Clinical, Endoscopic and Histologic Differences in Gastric Mucosa Between Younger and Older Adults: An Observational Study on the Aging Stomach
Abstract
1. Introduction
2. Materials and Methods
2.1. Study Design
2.2. Patients
- Prospective clinical and demographic database registry including age, gender, clinical indication for upper endoscopy and ongoing therapies with a special focus on antiplatelet, anticoagulant and PPIs. PPI therapy was defined as ongoing when drugs were suspended less than 7 days before endoscopy.
- Upper endoscopy, under deep sedation, was performed according to several quality indicators, including the use of virtual chromoendoscopy, preprocedural simethicone and fundus retroflexion [29].
- Endoscopic diagnoses were coded and collected in a predefined, standardized and searchable fashion. Antithrombotic therapy was managed according to international guidelines [30].
- Two biopsy specimens were systematically obtained from the antrum, another two from the body and were compared for histological features. When endoscopic lesions (e.g., polyps, ulcer) were evident, apart from the respective lesion biopsies, random biopsies from the opposite wall of the antrum/body were collected for analysis.
- Refusal to participate in the study.
- Pregnancy.
- Previously known gastric pathology (e.g., autoimmune gastritis, GC).
- Recent H. pylori eradication (within 12 months).
- Previous gastric surgery.
- Crohn’s disease.
- Chemoradiation and/or immunomodulatory therapy.
- Technical impossibility to obtain gastric biopsies.
2.3. Gastric Biopsy Analysis
2.4. Statystical Analysis
3. Results
3.1. Baseline Clinical Characteristics
3.2. Gastric Endoscopic Lesions
3.3. Gastric Histology
4. Discussion
5. Conclusions
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
Abbreviations
CCI | Charlson comorbidity index |
CAG | Chronic atrophic gastritis |
GC | Gastric cancer |
H. pylori | Helicobacter pylori |
IM | Intestinal metaplasia |
PPI | Proton pump inhibitor |
References
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Variables | 18–45 Years (n = 50) | ≥70 Years (n = 50) | p Value | |
---|---|---|---|---|
Age (SD) | 33.6 ± 8.1 years | 76.2 ± 4.1 years | ||
Gender | Male | 23 (46%) | 22 (44%) | 0.421 |
Female | 27 (54%) | 28 (56%) | ||
Charlson Comorbidity index | 0.2 ± 0.4 | 4.8 ± 1.6 | <0.001 | |
Ambulatory therapy | NSAID | 1 (2%) | 8 (16%) | <0.001 |
Antiplatelets | 3 (6%) | 16 (32%) | <0.001 | |
Anticoagulants | 2 (4%) | 8 (16%) | 0.023 | |
Proton pump inhibitors | 9 (18%) | 21 (42%) | <0.001 | |
Laboratory evaluation | Hemoglobin (SD) | 13.6 ± 1.3 | 12.9 ± 1.7 | 0.044 |
Iron (SD) | 82.3 ± 40.0 | 73.1 ± 32.6 | 0.377 | |
Folic acid (SD) | 5.4 ± 4.3 | 5.1 ± 4.8 | 0.234 | |
Vitamin B12 (SD) | 601 ± 87.6 | 549 ± 69.5 | 0.565 | |
Clinical indication for upper endoscopy | Dyspepsia | 23 (46%) | 17 (34%) | 0.079 |
Gastroesophageal reflux disease | 5 (10%) | 10 (20%) | 0.019 | |
Peptic ulcer disease | 10 (20%) | 9 (18%) | 0.401 | |
Dysphagia | 4 (8%) | 3 (6%) | 0.349 | |
Radiological findings | 3 (6%) | 2 (4%) | 0.325 | |
Gastric polyp | 2 (4%) | 4 (8.0%) | 0.202 | |
Diarrhea | 2 (4%) | 3 (6%) | 0.325 | |
Iron deficiency anemia | 1 (2%) | 2 (4%) | 0.281 |
Endoscopic Finding | 18–45 Years (n = 50) | ≥70 Years (n = 50) | p Value | |
---|---|---|---|---|
Normal mucosa | 25 (50%) | 10 (20%) | <0.001 | |
Erythema | 17 (34%) | 15 (30%) | 0.336 | |
Erosions | 5 (10%) | 8 (16%) | 0.189 | |
Peptic ulcer disease | Gastric ulcer | 1 (2%) | 4 (6%) | 0.004 |
Duodenal ulcer | 0 (0%) | 6 (12%) | ||
Gastric polyps | 2 (4%) | 7 (14%) | 0.041 |
Histologic Finding | 18–45 Years (n = 50) | ≥70 Years (n = 50) | p Value | |
---|---|---|---|---|
Normal mucosa | 22 (44%) | 2 (4%) | <0.001 | |
Reactive gastritis | 7 (14%) | 5 (10%) | 0.271 | |
Reactive gastritis H.pylori + | 3 (6%) | 0 (0%) | 0.0910 | |
Chronic gastritis | 19 (38%) | 28 (56%) | 0.004 | |
Chronic gastritis H.pylori + | 11 (22%) | 10 (20%) | 0.0681 | |
Intestinal metaplasia | OLGIM I | 2 (4%) | 2 (4%) | <0.001 |
OLGIM II | 0 (0%) | 3 (6%) | ||
OLGIM III | 0 (0%) | 5 (10%) | ||
OLGIM IV | 0 (0%) | 4 (8%) | ||
Intestinal metaplasia H.pylori + | 1 (2%) | 2 (4%) | 0.113 | |
Chronic atrophic gastritis | OLGA I | 2 (4%) | 3 (6%) | <0.001 |
OLGA II | 0 (0%) | 3 (6%) | ||
OLGA III | 0 (0%) | 4 (8%) | ||
OLGA IV | 0 (0%) | 4 (8%) | ||
Chronic atrophic gastritis H.pylori + | 1 (2%) | 2 (4%) | 0.113 | |
PPI-related gastric changes | 2 (4%) | 15 (30%) | <0.001 | |
H.pylori + | 0 (0%) | 0 (0%) |
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Vara-Luiz, F.; Mendes, I.; Palma, C.; Mascarenhas, P.; Teles, A.E.; Santos, I.C.; Nunes, G.; Patita, M.; Mocanu, I.; Pires, S.; et al. Clinical, Endoscopic and Histologic Differences in Gastric Mucosa Between Younger and Older Adults: An Observational Study on the Aging Stomach. Med. Sci. 2025, 13, 224. https://doi.org/10.3390/medsci13040224
Vara-Luiz F, Mendes I, Palma C, Mascarenhas P, Teles AE, Santos IC, Nunes G, Patita M, Mocanu I, Pires S, et al. Clinical, Endoscopic and Histologic Differences in Gastric Mucosa Between Younger and Older Adults: An Observational Study on the Aging Stomach. Medical Sciences. 2025; 13(4):224. https://doi.org/10.3390/medsci13040224
Chicago/Turabian StyleVara-Luiz, Francisco, Ivo Mendes, Carolina Palma, Paulo Mascarenhas, Ana Elisa Teles, Inês Costa Santos, Gonçalo Nunes, Marta Patita, Irina Mocanu, Sara Pires, and et al. 2025. "Clinical, Endoscopic and Histologic Differences in Gastric Mucosa Between Younger and Older Adults: An Observational Study on the Aging Stomach" Medical Sciences 13, no. 4: 224. https://doi.org/10.3390/medsci13040224
APA StyleVara-Luiz, F., Mendes, I., Palma, C., Mascarenhas, P., Teles, A. E., Santos, I. C., Nunes, G., Patita, M., Mocanu, I., Pires, S., Meira, T., Vieira, A., Pinto-Marques, P., Gomes-Pinto, D., & Fonseca, J. (2025). Clinical, Endoscopic and Histologic Differences in Gastric Mucosa Between Younger and Older Adults: An Observational Study on the Aging Stomach. Medical Sciences, 13(4), 224. https://doi.org/10.3390/medsci13040224