Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic

SIMPLE SUMMARY: Niclosamide, a drug used to treat tapeworm infection, has been shown to have potential as an anticancer drug. The mechanism proposed for this action is the drug-induced inhibition of multiple signaling pathways. Here we uncover an additional, but novel and hitherto unknown, mechanism...

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Autores principales: Sennoune, Souad R., Nandagopal, Gunadharini Dharmalingam, Ramachandran, Sabarish, Mathew, Marilyn, Sivaprakasam, Sathish, Jaramillo-Martinez, Valeria, Bhutia, Yangzom D., Ganapathy, Vadivel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9913174/
https://www.ncbi.nlm.nih.gov/pubmed/36765717
http://dx.doi.org/10.3390/cancers15030759
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author Sennoune, Souad R.
Nandagopal, Gunadharini Dharmalingam
Ramachandran, Sabarish
Mathew, Marilyn
Sivaprakasam, Sathish
Jaramillo-Martinez, Valeria
Bhutia, Yangzom D.
Ganapathy, Vadivel
author_facet Sennoune, Souad R.
Nandagopal, Gunadharini Dharmalingam
Ramachandran, Sabarish
Mathew, Marilyn
Sivaprakasam, Sathish
Jaramillo-Martinez, Valeria
Bhutia, Yangzom D.
Ganapathy, Vadivel
author_sort Sennoune, Souad R.
collection PubMed
description SIMPLE SUMMARY: Niclosamide, a drug used to treat tapeworm infection, has been shown to have potential as an anticancer drug. The mechanism proposed for this action is the drug-induced inhibition of multiple signaling pathways. Here we uncover an additional, but novel and hitherto unknown, mechanism for the anticancer efficacy of this antihelminthic. Niclosamide forces cancer cells to nutrient starvation by blocking macropinocytosis, SLC38A5-mediated amino acid entry and H(+)-coupled nutrient transport pathways. Macropinocytosis is a process by which cells take up extracellular fluid along with the components present in the fluid, and this process is stimulated by an alkaline pH in the cytoplasm. SLC38A5 is an amino acid transporter that is stimulated by an outwardly directed H(+) gradient. The function of niclosamide as a H(+) channel is responsible for the newly discovered actions of this drug reported here. The drug also inhibits SLC38A5 by direct interaction with the transporter. ABSTRACT: Niclosamide, a drug used to treat tapeworm infection, possesses anticancer effects by interfering with multiple signaling pathways. Niclosamide also causes intracellular acidification. We have recently discovered that the amino acid transporter SLC38A5, an amino acid-dependent Na(+)/H(+) exchanger, activates macropinocytosis in cancer cells via amino acid-induced intracellular alkalinization. Therefore, we asked whether niclosamide will block basal and SLC38A5-mediated macropinocytosis via intracellular acidification. We monitored macropinocytosis in pancreatic and breast cancer cells using TMR-dextran and the function of SLC38A5 by measuring Li(+)-stimulated serine uptake. The peptide transporter activity was measured by the uptake of glycylsarcosine. Treatment of the cancer cells with niclosamide caused intracellular acidification. The drug blocked basal and serine-induced macropinocytosis with differential potency, with an EC(50) of ~5 μM for the former and ~0.4 μM for the latter. The increased potency for amino acid-mediated macropinocytosis is due to direct inhibition of SLC38A5 by niclosamide in addition to the ability of the drug to cause intracellular acidification. The drug also inhibited the activity of the H(+)-coupled peptide transporter. We conclude that niclosamide induces nutrient starvation in cancer cells by blocking macropinocytosis, SLC38A5 and the peptide transporter. These studies uncover novel, hitherto unknown, mechanisms for the anticancer efficacy of this antihelminthic.
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spelling pubmed-99131742023-02-11 Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic Sennoune, Souad R. Nandagopal, Gunadharini Dharmalingam Ramachandran, Sabarish Mathew, Marilyn Sivaprakasam, Sathish Jaramillo-Martinez, Valeria Bhutia, Yangzom D. Ganapathy, Vadivel Cancers (Basel) Article SIMPLE SUMMARY: Niclosamide, a drug used to treat tapeworm infection, has been shown to have potential as an anticancer drug. The mechanism proposed for this action is the drug-induced inhibition of multiple signaling pathways. Here we uncover an additional, but novel and hitherto unknown, mechanism for the anticancer efficacy of this antihelminthic. Niclosamide forces cancer cells to nutrient starvation by blocking macropinocytosis, SLC38A5-mediated amino acid entry and H(+)-coupled nutrient transport pathways. Macropinocytosis is a process by which cells take up extracellular fluid along with the components present in the fluid, and this process is stimulated by an alkaline pH in the cytoplasm. SLC38A5 is an amino acid transporter that is stimulated by an outwardly directed H(+) gradient. The function of niclosamide as a H(+) channel is responsible for the newly discovered actions of this drug reported here. The drug also inhibits SLC38A5 by direct interaction with the transporter. ABSTRACT: Niclosamide, a drug used to treat tapeworm infection, possesses anticancer effects by interfering with multiple signaling pathways. Niclosamide also causes intracellular acidification. We have recently discovered that the amino acid transporter SLC38A5, an amino acid-dependent Na(+)/H(+) exchanger, activates macropinocytosis in cancer cells via amino acid-induced intracellular alkalinization. Therefore, we asked whether niclosamide will block basal and SLC38A5-mediated macropinocytosis via intracellular acidification. We monitored macropinocytosis in pancreatic and breast cancer cells using TMR-dextran and the function of SLC38A5 by measuring Li(+)-stimulated serine uptake. The peptide transporter activity was measured by the uptake of glycylsarcosine. Treatment of the cancer cells with niclosamide caused intracellular acidification. The drug blocked basal and serine-induced macropinocytosis with differential potency, with an EC(50) of ~5 μM for the former and ~0.4 μM for the latter. The increased potency for amino acid-mediated macropinocytosis is due to direct inhibition of SLC38A5 by niclosamide in addition to the ability of the drug to cause intracellular acidification. The drug also inhibited the activity of the H(+)-coupled peptide transporter. We conclude that niclosamide induces nutrient starvation in cancer cells by blocking macropinocytosis, SLC38A5 and the peptide transporter. These studies uncover novel, hitherto unknown, mechanisms for the anticancer efficacy of this antihelminthic. MDPI 2023-01-26 /pmc/articles/PMC9913174/ /pubmed/36765717 http://dx.doi.org/10.3390/cancers15030759 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Sennoune, Souad R.
Nandagopal, Gunadharini Dharmalingam
Ramachandran, Sabarish
Mathew, Marilyn
Sivaprakasam, Sathish
Jaramillo-Martinez, Valeria
Bhutia, Yangzom D.
Ganapathy, Vadivel
Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title_full Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title_fullStr Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title_full_unstemmed Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title_short Potent Inhibition of Macropinocytosis by Niclosamide in Cancer Cells: A Novel Mechanism for the Anticancer Efficacy for the Antihelminthic
title_sort potent inhibition of macropinocytosis by niclosamide in cancer cells: a novel mechanism for the anticancer efficacy for the antihelminthic
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9913174/
https://www.ncbi.nlm.nih.gov/pubmed/36765717
http://dx.doi.org/10.3390/cancers15030759
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