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微卫星不稳定性发生于儿童中枢神经系统肿瘤的不同亚型中,而成人中枢神经系统肿瘤中则不会发生。

Microsatellite instability occurs in distinct subtypes of pediatric but not adult central nervous system tumors.

作者信息

Alonso M, Hamelin R, Kim M, Porwancher K, Sung T, Parhar P, Miller D C, Newcomb E W

机构信息

Department of Pathology New York University School of Medicine, New York 10016, USA.

出版信息

Cancer Res. 2001 Mar 1;61(5):2124-8.

PMID:11280776
Abstract

Length alterations in microsatellite repeats, termed microsatellite instability (MSI), are found in 10-15% of sporadic colon, endometrial, and gastric cancers harboring defects in DNA mismatch repair (MMR) genes We used the microsatellite markers Big Adenine Tract (BAT) 26 and BAT-25 from the reference panel of five markers recommended by the National Cancer Institute to evaluate the incidence of MSI in 206 central nervous system tumors. We screened 102 pediatric and 104 adult cases representing 165 astrocytic and 41 nonastrocytic tumors. The overall incidence of MSI was 8% (16 of 206). All 16 tumors with MSI were found in pediatric rather than adult patients. MSI was associated with two distinct subtypes of pediatric tumors occurring in 27% (12 of 45) of WHO grade III and grade IV astrocytomas and 24% (4 of 17) of gangliogliomas We evaluated the difference in clinicopathological and genetic features among 45 high-grade pediatric astrocytomas by MSI status. The median survival for pediatric patients with MSI (n = 12) was 8 months compared with 15 months for those patients without MSI (n = 33; P = 0.18). The frequency of p53 gene mutations was 13% for pediatric patients with MSI (n = 8) compared with 47% for those patients without MSI (n = 19; P = 0.19). These results revealed a trend between MSI status and prog nosis and MSI status and frequency of p53 gene mutations. Our data suggest that pediatric high-grade astrocytomas can be attributed to two different genetic pathways: a MMR-deficient pathway and a MMR proficient pathway.

摘要

微卫星重复序列长度改变,即微卫星不稳定性(MSI),在10% - 15%散发的结肠癌、子宫内膜癌和胃癌中被发现,这些癌症存在DNA错配修复(MMR)基因缺陷。我们使用了美国国立癌症研究所推荐的五个标记物参考面板中的微卫星标记物大腺嘌呤序列(BAT)26和BAT - 25,来评估206例中枢神经系统肿瘤中MSI的发生率。我们筛查了102例儿科病例和104例成人病例,分别代表165例星形细胞瘤和41例非星形细胞瘤。MSI的总体发生率为8%(206例中的16例)。所有16例存在MSI的肿瘤均在儿科患者而非成人患者中发现。MSI与儿科肿瘤的两种不同亚型相关,分别发生在27%(45例中的12例)的世界卫生组织III级和IV级星形细胞瘤以及24%(17例中的4例)的神经节胶质瘤中。我们根据MSI状态评估了45例儿科高级别星形细胞瘤的临床病理和基因特征差异。MSI儿科患者(n = 12)的中位生存期为8个月,而无MSI的患者(n = 33)为15个月(P = 0.18)。MSI儿科患者(n = 8)中p53基因突变频率为13%,而无MSI的患者(n = 19)为47%(P = 0.19)。这些结果揭示了MSI状态与预后以及MSI状态与p53基因突变频率之间的一种趋势。我们的数据表明,儿科高级别星形细胞瘤可归因于两种不同的遗传途径:一种是MMR缺陷途径,另一种是MMR正常途径。

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