Concurrent -Amplified Secondary Angiosarcoma and Recurrent Carcinoma in the Breast: A Rare Presentation With Unique Clinical Features and Distinct Amplification Patterns.
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TL;DR
A patient who was previously diagnosed with invasive breast cancer and intraductal papilloma is presented, presenting with a new enlargement in her left axilla during follow-up, highlighting the importance of considering this phenomenon in differential diagnoses.
OpenAlex 토픽 ·
Vascular Tumors and Angiosarcomas
Cardiac tumors and thrombi
Soft tissue tumors and treatment
A patient who was previously diagnosed with invasive breast cancer and intraductal papilloma is presented, presenting with a new enlargement in her left axilla during follow-up, highlighting the impor
APA
Kristin J. Rybski, B X Zhang, et al. (2026). Concurrent -Amplified Secondary Angiosarcoma and Recurrent Carcinoma in the Breast: A Rare Presentation With Unique Clinical Features and Distinct Amplification Patterns.. International journal of surgical pathology, 34(3), 709-717. https://doi.org/10.1177/10668969251381319
MLA
Kristin J. Rybski, et al.. "Concurrent -Amplified Secondary Angiosarcoma and Recurrent Carcinoma in the Breast: A Rare Presentation With Unique Clinical Features and Distinct Amplification Patterns.." International journal of surgical pathology, vol. 34, no. 3, 2026, pp. 709-717.
PMID
41236876 ↗
Abstract 한글 요약
Secondary angiosarcoma of the breast is a rare and aggressive malignancy, with characteristic amplification. It typically arises in the field of prior radiation for breast cancer treatment, or rarely, in patients with a history of radical mastectomy with axillary lymph node dissection. Concurrent angiosarcoma and carcinoma in the same breast is exceedingly rare. In this report, we describe a rare occurrence of concurrent -amplified angiosarcoma in the breast skin and recurrent carcinoma in the breast parenchyma in a patient without any history of breast radiation or axillary lymph node dissection. In addition, both angiosarcoma and carcinoma were amplified, but with distinct amplification patterns. The angiosarcoma demonstrated a 5' only amplification with a breakpoint between the 5' and 3' probes, while the carcinoma harbored a large amplification on chromosome 8q24.21, encompassing both 5' and 3' . This case report highlights the occurrence of secondary angiosarcoma arising in a patient without a history of prior radiotherapy or an axillary dissection, as well as the rare concurrence of angiosarcoma and carcinoma in the same breast. More intriguingly, the distinct gene amplification patterns in the concurrent angiosarcoma and carcinoma reflect the complexity of the gene in the tumorigenesis of different types of malignancies and may explain the different levels of MYC protein expression on immunohistochemistry.
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