AKT Signaling Pathway in Invasive Ductal Carcinoma of the Breast: Correlation with ERα,ERβ and HER-2 Expression

Abstract

Aims and background

Estradiol exerts most of its effects by direct binding to the estrogen receptor in breast carcinoma, ERβ expression is a useful biomarker for breast cancer in a manner that is independent of ERα expression. However, studies evaluating ERβ expression with certain tumor variables, such as tumor grade and disease-free survival, had produced conflicting results. The Akt signaling pathway currently attracts considerable attention as a new target for effective therapeutic strategies. The current study attempted to compare the relative associations of variables including ERα, ERβ, HER-2/neu and AKT staining with the presence of metastases or survival.

Methods and study design

Immunohistochemical staining was employed to determine the expression of ERα, ERβ, pAkt and HER-2/neu in 110 cases of primary breast carcinoma.

Results

Positive ERα, ERβ, pAkt and HER-2/neu expressions were respectively observed in 46.4% (51/110), 59.1% (65/110), 40.9% (45/110) and 31.8% (35/110) of the tumors. pAkt was significantly associated with HER-2/neu overexpression (P <0.005) and axillary lymph node metastasis (P <0.05). However, there was no significant relationship between pAkt and ERα, ERβ, p53 (P >0.05) expressions. Survival analysis showed that pAkt positivity was associated with poor disease-free survival of the patients.

Conclusions

The current study suggested that activity of the Akt signaling pathway may indicate a poor prognosis in patients with breast carcinoma. The results implied that estrogen can activate the PI3K-Akt pathway through ERα and ERβ-independent mechanisms in breast cancer.

Keywords

Akt breast neoplasm estrogen receptor-α estrogen receptor-β HER-2

Get full access to this article

View all access options for this article.

References

Nakopoulou

, Lazaris

A.C.

, Panayotopoulou

E.G.

, Giannopoulou

, Givalos

, Markaki

, Keramopoulos

: The favourable prognostic value of oestrogen receptor β immunohistochemical expression in breast cancer. J Clin Pathol, 57: 523–528, 2004.

Balfe

P.J.

, McCann

A.H.

, Welch

H.M.

, Kerin

M.J.

: Estrogen receptor β and breast cancer. Eur J Surg Oncol, 30: 1043–1050, 2004.

Weihua

, Andersson

, Cheng

, Simpson

E.R.

, Warner

, Gustafsson

J.A.

: Update on estrogen signaling. FEBS Lett, 546: 17–24, 2003.

Omoto

, Eguchi

, Yamamoto-Yamaguchi

, Hayashi

: Estrogen receptor (ER) β1 and ERβcx/β2 inhibit ERα function differently in breast cancer cell line MCF7. Oncogene, 22: 5011–5020, 2003.

Zhou

, Tan

, Stone Hawthorne

, Klos

K.S.

, Lan

K.H.

, Yang

, Smith

T.L.

, Shi

, Yu

: Activation of the Akt/mammalian target of rapamycin/4E-BP1 pathway by ErbB2 overexpression predicts tumor progression in breast cancers. Clin Cancer Res, 10: 6779–6788, 2004.

Sengupta

, Jordan

V.C.

: Selective estrogen modulators as an anticancer tool: mechanisms of efficiency and resistance. Adv Exp Med Biol, 630: 206–219, 2008.

Clark

A.S.

, West

, Streicher

, Dennis

P.A.

: Constitutive and inducible Akt activity promotes resistance to chemotherapy, trastuzumab, or tamoxifen in breast cancer cells. Mol Cancer Ther, 1: 707–717, 2002.

Goldhirsch

, Glick

J.H.

, Gelber

R.D.

, Senn

H.J.

: Meeting highlights: international expert consensus on the primary therapy of early breast cancer. J Natl Cancer Inst, 90: 1601–1608, 1998.

Tokunaga

, Kimura

, Oki

, Ueda

, Futatsugi

, Mashino

, Yamamoto

, Ikebe

, Kakeji

, Baba

, Maehara

: Akt is frequently activated in HER2/neu-positive breast cancers and associated with poor prognosis among hormone treated patients. Int J Cancer, 118: 284–289, 2006.

10.

Freitas

, Moore

D.H.

, Michael

, Kelley

M.R.

: Studies of aporinic/apyrimidinic endonuclease/ref-1 expression in epithelial ovarian cancer: correlations with tumor progression and platinum resistance. Clin Cancer Res, 9: 4689–4694, 2003.

11.

Normanno

, Morabito

, De Luca

, Piccirillo

M.C.

, Gallo

, Maiello

M.R.

, Perrone

: Target-based therapies in breast cancer: current status and future perspectives. Endcr Relat Cancer, 16: 675–702, 2009.

12.

Massarweh

, Schiff

: Resistance to endocrine therapy in breast cancer: exploiting estrogen receptor/growth factor signaling crosstalk. Endocr Relat Cancer, Suppl 1: S15–24, 2006.

13.

Wallin

J.J.

, Guan

, Prior

W.W.

, Edgar

K.A.

, Kassees

, Sampath

, Belvin

, Friedman

L.S.

: Nuclear phospho-Akt increase predicts synergy of PI3K inhibition and doxorubicin in breast and ovarian cancer. Sci Transl Med, 2: 48ra66, 2010.

14.

Park

S.S.

, Kim

S.W.

: Activated Akt signaling pathway in invasive ductal carcinoma of the breast: correlation with HER2 overexpression. Oncol Rep, 18: 139–143, 2007.

15.

Jordan

V.C.

, O'Malley

B.W.

: Selective estrogen-receptor modulators and antihormonal resistance in breast cancer. J Clin Oncol, 25: 5815–5824, 2007.

16.

Tokunaga

, Kataoka

, Kimura

, Oki

, Mashino

, Nishida

, Koga

, Morita

, Kakeji

, Baba

, Ohno

, Maehara

: The association between Akt activation and resistance to hormone therapy in metastatic breast cancer. Eur J Cancer, 42: 629–635, 2006.

17.

Simoncini

, Hafezi-Moghadam

, Brazil

D.P.

, Ley

, Chin

W.W.

, Liao

J.K.

: Interaction of oestrogen receptor with the regulatory subunit of phosphatidylinositol-3-OH kinase. Nature (Lond), 407: 538–541, 2000.

18.

Pancholi

, Lykkesfeldt

A.E.

, Hilmi

, Banerjee

, Leary

, Drury

, Johnston

, Dowsett

, Martin

L.A.

: ERBB2 influences the subcellular localization of the estrogen receptor in tamoxifen-resistant MCF-7 cells leading to the activation of AKT and RPS6KA2. Endocr Relat Cancer, 15: 985–1002, 2008.

19.

Knuefermann

, Lu

, Liu

, Jin

, Liang

, Wu

, Schmidt

, Mills

G.B.

, Mendelsohn

, Fan

: HER2/PI3K/Akt activation leads to a multidrug resistance in human breast adenocarcinoma cells. Oncogene, 22: 3205–3212, 2003.

20.

Charlier

, Chariot

, Antoine

, Merville

M.P.

, Gielen

, Castronovo

: Tamoxifen and its active metabolite inhibit growth of estrogen receptor-negative MDA-MB-435 cells. Biochem Pharmacol, 49: 351–358, 1995.

21.

Speirs

, Carder

P.J.

, Lane

, Dodwell

, Lansdown

M.R.

, Hanby

A.M.

: Oestrogen receptor β: what it means for patients with breast cancer. Lancet Oncol, 5: 174–181, 2004.

22.

Duong

B.N.

, Elliott

, Frigo

D.E.

, Melnik

L.I.

, Vanhoy

, Tomchuck

, Lebeau

H.P.

, David

, Beckman

B.S.

, Alam

, Bratton

M.R.

, McLachlan

J.A.

, Burow

M.E.

: Akt regulation of estrtogen receptor β transcriptional activity in breast cancer. Cancer Res, 66: 8373–8381, 2006.