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通过血清胃蛋白酶原检测确定的癌症高危人群:无症状中年男性10年随访结果

Cancer high-risk subjects identified by serum pepsinogen tests: outcomes after 10-year follow-up in asymptomatic middle-aged males.

作者信息

Yanaoka Kimihiko, Oka Masashi, Mukoubayashi Chizu, Yoshimura Noriko, Enomoto Shotaro, Iguchi Mikitaka, Magari Hirohito, Utsunomiya Hirotoshi, Tamai Hideyuki, Arii Kenji, Ohata Hiroshi, Fujishiro Mitsuhiro, Takeshita Tatsuya, Mohara Osamu, Ichinose Masao

机构信息

Department of Gastroenterology, School of Medicine, Wakayama Medical University, Wakayama, Japan.

出版信息

Cancer Epidemiol Biomarkers Prev. 2008 Apr;17(4):838-45. doi: 10.1158/1055-9965.EPI-07-2762.

Abstract

BACKGROUND

Gastric cancer screening using the pepsinogen filter test is receiving wide recognition in Japan owing to convenience, freedom from discomfort or risk, efficiency, and economy. Because the long-term outcomes of cancer development in extensive atrophic gastritis detected by pepsinogen test are unclear, test-positive and test-negative subjects were investigated in a longitudinal cohort study.

METHODS

Subjects comprised 5,209 middle-aged men with measured serum pepsinogen levels who were followed for 10 years. Cancer development based on "atrophy-positive" and "atrophy-negative" criteria used for cancer screening was investigated.

RESULTS

During the study, 63 cases of cancer developed in the cohort, representing an incidence rate of 125 per 100,000 person-years. Pepsinogen test screening using the most widely used atrophy-positive criterion (pepsinogen I, < or =70 ng/mL; pepsinogen I/II ratio, < or =3.0) displayed 58.7% sensitivity, 73.4% specificity, and 2.6% positive predictive value. Cancer incidence rate was 276 per 100,000 person-years for the atrophy-positive group and 70 per 100,000 person-years for the atrophy-negative group. Incidence rate was higher in groups fulfilling stricter positive criteria detecting more extensive atrophy, reaching 424 per 100,000 person-years. In addition, 9.2% of atrophy-negative subjects with pepsinogen I of >70 ng/mL and pepsinogen I/II ratio of < or =3.0 (reflecting putative inflammation-based high pepsinogen II level) are at high risk for cancer, particularly diffuse-type cancer, with a cancer incidence rate comparable with atrophy-positive subjects (216 per 100,000 person-years).

CONCLUSION

Atrophy-positive subjects by pepsinogen filter test, particularly those fulfilling stricter criteria, and atrophy-negative subjects with low pepsinogen I/II ratio reflecting putative extensive active inflammation constitute populations at high risk for gastric cancer, requiring thorough endoscopic examination.

摘要

背景

由于方便、无不适或风险、高效及经济,使用胃蛋白酶原筛选试验进行胃癌筛查在日本正得到广泛认可。由于胃蛋白酶原试验检测出的广泛萎缩性胃炎患者癌症发生的长期结果尚不清楚,因此在一项纵向队列研究中对试验阳性和试验阴性的受试者进行了调查。

方法

研究对象包括5209名测量了血清胃蛋白酶原水平的中年男性,随访10年。基于用于癌症筛查的“萎缩阳性”和“萎缩阴性”标准调查癌症发生情况。

结果

在研究期间,队列中发生了63例癌症,发病率为每10万人年125例。使用最广泛应用的萎缩阳性标准(胃蛋白酶原I,≤70 ng/mL;胃蛋白酶原I/II比值,≤3.0)进行胃蛋白酶原试验筛查,显示敏感性为58.7%,特异性为73.4%,阳性预测值为2.6%。萎缩阳性组的癌症发病率为每10万人年276例,萎缩阴性组为每10万人年70例。满足更严格阳性标准(检测到更广泛萎缩)的组发病率更高,达到每10万人年424例。此外,胃蛋白酶原I>70 ng/mL且胃蛋白酶原I/II比值≤3.0(反映基于假定炎症的高胃蛋白酶原II水平)的萎缩阴性受试者中有9.2%患癌风险高,尤其是弥漫型癌症,其癌症发病率与萎缩阳性受试者相当(每10万人年216例)。

结论

胃蛋白酶原筛选试验的萎缩阳性受试者,尤其是那些满足更严格标准的受试者,以及胃蛋白酶原I/II比值低、反映假定广泛活动性炎症的萎缩阴性受试者,构成胃癌高危人群,需要进行全面的内镜检查。

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