Abstract

In a quest for prognostic biomarkers in early-stage colorectal cancer, we investigated NNMT (nicotinamide N-methyltransferase) in large cohorts of patients. Immunohistochemical examination of 679 patients illustrates that NNMT protein is predominantly expressed in the cancer stroma at varying levels, and about 20% of cancer tissues overexpress NNMT when compared to levels observed in normal colorectal mucosa. Clinical correlation analyses of 572 patients with early-stage cancers reveal that NNMT protein overexpression is significantly associated with shorter overall and disease-free survival, but no such correlation is found in late-stage colorectal cancer. Analyses of TCGA and CPTAC colorectal cancer cohorts show that NNMT mRNA expression is positively correlated with protein levels, is significantly higher in CIMP-high or MSI subtypes than in CIMP-low or MSS subtypes, and is positively correlated with its paralog INMT but not with its interaction partners such as PNMT, ADK, APP, ATF6, BMF, BRD4, CDC37, or CRYZ. In early-stage cancers, NNMT expression is higher in BRAF-mutated than in BRAF wild type tumors but is not affected by KRAS or PIK3CA mutation status. As a cancer stromal protein with important roles in metabolism and cancer epigenetics, NNMT is emerging as a promising biomarker for risk stratification of early-stage cancers.

Highlights

  • IntroductionIn the United States, the lifetime risk of developing colorectal cancer is about 1 in 23 for men and 1 in 25 for women according to the American Cancer Society

  • Colorectal cancer is among the most common cancers in both men and ­women[1]

  • We found that NNMT protein is weakly expressed in normal stromal cells of the lamina propria of benign colonic mucosa and can be significantly overexpressed in colorectal cancer tumor stromal cells but not in cancer cells (Figs. 1 and 2)

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Summary

Introduction

In the United States, the lifetime risk of developing colorectal cancer is about 1 in 23 for men and 1 in 25 for women according to the American Cancer Society. The death rate from colorectal cancer has been dropping in recent years, partially due to increased screening efforts and early d­ etection[2]. NNMT impairs the methylation balance of cancer cells by consuming methyl units, changes protein and gene methylation landscapes, and may result in hypomethylated histone and alteration of the epigenetic state of cancer c­ ells[6]. NNMT overexpression has been reported to decrease drug sensitivity and enhance chemoresistance in breast cancer, esophageal squamous cell carcinoma, and cell lines of colorectal cancer and m­ elanoma[26–29]. We sought to investigate whether NNMT is a prognostic marker in early-stage colorectal cancer

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