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Institute of Tumor Biology, University Medical Center, Martinister. 52, 20246 Hamburg, Germany
¹ Institute of Pathology, University of Münster, Münster, Germany
² Institute of Pathology, Institute of Pathology, Cologne, Germany
³ Departement de Biologie Clinique, Institut Gustave-Roussy Villejuif and Faculté des Sciences Pharmaceutiques et Biologiques de Paris, FRE2443 CNRS, Université René Decartes, Paris 5, France
⁴ Institute of Pathology, University of Basle, Basle, Switzerland
⁵ Institute of Immunology, University of Witten/Herdecke, Witten, Germany

(Requests for offprints should be addressed to B Brandt; Email: bu.brandt{at}uke.uni-hamburg.de)

Early placenta insulin-like growth factor (EPIL) is expressed by a subpopulation of the Her2-positive SKBR3 breast cancer cell line displaying high motility and transendothelial invasiveness in vitro, as recently shown by our group. As a consequence of this, we established cellular models by generating an EPIL-overexpressing SKBR3 cell line, knocked down EPIL by adding specific small interfering RNA (siRNA) to those cells and produced EPIL-enriched and depleted serum-free culture media. EPIL-expressing cells as well as EPIL-induced SKBR3 cells acquired a high capacity for transendothelial invasiveness. We observed a thin and outspread morphology caused by enhanced formation of lamellipodia, i.e. protrusions in the initial phase of motility. In parallel, Her2-positive MDAHer2 breast cancer cells also showed increased invasiveness when induced by EPIL-conditioned medium. A downstream signaling impact of EPIL could be observed in the form of reduced phosphorylation of Her2, erk1/2 and akt, while phospholipase C1 phophorylation remained unaffected. As an in vivo model for highly motile tumor cells, Paget’s disease of the nipple showed simultaneous EPIL and Her2 expression upon immunohistochemical examination using specific antibodies. Such experimental data have been translated to a clinical setting by using a prognostic tissue microarray established from 603 breast cancer cases. Survival data analysis found a significant association between expression levels of EPIL and 5-year overall survival that was dose dependent: EPIL (negative) 84%, EPIL (moderately positive) 77%, EPIL (strongly positive) 48% (P<0.005). One particular subgroup (7.6% of the cases with full clinical records) that comprised tumors simultaneously expressing EPIL and Her2 represented patients with the poorest 5-year overall survival. The results suggested that EPIL might be a cancer cell-produced growth factor that influences lateral Her2 signaling. Moreover, EPIL may be induced by factors apart from Her2 and may independently provide signaling for cancer invasion and motility.

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