Gene Expression of E-Selectin in Tissue and its Protein Level in Serum of Breast Cancer Patients

Abstract

Aims and background

This study aims to detect the expression of E-selectin in tissue and the serum level of its soluble form in patients with primary breast cancer and benign breast tumors and to correlate the results with the clinicopathological data of the subjects.

Methods

Fifty participants were included in the study and stratified into 3 subgroups. Group A comprised 30 patients with primary breast cancer, group B 9 patients with benign breast tumors, and group C 11 healthy control women undergoing reduction mammoplasty. E-selectin gene expression was investigated in breast tissues by PCR techniques and soluble E-selectin was measured in sera by ELISA.

Results

The E-selectin gene was expressed in 73.3% of group A, 44.4% of group B and 9.1% of group C. It was expressed in 61.5% of patients with grade 2 breast cancer and in 82.4% of patients with grade 3 breast cancer. E-selectin gene expression was detected in 60%, 73.3% and 100% of patients with stage II, III and IV tumors, respectively. It was detected in 81.8% of patients with node-positive primary breast cancer and in 50% of patients with node-negative cancer. PCR in situ hybridization was done to locate the site of E-selectin expression. E-selectin was found on the membranes of peritumoral endothelial cells while it was not found on breast epithelial cells. Serum levels of soluble E-selectin were significantly elevated in group A compared to groups B and C (P <0.001). They increased significantly with increasing breast cancer stage (P <0.001) and were significantly higher in patients with lymph node involvement than in patients without node involvement (P <0.001).

Conclusions

The studied marker showed associations with established prognostic parameters such as lymph node involvement and histological tumor grade. Further studies are needed to evaluate E-selectin as a possible target for antimetastat-ic therapy through modulation of the expression of the cell adhesion molecule. E-selectin can be regarded as a promising strategy in improving tumor therapy.

Keywords

breast cancer E-selectin gene expression

Get full access to this article

View all access options for this article.

References

Bewick

, Conlon

, Lee

, Parissenti

A.M.

, Zhang

, Gluck

: Evaluation of sICAM-1, sVCAM-1 and sE-selectin levels in patients with metastatic breast cancer receiving high-dose chemotherapy. Stem Cells Dev, 13: 281–294, 2004.

Zetter

B.R.

: Adhesion molecules in tumor metastasis. Semin Cancer Biol, 4: 219–229, 1993.

Frenette

P.S.

, Wagner

D.D.

: Adhesion molecules-part 1. N Engl J Med, 334: 1526–1529, 1996.

Frenette

P.S.

, Wagner

D.D.

: Adhesion molecules-part II: blood vessels and blood cells. N Engl J Med, 335: 43–45, 1996.

Meyer

, Hart

I.R.

: Mechanisms of tumour metastasis. Eur J Cancer, 34: 214–221, 1998.

Menger

M.D.

, Vollmar

: Adhesion molecules as determinants of disease: from molecular biology to surgical research. Br J Surg, 83: 588–601, 1996.

Gearing

A.J.

, Hemingway

, Pigott

, Hughes

, Rees

A.J.

, Cashman

S.J.

: Soluble forms of vascular adhesion molecules, E-selectin, ICAM-1, and VCAM-1: pathological significance. Ann NY Acad Sci, 667: 324–331, 1992.

Tesarova

, Kvasnicka

, Umlaufova

, Homolkova

, Kalousova

, Tesar

: Soluble adhesion molecules in female patients with breast carcinoma. Cas Lek Cesk, 142: 292–299, 2003.

Hebbar

, Peyrat

J.P.

: Significance of soluble endothelial molecule E-selectin in patients with breast cancer. Int J Biol Markers, 15: 15–21, 2000.

10.

Hebbar

, Revillion

, Louchez

M.M.

, Vilain

M.O.

, Fournier

, Bonneterre

, Peyrat

J.P.

: The relationship between concentrations of circulating soluble E-selectin and clinical, pathological, and biological features in patients with breast cancer. Clin Cancer Res, 4: 373–380, 1998.

11.

Eichbaum

M.H.

, de Rossi

T.M.

, Kaul

, Bastert

: Serum levels of soluble E-selectin are associated with the clinical course of metastatic disease in patients with liver metastases from breast cancer. Oncol Res, 14: 603–610, 2004.

12.

Hakomori

: Novel endothelial cell activation factor(s) released from activated platelets which induce E-selectin expression and tumor cell adhesion to endothelial cells: A preliminary note. Biochem Biophys Res Commun, 203: 605–613, 1994.

13.

Kaji

, Ishikura

, Kishimoto

, Omi

, Ishizu

, Kimura

: E-selectin expression induced by pancreas-carcinoma-derived interleukin-1 alpha results in enhanced adhesion of pancreas-carcinoma cells to endothelial cells. Int J Cancer, 60: 712–717, 1995.

14.

Bloom

, Richardson

: Histological grading and prognosis in breast cancer. Br J Cancer, 11: 359–363, 1957.

15.

American Joint Committee of Cancer (AJCC): Manual for staging of cancer, 3rd edition, JB Lippincott, Philadelphia, 1988.

16.

Heyl

, Handt

, Reister

, Gehlen

, Schroder

, Mitter-mayer

, Rath

: Elevated soluble adhesion molecules in women with preeclampsia. Do cytokines like tumor necrosis factor- and interleukin-1, cause endothelial activation? Eur J Obstet Gynecol Reprod Biol, 86: 35–41, 1999.

17.

Saunders

, Trapp

: Basic and clinical biostatistics, 2nd edition, pp 85–90, Appleton and Lange, Norwalk, USA, 1994.

18.

Valagussa

, Bonadonna

: Breast cancer. In: Cancer chemotherapy and biological response modifiers, Annual 19, Giaccone

, Schilsky

, Sondel

(Eds), pp 606–608, Elsevier Science BV, Amsterdam, 2001.

19.

Sheen-Chen

S.M.

, Eng

H.L.

, Huang

C.C.

, Chen

W.J.

: Serum levels of soluble E-selectin in women with breast cancer. Br J Surg, 91: 1578–1581, 2004.

20.

Izumi

, Taniuchi

, Tsuji

: Characterization of human colon carcinoma variant cells selected for sialyl Lex carbohydrate antigen: liver colonization and adhesion to vascular endothelial cells. Exp Cell Res, 216: 215–221, 1995.

21.

Lim

A.G.

, Jazrawi

, Levy

J.H.

, Deuds

A.C.

, Maxwell

J.D.

, Northfield

T.C.

: Soluble E-selectin and vascular cell adhesion molecule-1 (VCAM-1) in primary biliary cirrhosis. J Hepatol, 22: 416–422, 1995.

22.

Banks

R.E.

, Gearing

A.J.

, Hemingway

I.K.

, Norfolk

D.R.

, Perren

T.J.

, Selby

P.J.

: Circulating ICAM-1, E-selectin and VCAM-1 in human malignancies. Br J Cancer, 68: 122–124, 1993.

23.

Fox

S.B.

, Turner

G.D.

, Gatter

K.C.

, Harris

AL.

The increased expression of adhesion molecules ICAM-3, E- and P-se-lectins on breast cancer endothelium.

J Pathol, 177: 369–376, 1995.

24.

Narita

, Tunahashi

, Satoh

, Watanabe

, Sakamogo

, Takagi

: Association of expression of blood group related carbohydrate antigens with prognosis in breast cancer. Cancer, 7: 3044–3053, 1995.

25.

Narita

, Kawakami

, Matsuura

, Funahashi

, Kannagi

: Adhesion of breast cells to vascular endothelium mediated by sialyl Lewis x E-selectin. Breast Cancer, 3: 19–23, 1996.

26.

Biancone

, Araki

, Vassalli

, Stamenkovic

: Redirection of tumor metastasis by expression of E-selectin in vivo. J Exp Med, 183: 581–587, 1996.

27.

Matsuura

, Narita

, Mitsuoka

, Kimura

, Kannagi

, Imai

, Funahashi

, Takagi

: Increased concentration of soluble E-selectin in the sera of breast cancer patients. Anticancer Res, 17: 67–72, 1997.

28.

Nguyen

, Strubel

N.A.

, Bischoff

: A role for sialyl Lewis-X/A glycoconjugates in capillary morphogenesis. Nature, 365: 267–269, 1993.

29.

Koch

A.E.

, Halloran

M.M.

, Haskell

C.J.

, Shah

M.R.

, Polverimi

P.J.

: Angiogenesis mediated by soluble forms of E-selectin and vascular cell adhesion molecule-1. Nature, 376: 517–519, 1995.

30.

Griffioen

A.W.

, Damen

C.A.

, Blijham

G.H.

, Groenewegen

: Tumor angiogenesis is accompanied by a decreased inflammatory response of tumor-associated endothelium. Blood, 88: 667–673, 1996.

31.

O'Hanlon

D.M.

, Fitzsimons

, Lynch

, Tormey

, Malone

, Given

H.F.

: Soluble adhesion molecules (E-selectin, ICAM-1 and VCAM-1) in breast carcinoma. Eur J Cancer, 38: 2252–2257, 2002.

32.

Rosette

, Roth

R.B.

, Oeth

, Braun

, Kammerer

, Ekblom

, Denissenko

M.F.

: Role of ICAM1 in invasion of human breast cancer cells. Carcinogenesis, 26: 943–950, 2005.

33.

Matsuura

, Narita

, Mitsuoka

, Kimura

, Kannagi

, Imai

, Funahashi

, Takagi

: Increased level of circulating adhesion molecules in the sera of breast cancer patients with distant metastases. Jpn J Clin Oncol, 27: 35–39, 1997.