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原发性乳腺癌和腋窝淋巴结转移瘤中的等位基因失衡。

Allelic imbalance in primary breast carcinomas and metastatic tumors of the axillary lymph nodes.

作者信息

Ellsworth Rachel E, Ellsworth Darrell L, Neatrour David M, Deyarmin Brenda, Lubert Susan M, Sarachine Miranda J, Brown Patrick, Hooke Jeffrey A, Shriver Craig D

机构信息

Clinical Breast Care Project, Windber Research Institute, Windber, PA 15963, USA.

出版信息

Mol Cancer Res. 2005 Feb;3(2):71-7. doi: 10.1158/1541-7786.MCR-04-0180.

Abstract

Axillary lymph node status is the most important prognostic factor in predicting disease outcome in women with breast cancer. A number of chromosomal aberrations in primary breast tumors have been correlated with lymph node status and clinical outcome, but chromosomal changes particular to metastatic lymph node tumors have not been well studied. DNA samples isolated from laser-microdissected primary breast and metastatic axillary lymph node tumors from 25 women with invasive breast cancer were amplified using 52 microsatellite markers defining 26 chromosomal regions commonly deleted in breast cancer. Levels and patterns of allelic imbalance (AI) within and between breast and lymph node tumors were assessed to identify chromosomal alterations unique to primary or metastatic tumors and to examine the timing of metastatic potential. The overall frequency of AI in primary breast tumors (0.24) was significantly greater (P < 0.001) than that in lymph node tumors (0.10), and congruent AI events were observed for < 20% of informative markers. AI at chromosomes 11q23.3 and 17p13.3 occurred significantly more frequently (P < 0.05) in primary breast tumors alone; no chromosomal regions showed a significantly higher AI frequency in lymph nodes. Higher rates of AI in primary versus metastatic lymph node tumors suggest that acquisition of metastatic potential may be an early event in carcinogenesis, occurring before significant levels of AI accumulate in the primary tumor. In addition, patterns of AI were highly discordant between tumor types, suggesting that additional genetic alterations accumulated independently in the two cell populations.

摘要

腋窝淋巴结状态是预测乳腺癌女性疾病预后的最重要预后因素。原发性乳腺肿瘤中的一些染色体畸变已与淋巴结状态和临床结果相关,但转移性淋巴结肿瘤特有的染色体变化尚未得到充分研究。从25例浸润性乳腺癌女性患者的激光显微切割原发性乳腺肿瘤和转移性腋窝淋巴结肿瘤中分离的DNA样本,使用52个微卫星标记进行扩增,这些标记定义了26个在乳腺癌中常见缺失的染色体区域。评估乳腺肿瘤和淋巴结肿瘤内部及之间的等位基因不平衡(AI)水平和模式,以识别原发性或转移性肿瘤特有的染色体改变,并检查转移潜能的发生时间。原发性乳腺肿瘤中AI的总体频率(0.24)显著高于淋巴结肿瘤(0.10)(P < 0.001),并且在<20%的信息性标记中观察到一致的AI事件。仅在原发性乳腺肿瘤中,11q23.3和17p13.3染色体上的AI发生频率显著更高(P < 0.05);没有染色体区域在淋巴结中显示出显著更高的AI频率。原发性肿瘤与转移性淋巴结肿瘤中较高的AI发生率表明,转移潜能的获得可能是致癌过程中的早期事件,发生在原发性肿瘤中AI显著积累之前。此外,肿瘤类型之间的AI模式高度不一致,表明两个细胞群体中独立积累了额外的基因改变。

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