4.4 Article

Genomic Alterations in Primary Breast Cancers Compared with Their Sentinel and More Distal Lymph Node Metastases: An aCGH Study

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GENES CHROMOSOMES & CANCER
卷 48, 期 12, 页码 1091-1101

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WILEY
DOI: 10.1002/gcc.20711

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  1. Gattuso Chair in Breast Surgical Oncology
  2. Canadian Breast Cancer Research Alliance
  3. Canadian Institute for Health Research training program in Oncologic Molecular Pathology, Canada [STP-53912]

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Metastatic potential of breast cancer may be associated with specific genomic alterations and the earliest metastases are likely to be found in the sentinel lymph nodes (SLN). Using array comparative genomic hybridization (aCGH), we compared the genomes of primary breast invasive duct carcinomas (IDCs), their sentinel and more distal lymph node metastases, and IDCs without nodal metastasis. Thirty-three samples from 22 patients with IDC were subjected to aCGH: 8 IDC samples from patients without lymph node metastasis, I I IDCs associated with SLN metastases out of which 7 had paired samples of metastases, and 14 samples of lymph node metastases out of which 8 were sentinel-distal pairs from 4 patients. aCGH data were analyzed by correlation of genomic profiles, cluster analysis, segmentation, and peak identification. Quantitative real-time PCR was used for data validation. We observed high genomic similarity between primary tumors and their nodal metastases as well as between metastases to the sentinel and distal lymph nodes. Several recurrent alterations were detected preferentially in IDC associated with SLN metastases compared to IDCs without metastasis. Amplification within the 17q24.1-24.2(59.96-62.76 Mb) region was associated with presence of sentinel or distal lymph node metastases; larger tumor size and higher histological grade. In our samples, there were genomic events associated with metastatic progression, which could be detected in both primary tumors and LN metastases. Gain on 17q24.1-24.2 is a candidate region for further testing as a predictor of nodal metastasis. (C) 2009 Wiley-Liss, Inc.

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