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急性髓系白血病中FLT3突变与CD7表达的相关性

Correlation of FLT3 mutations with expression of CD7 in acute myeloid leukemia.

作者信息

Baqai Junaid, Crisan Domnita

机构信息

Department of Clinical Pathology, William Beaumont Hospital, Beaumont Health System, MI.

出版信息

Appl Immunohistochem Mol Morphol. 2015 Feb;23(2):104-8. doi: 10.1097/PDM.0000000000000034.

Abstract

FLT3 mutations are common in acute myeloid leukemia (AML), particularly in cases with normal karyotype. Internal tandem duplication (ITD) and also point mutations affecting aspartic acid 835 (D835) are reported. A previous study demonstrated aberrant expression of CD7 on blasts in de novo AML cases with FLT3/ITD mutations. Our study goals are to expand the evaluation of this association to a larger group of patients; to evaluate the association of aberrant CD7 expression in AMLs with D835 mutation, not previously done; to evaluate if aberrant CD7 expression may serve as a surrogate marker for predicting FLT3 mutational status; to evaluate if combined FLT3 with NPM1 mutational status has a better correlation with CD7 expression. The FLT3 mutational analysis was performed on DNA extracted from 149 previously diagnosed AML cases with cytogenetics and flow cytometry evaluation available. Of 149 patients, 28 were positive for FLT3; CD7 was positive in 13 of 20 ITD-positive cases, 5 of 6 D835-positive cases, and 1 of 2 ITD/D835-positive cases. The association of CD7 positivity and FLT3 positivity was found to be significant. However, CD7 expression has a low positive predictive value of 30% and a negative predictive value of 90%. Because of the low positive predictive value, CD7 expression cannot be used as a surrogate marker for FLT3 positivity; even though the negative predictive value is higher, some cases that are FLT3 positive may be missed if CD7 expression would be used for screening.

摘要

FLT3突变在急性髓系白血病(AML)中很常见,尤其是在核型正常的病例中。据报道存在内部串联重复(ITD)以及影响天冬氨酸835(D835)的点突变。先前的一项研究表明,在伴有FLT3/ITD突变的初发AML病例中,原始细胞上CD7表达异常。我们的研究目标是将这种关联的评估扩展到更大的患者群体;评估AML中异常CD7表达与D835突变的关联(此前未进行过此项研究);评估异常CD7表达是否可作为预测FLT3突变状态的替代标志物;评估FLT3与NPM1联合突变状态是否与CD7表达具有更好的相关性。对从149例先前诊断的AML病例中提取的DNA进行FLT3突变分析,这些病例有细胞遗传学和流式细胞术评估结果。在149例患者中,28例FLT3呈阳性;在20例ITD阳性病例中的13例、6例D835阳性病例中的5例以及2例ITD/D835阳性病例中的1例中,CD7呈阳性。发现CD7阳性与FLT3阳性之间存在显著关联。然而,CD7表达的阳性预测值低至30%,阴性预测值为90%。由于阳性预测值低,CD7表达不能用作FLT3阳性的替代标志物;即使阴性预测值较高,但如果将CD7表达用于筛查,一些FLT3阳性的病例可能会被漏诊。

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