1.Expression of LXR-β in human gastric cancer tissue and the effect of GW3965 on the proliferation of gastric cancer cell line SGC-7901.
Ran WANG ; Ruixin LI ; Qiaocheng WEN ; Kun PENG ; Xiangzhou TAN ; Zhikang CHEN
Journal of Central South University(Medical Sciences) 2016;41(2):127-133
		                        		
		                        			OBJECTIVE:
		                        			To examine the expression of liver X receptor-β (LXR-β) in human gastric cancer tissue, and to explore the effect of GW3965, an agonist of LXRs, on proliferation of gastric cancer cell line SGC-7901.
		                        		
		                        			METHODS:
		                        			The immunohistochemical assay was used to detect the expression of LXR-β, activating transcription factor 4 (ATF4) in gastric cancer tissues and the corresponding pericarcinoma tissues in 114 patients. Real-time quantitative PCR and Western blot were used to determine mRNA and protein levels of ATF4 and ATP-binding cassette 1 (ABCA1), one of the downstream target genes of LXRs, in SGC-7901 cells with or without GW3965 treatment. Cell counting kit-8 (CCK-8) assay was performed to detect cell proliferation. The expression of ATF4 was silenced by short hairpin RNA (shRNA).
		                        		
		                        			RESULTS:
		                        			The expressions of LXR-β and ATF-4 were obviously down-regulated in the gastric cancer tissues than that in the corresponding pericarcinoma tissues (both P<0.05). Compared with the control cells, GW3965 treatment inhibited proliferation of SGC-7901 cells and up-regulated ATF4 and ABCA1 expressions (both P<0.05). Knockdown of ATF4 can reverse the antiproliferative effect of GW3965 on SGC-7901 cells.
		                        		
		                        			CONCLUSION
		                        			The expression of LXR-β is decreased in human gastric cancer tissues, and activation of LXRs by GW3965 could inhibit the proliferation of SGC-7901 cells via ATF4.
		                        		
		                        		
		                        		
		                        			Activating Transcription Factor 4
		                        			;
		                        		
		                        			genetics
		                        			;
		                        		
		                        			metabolism
		                        			;
		                        		
		                        			Benzoates
		                        			;
		                        		
		                        			pharmacology
		                        			;
		                        		
		                        			Benzylamines
		                        			;
		                        		
		                        			pharmacology
		                        			;
		                        		
		                        			Cell Line, Tumor
		                        			;
		                        		
		                        			drug effects
		                        			;
		                        		
		                        			Cell Proliferation
		                        			;
		                        		
		                        			Gene Expression Regulation, Neoplastic
		                        			;
		                        		
		                        			Gene Silencing
		                        			;
		                        		
		                        			Humans
		                        			;
		                        		
		                        			Liver X Receptors
		                        			;
		                        		
		                        			Orphan Nuclear Receptors
		                        			;
		                        		
		                        			genetics
		                        			;
		                        		
		                        			metabolism
		                        			;
		                        		
		                        			RNA, Messenger
		                        			;
		                        		
		                        			genetics
		                        			;
		                        		
		                        			metabolism
		                        			;
		                        		
		                        			RNA, Small Interfering
		                        			;
		                        		
		                        			genetics
		                        			;
		                        		
		                        			Stomach Neoplasms
		                        			;
		                        		
		                        			pathology
		                        			;
		                        		
		                        			Up-Regulation
		                        			
		                        		
		                        	
            
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