Abstract
DEAD-box RNA helicase DDX21 (also named nucleolar RNA helicase 2) is a nuclear autoantigen with undefined roles in cancer. To explore possible roles of autoimmune recognition in cancer immunity, we examined DDX21 protein expression in colorectal cancer tissue and its association with patient clinical outcomes. Unbiased deep proteomic profiling of two independent colorectal cancer cohorts using mass spectrometry showed that DDX21 protein was significantly upregulated in cancer relative to benign mucosa. We then examined DDX21 protein expression in a validation group of 710 patients, 619 of whom with early stage and 91 with late stage colorectal cancers. DDX21 was detected mostly in the tumor cell nuclei, with high expression in some mitotic cells. High levels of DDX21 protein were found in 28% of stage I, 21% of stage II, 30% of stage III, and 32% of stage IV colorectal cancer cases. DDX21 expression levels correlated with non-mucinous histology in early stage cancers but not with other clinicopathological features such as patient gender, age, tumor location, tumor grade, or mismatch repair status in any cancer stage. Kaplan–Meier analyses revealed that high DDX21 protein levels was associated with longer survival in patients with early stage colorectal cancer, especially longer disease-free survival in patients with microsatellite instability (MSI) cancers, but no such correlations were found for the microsatellite stable subtype or late stage colorectal cancer. Univariate and multivariate analyses also identified high DDX21 protein expression as an independent favorable prognostic marker for early stage MSI colorectal cancer.
Highlights
Abbreviations CRC Colorectal cancer DDX21 DEAD-box RNA helicase 21 DFS Disease-free survival IHC Immunohistochemistry MMR Mismatch repair microsatellite stability (MSS) Microsatellite stability microsatellite instability (MSI) Microsatellite instability OS Overall survival
Using deep unbiased tissue proteomics by Fourier transform mass spectrometry[7,8,9,10], we found that proteomic profiling robustly separates colorectal cancer from benign mucosa (Fig. 1a,b)
We found high DDX21 protein expression in about 20–30% of colorectal cancer cases, regardless of cancer stage (Tables 1, 2)
Summary
Abbreviations CRC Colorectal cancer DDX21 DEAD-box RNA helicase 21 DFS Disease-free survival IHC Immunohistochemistry MMR Mismatch repair MSS Microsatellite stability MSI Microsatellite instability OS Overall survival. Target cellular proteins in particular pathways, not genes, there is a need for protein-based molecular biomarkers with an underlying functional pathophysiologic rationale. Such functional protein markers have the potential to offer more precise prognostic and predictive value, which would enable better risk stratification of early stage cancer after surgical removal and better selection of patients for adjuvant chemotherapy or immunotherapy, while avoiding overtreatment or immune-related adverse events[5,6]. We validated DDX21 protein expression in a large cohort of patients in order to evaluate the clinical prognostic significance of DDX21 in colorectal cancer, especially its potential as a prognostic marker for early stage cancer
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