Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy

Carbon monoxide and nitric oxide are two of the most important vasoprotective mediators. Their downregulation observed during vascular dysfunction, which is associated with cancer progression, leads to uncontrolled platelet activation. Therefore, the aim of our studies was to improve vasoprotection...

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Autores principales: Porshneva, Kseniia, Papiernik, Diana, Psurski, Mateusz, Łupicka-Słowik, Agnieszka, Matkowski, Rafał, Ekiert, Marcin, Nowak, Marcin, Jarosz, Joanna, Banach, Joanna, Milczarek, Magdalena, Goszczyński, Tomasz M., Sieńczyk, Marcin, Wietrzyk, Joanna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6587338/
https://www.ncbi.nlm.nih.gov/pubmed/31281522
http://dx.doi.org/10.7150/thno.31461
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author Porshneva, Kseniia
Papiernik, Diana
Psurski, Mateusz
Łupicka-Słowik, Agnieszka
Matkowski, Rafał
Ekiert, Marcin
Nowak, Marcin
Jarosz, Joanna
Banach, Joanna
Milczarek, Magdalena
Goszczyński, Tomasz M.
Sieńczyk, Marcin
Wietrzyk, Joanna
author_facet Porshneva, Kseniia
Papiernik, Diana
Psurski, Mateusz
Łupicka-Słowik, Agnieszka
Matkowski, Rafał
Ekiert, Marcin
Nowak, Marcin
Jarosz, Joanna
Banach, Joanna
Milczarek, Magdalena
Goszczyński, Tomasz M.
Sieńczyk, Marcin
Wietrzyk, Joanna
author_sort Porshneva, Kseniia
collection PubMed
description Carbon monoxide and nitric oxide are two of the most important vasoprotective mediators. Their downregulation observed during vascular dysfunction, which is associated with cancer progression, leads to uncontrolled platelet activation. Therefore, the aim of our studies was to improve vasoprotection and to decrease platelet activation during progression of mouse mammary gland cancer by concurrent use of CO and NO donors (CORM-A1 and DETA/NO, respectively). Methods: Mice injected intravenously with 4T1-luc2-tdTomato or orthotopically with 4T1 mouse mammary gland cancer cells were treated with CORM-A1 and DETA/NO. Ex vivo aggregation and activation of platelets were assessed in the blood of healthy donors and breast cancer patients. Moreover, we analyzed the compounds' direct effect on 4T1 mouse and MDA-MB-231 human breast cancer cells proliferation, adhesion and migration in vitro. Results: We have observed antimetastatic effect of combination therapy, which was only transient in orthotopic model. During early stages of tumor progression concurrent use of CORM-A1 and DETA/NO demonstrated vasoprotective ability (decreased endothelin-1, sICAM and sE-selectin plasma level) and downregulated platelets activation (decreased bound of fibrinogen and vWf to platelets) as well as inhibited EMT process. Combined treatment with CO and NO donors diminished adhesion and migration of breast cancer cells in vitro and inhibited aggregation as well as TGF-β release from breast cancer patients' platelets ex vivo. However, antimetastatic effect was not observed at a later stage of tumor progression which was accompanied by increased platelets activation and endothelial dysfunction related to a decrease of VASP level. Conclusion: The therapy was shown to have antimetastatic action and resulted in normalization of endothelial metabolism, diminution of platelet activation and inhibition of EMT process. The effect was more prominent during early stages of tumor dissemination. Such treatment could be applied to inhibit metastasis during the first stages of this process.
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spelling pubmed-65873382019-07-05 Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy Porshneva, Kseniia Papiernik, Diana Psurski, Mateusz Łupicka-Słowik, Agnieszka Matkowski, Rafał Ekiert, Marcin Nowak, Marcin Jarosz, Joanna Banach, Joanna Milczarek, Magdalena Goszczyński, Tomasz M. Sieńczyk, Marcin Wietrzyk, Joanna Theranostics Research Paper Carbon monoxide and nitric oxide are two of the most important vasoprotective mediators. Their downregulation observed during vascular dysfunction, which is associated with cancer progression, leads to uncontrolled platelet activation. Therefore, the aim of our studies was to improve vasoprotection and to decrease platelet activation during progression of mouse mammary gland cancer by concurrent use of CO and NO donors (CORM-A1 and DETA/NO, respectively). Methods: Mice injected intravenously with 4T1-luc2-tdTomato or orthotopically with 4T1 mouse mammary gland cancer cells were treated with CORM-A1 and DETA/NO. Ex vivo aggregation and activation of platelets were assessed in the blood of healthy donors and breast cancer patients. Moreover, we analyzed the compounds' direct effect on 4T1 mouse and MDA-MB-231 human breast cancer cells proliferation, adhesion and migration in vitro. Results: We have observed antimetastatic effect of combination therapy, which was only transient in orthotopic model. During early stages of tumor progression concurrent use of CORM-A1 and DETA/NO demonstrated vasoprotective ability (decreased endothelin-1, sICAM and sE-selectin plasma level) and downregulated platelets activation (decreased bound of fibrinogen and vWf to platelets) as well as inhibited EMT process. Combined treatment with CO and NO donors diminished adhesion and migration of breast cancer cells in vitro and inhibited aggregation as well as TGF-β release from breast cancer patients' platelets ex vivo. However, antimetastatic effect was not observed at a later stage of tumor progression which was accompanied by increased platelets activation and endothelial dysfunction related to a decrease of VASP level. Conclusion: The therapy was shown to have antimetastatic action and resulted in normalization of endothelial metabolism, diminution of platelet activation and inhibition of EMT process. The effect was more prominent during early stages of tumor dissemination. Such treatment could be applied to inhibit metastasis during the first stages of this process. Ivyspring International Publisher 2019-05-31 /pmc/articles/PMC6587338/ /pubmed/31281522 http://dx.doi.org/10.7150/thno.31461 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Porshneva, Kseniia
Papiernik, Diana
Psurski, Mateusz
Łupicka-Słowik, Agnieszka
Matkowski, Rafał
Ekiert, Marcin
Nowak, Marcin
Jarosz, Joanna
Banach, Joanna
Milczarek, Magdalena
Goszczyński, Tomasz M.
Sieńczyk, Marcin
Wietrzyk, Joanna
Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title_full Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title_fullStr Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title_full_unstemmed Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title_short Temporal inhibition of mouse mammary gland cancer metastasis by CORM-A1 and DETA/NO combination therapy
title_sort temporal inhibition of mouse mammary gland cancer metastasis by corm-a1 and deta/no combination therapy
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6587338/
https://www.ncbi.nlm.nih.gov/pubmed/31281522
http://dx.doi.org/10.7150/thno.31461
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