Detection of amplified int-2/FGF-3 gene in primary breast carcinomas using differential polymerase chain reaction

  • Authors:
    • Rakesh Naidu
    • Norhanom Abdul Wahab
    • Manmohan Yadav
    • Methil Kannan Kutty
    • Suseela Nair
  • View Affiliations

  • Published online on: August 1, 2001     https://doi.org/10.3892/ijmm.8.2.193
  • Pages: 193-198
Metrics: Total Views: 0 (Spandidos Publications: | PMC Statistics: )
Total PDF Downloads: 0 (Spandidos Publications: | PMC Statistics: )


Abstract

Amplification of int-2/FGF-3 gene was investigated by differential polymerase chain reaction (dPCR) in 440 archival primary breast carcinoma tissues. Of these, 23 were comedo ductal carcinoma in situ (DCIS), 18 were non-comedo DCIS, 41 were comedo DCIS with adjacent invasive ductal carcinomas, 19 were non-comedo DCIS with adjacent invasive ductal carcinomas, 270 were invasive ductal carcinomas, 33 were invasive lobular carcinomas, 21 were colloid carcinomas and 15 were medullary carcinomas. Int-2 was amplified in 22% (96/440) of the primary breast carcinomas. It was shown that int-2 was amplified in 13% (3/23) of the comedo DCIS, 17% (7/41) of the comedo DCIS and 29% (12/41) of the adjacent invasive ductal carcinomas, 26% (71/270) of the invasive ductal carcinomas, 18% (6/33) of the invasive lobular carcinomas, 10% (2/21) of the colloid carcinomas and 13% (2/15) of the medullary carcinomas. In contrast, int-2 was not amplified in non-comedo DCIS and invasive ductal carcinomas with adjacent non-comedo DCIS lesions. A significant association was observed between int-2 amplification in the in situ components and adjacent invasive lesion (P<0.05). All tumors with int-2 amplification in the in situ lesions (7/7) also demonstrated same degree of amplification in the adjacent invasive components. However, 9% (5/53) of the tumors with no amplified int-2 gene in the in situ components showed int-2 amplification in the adjacent invasive lesions. A significant relationship was noted between amplification of int-2 and lymph node metastases (P<0.05) and poorly differentiated tumors (P<0.05) but not with estrogen receptor status (P>0.05) and proliferation index (Ki-67 and PCNA) (P>0.05). In Malaysia, majority of the patients belong to younger age group (<50 years old) but a comparison of the age groups showed that the amplification of int-2 was not statistically associated with patient age (P>0.05). These observations indicate that amplification of int-2 tends to strengthen the view that int-2 may have the potential to be an indicator of poor prognosis regardless of the age of the patient. Moreover, the presence of int-2 amplification in preinvasive, preinvasive and adjacent invasive lesions, and invasive carcinomas suggest that int-2 could be a marker of genetic instability occurring in early and late stages of tumor development.

Related Articles

Journal Cover

August 2001
Volume 8 Issue 2

Print ISSN: 1107-3756
Online ISSN:1791-244X

Sign up for eToc alerts

Recommend to Library

Copy and paste a formatted citation
x
Spandidos Publications style
Naidu R, Wahab NA, Yadav M, Kutty MK and Nair S: Detection of amplified int-2/FGF-3 gene in primary breast carcinomas using differential polymerase chain reaction. Int J Mol Med 8: 193-198, 2001.
APA
Naidu, R., Wahab, N.A., Yadav, M., Kutty, M.K., & Nair, S. (2001). Detection of amplified int-2/FGF-3 gene in primary breast carcinomas using differential polymerase chain reaction. International Journal of Molecular Medicine, 8, 193-198. https://doi.org/10.3892/ijmm.8.2.193
MLA
Naidu, R., Wahab, N. A., Yadav, M., Kutty, M. K., Nair, S."Detection of amplified int-2/FGF-3 gene in primary breast carcinomas using differential polymerase chain reaction". International Journal of Molecular Medicine 8.2 (2001): 193-198.
Chicago
Naidu, R., Wahab, N. A., Yadav, M., Kutty, M. K., Nair, S."Detection of amplified int-2/FGF-3 gene in primary breast carcinomas using differential polymerase chain reaction". International Journal of Molecular Medicine 8, no. 2 (2001): 193-198. https://doi.org/10.3892/ijmm.8.2.193