Identification of DNA methylation-driven genes and construction of a nomogram to predict overall survival in pancreatic cancer

G C Deng; D C Sun; Q Zhou; Y Lv; H Yan; Q L Han; G H Dai

doi:10.1186/s12864-021-08097-w

Identification of DNA methylation-driven genes and construction of a nomogram to predict overall survival in pancreatic cancer

BMC Genomics. 2021 Nov 3;22(1):791. doi: 10.1186/s12864-021-08097-w.

Authors

G C Deng^{1

2}, D C Sun¹, Q Zhou¹, Y Lv¹, H Yan¹, Q L Han³, G H Dai^{4

5}

Affiliations

¹ Senior Department of Oncology, The Fifth Medical Center of Chinese People's Liberation Army (PLA)General Hospital, Beijing, China.
² School of Medicine, Nankai University, Tianjin, China.
³ Senior Department of Oncology, The Fifth Medical Center of Chinese People's Liberation Army (PLA)General Hospital, Beijing, China. [email protected].
⁴ Senior Department of Oncology, The Fifth Medical Center of Chinese People's Liberation Army (PLA)General Hospital, Beijing, China. [email protected].
⁵ School of Medicine, Nankai University, Tianjin, China. [email protected].

Abstract

Background: The incidence and mortality of pancreatic cancer (PC) has gradually increased. The aim of this study was to identify survival-related DNA methylation (DNAm)-driven genes and establish a nomogram to predict outcomes in patients with PC.

Methods: The gene expression, DNA methylation database, and PC clinical samples were downloaded from TCGA. DNAm-driven genes were identified by integrating analyses of gene expression and DNA methylation data. Survival-related DNAm-driven genes were screened via univariate, least absolute shrinkage and selection operator (LASSO), and multivariate Cox regression analyses to develop a risk score model for prognosis. Based on analyses of clinical parameters and risk score, a nomogram was built and validated. The independent cohort from GEO database were used for external validation.

Results: A total of 16 differentially expressed methylation-driven genes were identified. Based on LASSO Cox regression and multivariate Cox regression analysis, six genes (FERMT1, LIPH, LAMA3, PPP1R14D, NQO1, VSIG2) were chosen to develop the risk score model. In the Kaplan-Meier analysis, age, T stage, N stage, AJCC stage, radiation therapy history, tumor size, surgery type performed, pathological type, chemotherapy history, and risk score were potential prognostic factors in PC (P < 0.1). In the multivariate analysis, stage, chemotherapy, and risk score were significantly correlated to overall survival (P < 0.05). The nomogram was constructed with the three variables (stage, chemotherapy, and risk score) for predicting the 1-year, 2-year, and 3-year survival rates of PC patients. Nomogram performance was assessed by receiver operating characteristic (ROC) curves and calibration curves. 1-year, 2-year and 3-year AUC of nomogram model was 0.899, 0.765 and 0.776, respectively.

Conclusions: In our study, we successfully identified the six DNAm-driven genes (FERMT1, LIPH, LAMA3, PPP1R14D, NQO1, VSIG2) with a relationship to the outcomes of PC patients. The nomogram including stage, chemotherapy, and risk score could be used to predict survival in PC patients.

Keywords: DNA methylation; Nomogram; Pancreatic cancer; Prognosis; Risk score.

MeSH terms

DNA Methylation
Humans
Membrane Proteins
Neoplasm Proteins
Neoplasm Staging
Nomograms*
Pancreatic Neoplasms* / genetics
Prognosis

Substances

FERMT1 protein, human
Membrane Proteins
Neoplasm Proteins