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用于检测黑色素瘤中BRAF和NRAS突变的快速全自动平台的评估

Evaluation of a Rapid, Fully Automated Platform for Detection of BRAF and NRAS Mutations in Melanoma.

作者信息

Barel Fanny, Guibourg Briac, Lambros Laetitia, Le Flahec Glen, Marcorelles Pascale, Uguen Arnaud

机构信息

Department of Pathology, CHRU Brest, F-29220 Brest, France.

出版信息

Acta Derm Venereol. 2018 Jan 12;98(1):44-49. doi: 10.2340/00015555-2738.

Abstract

BRAF and NRAS genetic analyses are time-consuming and can delay treatment choices in patients with metastatic melanomas presenting with acute deterioration. We compared the rapid, real-time, fully automated molecular diagnosis platform Idylla™ with next-generation sequencing (NGS) and immunohistochemistry for detection of BRAF and NRAS mutations in 36 patients with metastatic melanomas. The Idylla™ NRAS-BRAF-EGFRS492R mutation assay (110 min per sample) detected BRAF and NRAS mutations in 15 and 17 samples, respectively. One NRAS mutation was different between NGS and Idylla™ (NRASG13C vs. NRASG12A/D). Four samples were BRAF and NRAS wild-type. The global concordance between NGS and Idylla™ assays was 97.2% (35/36 cases). Immunohistochemistry was positive only in 9/9 BRAFV600E- and 6/6 NRASQ61R-mutated samples with VE1 and SP174 antibodies, respectively. The Idylla™ platform is a valuable rapid molecular diagnosis tool to reduce the delay in BRAF and NRAS analyses-related treatment choices for patients with metastatic melanoma presenting with acute deterioration.

摘要

BRAF和NRAS基因分析耗时较长,可能会延误急性病情恶化的转移性黑色素瘤患者的治疗选择。我们将快速、实时、全自动分子诊断平台Idylla™与下一代测序(NGS)和免疫组化进行比较,以检测36例转移性黑色素瘤患者的BRAF和NRAS突变。Idylla™NRAS - BRAF - EGFRS492R突变检测法(每个样本110分钟)分别在15个和17个样本中检测到BRAF和NRAS突变。NGS与Idylla™检测到的一个NRAS突变不同(NRASG13C与NRASG12A/D)。4个样本为BRAF和NRAS野生型。NGS与Idylla™检测的总体一致性为97.2%(35/36例)。免疫组化仅在分别使用VE1和SP174抗体的9/9 BRAFV600E突变和6/6 NRASQ61R突变样本中呈阳性。Idylla™平台是一种有价值的快速分子诊断工具,可减少急性病情恶化的转移性黑色素瘤患者在BRAF和NRAS分析相关治疗选择上的延误。

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