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Characterization of the Recurrent 8p11-12 Amplicon Identifies PPAPDC1B, a Phosphatase Protein, as a New Therapeutic Target in Breast Cancer

¹ UMR 144, Centre National de la Recherche Scientifique, Institut Curie; ² Institut Curie, Centre de Recherche; ³ Institut Curie, Translational Research Department; ⁴ Institut National de la Sante et de la Recherche Medicale, U830, Institut Curie; ⁵ Département de Pathologie, Institut Curie; ⁶ Department of Surgery, Institut Curie; and ⁷ Unité de Génétique Somatique, Institut Curie, Paris, France

Requests for reprints: François Radvanyi, UMR 144, Centre National de la Recherche Scientifique, Institut Curie, 26 rue d'Ulm, 75248 Paris Cedex 05, France. Phone: 33-1-56-24-63-39; Fax: 33-1-56-24-63-49; E-mail: Francois.Radvanyi{at}curie.fr or Olivier Delattre, U830 Institut National de la Sante et de la Recherche Medicale, Institut Curie, 26 rue d'Ulm, 75248 Paris Cedex 05, France. Phone: 33-1-56-24-66-81; Fax: 33-1-56-24-66-30; E-mail: Olivier.Delattre{at}curie.fr.

Key Words: 8p11-12 amplicon • breast cancer • phosphatase

The 8p11-12 chromosome region is one of the regions most frequently amplified in breast carcinoma (10–15% of cases). Several genes within this region have been identified as candidate oncogenes, as they are both amplified and overexpressed. However, very few studies have explored the role of these genes in cell transformation, with the aim of identifying valuable therapeutic targets. An analysis of comparative genomic hybridization array and expression profiling data for a series of 152 ductal breast carcinomas and 21 cell lines identified five genes (LSM1, BAG4, DDHD2, PPAPDC1B, and WHSC1L1) within the amplified region as consistently overexpressed due to an increased gene copy number. The use of small interfering RNA to knock down the expression of each of these genes showed the major role played by two genes, PPAPDC1B and WHSC1L1, in regulating the survival and transformation of two different cell lines harboring the 8p amplicon. The role of these two genes in cell survival and cell transformation was also confirmed by long-term knockdown expression studies using short hairpin RNAs. The potential of PPAPDC1B, which encodes a transmembrane phosphatase, as a therapeutic target was further shown by the strong inhibition of growth of breast tumor xenografts displaying 8p11-12 amplification induced by the silencing of PPAPDC1B. The oncogenic properties of PPAPDC1B were further shown by its ability to transform NIH-3T3 fibroblasts, inducing their anchorage-independent growth. Finally, microarray experiments on PPAPDC1B knockdown indicated that this gene interfered with multiple cell signaling pathways, including the Janus-activated kinase-signal transducer and activator of transcription, mitogen-activated protein kinase, and protein kinase C pathways. PPAPDC1B may also potentiate the estrogen receptor pathway by down-regulating DUSP22. [Cancer Res 2008;68(17):7165–75]