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脑膜瘤中碱性磷酸酶活性的丧失:一种快速组织化学技术,表明1号染色体短臂远端一个假定的肿瘤抑制基因与进展相关的缺失。

Loss of alkaline phosphatase activity in meningiomas: a rapid histochemical technique indicating progression-associated deletion of a putative tumor suppressor gene on the distal part of the short arm of chromosome 1.

作者信息

Niedermayer I, Feiden W, Henn W, Steilen-Gimbel H, Steudel W I, Zang K D

机构信息

Department of Neuropathology, Medical School, University of Saarland, Homburg, Germany.

出版信息

J Neuropathol Exp Neurol. 1997 Aug;56(8):879-86.

PMID:9258258
Abstract

Apart from defined histomorphologic features, increased Ki-67 indices and various numeric and structural chromosome aberrations, meningiomas of the intermediate (WHO grade II, atypical meningioma) and anaplastic type (WHO grade III) are cytogenetically distinguished from common-type meningiomas (WHO grade I) by frequent loss of the distal part of the short arm of one chromosome 1 (1p-), which formerly proved to be an independent predictor of shorter recurrence-free intervals. Histochemically, loss of alkaline phosphatase activity (ALPL, liver/bone/kidney type, EC 3.1.3.1) was another frequent, specific finding in meningiomas with signs of dedifferentiation. In a prospective study including 66 meningiomas, all common-type meningiomas except one case (18/19) were reactive for ALPL, whereas 75% (30/39) of intermediate type and all anaplastic meningiomas (8/8) showed loss of enzyme activity in large areas of the tumor. Exclusively, the ALPL negative phenotype was associated with 1p loss (15/19). Our data suggest that ALPL, which is coded as a single copy gene on chromosome 1p36.1-p34, is a useful marker enzyme for the loss of a putative regulatory (tumor suppressor) gene on chromosome 1p, or that ALPL itself represents a new tumor suppressor gene homozygously inactivated in meningiomas.

摘要

除了明确的组织形态学特征、Ki-67指数增加以及各种数值和结构染色体畸变外,间变型(世界卫生组织II级,非典型脑膜瘤)和间变类型(世界卫生组织III级)脑膜瘤在细胞遗传学上与普通型脑膜瘤(世界卫生组织I级)的区别在于,常出现一条1号染色体短臂远端部分的缺失(1p-),此前已证明这是无复发生存期较短的独立预测指标。组织化学方面,碱性磷酸酶活性(ALPL,肝/骨/肾型,EC 3.1.3.1)缺失是具有去分化迹象的脑膜瘤中另一个常见的特异性发现。在一项纳入66例脑膜瘤的前瞻性研究中,除1例(18/19)外,所有普通型脑膜瘤的ALPL均呈阳性反应,而间变型脑膜瘤的75%(30/39)和所有间变脑膜瘤(8/8)在肿瘤大片区域显示酶活性缺失。仅ALPL阴性表型与1p缺失相关(15/19)。我们的数据表明,在1p36.1-p34染色体上作为单拷贝基因编码的ALPL,是1p上一个假定调控(肿瘤抑制)基因缺失的有用标记酶,或者ALPL本身代表一种在脑膜瘤中纯合失活的新肿瘤抑制基因。

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