首页> 外文期刊>Surgical Endoscopy >Comparison of COX-2, Ki-67, and BCL-2 expression in normal esophageal mucosa, Barrett's esophagus, dysplasia, and adenocarcinoma with postablation mucosa and implications for ablative therapies.
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Comparison of COX-2, Ki-67, and BCL-2 expression in normal esophageal mucosa, Barrett's esophagus, dysplasia, and adenocarcinoma with postablation mucosa and implications for ablative therapies.

机译:正常食管粘膜,Barrett食管,异型增生和腺癌伴消融后粘膜的COX-2,Ki-67和BCL-2表达的比较及其对消融治疗的意义。

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BACKGROUND: The neosquamous mucosa that replaces ablated esophageal endothelium after endoscopic mucosal ablation for Barrett's metaplasia or high-grade dysplasia (HGD) may retain buried glandular tissue. This study aimed to assess the neoplastic potential, cellular proliferation, and resistance to apoptosis of this buried glandular tissue by measuring COX-2, Ki-67, and BCL-2 expression in these tissues. METHODS: A prospectively collected database was sourced for esophageal biopsy specimens with normal histologic appearance, Barrett's metaplasia, HGD, adenocarcinoma, and postablation mucosa comprising ablated Barrett's and ablated HGD. Quantitative analysis of cellular markers was achieved immunohistochemically using monoclonal antibodies for the COX-2 enzyme (suggesting increased neoplastic potential), Ki-67 antigen (suggesting cellular proliferation), and BCL-2 oncoprotein (suggesting oncogenic resistance to apoptosis). Grading was performed by independent, blinded observers, and the pre- and postablation cellular disparities were subsequently noted. RESULTS: The buried glandular elements of postablation mucosa demonstrated universally greater COX-2, Ki-67, and BCL-2 expression than normal esophagus. Barrett's esophagus and adenocarcinoma expressed significantly greater COX-2 and Ki-67 at the deep glandular level than postablation mucosa. HGD demonstrated greater Ki-67 expression than the postablation tissue but only within the superficial glands. Overall, the expression of COX-2 correlated significantly with Ki-67 expression in deep glandular tissue. CONCLUSIONS: Ablation of pathologic mucosa in Barrett's esophagus and HGD reduces the expression of some markers of neoplastic behavior. However, the buried glandular tissue of the postablation mucosa still exhibits a higher expression than normal esophageal epithelium. This has potential implications for the follow-up treatment of these patients because it is unclear whether the true risk of neoplastic progression is adequately reduced. A more comprehensive study is required to address this issue.
机译:背景:由于Barrett上皮化生或高度不典型增生(HGD),内镜下黏膜消融后新鳞状黏膜替代了被消融的食管内皮细胞可能保留了腺体的埋藏组织。这项研究旨在通过测量这些组织中的COX-2,Ki-67和BCL-2表达来评估这些埋藏腺组织的瘤变潜力,细胞增殖和对细胞凋亡的抵抗力。方法:前瞻性收集数据库,以获取组织学正常,巴雷特化生,HGD,腺癌以及包括消融的Barrett和消融的HGD的消融后粘膜的食管活检标本。使用针对COX-2酶(建议增加肿瘤形成潜力),Ki-67抗原(建议细胞增殖)和BCL-2癌蛋白(建议对细胞凋亡的致癌性)的单克隆抗体,通过免疫组织化学对细胞标记物进行了定量分析。由独立的,不知情的观察者进行分级,随后记录消融前后的细胞差异。结果:消融后黏膜的腺体的埋藏普遍表现出比正常食管更高的COX-2,Ki-67和BCL-2表达。与消融后的粘膜相比,巴雷特的食道和腺癌在腺体深处表达的COX-2和Ki-67明显更高。 HGD表现出比消融后组织更高的Ki-67表达,但仅在浅腺内。总体而言,在深腺组织中,COX-2的表达与Ki-67的表达显着相关。结论:巴雷特食管和HGD的病理性黏膜消融可减少某些肿瘤行为标志物的表达。但是,消融后黏膜的腺体埋藏组织仍比正常食管上皮具有更高的表达。这对于这些患者的后续治疗具有潜在的意义,因为尚不清楚是否充分降低了肿瘤进展的真正风险。为了解决此问题,需要进行更全面的研究。

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