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p27KIP1和SKp2蛋白异常表达与人胶质瘤临床病理学关系的研究
引用本文:王艳芬,周洁,王磊,刘爽,龚岘. p27KIP1和SKp2蛋白异常表达与人胶质瘤临床病理学关系的研究[J]. 中国肿瘤临床与康复, 2008, 15(6)
作者姓名:王艳芬  周洁  王磊  刘爽  龚岘
作者单位:江苏省扬州市第一人民医院病理科
摘    要:目的探讨脑胶质瘤组织中p27~(KIP1)蛋白和S期激酶相关蛋白2(skp2)异常表达与临床病理因素的关系。方法应用免疫组化SP法检测45例胶质瘤和10例正常脑组织中p27~(KIP1)和Skp2蛋白表达情况。结果p27~(KIP1)和Skp2蛋白在正常脑组织和胶质瘤组织中的阳性表达率差异有显著性(P=0.033、P=0.005);p27~(KIP1)和Skp2蛋白表达水平与胶质瘤组织学分级相关(P<0.01),但与患者的性别、年龄及肿瘤大小无明显关系(P>0.05);Skp2阳性表达组和阴性表达组之间p27~(KIP1)蛋白阳性率差异有显著性(x~2=4.8458,P=0.028);胶质瘤组织中p27~(KIP1)蛋白和Skp2蛋白的表达呈负相关(r=-0.5477,P<0.05)。结论Skp2蛋白在胶质瘤组织中表达上调,加速了对p27~(KIP1)泛素化依赖的蛋白降解,使p27~(KIP1)蛋白表达降低,失去对细胞周期的调控并促进细胞异常增殖,从而参与了胶质瘤的发生和发展。

关 键 词:胶质瘤  p27~(KIP1)  S期激酶相关蛋白2  肿瘤抑制基因

Relationship between the abnormal expression of p27KIP1 and SKp2 proteins and clinicopathology of human glioma
WANG Yan-fen ZHOU Jie WANG Lei,et al. Relationship between the abnormal expression of p27KIP1 and SKp2 proteins and clinicopathology of human glioma[J]. Chinese Journal of Clinical Oncology and Rehabilitation, 2008, 15(6)
Authors:WANG Yan-fen ZHOU Jie WANG Lei  et al
Abstract:Objective To investigate the relationship between the abnormal expressions of p27~(KIP1) and SKp2 proteins in human glioma tissues and elinicopathology.Methods The expression of p27~(KIP1) and SKp2 proteins were examined by SP immunohistochemieal staining in 45 human glioma specimens and in 10 normal human brain tissue specimens.Results There was statistically significant difference in the positive rate of p27~(KIP1) and SKp2 proteins between glioma specimens and normal human brain tissues (P<0.05). The expression of p27~(KIP1) and SKp2 proteins was closely related with pathological grade of glioma tissues(P<0.01),but their expression in gliomas had no obvious relation to the sex,ages and sizes of tumor(P>0.05).There was statistically significant difference in the positive rate of p27~(KIP1) protein between the positive expression group and the negative expression group of Skp2 protein(X~2=4.8458,P=0.028).There was a negative correlation between expression of p27~(KIP1) and SKp2 proteins in glioma tissues (r=-0.5477,P<0.05).Conclusions Expression of Skp2 protein is up-regulated significantly in gliomas,and overexpres- sion of Skp2 reduces the protein level of p27~(KIP1) through ubiquitin-depondent protein degradation and causes disruption of cell cycle control and enhancement of the proliferative activity,indicating that Skp2 and p27~(KIP1) play important roles in oncogenesis and development of glioma.
Keywords:Glioma  p27~(KIP1)  S phase kinase protein 2(Skp2)  Tumor-suppressing gene
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