Increased Activator Protein-1 DNA Binding and c-Jun NH2-Terminal Kinase Activity in Human Breast Tumors with Acquired Tamoxifen Resistance

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Increased Activator Protein-1 DNA Binding and c-Jun NH₂-Terminal Kinase Activity in Human Breast Tumors with Acquired Tamoxifen Resistance¹

Stephen R. D. Johnston², Biao Lu, Gary K. Scott, Peter J. Kushner, Ian E. Smith, Mitchell Dowsett and Christopher C. Benz

Departments of Medicine [S. R. D. J., I. E. S.] and Academic Biochemistry [S. R. D. J., M. D.], Royal Marsden Hospital and Institute of Cancer Research, London, SW3 6JJ, England; and Department of Medicine and Cancer Research Institute [B. L., G. K. S., C. C. B.] and Metabolic Research Unit [P. J. K.], University of California, San Francisco, California 94143

Human breast tumors that are initially responsive to tamoxifen(TAM) eventually relapse during treatment. Estrogen receptor(ER) expression and function are often preserved in these tumors,and clinical evidence suggests that this relapse may be relatedto TAM’s known agonistic properties. ER can interact withthe activator protein-1 (AP-1) transcription factor complexthrough protein-protein interactions that are independent ofER DNA binding and, in certain ER-positive cells, this may allowTAM to exert an agonist response on AP-1-regulated genes. We,therefore, assessed both AP-1 DNA binding and the known AP-1activating enzyme, c-Jun NH₂-terminal kinase (JNK), in a panelof 30 ER-positive primary human breast tumors with acquiredTAM resistance, as compared to a matched panel of 27 untreatedcontrol ER-positive breast tumors and a separate control setof 14 primary tumors, which included 7 ER-positive tumors thatwere growth-arrested by 3 months of preoperative TAM. AP-1 DNAbinding activity was measured from cryopreserved tumor extractsusing a labeled oligonucleotide probe containing a consensusAP-1 response element by electrophoretic mobility shift assay.JNK was first extracted from the tumor lysates by incubationover a Sepharose-bound c-Jun(1–89) fusion protein, andits activity was then measured by chemiluminescent Western blotby detection of the phosphorylated product using a phospho-Jun(Ser-63)-specificprimary antibody. The set of control ER-positive breast tumorsgrowth arrested by TAM showed no significant difference fromuntreated control tumors in their AP-1 DNA binding and JNK activities.In contrast, there was a significant (P < 0.001) increasein mean AP-1 DNA binding activity for the panel of ER-positiveTAM-resistant (TAM-R) tumors as compared to its matched controlpanel of untreated tumors. Mean JNK activity in the TAM-R tumorswas also significantly higher than that found in the untreatedtumors (P = 0.038). Overall, there was no significant correlationbetween JNK activity and AP-1 DNA binding; however, regressionanalysis showed that, for any given level of JNK activity, theTAM-R tumors possessed a 3.5-fold increase in AP-1 DNA bindingactivity as compared to the untreated tumors. These findingsindicate that, when compared to untreated ER-positive primarybreast tumors, TAM-R tumors demonstrate significantly increasedlevels of AP-1 DNA binding and JNK activity, consistent withexperimental models suggesting that TAM-stimulated ER-positivetumor growth may be mediated by enhanced AP-1 transcriptionalactivity. These observations support the need for further evaluationof these markers in breast tumors as predictors of TAM resistance.

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