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Rac1 gene mutations in human brain tumours.

机译:人脑肿瘤中的Rac1基因突变。

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AIMS: Rac1 is a member of the Ras superfamily of small GTPase and plays a fundamental role in cytoskeleton reorganization, regulation of gene expression and cell proliferation, and cellular transformation. Though recent studies point to an involvement of rac1 in tumorigenesis, little is known about the alteration of rac1 gene in human brain tumours. METHODS: Reverse transcription-polymerase chain reaction (RT-PCR), TA cloning, and DNA sequencing were performed to detect rac1 gene mutations in the surgical specimens of 45 human brain tumours. RESULTS: Twelve of 45 cases had base changes in the rac1 gene. The frequency of rac1 alterations was seven of 18 meningiomas, three of 14 astrocytomas, one of seven pituitary adenomas, and one of four metastatic brain tumours. No mutation was detected in acoustic neurilemomas. The subtypes of seven meningiomas include three meningotheliomatous, two atypical, one transitional and one angioblastic meningioma. Three astrocytomas had rac1 gene mutation, including one grade II, one grade III, and one grade IV astrocytoma. All of single base changes were transitions, five of them being T to C transitions. Sites of rac1 mutation were found in codons 34, 41 (two cases), 42 (two cases), 43, 44, 46 and 58. These mutations are mainly localized in the putative effector-domain of rac1 gene and may enhance the activity of rac1, which increases the survival of brain tumours. CONCLUSION: Our results suggest that rac1 gene may play a role in some brain tumours of divergent histogenesis and that the alterations of rac1 gene may contribute to tumorigenesis and/or metastasis.
机译:目的:Rac1是小GTPase的Ras超家族的成员,在细胞骨架重组,基因表达和细胞增殖的调控以及细胞转化中起着基本作用。尽管最近的研究表明rac1参与肿瘤发生,但是关于rac1基因在人脑肿瘤中的改变知之甚少。方法:采用逆转录聚合酶链反应(RT-PCR),TA克隆和DNA测序技术检测45例人脑肿瘤手术标本中的rac1基因突变。结果:45例中有12例rac1基因发生碱基改变。 rac1改变的频率为18个脑膜瘤中的7个,14个星形细胞瘤中的3个,7个垂体腺瘤之一和4个转移性脑瘤之一。在听觉神经瘤中未检测到突变。七个脑膜瘤的亚型包括三个脑膜瘤,两个非典型性,一个过渡性和一个成血管性脑膜瘤。 3个星形细胞瘤具有rac1基因突变,包括1个II级,1个III级和1个IV级星形细胞瘤。所有单个基本更改都是过渡,其中五个是T到C的过渡。 rac1突变的位点位于密码子34、41(两个病例),42(两个病例),43、44、46和58密码子中。这些突变主要位于rac1基因的推定效应子域中,可能增强rac1基因的活性。 rac1,可增加脑肿瘤的存活率。结论:我们的结果提示rac1基因可能在某些组织分化程度不同的脑肿瘤中起作用,而rac1基因的改变可能有助于肿瘤的发生和/或转移。

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