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自动化评估DNA倍性、染色质组织和基质分数以预测II期结直肠癌患者的预后和辅助治疗反应。

Automated assessment of DNA ploidy, chromatin organization, and stroma fraction to predict prognosis and adjuvant therapy response in patients with stage II colorectal carcinoma.

作者信息

Zhao Zhixun, Zhang Xiaochen, Li Zhongwu, Gao Yibo, Guan Xu, Jiang Zheng, Liu Zheng, Yang Ming, Chen Haipeng, Ma Xiaolong, Yang Runkun, Lu Zhao, Liu Hengchang, Yang Lujing, Wu Aiwen, Zou Shuangmei, Wang Xishan

机构信息

Department of Colorectal Surgery, National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College Beijing, China.

Department of Gastroenterology and Hepatology, Institute of Clinical Medicine, Graduate School of Comprehensive Human Sciences, University of Tsukuba Tsukuba, Japan.

出版信息

Am J Cancer Res. 2021 Dec 15;11(12):6119-6132. eCollection 2021.

Abstract

DNA ploidy, tumor stroma, and chromatin organization have important implications in tumorigenesis and patient outcome. Automated image cytometry tools were developed to quantitatively measure DNA ploidy (P), stroma fraction (S), and chromatin organization or Nucleotyping (N). This study aimed to discover their clinical value in different stages of colorectal cancer (CRC) in a Chinese patient population. A total of 496 CRC patients of stages I, II, and LMCRC (liver metastatic CRC) were enrolled in this study. Stage II CRC patients with diploidy, low-stroma, or chromatin homogenous status predicted significantly higher 5-year OS and DFS. We constructed a PSN-panel enabled the stage II patients to be further stratified into low-, middle-, high-risk groups, the 5-year OS (89.5% 67.9% 60.9%, P<0.001) and DFS (86.0% 62.3% 53.6%, P<0.001) were stratified significantly. In addition, when combined the PSN-panel with T stage or MSS status in stage II patients, the PSN-low risk patients showed significant longer 5-year OS and DFS than the PSN-high risk patients in T3 (OS: 86.3% 65.3%, P=0.015; DFS: 83.5 59.8%, P=0.013) or MSS (OS: 86.4% 63.9%, P=0.005; DFS: 85.5 57.8%, P=0.003) patients. Finally, in the group of stage II patients with at least one high-risk factor (non-diploidy, high-stroma, chromatin heterogenous), patients who received adjuvant therapy showed significantly longer OS (72.1% 48.3%, P=0.007) and DFS (64.5% 43.9%, P=0.015) than those who did not receive adjuvant therapy. In contrast, P, S, N couldn't predict the prognosis of stage I and LMCRC patients. Overall, our data demonstrate that the PSN panel is an accurate prognostic tool that can guide treatment decisions for Chinese stage II CRC patients.

摘要

DNA倍体、肿瘤基质和染色质组织在肿瘤发生和患者预后方面具有重要意义。已开发出自动图像细胞术工具来定量测量DNA倍体(P)、基质分数(S)和染色质组织或核型分析(N)。本研究旨在在中国患者群体中发现它们在不同阶段结直肠癌(CRC)中的临床价值。本研究共纳入了496例I期、II期和肝转移结直肠癌(LMCRC)患者。II期结直肠癌患者中,二倍体、低基质或染色质均一状态的患者预测5年总生存期(OS)和无病生存期(DFS)显著更高。我们构建了一个PSN模型,可将II期患者进一步分层为低、中、高风险组,5年OS(89.5%、67.9%、60.9%,P<0.001)和DFS(86.0%、62.3%、53.6%,P<0.001)有显著分层。此外,在II期患者中将PSN模型与T分期或错配修复缺陷(MSS)状态相结合时,PSN低风险患者在T3期(OS:86.3%对65.3%,P=0.015;DFS:83.5对59.8%,P=0.013)或MSS期(OS:86.4%对63.9%,P=0.005;DFS:85.5对57.8%,P=0.003)的5年OS和DFS显著长于PSN高风险患者。最后,在至少有一个高风险因素(非二倍体、高基质、染色质异质性)的II期患者组中,接受辅助治疗的患者的OS(72.1%对

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