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溃疡性结肠炎患者盆腔回肠贮袋/肛管癌的危险因素

Risk factors for carcinoma of the pelvic ileal pouch/anal canal in ulcerative colitis.

作者信息

Elkowitz David, Daum Fredric, Markowitz James, Proccaccino John, Boas Eleonore, Cuomo Joanne, Kahn Ellen

机构信息

Department of Pathology, North Shore University Hospital, New York University School of Medicine, Manhasset, New York 11030, USA.

出版信息

Ann Clin Lab Sci. 2004 Spring;34(2):143-9.

Abstract

Patients with ulcerative colitis who undergo proctocolectomy and an ileal anal anastomosis (IPAA) require surveillance; dysplasia and carcinoma occur in both the small intestinal mucosa of the ileal pouch and the retained rectal mucosa as early as 2 yr after ileostomy closure. This study evaluated risk factors for carcinoma (eg, dysplasia, p53 overexpression, labeling index, and aneuploidy) in the small intestinal and rectal mucosa. Thirty patients (age 14-64 yr) with ulcerative colitis and IPAA were studied. The mean duration of ulcerative colitis prior to IPAA was 3 yr (range 6 mo-21 yr). Patients were followed by annual endoscopy and biopsies of the ileal pouch and rectal mucosa. Sections of small intestine and rectal mucosa were evaluated for inflammation and dysplasia, and by immunohistochemical stains Ki-67 (MIB-1) for a labeling index and for p53. Ploidy determination was performed by flow cytometry. Active inflammation of the small intestinal mucosa and the rectal mucosa was frequent and the labeling index of both the pouch and rectal mucosa was abnormal. Two patients had changes indefinite for dysplasia, one involving the small bowel mucosa of the pouch and the other the retained rectal mucosa. Fifteen of the 30 patients had overexpression of p53, 9 from the pouch, and 6 from the rectal mucosa. Overexpression of p53 was seen in both of the patients with indefinite dysplasia. Aneuploidy was noted in 3 patients: two from the pouch and one from the rectal mucosa. All aneuploidic specimens were p53-positive, but negative for dysplasia. In conclusion, most biopsies of the ileal pouch and rectal mucosa were inflamed. The labeling indexes of the small bowel and rectal mucosa were higher than normal. The risk factors for carcinoma (dysplasia, overexpression of p53, and aneuploidy) occurred in the small intestinal and the rectal mucosa. Overexpression of p53 was noted in 16 patients, dysplasia only in 2. Therefore, p53 overexpression and aneuploidy should be considered in the evaluation of surveillance biopsies of patients with ulcerative colitis with IPAA, whereas dysplasia is an insensitive marker.

摘要

接受全结肠直肠切除及回肠肛管吻合术(IPAA)的溃疡性结肠炎患者需要进行监测;早在回肠造口关闭后2年,发育异常和癌就会出现在回肠袋的小肠黏膜和保留的直肠黏膜中。本研究评估了小肠和直肠黏膜中癌的危险因素(如发育异常、p53过表达、标记指数和非整倍体)。对30例(年龄14 - 64岁)溃疡性结肠炎并接受IPAA的患者进行了研究。IPAA术前溃疡性结肠炎的平均病程为3年(范围6个月 - 21年)。通过每年对回肠袋和直肠黏膜进行内镜检查及活检对患者进行随访。对小肠和直肠黏膜切片进行炎症和发育异常评估,并通过免疫组化染色检测Ki - 67(MIB - 1)以获得标记指数和检测p53。通过流式细胞术进行倍性测定。小肠黏膜和直肠黏膜的活动性炎症很常见,回肠袋和直肠黏膜的标记指数均异常。2例患者有发育异常不明确的改变,1例累及回肠袋的小肠黏膜,另1例累及保留的直肠黏膜。30例患者中有15例p53过表达,9例来自回肠袋,6例来自直肠黏膜。2例发育异常不明确的患者均有p5过表达。3例患者出现非整倍体:2例来自回肠袋,1例来自直肠黏膜。所有非整倍体标本p53均为阳性,但发育异常为阴性。总之,大多数回肠袋和直肠黏膜活检显示有炎症。小肠和直肠黏膜的标记指数高于正常。癌的危险因素(发育异常、p53过表达和非整倍体)出现在小肠和直肠黏膜中。16例患者出现p53过表达,仅2例有发育异常。因此,在评估溃疡性结肠炎并接受IPAA患者的监测活检时,应考虑p53过表达和非整倍体,而发育异常是一个不敏感的标志物。

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