米非司酮通过调节岩藻糖基转移酶IV的表达抑制胚胎体外黏附  被引量:2

Mifepristone Inhibits the Adhesion of Embryos in vitro by Decreasing the Expression of Fucosyltransferase IV

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作  者:尉晓蔚[1] 刘帅[2] 刘佳[2] 燕秋[2] 

机构地区:[1]大连大学附属中山医院,大连116001 [2]大连医科大学,大连116044

出  处:《生殖与避孕》2014年第1期1-5,26,共6页Reproduction and Contraception

摘  要:目的:探讨米非司酮对人胚胎细胞JAR与人子宫内膜细胞RL95-2之间黏附的影响及其调控的分子机制。方法:采用黏附实验分别观察RU486以及岩藻糖基转移酶IV(FUT4)对JAR细胞与RL95-2细胞之间黏附的影响。采用RT-PCR以及Western blotting检测米非司酮对RL95-2细胞以及流产妇女子宫内膜中FUT4表达的调控。结果:①米非司酮抑制JAR细胞与RL95-2单层细胞之间的黏附;②米非司酮抑制RL95-2细胞以及流产妇女子宫内膜中FUT4基因和蛋白的表达;③FUT4质粒转染RL95-2细胞后,调节JAR细胞与RL95-2单层细胞之间的黏附。结论:米非司酮通过调节FUT4的表达抑制胚胎体外黏附。Objective: To investigate the effect of mifepristone on the adhesion of JAR cells to RL95-2 cells monolayer and its regulation mechanism. Methods: The adhesion of JAR cells to RL95-2 cells monolayer which was treated with mifepristone or fucosyltransferase IV (FUT4) plasmid was detected by cell counting. The regulation of mifepristone via FUT4 in RL95-2 cells and in human endometfial tissues was examined by RT-PCR and Western blotting. Results: 1) Mifepristone inhibited the adhesion of JAR cells to RL95-2 cells monolayer. 2) Mifepristone inhibited the expression of FUT4 in RL95-2 cells and in human endometrial tissues by RT-PCR and Western blotting. 3) The adhesion of JAR cells to RL95-2 cell monolayer was inhibited by FUT4-siRNA. Inversely, the percent of adhesion was promoted by FUT4 over-expression plasmid. Conclusion: Mifepristone inhibits the adhesion of embryos in vitro by decreasing the expression of FUT4.

关 键 词:米非司酮 岩藻糖基转移酶IV(FUT4) 子宫内膜 黏附 

分 类 号:R714.8[医药卫生—妇产科学]

 

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