A functional genomics approach for the identification of putative tumor suppressor genes: Dickkopf-1 as suppressor of HeLa cell transformation

doi:10.1093/carcin/bgg190

Carcinogenesis Advance Access originally published online on October 10, 2003

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Carcinogenesis, Vol. 25, No. 1, 47-59, January 2004
© Oxford University Press; all rights reserved

CANCER BIOLOGY

A functional genomics approach for the identification of putative tumor suppressor genes: Dickkopf-1 as suppressor of HeLa cell transformation

Andrei M. Mikheev¹, Svetlana A. Mikheeva², Binrong Liu³, Pinchas Cohen³ and Helmut Zarbl¹^,4

¹ Program in Cancer Biology, Division of Public Health, Fred Hutchinson Cancer Research Center Seattle, WA 98104-2092, USA, ² Department of Pediatrics, University of Washington Seattle, WA 98195, USA and ³ Department of Pediatrics, University of California, Los Angeles, CA 90095, USA

We described previously the isolation and characterization oftwo non-tumorigenic revertants from the HeLa cervical carcinomacell line, and demonstrated that loss of the transformed phenotypein these cells was the result of dominant somatic mutations.The goal of the present study was to use cDNA microarrays toidentify candidate tumor suppressors among the set of geneswhose increased expression correlated with loss of tumorigenicityin both revertants. Among the genes with significantly increasedexpression levels in both HA and HF revertants we identifiedInsulin Growth Factor Binding Protein-3 (IGFBP-3) and the Dickkopf-1(DKK-1) genes. Both of these genes encode secreted proteinsimplicated in the modulation cell growth and differentiation,and IGFBP-3 was shown previously to have tumor suppressing activity.To test the hypothesis that increased expression of IGFBP-3or the DKK-1 genes could have contributed to the suppressionof tumorigenicity in the revertants, we expressed IGFBP-3 orDKK-1 in HeLa cells, and assessed their effects on anchoragedependent and independent growth, and tumor formation in athymicnude mice. Ectopic expression of IGFBP-3 or DKK-1 resulted insignificantly decreased growth in soft agar. HeLa cells expressingectopic IGFBP-3 or DKK-1 showed statistically significant differencesin the kinetics of tumor formation. In any tumors that arosein animals injected with the IGFBP-3 expressing cells, therewas a complete loss of IGFBP-3 activity, as measured by bindingto IGF-1 and IGF-2 proteins. All tumors that arose after injectionof cells expressing DKK-1, invariably showed almost a completeloss of ectopic DKK-1 expression. The observations that lossof DKK-1 expression or IGFBP-3 activity was required for tumorigenicitysuggested that both proteins encode putative tumor suppressorgenes. We also show that while DKK-1 expression does not affectcell growth in vitro, the protein does sensitize cells to apoptosis.We also demonstrated that effect of DKK-1 was not due to inhibitionof ß-catenin/TCF4-regulated transcription. Taken together,our results indicate that somatic cell genetics combining withgene expression profiling may be a useful approach for the identificationof functional suppressors of malignant cell growth.

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