BMC Cancer (Dec 2006)

An association of a simultaneous nuclear and cytoplasmic localization of Fra-1 with breast malignancy

  • Chen Liyong,
  • Zhang Yan,
  • Zhang Dong,
  • Song Santai,
  • Song Yuhua,
  • Qian Lu,
  • Shi Ming,
  • Zhao Huibin,
  • Jiang Zefei,
  • Guo Ning

DOI
https://doi.org/10.1186/1471-2407-6-298
Journal volume & issue
Vol. 6, no. 1
p. 298

Abstract

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Abstract Background Overexpression of Fra-1 in fibroblasts causes anchorage-independent cell growth and oncogenic transformation. A high level of Fra-1 expression is found in various tumors and tumorigenic cell lines, suggesting that Fra-1 may be involved in malignant progression. This study aimed to investigate the significance of Fra-1 expression in breast carcinogenesis. Methods The expression of Fra-1 was investigated by immunohistochemistry in neoplastic breast diseases ranging from benign fibroadenoma to very aggressive undifferentiated carcinoma. The correlations of Fra-1 expression with other indicators of breast carcinoma prognosis (ER, PR and ErbB2 receptors) were analyzed. Results All neoplastic breast tissues, either benign or malignant breast tissues, were nuclear immunoreactive for Fra-1-recognizing antibody. The pattern of Fra-1 expression by benign neoplastic cells was predominantly nuclear. However, the nuclear/cytoplasmic concomitant immunoreactivity was observed in all types of breast carcinomas. A clear shift in Fra-1 immunoreactivity, from an exclusively nuclear to a simultaneous nuclear and cytoplasmic localization was noticed in ~90% of breast carcinomas. Conclusion The overall expression, pattern and intensity of Fra-1 proteins were correlated with breast oncogenesis. Overexpression of Fra-1, leading to a persistent high cytoplasmic accumulation, may play a role in the process of breast carcinogenesis.