伴有皮肤转移的乳腺癌的分子改变和预后。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Applied Bio Materials Pub Date : 2024-07-05 DOI:10.1186/s13000-024-01509-x

Yan Xu, Li Ding, Chao Li, Bin Hua, Sha Wang, Junli Zhang, Cuicui Liu, Rongyun Guo, YongQiang Zhang

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引用次数: 0

摘要

目的：皮肤转移（CM）占乳腺癌（BC）患者的5%-30%，对治疗反应差，预后不良。更好地了解转移所涉及的分子改变至关重要，这将有助于确定乳腺癌的诊断和疗效生物标志物：我们回顾性研究了13例经组织学或细胞学诊断为乳腺癌和CM的患者。我们从病历中提取了临床信息。我们使用新一代测序技术（NGS）分析了425个癌症相关基因的突变情况。此外，还对所有组织进行了免疫组化（IHC）分析。研究还评估了预后与各种临床和分子因素的关联：结果：半数以上的 Ki67 低患者（50%）的 T1 明显短于 Ki67 低组（≤50%）（中位 12.5 个月 vs. 50.0 个月，P = 0.036）。TP53、PIK3CA突变和TERT扩增组与较差的T2相关（中位11个月对36个月，P = 0.065；8个月对36个月，P = 0.013；7个月对36个月，P = 0.003）。所有P值均未经调整：我们比较了原发性乳腺癌组织和相应的CM组织的基因组特征，并讨论了可能导致晚期乳腺癌患者皮肤转移的潜在基因和通路。TP53、PIK3CA突变和TERT扩增可作为CM患者预后不良的生物标志物。

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Molecular alterations and prognosis of breast cancer with cutaneous metastasis.

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.

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来源期刊

ACS Applied Bio Materials Chemistry-Chemistry (all)

CiteScore

9.40

自引率

2.10%

发文量

464