Ivermectin inhibits HSP27 and potentiates efficacy of oncogene targeting in tumor models
Lucia Nappi, … , Gary D. Brayer, Martin Gleave
Lucia Nappi, … , Gary D. Brayer, Martin Gleave
Published December 17, 2019
Citation Information: J Clin Invest. 2020;130(2):699-714. https://doi.org/10.1172/JCI130819.
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Research Article Oncology

Ivermectin inhibits HSP27 and potentiates efficacy of oncogene targeting in tumor models

Abstract

HSP27 is highly expressed in, and supports oncogene addiction of, many cancers. HSP27 phosphorylation is a limiting step for activation of this protein and a target for inhibition, but its highly disordered structure challenges rational structure-guided drug discovery. We performed multistep biochemical, structural, and computational experiments to define a spherical 24-monomer complex composed of 12 HSP27 dimers with a phosphorylation pocket flanked by serine residues between their N-terminal domains. Ivermectin directly binds this pocket to inhibit MAPKAP2-mediated HSP27 phosphorylation and depolymerization, thereby blocking HSP27-regulated survival signaling and client-oncoprotein interactions. Ivermectin potentiated activity of anti–androgen receptor and anti-EGFR drugs in prostate and EGFR/HER2-driven tumor models, respectively, identifying a repurposing approach for cotargeting stress-adaptive responses to overcome resistance to inhibitors of oncogenic pathway signaling.

Authors

Lucia Nappi, Adeleke H. Aguda, Nader Al Nakouzi, Barbara Lelj-Garolla, Eliana Beraldi, Nada Lallous, Marisa Thi, Susan Moore, Ladan Fazli, Dulguun Battsogt, Sophie Stief, Fuqiang Ban, Nham T. Nguyen, Neetu Saxena, Evgenia Dueva, Fan Zhang, Takeshi Yamazaki, Amina Zoubeidi, Artem Cherkasov, Gary D. Brayer, Martin Gleave

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Figure 5

Ivermectin reverses taxane resistance in prostate cancer cells.

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Ivermectin reverses taxane resistance in prostate cancer cells. (A) Immu...
(A) Immunoblotting analysis of p-HSP27 and total HSP27 in PC3 parental (WT) and PC3 docetaxel-resistant (DR) cells. (B) Cell survival of PC3-DR treated with docetaxel (DTX), IVM, and the combination of both drugs for 4 days. Data shown as mean ± SEM; ****P < 0.0001 by ANOVA with Bonferroni’s correction. (C) Immunoblotting analysis of p-HSP27 and cleaved PARP in PC3-DR cells treated with increasing doses of IVM for 24 hours. (D) Tumor volume of PC3-DR xenografts treated with control (normal saline), IVM (10 mg/kg orally, every other day), micellar paclitaxel (0.5 mg i.v., 3 times per week, every other week), IVM (10 mg/kg by gavage, 3 times per week), and the combination of both drugs. Data shown as mean ± SEM; ****P < 0.0001; n = 8–14; compared by ANOVA followed by Tukey’s correction. (E) Representative images of immunohistochemical analysis of p-HSP27, TUNEL, and Ki-67 on PC3-DR xenografts treated as specified in D. Scale bars: 100 μm.