Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors

Bortezomib and the other licensed 20S proteasome inhibitors show robust activity against liquid tumors like multiple myeloma, but have disappointed against solid tumors including ovarian cancer. Consequently, interest is mounting in alternative non-peptide based drugs targeting the proteasome’s 19S...

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Autores principales: Anchoori, Ravi K., George, Logan, Tseng, Ssu-Hsueh, Lam, Brandon, Polkampally, Srinidhi, Amiano, Anjali D., Foran, Palmer, Tsingine, Hannah, Samanapally, Harideep, Carrizo Velasquez, Fernanda, Das, Samarjit, Xing, Deyin, Bin Salam, Ahmad, Karanam, Balasubramanyam, Hung, Chien-Fu, Roden, Richard B. S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8432795/
https://www.ncbi.nlm.nih.gov/pubmed/34506530
http://dx.doi.org/10.1371/journal.pone.0256937
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author Anchoori, Ravi K.
George, Logan
Tseng, Ssu-Hsueh
Lam, Brandon
Polkampally, Srinidhi
Amiano, Anjali D.
Foran, Palmer
Tsingine, Hannah
Samanapally, Harideep
Carrizo Velasquez, Fernanda
Das, Samarjit
Xing, Deyin
Bin Salam, Ahmad
Karanam, Balasubramanyam
Hung, Chien-Fu
Roden, Richard B. S.
author_facet Anchoori, Ravi K.
George, Logan
Tseng, Ssu-Hsueh
Lam, Brandon
Polkampally, Srinidhi
Amiano, Anjali D.
Foran, Palmer
Tsingine, Hannah
Samanapally, Harideep
Carrizo Velasquez, Fernanda
Das, Samarjit
Xing, Deyin
Bin Salam, Ahmad
Karanam, Balasubramanyam
Hung, Chien-Fu
Roden, Richard B. S.
author_sort Anchoori, Ravi K.
collection PubMed
description Bortezomib and the other licensed 20S proteasome inhibitors show robust activity against liquid tumors like multiple myeloma, but have disappointed against solid tumors including ovarian cancer. Consequently, interest is mounting in alternative non-peptide based drugs targeting the proteasome’s 19S regulatory particle subunit, including its ubiquitin receptor RPN13. RA183 and RA375 are more potent analogs of the prototypic inhibitor of RPN13 (iRPN13) called RA190, and they show promise for the treatment of ovarian cancer. Here we demonstrate that rendering these candidate RPN13 inhibitors chiral and asymmetric through the addition of a single methyl to the core piperidone moiety increases their potency against cancer cell lines, with the S-isomer being more active than the R-isomer. The enhanced cancer cell cytotoxicities of these compounds are associated with improved binding to RPN13 in cell lysates, ATP depletion by inhibition of glycolysis and mitochondrial electron chain transport, mitochondrial depolarization and perinuclear clustering, oxidative stress and glutathione depletion, and rapid accumulation of high molecular weight polyubiquitinated proteins with a consequent unresolved ubiquitin proteasome system (UPS) stress response. Cytotoxicity was associated with an early biomarker of apoptosis, increased surface annexin V binding. As for cisplatin, BRCA2 and ATM deficiency conferred increased sensitivity to these iRPN13s. Ubiquitination plays an important role in coordinating DNA damage repair and the iRPN13s may compromise this process by depletion of monomeric ubiquitin following its sequestration in high molecular weight polyubiquitinated protein aggregates. Indeed, a synergistic cytotoxic response was evident upon treatment of several ovarian cancer cell lines with either cisplatin or doxorubicin and our new candidate iRPN13s, suggesting that such a combination approach warrants further exploration for the treatment of ovarian cancer.
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spelling pubmed-84327952021-09-11 Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors Anchoori, Ravi K. George, Logan Tseng, Ssu-Hsueh Lam, Brandon Polkampally, Srinidhi Amiano, Anjali D. Foran, Palmer Tsingine, Hannah Samanapally, Harideep Carrizo Velasquez, Fernanda Das, Samarjit Xing, Deyin Bin Salam, Ahmad Karanam, Balasubramanyam Hung, Chien-Fu Roden, Richard B. S. PLoS One Research Article Bortezomib and the other licensed 20S proteasome inhibitors show robust activity against liquid tumors like multiple myeloma, but have disappointed against solid tumors including ovarian cancer. Consequently, interest is mounting in alternative non-peptide based drugs targeting the proteasome’s 19S regulatory particle subunit, including its ubiquitin receptor RPN13. RA183 and RA375 are more potent analogs of the prototypic inhibitor of RPN13 (iRPN13) called RA190, and they show promise for the treatment of ovarian cancer. Here we demonstrate that rendering these candidate RPN13 inhibitors chiral and asymmetric through the addition of a single methyl to the core piperidone moiety increases their potency against cancer cell lines, with the S-isomer being more active than the R-isomer. The enhanced cancer cell cytotoxicities of these compounds are associated with improved binding to RPN13 in cell lysates, ATP depletion by inhibition of glycolysis and mitochondrial electron chain transport, mitochondrial depolarization and perinuclear clustering, oxidative stress and glutathione depletion, and rapid accumulation of high molecular weight polyubiquitinated proteins with a consequent unresolved ubiquitin proteasome system (UPS) stress response. Cytotoxicity was associated with an early biomarker of apoptosis, increased surface annexin V binding. As for cisplatin, BRCA2 and ATM deficiency conferred increased sensitivity to these iRPN13s. Ubiquitination plays an important role in coordinating DNA damage repair and the iRPN13s may compromise this process by depletion of monomeric ubiquitin following its sequestration in high molecular weight polyubiquitinated protein aggregates. Indeed, a synergistic cytotoxic response was evident upon treatment of several ovarian cancer cell lines with either cisplatin or doxorubicin and our new candidate iRPN13s, suggesting that such a combination approach warrants further exploration for the treatment of ovarian cancer. Public Library of Science 2021-09-10 /pmc/articles/PMC8432795/ /pubmed/34506530 http://dx.doi.org/10.1371/journal.pone.0256937 Text en © 2021 Anchoori et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Anchoori, Ravi K.
George, Logan
Tseng, Ssu-Hsueh
Lam, Brandon
Polkampally, Srinidhi
Amiano, Anjali D.
Foran, Palmer
Tsingine, Hannah
Samanapally, Harideep
Carrizo Velasquez, Fernanda
Das, Samarjit
Xing, Deyin
Bin Salam, Ahmad
Karanam, Balasubramanyam
Hung, Chien-Fu
Roden, Richard B. S.
Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title_full Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title_fullStr Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title_full_unstemmed Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title_short Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors
title_sort chirality and asymmetry increase the potency of candidate adrm1/rpn13 inhibitors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8432795/
https://www.ncbi.nlm.nih.gov/pubmed/34506530
http://dx.doi.org/10.1371/journal.pone.0256937
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