Abstract
BackgroundThe dysfunction of myc-related zinc finger protein (MAZ) has been proven to contribute to tumorigenesis and development of multiple cancer types. However, the biological roles and clinical significance of MAZ in clear cell renal carcinoma (ccRCC) remain unclear.MethodsMAZ expression was examined in ccRCC and normal kidney tissue by quantitative real-time PCR and Western blot. Statistical analysis was used to evaluate the clinical correlation between MAZ expression and clinicopathological characteristics to determine the relationship between MAZ expression and the survival of ccRCC patients. The biological roles of MAZ in cells were investigated in vitro using MTT and colony assays. Luciferase reporter assays and chromatin immunoprecipitation (ChIP) were used to investigate the relationship between MAZ and its potential downstream signaling molecules.ResultsMAZ expression is elevated in ccRCC tissues, and higher levels of MAZ were correlated with poor survival of patients with ccRCC. MAZ upregulation elevates the proliferation ability of ccRCC cells in vitro, whereas silencing MAZ represses this ability. Our results further reveal that MAZ promotes cell growth, which is dependent on ERK signaling. Importantly, we found that MAZ positively regulates MAP2K2 expression in ccRCC cells. Mechanistically, MAZ binds to the MAP2K2 promoter and increases MAP2K2 transcription. Furthermore, MAP2K2 levels were shown to be increased in ccRCC tissues and to be associated with a poor prognosis of ccRCC patients. MAP2K2 upregulation activates the ERK signaling pathway and promotes ccRCC progression.ConclusionThese results reveal that the MAZ/MAP2K2/ERK signaling axis plays a crucial role in promoting ccRCC progression, which suggests the potential therapeutic utility of MAZ in ccRCC.
Highlights
The dysfunction of myc-related zinc finger protein (MAZ) has been proven to contribute to tumorigen‐ esis and development of multiple cancer types
The results showed that the expression of MAZ significantly increased in clear cell renal carcinoma (ccRCC) tissues than that in normal kidney tissues (Fig. 1B–D)
Using Kaplan–Meier correlation analysis we found that higher MAZ mRNA levels in ccRCC patients predict poorer overall survival in TCGA database (Fig. 1G)
Summary
The dysfunction of myc-related zinc finger protein (MAZ) has been proven to contribute to tumorigen‐ esis and development of multiple cancer types. The biological roles and clinical significance of MAZ in clear cell renal carcinoma (ccRCC) remain unclear. It has been confirmed that many genes are involved in the progress of ccRCC [7, 8], but the underlying molecular mechanism is still unclear. Myc-related zinc finger protein (MAZ) is encoded by a 2.7 kb gene on chromosome 16p11.2 and is a protein composed of 477 amino acids [9]. The MAZ, which is a downstream gene of the oncoprotein Cyr61/CCN1, promotes pancreatic cancer cell migration and invasion via CRAF-ERK signaling [12]. The clinical significance and biological function of MAZ in ccRCC remain unclear
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