Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases

The heparan sulfate (HS) mimic/heparanase inhibitor roneparstat (SST0001) shows antitumor activity in preclinical sarcoma models. We hypothesized that this 100% N-acetylated and glycol-split heparin could interfere with the functions of several receptor tyrosine kinases (RTK) coexpressed in sarcomas...

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Autores principales: Cassinelli, Giuliana, Favini, Enrica, Dal Bo, Laura, Tortoreto, Monica, De Maglie, Marcella, Dagrada, Gianpaolo, Pilotti, Silvana, Zunino, Franco, Zaffaroni, Nadia, Lanzi, Cinzia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5216983/
https://www.ncbi.nlm.nih.gov/pubmed/27374103
http://dx.doi.org/10.18632/oncotarget.10292
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author Cassinelli, Giuliana
Favini, Enrica
Dal Bo, Laura
Tortoreto, Monica
De Maglie, Marcella
Dagrada, Gianpaolo
Pilotti, Silvana
Zunino, Franco
Zaffaroni, Nadia
Lanzi, Cinzia
author_facet Cassinelli, Giuliana
Favini, Enrica
Dal Bo, Laura
Tortoreto, Monica
De Maglie, Marcella
Dagrada, Gianpaolo
Pilotti, Silvana
Zunino, Franco
Zaffaroni, Nadia
Lanzi, Cinzia
author_sort Cassinelli, Giuliana
collection PubMed
description The heparan sulfate (HS) mimic/heparanase inhibitor roneparstat (SST0001) shows antitumor activity in preclinical sarcoma models. We hypothesized that this 100% N-acetylated and glycol-split heparin could interfere with the functions of several receptor tyrosine kinases (RTK) coexpressed in sarcomas and activated by heparin-binding growth factors. Using a phospho-proteomic approach, we investigated the drug effects on RTK activation in human cell lines representative of different sarcoma subtypes. Inhibition of FGF, IGF, ERBB and PDGF receptors by the drug was biochemically and functionally validated. Roneparstat counteracted the autocrine loop induced by the COL1A1/PDGFB fusion oncogene, expressed in a human dermatofibrosarcoma protuberans primary culture and in NIH3T3(COL1A1/PDGFB) transfectants, inhibiting cell anchorage-independent growth and invasion. In addition, roneparstat inhibited the activation of cell surface PDGFR and PDGFR-associated FAK, likely contributing to the reversion of NIH3T3(COL1A1/PDGFB) cell transformed and pro-invasive phenotype. Biochemical and histological/immunohistochemical ex vivo analyses confirmed a reduced activation of ERBB4, EGFR, INSR, IGF1R, associated with apoptosis induction and angiogenesis inhibition in a drug-treated Ewing's sarcoma family tumor xenograft. The combination of roneparstat with irinotecan significantly improved the antitumor effect against A204 rhabdoid xenografts resulting in a high rate of complete responses and cures. These findings reveal that roneparstat exerts a multi-target inhibition of RTKs relevant in the pathobiology of different sarcoma subtypes. These effects, likely cooperating with heparanase inhibition, contribute to the antitumor efficacy of the drug. The study supports heparanase/HS axis targeting as a valuable approach in combination therapies of different sarcoma subtypes providing a preclinical rationale for clinical investigation.
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spelling pubmed-52169832017-01-17 Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases Cassinelli, Giuliana Favini, Enrica Dal Bo, Laura Tortoreto, Monica De Maglie, Marcella Dagrada, Gianpaolo Pilotti, Silvana Zunino, Franco Zaffaroni, Nadia Lanzi, Cinzia Oncotarget Research Paper The heparan sulfate (HS) mimic/heparanase inhibitor roneparstat (SST0001) shows antitumor activity in preclinical sarcoma models. We hypothesized that this 100% N-acetylated and glycol-split heparin could interfere with the functions of several receptor tyrosine kinases (RTK) coexpressed in sarcomas and activated by heparin-binding growth factors. Using a phospho-proteomic approach, we investigated the drug effects on RTK activation in human cell lines representative of different sarcoma subtypes. Inhibition of FGF, IGF, ERBB and PDGF receptors by the drug was biochemically and functionally validated. Roneparstat counteracted the autocrine loop induced by the COL1A1/PDGFB fusion oncogene, expressed in a human dermatofibrosarcoma protuberans primary culture and in NIH3T3(COL1A1/PDGFB) transfectants, inhibiting cell anchorage-independent growth and invasion. In addition, roneparstat inhibited the activation of cell surface PDGFR and PDGFR-associated FAK, likely contributing to the reversion of NIH3T3(COL1A1/PDGFB) cell transformed and pro-invasive phenotype. Biochemical and histological/immunohistochemical ex vivo analyses confirmed a reduced activation of ERBB4, EGFR, INSR, IGF1R, associated with apoptosis induction and angiogenesis inhibition in a drug-treated Ewing's sarcoma family tumor xenograft. The combination of roneparstat with irinotecan significantly improved the antitumor effect against A204 rhabdoid xenografts resulting in a high rate of complete responses and cures. These findings reveal that roneparstat exerts a multi-target inhibition of RTKs relevant in the pathobiology of different sarcoma subtypes. These effects, likely cooperating with heparanase inhibition, contribute to the antitumor efficacy of the drug. The study supports heparanase/HS axis targeting as a valuable approach in combination therapies of different sarcoma subtypes providing a preclinical rationale for clinical investigation. Impact Journals LLC 2016-06-25 /pmc/articles/PMC5216983/ /pubmed/27374103 http://dx.doi.org/10.18632/oncotarget.10292 Text en Copyright: © 2016 Cassinelli et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Cassinelli, Giuliana
Favini, Enrica
Dal Bo, Laura
Tortoreto, Monica
De Maglie, Marcella
Dagrada, Gianpaolo
Pilotti, Silvana
Zunino, Franco
Zaffaroni, Nadia
Lanzi, Cinzia
Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title_full Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title_fullStr Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title_full_unstemmed Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title_short Antitumor efficacy of the heparan sulfate mimic roneparstat (SST0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
title_sort antitumor efficacy of the heparan sulfate mimic roneparstat (sst0001) against sarcoma models involves multi-target inhibition of receptor tyrosine kinases
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5216983/
https://www.ncbi.nlm.nih.gov/pubmed/27374103
http://dx.doi.org/10.18632/oncotarget.10292
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