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癌症生物学还是监测不力?一项关于结肠镜检查后结肠炎相关结直肠癌的多中心回顾性分析

Cancer Biology or Ineffective Surveillance? A Multicentre Retrospective Analysis of Colitis-Associated Post-Colonoscopy Colorectal Cancers.

作者信息

Kabir Misha, Thomas-Gibson Siwan, Ahmad Ahmir, Kader Rawen, Al-Hillawi Lulia, Mcguire Joshua, David Lewis, Shah Krishna, Rao Rohit, Vega Roser, East James E, Faiz Omar D, Hart Ailsa L, Wilson Ana

机构信息

Division of GI Services, University College London Hospitals NHS Foundation Trust, 250 Euston Road, London NW1 2PG, UK.

Imperial College London, London, UK.

出版信息

J Crohns Colitis. 2024 May 31;18(5):686-694. doi: 10.1093/ecco-jcc/jjad189.

Abstract

BACKGROUND AND AIMS

Inflammatory bowel disease [IBD] is associated with high rates of post-colonoscopy colorectal cancer [PCCRC], but further in-depth qualitative analyses are required to determine whether they result from inadequate surveillance or aggressive IBD cancer evolution.

METHODS

All IBD patients who had a colorectal cancer [CRC] diagnosed between January 2015 and July 2019 and a recent [<4 years] surveillance colonoscopy at one of four English hospital trusts underwent root cause analyses as recommended by the World Endoscopy Organisation to identify plausible PCCRC causative factors.

RESULTS

In total, 61% [n = 22/36] of the included IBD CRCs were PCCRCs. They developed in patients with high cancer risk factors [77.8%; n = 28/36] requiring annual surveillance, yet 57.1% [n = 20/35] had inappropriately delayed surveillance. Most PCCRCs developed in situations where [i] an endoscopically unresectable lesion was detected [40.9%; n = 9/22], [ii] there was a deviation from the planned management pathway [40.9%; n = 9/22], such as service-, clinician- or patient-related delays in acting on a detected lesion, or [iii] lesions were potentially missed as they were typically located within areas of active inflammation or post-inflammatory change [36.4%; n = 8/22].

CONCLUSIONS

IBD PCCRC prevention will require more proactive strategies to reduce endoscopic inflammatory burden, and to improve lesion optical characterization, adherence to recommended surveillance intervals, and patient acceptance of prophylactic colectomy. However, the significant proportion appearing to originate from non-adenomatous-looking mucosa which fail to yield neoplasia on biopsy yet display aggressive cancer evolution highlights the limitations of current surveillance. Emerging molecular biomarkers may play a role in enhancing cancer risk stratification in future clinical practice.

摘要

背景与目的

炎症性肠病(IBD)与结肠镜检查后结直肠癌(PCCRC)的高发病率相关,但需要进一步深入的定性分析来确定其是源于监测不足还是IBD癌症的侵袭性进展。

方法

对2015年1月至2019年7月期间被诊断为结直肠癌(CRC)且在四个英国医院信托机构之一近期(<4年)接受过监测结肠镜检查的所有IBD患者,按照世界内镜组织的建议进行根本原因分析,以确定可能的PCCRC致病因素。

结果

纳入的IBD CRC患者中,共有61%(n = 22/36)为PCCRC。这些病例发生在具有高癌症风险因素的患者中(77.8%;n = 28/36),需要每年进行监测,但57.1%(n = 20/35)的患者监测被不恰当地延迟。大多数PCCRC发生在以下情况:(i)检测到内镜下不可切除的病变(40.9%;n = 9/22);(ii)偏离计划的管理路径(40.9%;n = 9/22),例如因服务、临床医生或患者相关原因导致对检测到的病变处理延迟;或(iii)病变可能被漏诊,因为它们通常位于活动性炎症或炎症后改变区域(36.4%;n = 8/22)。

结论

预防IBD PCCRC需要更积极的策略,以减轻内镜下炎症负担,改善病变的光学特征,遵守推荐的监测间隔,并提高患者对预防性结肠切除术的接受度。然而,相当一部分PCCRC似乎起源于活检时未发现肿瘤但显示侵袭性癌症进展的非腺瘤样黏膜,这凸显了当前监测的局限性。新兴的分子生物标志物可能在未来临床实践中增强癌症风险分层方面发挥作用。

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