使用靶向激酶组测序对三阴性乳腺癌进行突变分析。
Mutational Analysis of Triple-Negative Breast Cancer Using Targeted Kinome Sequencing.
作者信息
Yoo Tae-Kyung, Lee Woo Seung, Kim Jisun, Kim Min Kyoon, Park In-Ae, Kim Ju Han, Han Wonshik
机构信息
Department of Surgery, Seoul St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Seoul, Korea.
Division of Biomedical Informatics, Seoul National University College of Medicine, Seoul, Korea.
出版信息
J Breast Cancer. 2022 Jun;25(3):164-177. doi: 10.4048/jbc.2022.25.e15. Epub 2022 Apr 20.
PURPOSE
Triple-negative breast cancer (TNBC) does not have defined therapeutic targets and is currently treated with chemotherapy only. Kinase dysregulation triggers cancer cell proliferation and metastasis and is a crucial therapeutic target for cancer. In this study, targeted kinome sequencing of TNBC tumors was performed to assess the association between kinome gene alterations and disease outcomes in TNBC.
METHODS
A kinome gene panel consisting of 612 genes was used for the targeted sequencing of 166 TNBC samples and matched normal tissues. Analyses of the significantly mutated genes were performed. Genomic differences between Asian and non-Asian patients with TNBC were evaluated using two Asian TNBC datasets (from Seoul National University Hospital [SNUH] and Fudan University Shanghai Cancer Center [FUSCC]) and three non-Asian TNBC datasets (The Cancer Genome Atlas [TCGA], METABRIC, and Gustave Roussy). The prognostic value of kinome gene mutations was evaluated using tumor mutational burden (TMB) and oncogenic pathway analyses. Mutational profiles from the TCGA were used for validation.
RESULTS
The significantly mutated genes included (60% of patients), (21%), (8%), and (8%). Compared with data from non-Asian public databases, the mutation rates of p.H1047R/Q were significantly higher in the SNUH cohort ( = 0.003, 0.048, and 0.032, respectively). This was verified using the FUSCC dataset ( = 0.003, 0.078, and 0.05, respectively). The TMB-high group showed a trend toward longer progression-free survival in our cohort and the TCGA TNBC cohort ( = 0.041 and 0.195, respectively). Kinome gene alterations in the Wnt pathway in patients with TNBC were associated with poor survival in both datasets ( = 0.002 and 0.003, respectively).
CONCLUSION
Comprehensive analyses of kinome gene alterations in TNBC revealed genomic alterations that offer therapeutic targets and should help identify high-risk patients more precisely in future studies.
目的
三阴性乳腺癌(TNBC)没有明确的治疗靶点,目前仅采用化疗进行治疗。激酶失调会引发癌细胞增殖和转移,是癌症的关键治疗靶点。在本研究中,对TNBC肿瘤进行靶向激酶组测序,以评估激酶组基因改变与TNBC疾病预后之间的关联。
方法
使用包含612个基因的激酶组基因panel对166例TNBC样本及匹配的正常组织进行靶向测序。对显著突变基因进行分析。利用两个亚洲TNBC数据集(来自首尔国立大学医院[SNUH]和复旦大学附属肿瘤医院[FUSCC])以及三个非亚洲TNBC数据集(癌症基因组图谱[TCGA]、METABRIC和古斯塔夫·鲁西研究所)评估亚洲和非亚洲TNBC患者之间的基因组差异。使用肿瘤突变负荷(TMB)和致癌途径分析评估激酶组基因突变的预后价值。来自TCGA的突变谱用于验证。
结果
显著突变基因包括(60%的患者)、(21%)、(8%)和(8%)。与非亚洲公共数据库的数据相比,SNUH队列中p.H1047R/Q的突变率显著更高(分别为=0.003、0.048和0.032)。使用FUSCC数据集对此进行了验证(分别为=0.003、0.078和0.05)。在我们的队列和TCGA TNBC队列中,TMB高的组显示出无进展生存期更长的趋势(分别为=0.041和0.195)。TNBC患者Wnt途径中的激酶组基因改变与两个数据集中的不良生存相关(分别为=0.002和0.003)。
结论
对TNBC中激酶组基因改变的综合分析揭示了可提供治疗靶点的基因组改变,并应有助于在未来研究中更精确地识别高危患者。
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