Zoning of mucosal phenotype, dysplasia, and telomerase activity measured by telomerase repeat assay protocol in Barrett's esophagus.

Neoplasia (New York, N.Y.) Pub Date : 2004-01-01
James J Going, Aileen J Fletcher-Monaghan, Lisa Neilson, Bea A Wisman, Ate van der Zee, Robert C Stuart, W Nicol Keith
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Abstract

Glandular dysplasia in Barrett's esophagus may regress spontaneously but can also progress to cancer. The human telomerase RNA template and the human telomerase reverse transcriptase enzyme which do not, of themselves, correlate strongly with telomerase activity, are too often overexpressed in Barrett's dysplasia to predict individual cancer risk. This study relates telomerase activity, mucosal phenotype, and dysplasia in Barrett's esophagus. Biopsies (n = 256) from squamous esophagus, columnar-lined esophagus every 2 cm, esophago-gastric junction, gastric body, and antrum from 32 patients with long-segment Barrett's esophagus were evaluated by telomerase repeat assay protocol (TRAP). Three biopsies for histology (n = 794) were simultaneously taken at each anatomical level. These and all prior and subsequent biopsies (n = 1917) were reviewed for mucosal phenotypes and dysplasia severity. Intestinal-type Barrett's mucosa was present at all levels in Barrett's esophagus. At least one Barrett's biopsy was TRAP(+) in 22 of 32 patients. TRAP positivity of intestinal-type Barrett's mucosa increased distally, possibly as a consequence of mucosal exposure to acid or bile reflux. Native gastric mucosa was rarely TRAP(+) (1/31 corpus, 2/32 antrum), whereas native squamous mucosa usually was TRAP(+) (31/32). Dysplasia almost always involved intestinal-type Barrett's mucosa (85/87; P <.00001), without evidence of proximal-distal zoning. TRAP could be positive without dysplasia and negative in extensive, even high-grade, dysplasia. TRAP activity merits evaluation as a candidate biomarker for increased risk of persistent dysplasia and cancer progression in Barrett's esophagus.

用端粒酶重复测定法测定Barrett食管粘膜表型、发育不良和端粒酶活性的分区。
巴雷特食管腺体发育不良可自行消退,但也可发展为癌症。人类端粒酶RNA模板和人类端粒酶逆转录酶本身与端粒酶活性没有很强的相关性,它们在巴雷特发育不良中经常过度表达,无法预测个体的癌症风险。本研究将端粒酶活性、粘膜表型和Barrett食管发育不良联系起来。采用端粒酶重复测定法(TRAP)对32例长段Barrett食管患者的鳞状食管、每2cm有柱状排列的食管、食管-胃交界、胃体和胃窦进行活检(n = 256)。在每个解剖水平同时进行3次组织学活检(n = 794)。这些以及所有先前和随后的活检(n = 1917)被回顾了粘膜表型和发育不良的严重程度。Barrett食管各级均有肠型Barrett粘膜。32例患者中有22例至少一次Barrett活检为TRAP(+)。肠型巴雷特粘膜TRAP阳性远端升高,可能是由于粘膜暴露于酸或胆汁反流所致。天然胃粘膜很少呈TRAP(+)(1/31体,2/32胃窦),而天然鳞状黏膜通常呈TRAP(+)(31/32)。发育不良几乎总是累及肠型巴雷特粘膜(85/87;P
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