Clinical and molecular implications of sex differences in surgically treated early-onset gastric cancer.
[BACKGROUND] Gastric cancer predominantly occurs in middle-aged and elderly individuals, whereas cases arising in individuals before the age of 45 years are defined as early-onset gastric cancer (EOGC
APA
Li B, Sun Z, et al. (2025). Clinical and molecular implications of sex differences in surgically treated early-onset gastric cancer.. Gastroenterology report, 13, goaf099. https://doi.org/10.1093/gastro/goaf099
MLA
Li B, et al.. "Clinical and molecular implications of sex differences in surgically treated early-onset gastric cancer.." Gastroenterology report, vol. 13, 2025, pp. goaf099.
PMID
41282549
Abstract
[BACKGROUND] Gastric cancer predominantly occurs in middle-aged and elderly individuals, whereas cases arising in individuals before the age of 45 years are defined as early-onset gastric cancer (EOGC). The biological and clinical characteristics of EOGC remain insufficiently understood. This study aimed to investigate the sex-specific clinicopathological and molecular features of EOGC.
[METHODS] We retrospectively analysed a large cohort of 4,903 gastric cancer patients, including 410 EOGC patients, to compare survival outcomes and clinicopathological features between EOGC patients and late-onset gastric cancer (LOGC) patients and between male and female EOGC patients. Additionally, transcriptome and genome sequencing data from a public Korean EOGC cohort were analysed to identify sex-specific molecular alterations, which were further validated in a Chinese EOGC cohort by using immunohistochemistry.
[RESULTS] Overall survival was significantly shorter in the LOGC group than in the EOGC group. In contrast, EOGC patients were characterized by a greater proportion of females, later T and N stages, more tumours located in the middle third of the stomach, a higher prevalence of diffuse and signet ring cell types, poorer differentiation, smaller tumour size, and lower HER2- and Ki67-positive rates. Among patients with EOGC, females accounted for the majority but had worse outcomes; these female EOGC patients were diagnosed earlier, presented with high proportions of lymph node metastasis and advanced stage, and a higher incidence of differentiated diffuse-type tumours than male EOGC patients. Molecular analyses further revealed female-specific expression upregulation, increased mutation numbers, and distinct immune infiltration patterns, which were validated in a Chinese cohort.
[CONCLUSION] EOGC displays pronounced sex-specific clinicopathological and molecular features. These findings highlight the need for sex-based considerations in understanding EOGC biology and tailoring clinical management strategies.
[METHODS] We retrospectively analysed a large cohort of 4,903 gastric cancer patients, including 410 EOGC patients, to compare survival outcomes and clinicopathological features between EOGC patients and late-onset gastric cancer (LOGC) patients and between male and female EOGC patients. Additionally, transcriptome and genome sequencing data from a public Korean EOGC cohort were analysed to identify sex-specific molecular alterations, which were further validated in a Chinese EOGC cohort by using immunohistochemistry.
[RESULTS] Overall survival was significantly shorter in the LOGC group than in the EOGC group. In contrast, EOGC patients were characterized by a greater proportion of females, later T and N stages, more tumours located in the middle third of the stomach, a higher prevalence of diffuse and signet ring cell types, poorer differentiation, smaller tumour size, and lower HER2- and Ki67-positive rates. Among patients with EOGC, females accounted for the majority but had worse outcomes; these female EOGC patients were diagnosed earlier, presented with high proportions of lymph node metastasis and advanced stage, and a higher incidence of differentiated diffuse-type tumours than male EOGC patients. Molecular analyses further revealed female-specific expression upregulation, increased mutation numbers, and distinct immune infiltration patterns, which were validated in a Chinese cohort.
[CONCLUSION] EOGC displays pronounced sex-specific clinicopathological and molecular features. These findings highlight the need for sex-based considerations in understanding EOGC biology and tailoring clinical management strategies.
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