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CD10 immunohistochemistry stains enteric mucosa, but negative staining is unreliable in the setting of active enteritis

机译:CD10免疫组化染色可检测肠黏膜,但在活动性肠炎的情况下阴性染色不可靠

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Ileal pouch–anal anastomosis is the definitive therapy for ulcerative colitis that is refractory to medical treatment or that has developed neoplasia. Patients with this procedure are routinely followed using directed endoscopic biopsies to monitor for dysplasia in the rectal cuff, residual/recurrent ulcerative colitis, and nonspecific acute inflammation of the ileal pouch (pouchitis), which have different clinical management and outcomes. Thus, accurate localization of mucosal biopsies is crucial to a definitive histological diagnosis, but is complicated by overlapping clinical presentations of pouchitis and ulcerative colitis, post-surgical and inflammatory changes to the mucosa, and altered endoscopic anatomy, resulting in difficulty determining whether a mucosal biopsy is ileal or rectal in origin for both the endoscopist and the pathologist. We explored the utility of CD10 immunohistochemistry to aid diagnosis in this clinical setting by highlighting the enteric mucosa, based on previous studies showing its utility in brush border staining and in the diagnosis of microvillous inclusion disease. We found uniformly positive CD10 immunostaining in normal enteric mucosa, but variable loss of expression in the setting of active enteritis. Specifically, CD10 staining was lost in up to 10% of the mucosa in 1/12 ileostomies and 4/13 enteric anastomoses, in 10–80% of the mucosa in 9/10 cases of Crohn's ileitis, in 10–60% of the mucosa in 7/16 ileal pouches, and in 20–90% of the mucosa in 6/8 cases of backwash ileitis, usually in the presence of active inflammation. There was no CD10 expression by normal or diseased colonic mucosa. Therefore, while CD10 immunostaining identifies normal enteric mucosa with 100% specificity, negative staining does not definitively exclude small intestinal mucosa in the setting of active enteritis, a common condition in ileal pouch mucosa.
机译:回肠囊袋-肛门吻合术是溃疡性结肠炎的权威疗法,对于溃疡性结肠炎,药物治疗无效或已发展为肿瘤。定期对该患者进行常规的定向内镜活检,以监测直肠套囊的增生,残余/复发性溃疡性结肠炎以及回肠囊的非特异性急性炎症(囊炎),这些患者的临床治疗和结局不同。因此,粘膜活检的准确定位对于确定的组织学诊断至关重要,但由于囊袋炎和溃疡性结肠炎的临床表现重叠,粘膜的手术后和炎性变化以及内窥镜解剖结构的改变,使诊断困难,这使得确定粘膜是否对于内镜医师和病理学家而言,活检起源于回肠或直肠。我们基于以前的研究显示了其在刷缘染色和微绒毛包涵体疾病诊断中的应用,探索了CD10免疫组织化学通过强调肠粘膜来辅助诊断的临床应用。我们在正常肠粘膜中发现了统一阳性的CD10免疫染色,但在活动性肠炎的情况下表达的变化却不尽相同。具体而言,在1/12的回肠切开术和4/13的肠吻合术中,多达10%的粘膜丧失了CD10染色,在9/10的克罗恩氏回肠炎中,粘膜的10–80%丧失了粘膜CD10染色,通常在有活动性炎症的情况下,在7/16回肠囊中有黏膜,在6/8例反冲洗性回肠炎中有20-90%的黏膜。正常或患病的结肠粘膜无CD10表达。因此,尽管CD10免疫染色以100%的特异性鉴定出正常的肠粘膜,但在活动性肠炎(回肠囊粘膜的常见情况)中,阴性染色并不能明确地排除小肠粘膜。

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