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首页> 外文期刊>Applied immunohistochemistry and molecular morphology: AIMM >Detection of IDH1 R132H mutation in acute myeloid leukemia by mutation-specific immunohistochemistry.
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Detection of IDH1 R132H mutation in acute myeloid leukemia by mutation-specific immunohistochemistry.

机译:突变特异性免疫组织化学检测急性髓性白血病IDH1 R132H突变。

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摘要

IDH1 mutations are present but are uncommon in acute myeloid leukemia (AML) and although prognostically favorable in gliomas their clinical significance in AML is unclear. Some have associated IDH1 mutations with inferior outcome, whereas others found no association with prognosis. Complicating these analyses is the need to sequence IDH1 from leukemic blasts, which is technically challenging and not yet routine. Mutation-specific antibodies enable robust, cost-effective detection of mutations in routine biopsy samples. Immunohistochemistry for the R132H mutation-specific antibody was performed in a tissue microarray containing 159 cases of AML, detecting the R132H mutation in 7 cases (4.4%). Positivity was associated with intermediate risk cytogenetics. Our results demonstrate an association between the R132H IDH1 mutation and intermediate risk cytogenetics in AML, suggesting that R132H IDH1 mutation may be associated with improved clinical outcome and demonstrate the feasibility of using mutation-specific antibodies to genotype and subclassify AML.
机译:存在IDH1突变,但在急性髓性白血病(AML)中罕见,但虽然在胶质瘤中预期有利于其在AML中的临床意义尚不清楚。有些人具有较差的IDH1突变,而其他人发现没有与预后的关联。使这些分析复杂化是需要从白血病爆炸中序列IDH1,这在技术上挑战并且尚未常规。突变特异性抗体能够稳健,经济有效地检测常规活检样品中的突变。 R132H突变特异性抗体的免疫组化在含有159例AML的组织微阵列中进行,检测7例中的R132H突变(4.4%)。阳性与中间风险细胞遗传学有关。我们的结果证明了AML中的R132H IDH1突变和中间风险细胞遗传学之间的关联,表明R132H IDH1突变可能与改善的临床结果相关,并证明使用突变特异性抗体与基因型和亚类分类AML的可行性。

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