Accuracy of screening for gastric cancer using serum pepsinogen concentrations

Kitahara, Fumiaki; Kobayashi, Kenichi; Satô, Tadashi; Kojima, Yuichiro; Araki, Tsutomu; Fujino, Masayuki

doi:10.1136/gut.44.5.693

Cited by 206 publications

(218 citation statements)

References 10 publications

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“…Therefore, the two tests gave positive results to largely distinctive subgroups in a population, and detected gastric cancers in different subgroups. Consequently, the sensitivity of serum pepsinogens may be decreased if the test is repeated in the same population, as suggested by the finding of Kitahara et al [45]. In contrast, the sensitivity of photofluorography would not change substantially even when the test is repeated, as they had already been conducted repeatedly in the study populations.…”

Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 89%

“…Studies of serum pepsinogens have so far focused on establishing an optimal cut-off point and quantifying the sensitivity and specificity. Table 7 summarizes studies examining the accuracy of serum pepsinogen measurement in a general population setting [43][44][45]. Table 8 presents the results of two studies comparing the accuracy of photofluorography and serum pepsinogens in a single population [46,47].…”

Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 99%

“…Therefore, a test that is highly sensitive for the initial prevalent screening may be less so for the subsequent incident screenings. Kitahara et al [45] report the accuracy of serum pepsinogens separately in "cross-sectional" and "prospective" evaluations, in which the former basically represents prevalent screening and the latter, incident screening. The observed sensitivity was high in the "cross-sectional" examination (84.6% or 10/13), but was substantially reduced in the "prospective" evaluation (40.0% or 4/10).…”

Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 99%

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Screening for gastric cancer in Japan

2000

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In Japan, mass screening for gastric cancer with photofluorography was initiated in 1960. At present, over 6 million people are screened annually. The sensitivity and specificity of photofluorography are 70%-90% and 80%-90%, respectively. The 5-year survival rate is 15%-30% better in screendetected cancers than in symptom-diagnosed cases. Although no randomized controlled trials have been reported, cohort and case-control studies generally showed a decreased risk of mortality from gastric cancer in the screened subjects. The summary odds ratio (95% confidence interval) of three casecontrol studies for ever screened versus never screened subjects was 0.39 (0.29-0.52) for men and 0.50 (0.34-0.72) for women. Substantial evidence indicates that the Japanese screening program with photofluorography is effective in reducing the mortality from gastric cancer. The measurement of serum pepsinogens has recently drawn attention as an alternative to photofluorography, given its lower cost and simplicity. Some studies have suggested a comparable accuracy for the two methods. However, these investigations may have overestimated the relative sensitivity of serum pepsinogen testing compared with photofluorography, because serum pepsinogen testing was conducted as prevalent screening, while photofluorography was done as incident screening. Furthermore, no studies have directly examined whether the screening with serum pepsinogens reduced gastric cancer mortality. Therefore, at present, evidence is insufficient to determine the benefit of this program.

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Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 89%

Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 99%

Section: Serum Pepsinogen Measurements As a Screening Testmentioning

confidence: 99%

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Screening for gastric cancer in Japan

2000

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“…thus, a full understanding of the molecular mechanism of carcinogenesis and identification of biomarkers for the early diagnosis and effective treatment of human GC are crucial. Although several serum biomarkers have been researched as new invasive tools for screening GC (6)(7)(8)(9), these serum tests are not available as screening or surveillance tests due to their low specificity and sensitivity (9). Biomarkers derived from tumor tissues may provide higher sensitivity and specificity than those from serum (10), yet tissue specimens must be obtained by invasive means involving endoscopy and biopsy.…”

Section: Introductionmentioning

confidence: 99%

Tissue metabolomic fingerprinting reveals metabolic disorders associated with human gastric cancer morbidity

Wang²,

Liu³

et al. 2011

Oncol Rep

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Abstract. the principal way to improve the outcome of gastric cancer (GC) is to predict carcinogenesis and metastasis at an early stage. the aims of the present study were to test the hypothesis that distinct metabolic profiles are reflected in GC tissues and to further explore potential biomarkers for GC diagnosis. Gas chromatography/mass spectrometry (GC/Ms) was utilized to analyze tissue metabolites from 30 GC patients. A diagnostic model for GC was constructed using orthogonal partial least squares discriminant analysis (OpLs-DA), and the metabolomic data were analyzed using the non-parametric Wilcoxon rank sum test to identify the metabolic tissue biomarkers for GC. Over 100 signals were routinely detected in one single total ion current (tIC) chromatogram, and the OPLS-DA model generated from the metabolic profile of the tissues adequately discriminated the GC tissues from the normal mucosae. Among the low-molecular-weight endogenous metabolites, a total of 41 compounds, such as amino acids, organic acids, carbohydrates, fatty acids and steroids, were detected, and 15 differential metabolites were identified with significant difference (p<0.05). A total of 20 variables were noted which contributed to a great extent in the discriminating OpLs-DA model (VIp value >1.0), among which 12 metabolites were identified using both VIP values (VIP >1) and the Wilcoxon test (p<0.05). In conclusion, the identification of the metabolites associated with GC morbidity potentially revealed perturbations of glycolysis, fatty acid β-oxidation, cholesterol and amino acid metabolism. these results suggest that tissue metabolic profiles have great potential in detecting GC and may aid in understanding its underlying mechanisms.

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“…When measurement of serum Pepsinogen concentrations are used as a screening test for gastric cancer, they achieve a sensitivity of > 80% and specificity of > 70%. 65 Anti-parietal cell antibody is well known as an autoantibody in pernicious anaemia. Anti-parietal cell antibody is also an auto-antibody in H. pylori associated gastritis.…”

Section: Screening For H Pylorimentioning

confidence: 99%

Test and treat or test and scope for Helicobacter pylori infection. Any change in gastric cancer prevention?

Loughlin

Sebastian

O'Connor

et al. 2003

Aliment Pharmacol Ther

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SUMMARYA 'test and treat' strategy is advocated for patients with dyspepsia under the age of 45 years, with endoscopy reserved for those with alarm symptoms or aged over 45 years. One of the consequences of this strategy will be a reduction in population infection rates of Helicobacter pylori. It is now clear that H. pylori is one of the prime initiators of gastric cancer with up to 70% of gastric cancers attributable to H. pylori. What remains unclear is if H. pylori reduction will lead to a reduction in gastric cancer.

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Accuracy of screening for gastric cancer using serum pepsinogen concentrations

Cited by 206 publications

References 10 publications

Screening for gastric cancer in Japan

Screening for gastric cancer in Japan

Tissue metabolomic fingerprinting reveals metabolic disorders associated with human gastric cancer morbidity

Test and treat or test and scope for Helicobacter pylori infection. Any change in gastric cancer prevention?

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