Identifying individualized prognostic signature and unraveling the molecular mechanism of recurrence in early-onset colorectal cancer

Identifying individualized prognostic signature and unraveling the molecular mechanism of recurrence in early-onset colorectal cancer

Background The incidence and mortality of early-onset colorectal cancer (EOCRC; < 50 years old) is increasing worldwide, with a high recurrence rate. The inherent heterogeneity of EOCRC makes its treatment challenging. Hence, to further understand the biology and reveal the molecular mechanisms o...

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Veröffentlicht in:European journal of medical research 2023-11, Vol.28 (1), p.1-533, Article 533
Hauptverfasser: Yang, Jia, Zhao, Yuting, Yuan, Rongqiang, Wang, Yongtong, Wang, Shiyi, Chang, Zhiqiang, Zhao, Wenyuan
Format: Artikel
Sprache:eng
Schlagworte:
Age
Analysis
Annexins
Biomarkers
Cancer
Chemotherapy
Colorectal cancer
Development and progression
Early-onset colorectal cancer
Gene expression
Genes
Health aspects
Immune microenvironment
Leukocytes
Mann-Whitney U test
Medical prognosis
Mortality
Mutation
Oncology, Experimental
Patients
Prognostic signature
Proteins
Recurrence-associated genes
Relative expression ordering
Survival analysis
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Zusammenfassung:Background The incidence and mortality of early-onset colorectal cancer (EOCRC; < 50 years old) is increasing worldwide, with a high recurrence rate. The inherent heterogeneity of EOCRC makes its treatment challenging. Hence, to further understand the biology and reveal the molecular mechanisms of EOCRC, a recurrence risk signature is needed to guide clinical management. Methods Based on the relative expression orderings (REOs) of genes in each sample, a prognostic signature was developed and validated utilizing multiple independent datasets. The underlying molecular mechanisms between distinct prognostic groups were explored via integrative analysis of multi-omics data. Results The prognostic signature consisting of 6 gene pairs (6-GPS) could predict the recurrence risk for EOCRC at the individual level. High-risk EOCRC classified by 6-GPS showed a poor prognosis but a good response to adjuvant chemotherapy. Moreover, high-risk EOCRC was characterized by epithelial-mesenchymal transition (EMT) and enriched angiogenesis, and had higher mutation burden, immune cell infiltration, and PD-1/PD-L1 expression. Furthermore, we identified four genes associated with relapse-free survival in EOCRC, including SERPINE1, PECAM1, CDH1, and ANXA1. They were consistently differentially expressed at the transcriptome and proteome levels between high-risk and low-risk EOCRCs. They were also involved in regulating cancer progression and immune microenvironment in EOCRC. Notably, the expression of SERPINE1 and ANXA1 positively correlated with M2-like macrophage infiltration. Conclusion Our results indicate that 6-GPS can robustly predict the recurrence risk of EOCRC, and that SERPINE1, PECAM1, CDH1, and ANXA1 may serve as potential therapeutic targets. This study provides valuable information for the precision treatment of EOCRC. Keywords: Early-onset colorectal cancer, Prognostic signature, Relative expression ordering, Recurrence-associated genes, Immune microenvironment
ISSN:2047-783X
0949-2321
2047-783X
DOI:10.1186/s40001-023-01491-y