胃粘膜萎缩血清学标记物在胃癌前病变筛查和癌症预防中的有效性。

IF 1.4 Q4 GASTROENTEROLOGY & HEPATOLOGY World Journal of Gastrointestinal Endoscopy Pub Date : 2024-08-16 DOI:10.4253/wjge.v16.i8.462
Sergey M Kotelevets, Sergey A Chekh, Sergey Z Chukov
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引用次数: 0

摘要

背景:需要新的标记物来提高萎缩性胃炎血清学筛查的有效性:目的:开发一种成本效益高、灵敏度高的萎缩性胃炎血清学筛查方法:采用可视内镜木村-泷本法筛选出的169名萎缩性胃炎患者中,有165人采用更新的木村-泷本法显示出组织学上的黏膜萎缩。所有169名患者均使用GastroPanel®(Biohit Plc,芬兰赫尔辛基)检测了餐后胃泌素-17(G17)和胃蛋白酶原-1(PG1)的水平:我们根据木村-竹本分类系统,采用五例胃黏膜活检组织学标准来评估 G17 在检测胃黏膜萎缩方面的敏感性。我们还比较了检测到的胃黏膜萎缩组织学程度与作为萎缩性胃炎标志物的 G17 和 PG1 血清学水平之间的形态功能关系。对于单灶重度萎缩性胃炎的检测,餐后G17血清学水平(范围:0-4 pmol/L)的灵敏度为62.2%,G17血清学水平(范围:0-10 pmol/L)的灵敏度为100%。根据木村-竹本(Kimura-Takemoto)分类法确定胃黏膜萎缩的严重程度时,PG1的水平与组织学萎缩程度之间没有发现很强的相关性。在所介绍的一名 63 岁多灶性萎缩性胃炎患者的临床病例中,经过五个月的凝乳酶替代疗法后,萎缩的血清学标志物--餐后 G17 的长期动态变化明显呈阳性:结论:通过评估餐后 G17 对多灶性萎缩性胃炎进行血清学筛查是一种成本效益高、灵敏度高的方法。根据悉尼体系,餐后 G17 是比胃活检的形态学检查更早的萎缩性胃炎消退标志物。因此,建议将餐后 G17 用于萎缩性胃炎治疗后的动态监测。
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Effectiveness of serological markers of gastric mucosal atrophy in the gastric precancer screening and in cancer prevention.

Background: New markers are needed to improve the effectiveness of serological screening for atrophic gastritis.

Aim: To develop a cost-effective method for serological screening of atrophic gastritis with a high level of sensitivity.

Methods: Of the 169 patients with atrophic gastritis, selected by the visual endoscopic Kimura-Takemoto method, 165 showed histological mucosal atrophy using the updated Kimura-Takemoto method. All 169 patients were examined for postprandial levels of gastrin-17 (G17) and pepsinogen-1 (PG1) using GastroPanel® (Biohit Plc, Helsinki, Finland).

Results: We used the histological standard of five biopsies of the gastric mucosa, in accordance with the Kimura-Takemoto classification system to assess the sensitivity of G17 in detecting gastric mucosal atrophy. We also compared the morpho-functional relationships between the detected histological degree of gastric mucosal atrophy and the serological levels of G17 and PG1, as the markers of atrophic gastritis. The sensitivity of postprandial G17 was 62.2% for serological levels of G17 (range: 0-4 pmol/L) and 100% for serological G17 (range: 0-10 pmol/L) for the detection of monofocal severe atrophic gastritis. No strong correlation was found between the levels of PG1 and degree of histological atrophy determined by the Kimura-Takemoto classification system to identify the severity of mucosal atrophy of the gastric corpus. In the presented clinical case of a 63-year-old man with multifocal atrophic gastritis, there is a pronounced positive long-term dynamics of the serological marker of atrophy - postprandial G17, after five months of rennet replacement therapy.

Conclusion: Serological screening of multifocal atrophic gastritis by assessment of postprandial G17 is a cost-effective method with high sensitivity. Postprandial G17 is an earlier marker of regression of atrophic gastritis than a morphological examination of a gastric biopsy in accordance with the Sydney system. Therefore, postprandial G17 is recommended for dynamic monitoring of atrophic gastritis after treatment.

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来源期刊
World Journal of Gastrointestinal Endoscopy
World Journal of Gastrointestinal Endoscopy GASTROENTEROLOGY & HEPATOLOGY-
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1164
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