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大肠髓样型低分化腺癌:一种以微卫星不稳定和生存期改善为特征的独特临床病理实体。

Medullary-type poorly differentiated adenocarcinoma of the large bowel: a distinct clinicopathologic entity characterized by microsatellite instability and improved survival.

作者信息

Lanza G, Gafà R, Matteuzzi M, Santini A

机构信息

Department of Experimental and Diagnostic Medicine, Section of Anatomic Pathology, University of Ferrara, and Division of Clinical Oncology, St Anna Hospital, Ferrara, Italy.

出版信息

J Clin Oncol. 1999 Aug;17(8):2429-38. doi: 10.1200/JCO.1999.17.8.2429.

DOI:10.1200/JCO.1999.17.8.2429
PMID:10561306
Abstract

PURPOSE

Recent studies suggest the existence of a distinct class of poorly differentiated large bowel adenocarcinomas, usually termed medullary-type adenocarcinomas (MTAs). The aim of the present study was to accurately define the clinical, histopathologic, biologic, and genetic features of this tumor type.

MATERIALS AND METHODS

Among 1,265 surgically resected sporadic colorectal carcinomas, 45 MTAs were identified on the basis of the following criteria: predominantly solid growth pattern (at least 70% of the tumor area) and lack of marked nuclear pleomorphism. The clinicopathologic, biologic, and genetic characteristics of MTAs were compared with those of a series of 457 common glandular colorectal adenocarcinomas.

RESULTS

The significantly different clinicopathologic features of MTAs were proximal location, large size, invasion into adjacent organs, expanding pattern of growth, low incidence of distant metastases, more frequent conspicuous peritumoral lymphocytic infiltration, and Crohn's-like lymphoid reaction. Furthermore, young patients with MTAs often demonstrated a family history highly suggestive of a hereditary background. Unlike glandular adenocarcinomas, the large majority of MTAs were DNA diploid by flow cytometric analysis (21 of 25, 84%) and p53 negative by immunohistochemistry (36 of 41, 87.8%). In addition, 18 of the 20 MTAs examined by DNA microsatellite analysis demonstrated widespread microsatellite instability (90% of cases). Patients with MTAs showed a better clinical outcome with respect to patients with common poorly differentiated adenocarcinomas (PDAs) (P <.0001) and well- or moderately differentiated adenocarcinomas (WMDAs) (P =.133). In particular, none of the 33 patients with completely resectable stage II and III MTAs developed tumor recurrence during the observation period. Conversely, 24.7% of patients with stage II and III WMDAs and 48.9% of patients with stage II and III PDAs, who had undergone curative surgical resection, died of recurrent disease (P =.01 and P <.0001, respectively).

CONCLUSION

All these data strongly indicate that MTAs represent a distinct pathologic entity, with specific histologic appearance and peculiar clinical and genetic features. These tumors need to be classified separately from other poorly differentiated colorectal carcinomas.

摘要

目的

近期研究提示存在一类独特的低分化大肠腺癌,通常称为髓样型腺癌(MTA)。本研究的目的是准确界定该肿瘤类型的临床、组织病理学、生物学及遗传学特征。

材料与方法

在1265例手术切除的散发性结直肠癌中,根据以下标准确定了45例MTA:主要为实性生长模式(至少占肿瘤面积的70%)且无明显核异型性。将MTA的临床病理、生物学及遗传学特征与457例常见的腺性结直肠腺癌进行比较。

结果

MTA显著不同的临床病理特征为位置靠近近端、体积大、侵犯相邻器官、呈膨胀性生长方式、远处转移发生率低、瘤周淋巴细胞浸润更常见且明显以及克罗恩样淋巴反应。此外,患有MTA的年轻患者常显示出高度提示遗传背景的家族史。与腺性腺癌不同,通过流式细胞术分析,绝大多数MTA为DNA二倍体(25例中的21例,84%),通过免疫组织化学检测p53为阴性(41例中的36例,87.8%)。此外,在通过DNA微卫星分析检测的20例MTA中,有18例显示广泛的微卫星不稳定性(90%的病例)。与常见的低分化腺癌(PDA)患者(P <.0001)和高分化或中分化腺癌(WMDA)患者(P =.133)相比,MTA患者显示出更好的临床结局。特别是,33例II期和III期可完全切除的MTA患者在观察期内均未发生肿瘤复发。相反,接受根治性手术切除的II期和III期WMDA患者中有24.7%以及II期和III期PDA患者中有48.9%死于复发性疾病(分别为P =.01和P <.0001)。

结论

所有这些数据强烈表明MTA代表一种独特的病理实体,具有特定的组织学表现以及独特的临床和遗传学特征。这些肿瘤需要与其他低分化结直肠癌分开分类。

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