慢性同种移植肾病大鼠肾组织中Smurf 2的表达及作用(1)
 |
| 第1页 |
参见附件(2983KB,3页)。
【摘要】 目的 观察Smad泛素化调节因子2(Smurf 2)在慢性移植肾病(CAN)大鼠肾组织的表达及其与CAN大鼠肾脏功能改变、病理学改变之间的关系,探讨Smurf 2在CAN中的作用。 方法 实验组采用近交系大鼠的同种异基因动物间的左肾原位移植,雄性F344大鼠40只为供体,雄性LEW大鼠40只为受体,移植手术后第10天行右肾切除术,对照组采用单肾切除术的雄性大鼠25只。分别于4、8、12、16周及24周处死大鼠,做肾功能、移植肾组织学检测,并借助免疫印迹、逆转录多聚酶联反应方法检测肾组织中Smurf 2 mRNA、Smurf 2蛋白的表达。结果 移植组大鼠尿蛋白定量、血清肌酐水平于移植后16周时显著增高,24周时更为显著。Smurf 2 mRNA、Smurf 2蛋白在移植后随疾病进展逐渐升高,24周时达高峰。相关分析显示,肾移植大鼠Smurf 2表达水平与24 h尿蛋白定量、血清肌酐水平、肾间质纤维化程度呈正相关(P<0.05,P<0.01)。结论 Smurf 2在CAN发病机制中起作用。
【关键词】 慢性移植肾病;Smurf 2;表达
Expression and role of Smurf 2 on chronic allograft nephropathy
JIA Ning, WANG Han, ZHENG Jing, et al.
Department of Nephrology,The Fifth Affiliated Hospital of Sun YetSen University,Zhuhai 519000,China
【Abstract】 Objective
To investigate expression and role of Smad ubiquitination regulatory factor2(Smurf 2)on the rat kidney of chronic allograft nephropathy(CAN)model. Methods The kidney of Fisher(F344)rats were orthotopically transplanted into Lewis recipients.Animals were harvested respectively at 4,8,12,16,24weeks after transplantation for renal fuction and histologycal examination.The expression of Smurf 2 was determinated with RTPCR and Westernblot.Results The expression of Smurf 2 mRNA and protein was increased on allograft, and the peak of two was at week24 after transplantation. The expression of increasd Smurf 2 were significantly positively correlated with 24hour urine protein extent,serum creatinine levels in CAN rats(P<0.05,P<0.01).Conclusion The increased of Smurf 2 might play a role in the mechanism of CAN.
【Key words】
Chronic allograft nephropathy; Smurf 2;Experssion
基金项目:广东省科技厅科技计划项目基金资助项目(项目编号:2008B030301084)
作者单位:519000珠海,中山大学附属第五医院肾内科(贾宁 郑晶 周文英),神经外科(王汉)
通讯作者:王汉
慢性移植肾病(chronic allograft nephropathy,CAN)是导致移植肾晚期失功的主要原因[1],其发病机制尚不清楚。转化生长因子β1(transforming growth factorβ1, TGFβ1)在CAN的发生过程中起重要作用[1,6,7]。Smad 泛素化调节因子 2(Smad ubiquitin regulatory factor 2,Smurf 2)在调节TGFβ1/Smads信号通路中起关键的作用[4]。本研究旨在观察Smurf 2在慢性移植肾病(CAN)大鼠肾组织的表达及其与CAN大鼠肾脏功能改变、病理学改变之间的关系,探讨Smurf 2在CAN中的作用 ......
您现在查看是摘要介绍页,详见PDF附件(2983KB,3页)。