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原发性人脑肿瘤的微卫星不稳定性分析

Microsatellite instability analysis of primary human brain tumors.

作者信息

Zhu J, Guo S Z, Beggs A H, Maruyama T, Santarius T, Dashner K, Olsen N, Wu J K, Black P

机构信息

Neurosurgical Laboratory, Brigham & Women's Hospital, Children's Hospital, Dana-Farber Cancer Institute, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

Oncogene. 1996 Apr 4;12(7):1417-23.

PMID:8622857
Abstract

Microsatellite instability, as shown by the presence of additional alleles or shifts of electrophoretic mobility at simple sequence tandem repeat loci, has been demonstrated in hereditary and sporadic colorectal tumors and many other tumor types. To study microsatellite instability in human brain tumors, we examined a total of 144 sporadic neoplasms. These included 33 astrocytic tumors, 23 oligodendrogliomas, six gangliogliomas, 41 meningiomas, 10 vestibular schwannomas and 31 pituitary adenomas. Di-, tri- and tetranucleotide repeat microsatellite markers localized on chromosome 4 and 9, X, 13 and 22, respectively, were used to assess whether instability was a significant aspect of their abnormal chromosomal pattern. Instability of microsatellite markers was detected in four oligodendrogliomas (17.4%), one pituitary adenoma (3.2%), one meningioma (2.4%), one astrocytic tumor (3.0%) and not at all in gangliogliomas and schwannomas. Therefore, our results suggest that the microsatellite instability which occurs in colorectal cancers with defective mismatch repair is infrequent in many types of human brain tumors and that the lower level of instability observed in brain tumors may be reflective of other mechanisms of genetic instability.

摘要

微卫星不稳定性,表现为简单序列串联重复位点出现额外等位基因或电泳迁移率改变,已在遗传性和散发性结直肠癌及许多其他肿瘤类型中得到证实。为研究人脑肿瘤中的微卫星不稳定性,我们共检测了144例散发性肿瘤。其中包括33例星形细胞瘤、23例少突胶质细胞瘤、6例神经节胶质瘤、41例脑膜瘤、10例前庭神经鞘瘤和31例垂体腺瘤。分别位于4号和9号染色体、X染色体、13号和22号染色体上的二核苷酸、三核苷酸和四核苷酸重复微卫星标记,用于评估不稳定性是否是其异常染色体模式的一个重要方面。在4例少突胶质细胞瘤(17.4%)、1例垂体腺瘤(3.2%)、1例脑膜瘤(2.4%)、1例星形细胞瘤(3.0%)中检测到微卫星标记不稳定性,而在神经节胶质瘤和神经鞘瘤中未检测到。因此,我们的结果表明,在错配修复缺陷的结直肠癌中出现的微卫星不稳定性在许多类型的人脑肿瘤中并不常见,并且在脑肿瘤中观察到的较低水平的不稳定性可能反映了其他遗传不稳定机制。

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