sampling. We have realized an unusually dense multi-region sampling scheme in a cohort of 26 colorectal cancer patients with peritoneal metastases, reconstructing the evolutionary history of on average 28.8 tissue samples per patient with a microsatellite-based fingerprinting assay. To assess metastatic randomness, we evaluate inter- and intra-metastatic heterogeneity relative to the primary tumor and find that peritoneal metastases are more heterogeneous than liver metastases but less diverse than locoregional metastases. Metachronous peritoneal metastases exposed to systemic chemotherapy show significantly higher inter-lesion diversity than synchronous, untreated metastases. Projection of peritoneal metastasis origins onto a spatial map of the primary tumor reveals that they often originate at the deep-invading edge, in contrast to liver and lymph node metastases which exhibit no such preference. Furthermore, peritoneal metastases typically do not share a common subclonal origin with distant metastases in more remote organs. Synthesizing these insights into an evolutionary portrait of peritoneal metastases, we conclude that the peritoneal-metastatic process imposes milder selective pressures onto disseminating cancer cells than the liver-metastatic process. Peritoneal metastases' unique evolutionary features have potential implications for staging and treatment.

摘要

人类中的转移是由大多数原发性肿瘤细胞完成的,还是需要一种特殊特征的进化,这仍然是一个悬而未决的问题。评估转移是否由原发性肿瘤谱系的非随机亚群形成,需要进行广泛且难以实施的采样。我们在一组26例患有腹膜转移的结直肠癌患者中实现了一种异常密集的多区域采样方案,使用基于微卫星的指纹分析方法重建了每位患者平均28.8个组织样本的进化历史。为了评估转移的随机性,我们评估了相对于原发性肿瘤的转移间和转移内异质性,发现腹膜转移比肝转移更具异质性,但比局部区域转移的多样性更低。接受全身化疗的异时性腹膜转移显示出比同步、未治疗的转移更高的病灶间多样性。将腹膜转移起源投射到原发性肿瘤的空间图谱上发现,它们通常起源于深度浸润边缘,这与肝转移和淋巴结转移不同,后者没有这种偏好。此外,腹膜转移通常与更远处器官的远处转移没有共同的亚克隆起源。将这些见解综合成腹膜转移的进化图景,我们得出结论,与肝转移过程相比,腹膜转移过程对播散癌细胞施加的选择性压力较小。腹膜转移的独特进化特征对分期和治疗具有潜在影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/281c/11463674/7ceb33800a99/nihpp-2024.09.25.614736v1-f0001.jpg

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