RT Journal Article SR Electronic T1 Connexin43 pseudogene in breast cancer cells offers a novel therapeutic target JF Molecular Cancer Therapeutics JO Mol Cancer Ther FD American Association for Cancer Research SP 786 OP 793 DO 10.1158/1535-7163.MCT-08-0930 VO 8 IS 4 A1 Bier, Andrew A1 Oviedo-Landaverde, Irene A1 Zhao, Jing A1 Mamane, Yael A1 Kandouz, Mustapha A1 Batist, Gerald YR 2009 UL http://mct.aacrjournals.org/content/8/4/786.abstract AB Connexin43 (Cx43) is often deregulated in breast cancer tissue compared with normal adjacent tissue. Stable reexpression of Cx43 in cancer slows growth and renders the cells more sensitive to cytotoxic chemotherapeutics. Pseudogenes are often considered nonfunctional copies of DNA. The Cx43 pseudogene (ΨCx43) possesses all the features of an expressed gene and is exclusively transcribed in breast cancer cell lines and not in normal cells. ΨCx43 can be translated in vivo, and its protein exhibits growth-suppressive behavior similar to Cx43. We showed that ΨCx43 binds to the polyribosomes in breast cancer cells and that exogenous expression of ΨCx43 induces translational inhibition of Cx43. Furthermore, ΨCx43 is translated and binds more efficiently to the translational machinery than does Cx43 in an in vitro system. Following knockdown of ΨCx43 in breast cancer cells, we observed an increase in Cx43 RNA and protein. This results in increased cellular sensitivity to cytotoxic chemotherapy. Our results show that ΨCx43 acts as a posttranscriptional regulator of Cx43 in breast cancer cells, and that this represents an example of the regulation of genes by pseudogenes with potential therapeutic implications in cancer. [Mol Cancer Ther 2009;8(4):786–93]