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炎症性肠病相关结直肠癌及相关黏膜病变的形态学、免疫组化和分子特征——单机构经验

Morphological, immunohistochemical and molecular features of inflammatory bowel disease associated colorectal carcinoma and associated mucosal lesions - Single institution experience.

作者信息

Kamarádová Kateřina, Vošmiková Hana, Rozkošová Kateřina, Ryška Aleš, Tachecí Ilja, Laco Jan

机构信息

The Fingerland Department of Pathology, Charles University Faculty of Medicine and University Hospital Hradec Králové, Sokolská 581, Hradec Králové, 500 03, Czech Republic.

2nd Department of Internal Medicine-Gastroenterology, Charles University Faculty of Medicine and University Hospital Hradec Králové, Sokolská 581, Hradec Králové, 500 03, Czech Republic.

出版信息

Pathol Res Pract. 2019 Apr;215(4):730-737. doi: 10.1016/j.prp.2019.01.010. Epub 2019 Jan 11.

DOI:10.1016/j.prp.2019.01.010
PMID:30679085
Abstract

BACKGROUND

Patients with inflammatory bowel disease (IBD) - ulcerative colitis (UC) and Crohn's disease (CD) have an elevated risk of developing colorectal carcinoma (CRC). Major risk factor in IBD patients is the continuous chronic inflammation leading to development of dysplasia and carcinoma. Nevertheless, other types of non-conventional but suspicious mucosal changes serrated change/dysplasia, NOS and villous hypermucinous change, have also been reported in IBD patients. Preneoplastic potential of these lesions is still not well elucidated.

AIMS

The aim of this study was identification of IBD-associated CRCs focusing on finding related precursor lesions in the surgical specimen or in archival biopsy samples followed by a detailed morphological, immunohistochemical and molecular evaluation. For the purpose of the study the mucosal lesions were divided into conventional IBD-associated dysplasia and non-conventional lesions that were merged under a provisory term of putative preneoplastic lesions (PPL).

METHODS

A total of 309 consecutive IBD colectomy specimens diagnosed during a 10-year period were reviewed. Detailed morphological evaluation, immunohistochemical analysis of mismatch repair (MMR) proteins, p53 and O-methylguanine DNA methyltransferase (MGMT) expression and molecular analysis for KRAS, NRAS and BRAF gene mutation were performed in the retrieved CRC cases as well as in the detected dysplasia and PPLs of these patients.

RESULTS

We identified 11 cases of morphologically heterogenous IBD-associated CRCs, occurring in 5 males and 6 females, aged 26-79 years (mean 44 years). A total of 22 mucosal lesions were revealed in 8 CRC patients comprising conventional IBD-associated dysplasia (4 lesions), PPLs as serrated change/dysplasia NOS (11 lesions), villous hypermucinous change (5 lesions), and two true serrated lesions (one sessile serrated adenoma and one traditional serrated adenoma). More than one type of lesion was found in 6 patients. Seven CRC cases harbored mutation of KRAS/NRAS and one case of BRAF. Two patients with KRAS-mutated CRC showed the same mutation in PPL in the same specimen (one serrated change NOS and one TSA with high-grade dysplasia). Similarly, one BRAF-mutated carcinoma case presented the same mutation in serrated change/dysplasia, NOS in the same specimen. Of the CRCs, two showed deficient MMR system profile, six presented with loss of MGMT expression, and six showed aberrant p53 expression. PPLs showed deficient MGMT expression (14 cases) and aberrant p53 (10 cases) as well.

CONCLUSION

IBD-associated CRCs are very heterogeneous entities. Besides conventional IBD-related dysplasia, other types of mucosal lesions may be associated with long lasting IBD and CRC e.g. villous hypermucinous change and serrated change/dysplasia, NOS. Since these lesions share certain genetic or immunohistochemical changes with the related CRC, a suspicion is raised that these lesions may also have preneoplastic potential. Awareness of these changes is necessary to prevent their missing and under-reporting, and further studies of these lesions should be carried out.

摘要

背景

炎症性肠病(IBD)患者,即溃疡性结肠炎(UC)和克罗恩病(CD)患者,患结直肠癌(CRC)的风险升高。IBD患者的主要风险因素是持续的慢性炎症,导致发育异常和癌变。然而,在IBD患者中也报告了其他类型的非传统但可疑的黏膜变化,即锯齿状变化/发育异常,未另行分类(NOS)和绒毛状高黏液变化。这些病变的癌前潜能仍未得到充分阐明。

目的

本研究的目的是识别与IBD相关的结直肠癌,重点是在手术标本或存档活检样本中找到相关的前驱病变,然后进行详细的形态学、免疫组织化学和分子评估。为了本研究的目的,黏膜病变被分为传统的与IBD相关的发育异常和非传统病变,后者在一个暂定的癌前病变(PPL)术语下合并。

方法

回顾了10年间诊断的309例连续的IBD结肠切除术标本。对检索到的结直肠癌病例以及这些患者检测到的发育异常和PPL进行了详细的形态学评估、错配修复(MMR)蛋白、p53和O-甲基鸟嘌呤DNA甲基转移酶(MGMT)表达的免疫组织化学分析以及KRAS、NRAS和BRAF基因突变的分子分析。

结果

我们识别出11例形态学上异质性的与IBD相关的结直肠癌,发生在5名男性和6名女性中,年龄在26 - 79岁(平均44岁)。8例结直肠癌患者共发现22处黏膜病变,包括传统的与IBD相关的发育异常(4处病变)、作为锯齿状变化/发育异常NOS的PPL(11处病变)、绒毛状高黏液变化(5处病变)以及两处真正的锯齿状病变(1处无蒂锯齿状腺瘤和1处传统锯齿状腺瘤)。6例患者发现不止一种类型的病变。7例结直肠癌病例存在KRAS/NRAS突变,1例存在BRAF突变。2例KRAS突变的结直肠癌患者在同一标本的PPL中显示相同的突变(1处锯齿状变化NOS和1处高级别发育异常的传统锯齿状腺瘤)。同样,1例BRAF突变的癌病例在同一标本的锯齿状变化/发育异常NOS中呈现相同的突变。在结直肠癌中,2例显示错配修复系统缺陷,6例呈现MGMT表达缺失,6例显示p53表达异常。PPL也显示MGMT表达缺失(14例)和p53异常(10例)。

结论

与IBD相关的结直肠癌是非常异质性的实体。除了传统的与IBD相关的发育异常外,其他类型的黏膜病变可能与长期的IBD和结直肠癌相关,例如绒毛状高黏液变化和锯齿状变化/发育异常NOS。由于这些病变与相关的结直肠癌有某些基因或免疫组织化学变化,有人怀疑这些病变也可能具有癌前潜能。认识到这些变化对于防止其漏诊和报告不足是必要的,并且应该对这些病变进行进一步研究。

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