Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm

Background/Aims The relationship between the serum pepsinogen (sPG) level and changes in gastric mucosa has been well studied. Here, we evaluated the usefulness of sPG (I, II, I/II ratio) and intragastric pH as a biomarker of severe gastric atrophy in gastric neoplastic lesions. Methods A total of 1...

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Main Authors: Jae Hwang Cha, Jin Seok Jang
Format: Article
Language:English
Published: The Korean Association of Internal Medicine 2020-05-01
Series:The Korean Journal of Internal Medicine
Subjects:
Online Access:http://www.kjim.org/upload/pdf/kjim-2018-282.pdf
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spelling doaj-e0425402853a4ee8837f3f97ab57ffb12021-08-10T04:41:12ZengThe Korean Association of Internal MedicineThe Korean Journal of Internal Medicine1226-33032005-66482020-05-0135355055810.3904/kjim.2018.282170138Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasmJae Hwang Cha0Jin Seok Jang1 Department of Internal Medicine, Dong-A University College of Medicine, Busan, Korea Department of Internal Medicine, Dong-A University College of Medicine, Busan, KoreaBackground/Aims The relationship between the serum pepsinogen (sPG) level and changes in gastric mucosa has been well studied. Here, we evaluated the usefulness of sPG (I, II, I/II ratio) and intragastric pH as a biomarker of severe gastric atrophy in gastric neoplastic lesions. Methods A total of 186 consecutive Korean patients with gastric neoplastic lesions underwent endoscopic submucosal dissection (ESD) in this study. The serologic atrophy group had sPG I level ≤ 70 ng/mL and an sPG I/II ratio ≤ 3.0. Before ESD, overnight fasting venous blood and gastric juice samples were collected to measure the sPG level and intragastric pH. The degree of gastric atrophy was estimated by endoscopy, and the rapid urease test was performed to investigate Helicobacter pylori infection. Results Patients who met the criteria of serologic atrophy showed more severe endoscopic atrophic changes (61% vs. 18%, p = 0.000). Older patients and those with more atrophic changes at the gastric upper body demonstrated both a lower sPG I level and a lower PG I/II ratio and more severe endoscopic atrophy. The sPG I/II ratio was the lowest in low grade dysplasia than in high grade dysplasia and early gastric cancer (EGC) (p = 0.015). In addition, patients who tested negative for serologic atrophy and H. pylori showed the lowest intragastric pH (p = 0.000). Conclusions A low sPG I level and a low I/II ratio were correlated with the severity of gastric atrophy in gastric neoplastic lesions, thus indicating it to be a sensitive biomarker of gastric precancerous lesions or EGC.http://www.kjim.org/upload/pdf/kjim-2018-282.pdfpepsinogensstomach neoplasmsgastric mucosaatrophy
collection DOAJ
language English
format Article
sources DOAJ
author Jae Hwang Cha
Jin Seok Jang
spellingShingle Jae Hwang Cha
Jin Seok Jang
Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
The Korean Journal of Internal Medicine
pepsinogens
stomach neoplasms
gastric mucosa
atrophy
author_facet Jae Hwang Cha
Jin Seok Jang
author_sort Jae Hwang Cha
title Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
title_short Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
title_full Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
title_fullStr Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
title_full_unstemmed Clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
title_sort clinical correlation between serum pepsinogen level and gastric atrophy in gastric neoplasm
publisher The Korean Association of Internal Medicine
series The Korean Journal of Internal Medicine
issn 1226-3303
2005-6648
publishDate 2020-05-01
description Background/Aims The relationship between the serum pepsinogen (sPG) level and changes in gastric mucosa has been well studied. Here, we evaluated the usefulness of sPG (I, II, I/II ratio) and intragastric pH as a biomarker of severe gastric atrophy in gastric neoplastic lesions. Methods A total of 186 consecutive Korean patients with gastric neoplastic lesions underwent endoscopic submucosal dissection (ESD) in this study. The serologic atrophy group had sPG I level ≤ 70 ng/mL and an sPG I/II ratio ≤ 3.0. Before ESD, overnight fasting venous blood and gastric juice samples were collected to measure the sPG level and intragastric pH. The degree of gastric atrophy was estimated by endoscopy, and the rapid urease test was performed to investigate Helicobacter pylori infection. Results Patients who met the criteria of serologic atrophy showed more severe endoscopic atrophic changes (61% vs. 18%, p = 0.000). Older patients and those with more atrophic changes at the gastric upper body demonstrated both a lower sPG I level and a lower PG I/II ratio and more severe endoscopic atrophy. The sPG I/II ratio was the lowest in low grade dysplasia than in high grade dysplasia and early gastric cancer (EGC) (p = 0.015). In addition, patients who tested negative for serologic atrophy and H. pylori showed the lowest intragastric pH (p = 0.000). Conclusions A low sPG I level and a low I/II ratio were correlated with the severity of gastric atrophy in gastric neoplastic lesions, thus indicating it to be a sensitive biomarker of gastric precancerous lesions or EGC.
topic pepsinogens
stomach neoplasms
gastric mucosa
atrophy
url http://www.kjim.org/upload/pdf/kjim-2018-282.pdf
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