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作 者:蔡锋[1] 姚勇[1] 焦永辉[1] 代从新[1] 刘小海[1] 王任直[1]
机构地区:[1]中国医学科学院北京协和医学院北京协和医院神经外科,100730
出 处:《神经疾病与精神卫生》2013年第2期117-120,124,共5页Journal of Neuroscience and Mental Health
基 金:基金项目:国家自然科学基金面上项目(81072084)
摘 要:目的检测miR-134在正常垂体组织和各垂体腺瘤亚型中的表达情况,分析其表达水平与无功能垂体腺瘤(NFPA)增殖侵袭能力的相关性。方法收集垂体腺瘤标本52例(NFPA33例,PRL腺瘤5例,GH腺瘤9例,ACTH腺瘤5例)和尸检正常腺垂体4例及临床相关病例资料,利用免疫组织化学、实时荧光定量PCR(qRT—PCR)等实验技术检测miR-134、MEG3和Ki-67等在各标本中的表达量,并结合病例资料分析数据。结果mIR-134在NFPA中表达水平明显低于其他类型垂体腺瘤和正常腺垂体(P〈0.01);并且miR-134的表达水平与NFPA患者发病年龄、肿瘤细胞Ki-67阳性率及肿瘤侵袭性呈负相关(P〈0.01)。结论miR-134表达下调可能是NFPA肿瘤发生及肿瘤呈侵袭样生长的重要原因之一;miR-134有望成为用于NFPA诊疗的新靶点。Objective To investigate the expression of miR-134 in pituitary normal tissues and all types of pituitary adenomas and to assess the relationship between its expression level and clinically non--functioning pituitary adenoma (NFPA) cells' proliferation and invasiveness. Methods Sporadic pi- tuitary adenoma specimens ( n =52,NFPA 33,PRL 5,GH 9 and ACTH 5) with their clinical data and normal pituitary glands ( n = 4) were collected from autopsy. The expression of miR--134, MEG3 and Ki--67 were quantitatively examined using immunohistochemistry and quantitative real--time reverse transcriptase polymerase chain reaction techniques. The differential expression of miR--134 and MEG3 in pituitary normal and tumor tissues and the association of miR-- 134 expression with NFPA tumor cells' proliferation and invasiveness were evaluated by statistical tests. Results The expression level of miR-- 134 in NFPA was extremely lower than that in pituitary normal tissues and other types of pituitary adenomas (P ~ 0.01). Moreover, the expression level of miR--134 in NFPA was negatively correlated to the age at diagnosis (P = 0. 027), the percentage of Ki--67 in NFPA tissues (P % 0. 001) and tumor invasiveness (P -- 0. 008). Conclusions The down--regulation of miR--134 expression may lead to the tumorigenesis of NFPA and contribute to tumor cells' high proliferation and the phenotype of invasive- ness. Consequently, miR--134 may become a novel biomarker for the diagnosis and a potential therapeu- tic target for the treatment of NFPA in the future.
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