T Ihamäki scite author profile

Relative risk (RR) and cumulative risk of gastric cancer (GCA) were calculated for different grades of atrophic gastritis (AG) of the antrum and body. Cross-sectional data on the occurrence of AG in a representative population sample (371 subjects), and Finnish Cancer Registry data on GCA were used in the calculations. The RR was increased significantly in severe AG of the antrum and the body (18.1 and 4.6 times, respectively), but not significantly in the less severe grades of AG. As a risk factor, severe antral and body gastritis were independent of each other. The cumulative risk, i.e., the probability of contracting GCA within the following 10 years in age groups 50-54 . . . 70-74 years was calculated to vary from 2.3% to 9.3% and from 8.7% to 31.9% in severe antral AG and from 0.9% to 4.5% and from 3.6% to 16.6% in severe body AG in males and females, respectively.

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Long-Term Course and Consequences ofHelicobacter pylorigastritis Results of a 32-Year Follow-up Study

Valle

Kekki

Sipponen

et al. 1996

Scandinavian Journal of Gastroenterology

243

158

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Serum Pepsinogen I and Serum Gastrin in the Screening of Severe Atrophic Corpus Gastritis

Kekki

Samloff²,

Varis³

et al. 1991

Scandinavian Journal of Gastroenterology

122

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Kekki M, Samloff IM, Varis K, Ihamaki T. Serum pepsinogen I and serum gastrin in thc screening of severe atrophic corpus gastritis. Scand J Gastroentcrol 1991, 26(suppl 186). 109-1 16The possibilities to screen atrophic corpus gastritis with serum pepsinogen 1 (S-PGI) and serum gastrin (S-gastrin) concentrations have been studied in 774 subjects: 71 index subjects selected from a general population at random, 353 of their first-degree relatives, 276 first-degree relatives of patients with gastric cancer, 53 patients with pernicious anaemia, and 21 of their relatives. Discrimination function analysis was calculated from members of random and gastric carcinoma families. S-PGI <30 ng/ml had a high sensitivity for severe diffuse atrophic corpus gastritis (SDAG) alone (89.5%) and SDAG + severe patchy atrophic corpus gastritis (SPAG) (89.1 %). Respective figures for specificity were 91 3 % and 94.8%. The discriminatory power of S-PGI 4 0 ng/ml and S-PGI <25 ng/ml was of the same order. The sensitivity of low S-PGI decreased sharply in detection of slighter forms of atrophic corpus gastritis. The sensitivity of S-gastrin >lo0 pmol/l to discriminate SDAG was 57.9% and SDAG+SPAG 58.7%. Respective figures for specificity were 90.2% and 92.2%. Diffuse and patchy atrophic changes behaved similarly regarding S-PGI and S-gastrin mean concentrations. Accordingly, the biopsy specimen with the severest atrophic changes indicates the degree of atrophy, which associates closely with the changes in S-PGI and S-gastrin. In conclusion, severe atrophic (diffuse or patchy) corpus gastritis may be screened from a general population with high sensitivity and specificity by low S-PGI <30 ng/ml, whereas an increased level of S-gastrin is too insensitive for this.

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Fasting Levels of Serum Gastrin in Different Functional and Morphologic States of the Antrofundal Mucosa: An Analysis of 860 Subjects

Sipponen

Valle

Varis

et al. 1990

Scandinavian Journal of Gastroenterology

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The relationship of fasting serum gastrin (FSG) levels to the histologic state of antral and body mucosa and to the stimulated acid output (PAO) was examined in 860 subjects. The FSG levels correlated with PAO and atrophy of the body mucosa: the FSG increased linearly with an increase in the grade of body atrophy and increased exponentially when the PAO decreased from 'normal' (greater than 10 meq/h) to zero. In subjects with achlorhydria or marked hypochlorhydria (PAO less than 1.1 meq/h) accompanying moderate or severe atrophy in the gastric body mucosa, FSG decreased linearly with increasing grade of atrophy in the antral mucosa. No such relationship between antral atrophy and FSG was found in subjects who had a PAO above 1.1 meq/h or who had non-atrophic gastric body mucosa. We conclude that the state of the antral mucosa influences the FSG level, but only when the function of antral G cells is maximal--that is, in achlorhydric or nearly achlorhydric conditions in which the inhibitory effect of intragastric acidity on the G cells' secretion of gastrin into the circulation is minimal.

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T Ihamäki

Relationships Among Serum Pepsinogen I, Serum Pepsinogen II, and Gastric Mucosal Histology

Gastric cancer risk in chronic atrophic gastritis: Statistical calculations of cross‐sectional data

Long-Term Course and Consequences ofHelicobacter pylorigastritis Results of a 32-Year Follow-up Study

Serum Pepsinogen I and Serum Gastrin in the Screening of Severe Atrophic Corpus Gastritis

Fasting Levels of Serum Gastrin in Different Functional and Morphologic States of the Antrofundal Mucosa: An Analysis of 860 Subjects

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