Antibody mediated CDCP1 degradation as mode of action for cancer targeted therapy

Gwendlyn Kollmorgen; Gerhard Niederfellner; Alexander Lifke; Gloria J Spohn; Natascha Rieder; Suzana Vega Harring; Frieder Bauss; Helmut Burtscher; Reiner Lammers; Birgit Bossenmaier

doi:10.1016/j.molonc.2013.08.009

Antibody mediated CDCP1 degradation as mode of action for cancer targeted therapy

Mol Oncol. 2013 Dec;7(6):1142-51. doi: 10.1016/j.molonc.2013.08.009. Epub 2013 Sep 3.

Authors

Gwendlyn Kollmorgen¹, Gerhard Niederfellner, Alexander Lifke, Gloria J Spohn, Natascha Rieder, Suzana Vega Harring, Frieder Bauss, Helmut Burtscher, Reiner Lammers, Birgit Bossenmaier

Affiliation

¹ Discovery Oncology, Pharmaceutical Research and Early Development (pRED), Roche Diagnostics GmbH, Nonnenwald 2, 82377 Penzberg, Germany.

Abstract

CUB-domain-containing-protein-1 (CDCP1) is an integral membrane protein whose expression is up-regulated in various cancer types. Although high CDCP1 expression has been correlated with poor prognosis in lung, breast, pancreas, and renal cancer, its functional role in tumor formation or progression is incompletely understood. So far it has remained unclear, whether CDCP1 is a useful target for antibody therapy of cancer and what could be a desired mode of action for a therapeutically useful antibody. To shed light on these questions, we have investigated the cellular effects of a therapeutic antibody candidate (RG7287). In focus formation assays, prolonged RG7287 treatment prevented the loss of contact inhibition caused by co-transformation of NIH3T3 cells with CDCP1 and Src. In a xenograft study, MCF7 cells stably overexpressing CDCP1 reached the predefined tumor volume faster than the parental MCF7 cells lacking endogenous CDCP1. This tumor growth advantage was abolished by RG7287 treatment. In vitro, RG7287 induced rapid tyrosine phosphorylation of CDCP1 by Src, which was accompanied by translocation of CDCP1 to a Triton X-100 insoluble fraction of the plasma membrane. Triggering these effects required bivalency of the antibody suggesting that it involves CDCP1 dimerization or clustering. However, this initial activation of CDCP1 was only transient and prolonged RG7287 treatment induced internalization and down-regulation of CDCP1 in different cancer cell lines. Antibody stimulated CDCP1 degradation required Src activity and was proteasome dependent. Also in three different xenograft models with endogenous CDCP1 expression RG7287 treatment resulted in significant tumor growth inhibition concomitant with substantially reduced CDCP1 levels as judged by immunohistochemistry and Western blotting. Thus, despite transiently activating CDCP1 signaling, the RG7287 antibody has a therapeutically useful mode of action.

Keywords: Antibody therapy; CDCP1; Contact inhibition; Src.

MeSH terms

Animals
Antibodies, Neoplasm / pharmacology*
Antigens, CD* / metabolism
Antigens, Neoplasm* / metabolism
Cell Adhesion Molecules* / antagonists & inhibitors
Cell Adhesion Molecules* / metabolism
Cell Line, Tumor
Cell Membrane / metabolism*
Cell Membrane / pathology
Humans
Membrane Glycoproteins* / antagonists & inhibitors
Membrane Glycoproteins* / metabolism
Mice
NIH 3T3 Cells
Neoplasm Proteins* / antagonists & inhibitors
Neoplasm Proteins* / metabolism
Neoplasms, Experimental* / drug therapy
Neoplasms, Experimental* / metabolism
Neoplasms, Experimental* / pathology
Proteolysis / drug effects*
Xenograft Model Antitumor Assays

Substances

Antibodies, Neoplasm
Antigens, CD
Antigens, Neoplasm
CDCP1 protein, human
CDCP1 protein, mouse
Cell Adhesion Molecules
Membrane Glycoproteins
Neoplasm Proteins