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author Gil, Veronica
Miranda, Susana
Riisnaes, Ruth
Gurel, Bora
D’Ambrosio, Mariantonietta
Vasciaveo, Alessandro
Crespo, Mateus
Ferreira, Ana
Brina, Daniela
Troiani, Martina
Sharp, Adam
Sheehan, Beshara
Christova, Rossitza
Seed, George
Figueiredo, Ines
Lambros, Maryou
Dolling, David
Rekowski, Jan
Alajati, Abdullah
Clarke, Matthew
Pereira, Rita
Flohr, Penny
Fowler, Gemma
Boysen, Gunther
Sumanasuriya, Semini
Bianchini, Diletta
Rescigno, Pasquale
Aversa, Caterina
Tunariu, Nina
Guo, Christina
Paschalis, Alec
Bertan, Claudia
Buroni, Lorenzo
Ning, Jian
Carreira, Suzanne
Workman, Paul
Swain, Amanda
Califano, Andrea
Shen, Michael M.
Alimonti, Andrea
Neeb, Antje
Welti, Jonathan
Yuan, Wei
de Bono, Johann
author_facet Gil, Veronica
Miranda, Susana
Riisnaes, Ruth
Gurel, Bora
D’Ambrosio, Mariantonietta
Vasciaveo, Alessandro
Crespo, Mateus
Ferreira, Ana
Brina, Daniela
Troiani, Martina
Sharp, Adam
Sheehan, Beshara
Christova, Rossitza
Seed, George
Figueiredo, Ines
Lambros, Maryou
Dolling, David
Rekowski, Jan
Alajati, Abdullah
Clarke, Matthew
Pereira, Rita
Flohr, Penny
Fowler, Gemma
Boysen, Gunther
Sumanasuriya, Semini
Bianchini, Diletta
Rescigno, Pasquale
Aversa, Caterina
Tunariu, Nina
Guo, Christina
Paschalis, Alec
Bertan, Claudia
Buroni, Lorenzo
Ning, Jian
Carreira, Suzanne
Workman, Paul
Swain, Amanda
Califano, Andrea
Shen, Michael M.
Alimonti, Andrea
Neeb, Antje
Welti, Jonathan
Yuan, Wei
de Bono, Johann
author_sort Gil, Veronica
collection PubMed
description It has been recognized for decades that ERBB signaling is important in prostate cancer, but targeting ERBB receptors as a therapeutic strategy for prostate cancer has been ineffective clinically. However, we show here that membranous HER3 protein is commonly highly expressed in lethal prostate cancer, associating with reduced time to castration resistance (CR) and survival. Multiplex immunofluorescence indicated that the HER3 ligand NRG1 is detectable primarily in tumor-infiltrating myelomonocytic cells in human prostate cancer; this observation was confirmed using single-cell RNA sequencing of human prostate cancer biopsies and murine transgenic prostate cancer models. In castration-resistant prostate cancer (CRPC) patient-derived xenograft organoids with high HER3 expression as well as mouse prostate cancer organoids, recombinant NRG1 enhanced proliferation and survival. Supernatant from murine bone marrow–derived macrophages and myeloid-derived suppressor cells promoted murine prostate cancer organoid growth in vitro, which could be reversed by a neutralizing anti-NRG1 antibody and ERBB inhibition. Targeting HER3, especially with the HER3-directed antibody–drug conjugate U3-1402, exhibited antitumor activity against HER3-expressing prostate cancer. Overall, these data indicate that HER3 is commonly overexpressed in lethal prostate cancer and can be activated by NRG1 secreted by myelomonocytic cells in the tumor microenvironment, supporting HER3-targeted therapeutic strategies for treating HER3-expressing advanced CRPC. SIGNIFICANCE: HER3 is an actionable target in prostate cancer, especially with anti-HER3 immunoconjugates, and targeting HER3 warrants clinical evaluation in prospective trials.
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spelling pubmed-89323362022-06-15 HER3 Is an Actionable Target in Advanced Prostate Cancer Gil, Veronica Miranda, Susana Riisnaes, Ruth Gurel, Bora D’Ambrosio, Mariantonietta Vasciaveo, Alessandro Crespo, Mateus Ferreira, Ana Brina, Daniela Troiani, Martina Sharp, Adam Sheehan, Beshara Christova, Rossitza Seed, George Figueiredo, Ines Lambros, Maryou Dolling, David Rekowski, Jan Alajati, Abdullah Clarke, Matthew Pereira, Rita Flohr, Penny Fowler, Gemma Boysen, Gunther Sumanasuriya, Semini Bianchini, Diletta Rescigno, Pasquale Aversa, Caterina Tunariu, Nina Guo, Christina Paschalis, Alec Bertan, Claudia Buroni, Lorenzo Ning, Jian Carreira, Suzanne Workman, Paul Swain, Amanda Califano, Andrea Shen, Michael M. Alimonti, Andrea Neeb, Antje Welti, Jonathan Yuan, Wei de Bono, Johann Cancer Res Translational Science It has been recognized for decades that ERBB signaling is important in prostate cancer, but targeting ERBB receptors as a therapeutic strategy for prostate cancer has been ineffective clinically. However, we show here that membranous HER3 protein is commonly highly expressed in lethal prostate cancer, associating with reduced time to castration resistance (CR) and survival. Multiplex immunofluorescence indicated that the HER3 ligand NRG1 is detectable primarily in tumor-infiltrating myelomonocytic cells in human prostate cancer; this observation was confirmed using single-cell RNA sequencing of human prostate cancer biopsies and murine transgenic prostate cancer models. In castration-resistant prostate cancer (CRPC) patient-derived xenograft organoids with high HER3 expression as well as mouse prostate cancer organoids, recombinant NRG1 enhanced proliferation and survival. Supernatant from murine bone marrow–derived macrophages and myeloid-derived suppressor cells promoted murine prostate cancer organoid growth in vitro, which could be reversed by a neutralizing anti-NRG1 antibody and ERBB inhibition. Targeting HER3, especially with the HER3-directed antibody–drug conjugate U3-1402, exhibited antitumor activity against HER3-expressing prostate cancer. Overall, these data indicate that HER3 is commonly overexpressed in lethal prostate cancer and can be activated by NRG1 secreted by myelomonocytic cells in the tumor microenvironment, supporting HER3-targeted therapeutic strategies for treating HER3-expressing advanced CRPC. SIGNIFICANCE: HER3 is an actionable target in prostate cancer, especially with anti-HER3 immunoconjugates, and targeting HER3 warrants clinical evaluation in prospective trials. American Association for Cancer Research 2021-12-15 2021-11-09 /pmc/articles/PMC8932336/ /pubmed/34753775 http://dx.doi.org/10.1158/0008-5472.CAN-21-3360 Text en ©2021 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license.
spellingShingle Translational Science
Gil, Veronica
Miranda, Susana
Riisnaes, Ruth
Gurel, Bora
D’Ambrosio, Mariantonietta
Vasciaveo, Alessandro
Crespo, Mateus
Ferreira, Ana
Brina, Daniela
Troiani, Martina
Sharp, Adam
Sheehan, Beshara
Christova, Rossitza
Seed, George
Figueiredo, Ines
Lambros, Maryou
Dolling, David
Rekowski, Jan
Alajati, Abdullah
Clarke, Matthew
Pereira, Rita
Flohr, Penny
Fowler, Gemma
Boysen, Gunther
Sumanasuriya, Semini
Bianchini, Diletta
Rescigno, Pasquale
Aversa, Caterina
Tunariu, Nina
Guo, Christina
Paschalis, Alec
Bertan, Claudia
Buroni, Lorenzo
Ning, Jian
Carreira, Suzanne
Workman, Paul
Swain, Amanda
Califano, Andrea
Shen, Michael M.
Alimonti, Andrea
Neeb, Antje
Welti, Jonathan
Yuan, Wei
de Bono, Johann
HER3 Is an Actionable Target in Advanced Prostate Cancer
title HER3 Is an Actionable Target in Advanced Prostate Cancer
title_full HER3 Is an Actionable Target in Advanced Prostate Cancer
title_fullStr HER3 Is an Actionable Target in Advanced Prostate Cancer
title_full_unstemmed HER3 Is an Actionable Target in Advanced Prostate Cancer
title_short HER3 Is an Actionable Target in Advanced Prostate Cancer
title_sort her3 is an actionable target in advanced prostate cancer
topic Translational Science
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8932336/
https://www.ncbi.nlm.nih.gov/pubmed/34753775
http://dx.doi.org/10.1158/0008-5472.CAN-21-3360
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