PT - JOURNAL ARTICLE AU - Meteoglu, Ibrahim AU - Dikicioglu, Emel AU - Erkus, Muhan AU - Culhaci, Nil AU - Kacar, Furuzan AU - Ozkara, Esra AU - Uyar, Meral TI - Breast carcinogenesis. Transition from hyperplasia to invasive lesions DP - 2005 Dec 01 TA - Saudi Medical Journal PG - 1889--1896 VI - 26 IP - 12 4099 - http://smj.org.sa/content/26/12/1889.short 4100 - http://smj.org.sa/content/26/12/1889.full SO - Saudi Med J2005 Dec 01; 26 AB - OBJECTIVE: To examine the balance loss between proliferation and apoptosis that play a role in breast cancer development, and to explore the places of various genes and molecules within this process in this supposed multistep process.METHODS: We obtained the specimens from 40 patients between 2002 and 2004 at the Department of Pathology, Medical Faculty, Adnan Menderes University, Aydin, Turkey. We categorized the lesions ductal hyperplasia (DH), atypical ductal hyperplasia (ADH), in situ ductal carcinoma (DCIS), and invasive ductal carcinoma (IDC). We determined the tumor size, histological grade and lymph node status of invasive cases and we used nottingham prognostic index (NPI). We applied ER, PR, c-erbB2, p53, Ki-67, bcl-2, dUTP nick end labeling (TUNEL), breast cancer gene-1, matrix metalloproteinases-1 and tissue inhibitor matrix metalloproteinases-1 stains to each lesion using the immunohistochemical method.RESULTS: We observed that ER and PR decreased in ADH when compared with DH (p=0.0001 and p=0.019). However, we determined that in DCIS as c-erbB2 (p=0,005) and Ki-67 (p=0.004) increase, TUNEL (p=0.04) and bcl-2 (p=0.005) decrease, when compared with ADH. When compared with DCIS lesions, we observed the existence of a higher c-erbB2 (p=0,003) and a lower TUNEL (p=0,012) in invasive tumors. Furthermore, we found that there is a higher MMP-1 (p=0,04) in invasive lesions, when compared with non-invasive lesions. We detected higher PR (p=0,049), lower TUNEL and c-erbB2 (p=0,017) in low grade group of NPI, when compared with high grade group of NPI.CONCLUSION: As a result, it has been shown that together with increase in proliferation, decrease in apoptosis, too, contributes to the proliferation/apoptosis imbalance that occurs in breast carcinogenesis. Increase in proliferation and decrease in apoptosis are parallel with the progression of lesions. We also showed that the changes, beginning with loss of ER and PR in ADH step, can cause malign transformation, which is especially notable both in DCIS step due to Ki-67 and c-erbB2 increase, and also with bcl-2 and TUNEL decrease.