2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels

Targeted delivery of therapeutic compounds to particular cell types such that they only affect the target cells is of great clinical importance since it can minimize undesired side effects. For example, typical chemotherapeutic treatments used in the treatment of neoplastic disorders are cytotoxic n...

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Autores principales: Neumann-Raizel, Hagit, Shilo, Asaf, Lev, Shaya, Mogilevsky, Maxim, Katz, Ben, Shneor, David, Shaul, Yoav D., Leffler, Andreas, Gabizon, Alberto, Karni, Rotem, Honigman, Alik, Binshtok, Alexander M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6804401/
https://www.ncbi.nlm.nih.gov/pubmed/31680972
http://dx.doi.org/10.3389/fphar.2019.01198
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author Neumann-Raizel, Hagit
Shilo, Asaf
Lev, Shaya
Mogilevsky, Maxim
Katz, Ben
Shneor, David
Shaul, Yoav D.
Leffler, Andreas
Gabizon, Alberto
Karni, Rotem
Honigman, Alik
Binshtok, Alexander M.
author_facet Neumann-Raizel, Hagit
Shilo, Asaf
Lev, Shaya
Mogilevsky, Maxim
Katz, Ben
Shneor, David
Shaul, Yoav D.
Leffler, Andreas
Gabizon, Alberto
Karni, Rotem
Honigman, Alik
Binshtok, Alexander M.
author_sort Neumann-Raizel, Hagit
collection PubMed
description Targeted delivery of therapeutic compounds to particular cell types such that they only affect the target cells is of great clinical importance since it can minimize undesired side effects. For example, typical chemotherapeutic treatments used in the treatment of neoplastic disorders are cytotoxic not only to cancer cells but also to most normal cells when exposed to a critical concentration of the compound. As such, many chemotherapeutics exhibit severe side effects, often prohibiting their effective use in the treatment of cancer. Here, we describe a new means for facilitated delivery of a clinically used chemotherapy compound' doxorubicin, into hepatocellular carcinoma cell line (BNL1 ME). We demonstrate that these cells express a large pore, cation non-selective transient receptor potential (TRP) channel V2. We utilized this channel to shuttle doxorubicin into BNL1 ME cells. We show that co-application of either cannabidiol (CBD) or 2-APB, the activators of TRPV2 channels, together with doxorubicin leads to significantly higher accumulation of doxorubicin in BNL1 ME cells than in BNL1 ME cells that were exposed to doxorubicin alone. Moreover, we demonstrate that sub-effective doses of doxorubicin when co-applied with either 2-APB or CBD lead to a significant decrease in the number of living BNL1 ME cell and BNL1 ME cell colonies in comparison to application of doxorubicin alone. Finally, we demonstrate that the doxorubicin-mediated cell death is significantly more potent, requiring an order of magnitude lower dose, when co-applied with CBD than with 2-APB. We suggest that CBD may have a dual effect in promoting doxorubicin-mediated cell death by facilitating the entry of doxorubicin via TRPV2 channels and preventing its clearance from the cells by inhibiting P-glycoprotein ATPase transporter. Collectively, these results provide a foundation for the use of large pore cation-non selective channels as “natural” drug delivery systems for targeting specific cell types.
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spelling pubmed-68044012019-11-03 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels Neumann-Raizel, Hagit Shilo, Asaf Lev, Shaya Mogilevsky, Maxim Katz, Ben Shneor, David Shaul, Yoav D. Leffler, Andreas Gabizon, Alberto Karni, Rotem Honigman, Alik Binshtok, Alexander M. Front Pharmacol Pharmacology Targeted delivery of therapeutic compounds to particular cell types such that they only affect the target cells is of great clinical importance since it can minimize undesired side effects. For example, typical chemotherapeutic treatments used in the treatment of neoplastic disorders are cytotoxic not only to cancer cells but also to most normal cells when exposed to a critical concentration of the compound. As such, many chemotherapeutics exhibit severe side effects, often prohibiting their effective use in the treatment of cancer. Here, we describe a new means for facilitated delivery of a clinically used chemotherapy compound' doxorubicin, into hepatocellular carcinoma cell line (BNL1 ME). We demonstrate that these cells express a large pore, cation non-selective transient receptor potential (TRP) channel V2. We utilized this channel to shuttle doxorubicin into BNL1 ME cells. We show that co-application of either cannabidiol (CBD) or 2-APB, the activators of TRPV2 channels, together with doxorubicin leads to significantly higher accumulation of doxorubicin in BNL1 ME cells than in BNL1 ME cells that were exposed to doxorubicin alone. Moreover, we demonstrate that sub-effective doses of doxorubicin when co-applied with either 2-APB or CBD lead to a significant decrease in the number of living BNL1 ME cell and BNL1 ME cell colonies in comparison to application of doxorubicin alone. Finally, we demonstrate that the doxorubicin-mediated cell death is significantly more potent, requiring an order of magnitude lower dose, when co-applied with CBD than with 2-APB. We suggest that CBD may have a dual effect in promoting doxorubicin-mediated cell death by facilitating the entry of doxorubicin via TRPV2 channels and preventing its clearance from the cells by inhibiting P-glycoprotein ATPase transporter. Collectively, these results provide a foundation for the use of large pore cation-non selective channels as “natural” drug delivery systems for targeting specific cell types. Frontiers Media S.A. 2019-10-15 /pmc/articles/PMC6804401/ /pubmed/31680972 http://dx.doi.org/10.3389/fphar.2019.01198 Text en Copyright © 2019 Neumann-Raizel, Shilo, Lev, Mogilevsky, Katz, Shneor, Shaul, Leffler, Gabizon, Karni, Honigman and Binshtok http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Neumann-Raizel, Hagit
Shilo, Asaf
Lev, Shaya
Mogilevsky, Maxim
Katz, Ben
Shneor, David
Shaul, Yoav D.
Leffler, Andreas
Gabizon, Alberto
Karni, Rotem
Honigman, Alik
Binshtok, Alexander M.
2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title_full 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title_fullStr 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title_full_unstemmed 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title_short 2-APB and CBD-Mediated Targeting of Charged Cytotoxic Compounds Into Tumor Cells Suggests the Involvement of TRPV2 Channels
title_sort 2-apb and cbd-mediated targeting of charged cytotoxic compounds into tumor cells suggests the involvement of trpv2 channels
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6804401/
https://www.ncbi.nlm.nih.gov/pubmed/31680972
http://dx.doi.org/10.3389/fphar.2019.01198
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