首页> 美国卫生研究院文献>Journal of Histochemistry and Cytochemistry >Differential Activity of NADPH-Producing Dehydrogenases Renders Rodents Unsuitable Models to Study IDH1R132 Mutation Effects in Human Glioblastoma
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Differential Activity of NADPH-Producing Dehydrogenases Renders Rodents Unsuitable Models to Study IDH1R132 Mutation Effects in Human Glioblastoma

机译:产生NADPH的脱氢酶的差异活性导致啮齿类动物研究人胶质母细胞瘤IDH1R132突变效应的不合适模型

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摘要

The somatic IDH1R132 mutation in the isocitrate dehydrogenase 1 gene occurs in high frequency in glioma and in lower frequency in acute myeloid leukemia and thyroid cancer but not in other types of cancer. The mutation causes reduced NADPH production capacity in glioblastoma by 40% and is associated with prolonged patient survival. NADPH is a major reducing compound in cells that is essential for detoxification and may be involved in resistance of glioblastoma to treatment. IDH has never been considered important in NADPH production. Therefore, the authors investigated NADPH-producing dehydrogenases using in silico analysis of human cancer gene expression microarray data sets and metabolic mapping of human and rodent tissues to determine the role of IDH in total NADPH production. Expression of most NADPH-producing dehydrogenase genes was not elevated in 34 cancer data sets except for IDH1 in glioma and thyroid cancer, indicating an association with the IDH1 mutation. IDH activity was the main provider of NADPH in human normal brain and glioblastoma, but its role was modest in NADPH production in rodent brain and other tissues. It is concluded that rodents are a poor model to study consequences of the IDH1R132 mutation in glioblastoma.
机译:异柠檬酸脱氢酶1基因的体细胞IDH1 R132 突变在神经胶质瘤中高发,在急性髓细胞性白血病和甲状腺癌中低发,而在其他类型的癌症中不高。该突变导致胶质母细胞瘤中NADPH的生产能力降低了40%,并与患者生存期延长有关。 NADPH是细胞中主要的还原性化合物,对于排毒至关重要,并且可能与胶质母细胞瘤对治疗的耐药性有关。 IDH在NADPH生产中从未被认为很重要。因此,作者使用计算机模拟人类癌症基因表达微阵列数据集以及人类和啮齿动物组织的代谢图谱研究了产生NADPH的脱氢酶,以确定IDH在总NADPH产生中的作用。除胶质瘤和甲状腺癌中的IDH1外,在34个癌症数据集中,大多数产生NADPH的脱氢酶基因的表达均未升高,表明与IDH1突变有关。 IDH活性是人类正常脑和胶质母细胞瘤中NADPH的主要提供者,但它在啮齿动物脑和其他组织中NADPH产生中的作用适中。结论是,啮齿类动物不是研究胶质母细胞瘤中IDH1 R132 突变后果的不良模型。

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