首页 / 院系成果 / 成果详情页

Molecular alterations and prognosis of breast cancer with cutaneous metastasis 期刊论文

编号：

67E67C4B5E0E9F1FB33789DEC672575E
作者：

Xu, Yan(许焱)#^[1]Ding, Li(丁丽)^[1]Li, Chao(李超)^[1]Hua, Bin(华彬)^[1]Wang, Sha^[2];Zhang, Junli^[2];Liu, Cuicui^[2];Guo, Rongyun^[2];Zhang, Yongqiang(张永强)*^[1]
语种：

英文
期刊：

DIAGNOSTIC PATHOLOGY ISSN：1746-1596 2024 年 19 卷 1 期 ; JUL 5
收录：
关键词：

Cutaneous metastasis Breast cancer Next-generation sequencing-NGS Genomic analysis Prognosis
摘要：

Purpose Cutaneous metastasis (CM) accounts for 5-30% of patients with breast cancer (BC) and presents unfavorable response to treatment and poor prognosis. A better understanding of the molecular alterations involved in metastasis is essential, which would help identify diagnostic and efficacy biomarkers for CM. Materials: We retrospectively reviewed a total of 13 patients with histological or cytological diagnosis of breast cancer and CM. Clinical information was extracted from the medical records. The mutational landscape of matched primary tumors with their lymph nodes or CM tissues were analyzed using next-generation sequencing (NGS) of 425 cancer-relevant genes. All tissues were also analyzed by immunohistochemistry (IHC). The association of prognosis with various clinical and molecular factors was also evaluated. Results More than half of the patients were Ki67 low (< 50%, 53.7%). Most patients (12, 92.3%) had other metastasis sites other than skin. The median time from diagnosis to the presentation of CM (T1) was 15 months (range: 0-94 months) and the median time from CM to death (T2) was 13 months (range 1-78). The most frequently altered genes across the three types of tissues were TP53 (69.6%, 16/23), PIK3CA (34.8%, 8/23), and MYC (26.1%). The number of alterations in CM tends to be higher than in primary tumors (median 8 vs. 6, P = 0.077). Copy number loss in STK11, copy number gain in FGFR4, TERT, AR, FLT4 and VEGFA and mutations in ATRX, SRC, AMER1 and RAD51C were significantly enriched in CM (all P < 0.05). Ki67 high group (> 50%) showed significantly shorter T1 than the Ki67 low group (<= 50%) (median 12.5 vs. 50.0 months, P = 0.036). TP53, PIK3CA mutations, and TERT amplification group were associated with inferior T2 (median 11 vs. 36 months, P = 0.065; 8 vs. 36 months, P = 0.013, 7 vs. 36 months, P = 0.003, respectively). All p values were not adjusted. Conclusion We compared the genomic features of primary breast cancer tissues with their corresponding CM tissues and discussed potential genes and pathways that may contribute to the skin metastasis of advanced breast cancers patients. TP53, PIK3CA mutant, and TERT amplification may serve as biomarkers for poor prognosis for CM patients.
推荐引用方式
GB/T 7714：

Xu Yan,Ding Li,Li Chao, et al. Molecular alterations and prognosis of breast cancer with cutaneous metastasis [J].DIAGNOSTIC PATHOLOGY,2024,19(1).
APA：

Xu Yan,Ding Li,Li Chao,Hua Bin,&Zhang Yongqiang.(2024).Molecular alterations and prognosis of breast cancer with cutaneous metastasis .DIAGNOSTIC PATHOLOGY,19(1).
MLA：

Xu Yan, et al. "Molecular alterations and prognosis of breast cancer with cutaneous metastasis" .DIAGNOSTIC PATHOLOGY 19,1(2024).
入库时间：

2024/7/25 13:47:48
更新时间：

2024/7/25 13:47:48
条目包含文件：

文件类型：PDF,文件大小：

正在加载全文

未找到全文

浏览次数：223  下载次数：0

分享到：

浏览次数：223

下载次数：0

打印次数：1