台湾地区原发性黏液性卵巢癌中 BRAF 突变的高频发生。

High frequency of BRAF mutations in primary mucinous ovarian carcinoma of Taiwanese patients.

机构信息

Department of Pathology, Chung-Shan Medical University, Taichung, Taiwan; Department of Pathology, Chung-Shan Medical University Hospital, Taichung, Taiwan.

Department of Statistics and Informatics Science, Providence University, Taichung, Taiwan.

出版信息

Taiwan J Obstet Gynecol. 2021 Nov;60(6):1072-1077. doi: 10.1016/j.tjog.2021.09.019.

DOI:10.1016/j.tjog.2021.09.019

PMID:34794740

Abstract

OBJECTIVE

Considering the clinical evidence of BRAF inhibitors that can treat melanoma patients successfully, we aimed to investigate the status of BRAF mutations of primary mucinous ovarian carcinomas (MOC) in Taiwanese women, and apply the emerging paradigm classification of BRAF mutation groups.

MATERIALS AND METHODS

20 archived primary MOC samples were analyzed. The BRAF mutations of activation segment (exon 15), CR3 (conserved regions 3), kinase domain of the BRAF gene were analyzed using the highly sensitive BRAF mutant enriched kit (FemtoPath®) with Sanger sequencing method. Additionally, we extended our prior reported data of HER2 aberrations and KRAS mutation into this study in order to compare with the status of BRAF mutation.

RESULTS

Of them (n = 20), 16 (80%) harbored BRAF missense mutations. Their mutation profile and case number (n) were categorized as (1) class I: V600E (n=1), V600M (n = 1); (2) class II: A598V (n = 1), T599I (n = 10); (3) class III: none (n = 0); and (4) unclassified variants: S602F (n = 2), T599I/S602F (n = 1). The BRAF S602F is novel. The prevalence of BRAF mutation is significantly higher than either HER2 mutation (80% vs. 35%; p = 0.022) or HER2 amplification (80% vs. 35%; p = 0.022). However, the mutation rates of BRAF and KRAS were not significantly different (80% vs. 60%; p = 0.289).

CONCLUSION

Activating BRAF mutation, HER2 amplification, HER2 mutation and KRAS mutation were not mutually exclusive. However, they may even have a synergistic effect in tumorigenesis. BRAF mutation is not uncommon in primary MOC of Taiwanese. The BRAF mutant (T599I) stands the majority. We suggested that there was a lower potential response to the existing V600 BRAF inhibitors, but may be responsive to dual BRAF plus MEK inhibitors or single MEK inhibitor. Further studies are warranted to investigate the clinical benefits of newly targeted therapy in recurrent or advanced stage primary MOC patients carrying different classes of BRAF mutation.

摘要

目的

鉴于 BRAF 抑制剂在成功治疗黑色素瘤患者方面的临床证据，我们旨在研究 BRAF 突变在台湾女性原发性黏液性卵巢癌（MOC）中的状态，并应用新兴的 BRAF 突变组分类范式。

材料和方法

分析了 20 例存档的原发性 MOC 样本。使用高灵敏度的 BRAF 突变富集试剂盒（FemtoPath®）和 Sanger 测序方法，分析 BRAF 基因激活片段（外显子 15）、CR3（保守区域 3）和激酶结构域的 BRAF 突变。此外，我们将之前报道的 HER2 异常和 KRAS 突变数据扩展到本研究中，以便与 BRAF 突变状态进行比较。

结果

其中 16 例（80%）存在 BRAF 错义突变。它们的突变谱和病例数（n）分为（1）I 类：V600E（n=1），V600M（n=1）；（2）II 类：A598V（n=1），T599I（n=10）；（3）III 类：无（n=0）；和（4）未分类变体：S602F（n=2），T599I/S602F（n=1）。BRAF S602F 是新发现的。BRAF 突变的发生率明显高于 HER2 突变（80% vs. 35%；p=0.022）或 HER2 扩增（80% vs. 35%；p=0.022）。然而，BRAF 和 KRAS 的突变率没有显著差异（80% vs. 60%；p=0.289）。

结论

激活的 BRAF 突变、HER2 扩增、HER2 突变和 KRAS 突变并非相互排斥，而是可能在肿瘤发生中具有协同作用。BRAF 突变在台湾原发性 MOC 中并不罕见。BRAF 突变（T599I）占多数。我们建议，对现有的 V600 BRAF 抑制剂的潜在反应较低，但可能对双重 BRAF 加 MEK 抑制剂或单一 MEK 抑制剂有反应。需要进一步研究以探讨携带不同类型 BRAF 突变的复发性或晚期原发性 MOC 患者新靶向治疗的临床获益。