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Dysplasia is more common in the distal than proximal colon in ulcerative colitis surveillance

机译:在溃疡性结肠炎监测中,异型增生在远端远比近端结肠更为常见

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Background: In patients with long-standing ulcerative colitis (UC), current dysplasia surveillance guidelines recommend four-quadrant biopsies every 10 cm throughout the colon. However, this may be inefficient if neoplastic lesions are localized in particular segments of the colorectum. The aim was to determine whether a difference exists in the anatomic distribution of dysplasia discovered in UC patients undergoing colonoscopic surveillance. Methods: From an institutional database of over 700 patients with UC who underwent two or more surveillance colonoscopies between 1994-2006, we identified all patients with flat (endoscopically invisible) low-grade dysplasia (fLGD) or advanced neoplasia (colorectal cancer [CRC] or high-grade dysplasia [HGD]). Pathology reports were reviewed regarding the anatomic location of all dysplastic lesions. Fisher's exact test was used to compare the frequencies of neoplasia among the different colonic segments. Results: We identified 103 patients who progressed to any neoplasia (fLGD, HGD, or CRC). These patients underwent a total of 396 colonoscopies. The mean age at first surveillance colonoscopy was 48.6 years, with a mean UC disease duration of 18.2 years; 100% had extensive disease. Fifty-five patients developed advanced neoplasia. The rectosigmoid was found to have a significantly greater number of biopsies positive for advanced neoplasia and for any neoplasia compared to all other colonic segments (P < 0.0007); 71.2% of all advanced neoplasia was in the rectosigmoid. Conclusions: The majority of dysplastic lesions identified in a surveillance program was detected in the rectosigmoid. Endoscopists should consider taking a greater percentage of biopsies in these segments as opposed to more proximal areas.
机译:背景:对于患有长期溃疡性结肠炎(UC)的患者,当前的发育异常监测指南建议在整个结肠中每10厘米进行四象限活检。但是,如果肿瘤性病变位于结肠直肠的特定部分,则效率可能较低。目的是确定在接受结肠镜检查的UC患者中发现的发育异常的解剖分布是否存在差异。方法:从1994年至2006年间接受两次或两次以上结肠镜检查的700余例UC患者的机构数据库中,我们确定了所有患有扁平(内窥镜下看不见)低度不典型增生(fLGD)或晚期肿瘤(结直肠癌[CRC])的患者或高度不典型增生[HGD])。回顾了有关所有发育不良病变的解剖位置的病理报告。 Fisher精确检验用于比较不同结肠段之间的瘤形成频率。结果:我们鉴定出103名进展为任何赘生物(fLGD,HGD或CRC)的患者。这些患者总共接受了396例结肠镜检查。初次监测结肠镜检查的平均年龄为48.6岁,平均UC病程为18.2年。 100%有广泛疾病。五十五名患者发展为晚期肿瘤。与所有其他结肠节段相比,发现直肠乙状结肠活检对于晚期赘生物和任何赘生物呈阳性的数量要多得多(P <0.0007)。所有晚期肿瘤的71.2%位于直肠乙状结肠。结论:在监视程序中发现的大多数增生性病变在直肠乙状结肠中被检测到。内镜医师应考虑在这些部位进行更大比例的活检,而不是近端区域。

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