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胃窦和胃体均检出时,肠化生进展的风险显著增加。

Risk of Progression of Gastric Intestinal Metaplasia Is Significantly Greater When Detected in Both Antrum and Body.

机构信息

Gastroenterology Department, Trinity College Dublin, Tallaght University Hospital, Belgard Avenue, Tallaght, Dublin, D24 NR0A, Ireland.

Histopathology Department, Trinity College Dublin, Tallaght University Hospital, Dublin, Ireland.

出版信息

Dig Dis Sci. 2021 Oct;66(10):3470-3475. doi: 10.1007/s10620-020-06659-8. Epub 2020 Oct 23.

Abstract

BACKGROUND

Gastric cancer (GC) is the fifth leading cause of cancer-related death worldwide. GC is usually preceded by a cascade of well-defined precursor lesions, set in place by an environmental trigger (H. pylori) including intestinal metaplasia (GIM) and dysplasia.

AIMS

To investigate the rates of progression of GIM to dysplasia and GC in a region of low gastric cancer incidence.

METHODS

We identified all patients diagnosed with GIM between January 1, 2008, and June 30, 2012. Any repeat upper endoscopy more than 1 year after index diagnosis and before December 31, 2018, was considered follow-up. Carcinomas the bulk of which were macroscopically located below the OGJ were considered primary gastric cancer.

RESULTS

Progression to more advanced lesions was observed in six patients (0.6%). Four patients (three male) developed GC at median age 74 years (SD 6). Two patients progressed to dysplasia (one male) at median age 71 years (SD 4). Patients with GIM in both gastric antrum and body were significantly more likely to progress than those with GIM in only one location (3.1% vs. 0.4%) (p value 0.017). Fifty-eight patients who had H. pylori eradicated were followed up. No progression to dysplasia or GC was noted in this group, with 28 patients having persistent GIM at follow-up.

CONCLUSION

Patients with GIM in both antrum and body had a significantly increased risk of progression and warrant close attention. This is comparable to routinely followed premalignant conditions such as Barrett's esophagus and Colonic Polyps, and appropriate surveillance protocols should be followed in this group.

摘要

背景

胃癌(GC)是全球第五大致癌相关死亡原因。GC 通常由一系列明确的前驱病变引起,这些病变由环境触发因素(H. pylori)引起,包括肠上皮化生(GIM)和异型增生。

目的

在胃癌发病率较低的地区,研究 GIM 向异型增生和 GC 进展的发生率。

方法

我们确定了 2008 年 1 月 1 日至 2012 年 6 月 30 日期间诊断为 GIM 的所有患者。任何在索引诊断后 1 年以上且在 2018 年 12 月 31 日之前进行的重复上内窥镜检查均被视为随访。大体上位于 OGJ 以下的大部分为癌的肿瘤被认为是原发性胃癌。

结果

六名患者(0.6%)观察到进展为更高级别的病变。四名患者(三名男性)在 74 岁(标准差 6 岁)时发展为 GC。两名患者在 71 岁(标准差 4 岁)时进展为异型增生(一名男性)。GIM 同时发生在胃窦和体部的患者比仅在一个部位发生 GIM 的患者更有可能进展(3.1%比 0.4%)(p 值 0.017)。58 名接受 H. pylori 根除的患者接受了随访。在该组中未观察到异型增生或 GC 进展,28 名患者在随访时仍存在持续性 GIM。

结论

GIM 同时发生在胃窦和体部的患者进展的风险显著增加,需要密切关注。这与 Barrett 食管和结肠息肉等常规随访的癌前病变相当,应在该组中遵循适当的监测方案。

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