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Published May 2017 | Accepted Version + Supplemental Material
Journal Article Open

A pyrrole-imidazole polyamide is active against enzalutamide-resistant prostate cancer

Abstract

The LREX' prostate cancer model is resistant to the antiandrogen enzalutamide via activation of an alternative nuclear hormone receptor (NHR), glucocorticoid receptor (GR), which has similar DNA binding specificity to the androgen receptor (AR). Small molecules that target DNA to interfere with protein-DNA interactions may retain activity against enzalutamide-resistant prostate cancers where ligand binding domain antagonists are ineffective. We reported previously that a pyrrole-imidazole (Py-Im) polyamide designed to bind the consensus androgen response element half-site has antitumor activity against hormone-sensitive prostate cancer. In enzalutamide-resistant LREX' cells, Py-Im polyamide interfered with both androgen receptor- and glucocorticoid receptor-driven gene expression, while enzalutamide interfered with only that of androgen receptor. Genomic analyses indicated immediate interference with the androgen receptor transcriptional pathway. Long-term treatment with Py-Im polyamide demonstrated a global decrease in RNA levels consistent with inhibition of transcription. The polyamide was active against two enzalutamide-resistant xenografts with minimal toxicity. Overall, our results identify Py-Im polyamide as a promising therapeutic strategy in enzalutamide-resistant prostate cancer.

Additional Information

© 2017 American Association for Cancer Research. Received September 14, 2016. Revision received January 5, 2017. Accepted March 8, 2017. Published OnlineFirst March 30, 2017. The authors thank Rochelle Diamond at the Caltech flow cytometry facility for assistance. Disclosure of Potential Conflicts of Interest: F. Yang is the vice president (research) at and has ownership interest (including patents) in Gene Sciences, Inc. N.G. Nickols has ownership interest (including patents) in Gene Sciences, Inc. P.B. Dervan is the founder of, has ownership interest (including patents) in, and is a consultant/advisory board member for Gene Sciences, Inc. No potential conflicts of interest were disclosed by the other authors. Authors' Contributions: Conception and design: A.A. Kurmis, F. Yang, N.G. Nickols, P.B. Dervan; Development of methodology: A.A. Kurmis, F. Yang, T.R. Welch; Acquisition of data (provided animals, acquired and managed patients, provided facilities, etc.): A.A. Kurmis, F. Yang, T.R. Welch, N.G. Nickols; Analysis and interpretation of data (e.g., statistical analysis, biostatistics, computational analysis): A.A. Kurmis, F. Yang, N.G. Nickols, P.B. Dervan; Writing, review, and/or revision of the manuscript: A.A. Kurmis, F. Yang, N.G. Nickols, P.B. Dervan; Administrative, technical, or material support (i.e., reporting or organizing data, constructing databases): N.G. Nickols; Study supervision: P.B. Dervan. Grant Support: This work was supported by NIH grants GM27681 to P.B. Dervan and T32GM007616 to A.A. Kurmis.

Attached Files

Accepted Version - 0008-5472.CAN-16-2503.full.pdf

Supplemental Material - 00085472can162503-sup-171698_1_supp_3798002_2m21yt_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810768_jmj1yv_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810769_jmj1yw_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810770_wmw1yw_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810771_6m61yw_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810772_tmt1yx_eps_zip.zip

Supplemental Material - 00085472can162503-sup-171698_1_supp_3810773_gmg1yx_eps_zip.zip

Supplemental Material - 171698_1_supp_3811292_2jby6b.docx

Files

00085472can162503-sup-171698_1_supp_3810768_jmj1yv_eps_zip.zip

Additional details

Created:
August 19, 2023
Modified:
October 25, 2023