| Literature DB >> 27315569 |
Mitsuro Kanda1, Dai Shimizu1, Tsutomu Fujii1, Haruyoshi Tanaka1, Masahiro Shibata1, Naoki Iwata1, Masamichi Hayashi1, Daisuke Kobayashi1, Chie Tanaka1, Suguru Yamada1, Goro Nakayama1, Hiroyuki Sugimoto1, Masahiko Koike1, Michitaka Fujiwara1, Yasuhiro Kodera1.
Abstract
Identification of novel gastric cancer (GC)-related molecules is necessary to improve management of patients with GC in both diagnostic and therapeutic aspects. The aim of the present study was to determine whether protein arginine methyltransferase 5 (PRMT5) acts as an oncogene in the progression of GC and whether it serves as a novel diagnostic marker and therapeutic target. We conducted global expression profiling of GC cell lines and RNA interference experiments to evaluate the effect of PRMT5 expression on the phenotype of GC cells. We analysed tissues of 179 patients with GC to assess the association of PRMT5 mRNA levels with clinicopathological factors. Differential expression of PRMT5 mRNA by GC cell lines correlated positively with the levels of GEMIN2, STAT3 and TGFB3. PRMT5 knockdown reduced the proliferation, invasion and migration of a GC cell line. PRMT5 mRNA levels were significantly higher in GC tissues than the corresponding adjacent normal tissues and were independent of tumour depth, differentiation and lymph node metastasis. High PRMT5 expression was an independent risk factor of positive peritoneal lavage cytology (odds ratio 3.90, P=0.003) and decreased survival. PRMT5 enhances the malignant phenotype of GC cell lines and its expression in gastric tissues may serve as a biomarker for patient stratification and a potential target of therapy.Entities:
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Year: 2016 PMID: 27315569 DOI: 10.3892/ijo.2016.3584
Source DB: PubMed Journal: Int J Oncol ISSN: 1019-6439 Impact factor: 5.650