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Research ArticleSpecial Section Articles

δ-Tocopherol Effect on Endocytosis and its Combination with Enzyme Replacement Therapy for Lysosomal Disorders: a New Type of Drug Interaction?

Rachel L Manthe, Jeffrey A Rappaport, Yan Long, Melani Solomon, Vinay Veluvolu, Michael Hildreth, Dencho Gugutkov, Juan Marugan, Wei Zheng and Silvia Muro
Journal of Pharmacology and Experimental Therapeutics May 17, 2019, jpet.119.257345; DOI: https://doi.org/10.1124/jpet.119.257345
Rachel L Manthe
1 University of Maryland;
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Jeffrey A Rappaport
1 University of Maryland;
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Yan Long
2 National Institutes of Health;
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Melani Solomon
1 University of Maryland;
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Vinay Veluvolu
1 University of Maryland;
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Michael Hildreth
1 University of Maryland;
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Dencho Gugutkov
3 Institute for Bioengineering of Catalonia;
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Juan Marugan
4 National Institute of Health;
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Wei Zheng
2 National Institutes of Health;
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Silvia Muro
5 University of Maryland, ICREA, and IBEC
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Abstract

Induction of lysosomal exocytosis alleviates lysosomal storage of undigested metabolites in cell models of lysosomal disorders (LDs). However, whether this strategy affects other vesicular compartments, e.g., those involved in endocytosis, is unknown. This is important both to predict side effects and to use this strategy in combination with therapies which require endocytosis for intracellular delivery, such as lysosomal enzyme replacement therapy (ERT). We investigated this using δ-tocopherol as a model previously shown to induce lysosomal exocytosis and cell models of type A Niemann-Pick disease, a LD characterized by acid sphingomyelinase (ASM) deficiency and sphingomyelin storage. δ-tocopherol and derivative CF3-T reduced net accumulation of fluid-phase, ligands, and polymer particles via phagocytic, caveolae-, clathrin-, and cell adhesion molecule (CAM)-mediated pathways, yet the latter route was less affected due to receptor overexpression. In agreement, δ-tocopherol lowered uptake of recombinant ASM by deficient cells (known to occur via the clathrin pathway) and via targeting intercellular adhesion molecule-1 (associated to the CAM pathway). However, the net enzyme activity delivered and lysosomal storage attenuation were greater via the latter route. Data suggest stimulation of exocytosis by tocopherols is not specific of lysosomes and affects endocytic cargo. However, this effect was transient and became unnoticeable several hours after tocopherol removal. Therefore, induction of exocytosis in combination with therapies requiring endocytic uptake, such as ERT, may represent a new type of drug interaction, yet this strategy could be valuable if properly timed for minimal interference.

SIGNIFICANCE STATEMENT N/A

  • cell trafficking
  • cellular transport
  • drug delivery
  • drug interactions
  • drug targeting
  • exocytosis
  • recombinant proteins
  • vitamin E
  • The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics: 385 (3)
Journal of Pharmacology and Experimental Therapeutics
Vol. 385, Issue 3
1 Jun 2023
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Research ArticleSpecial Section Articles

δ-Tocopherol Effect on Endocytosis and its Combination with Enzyme Replacement Therapy for Lysosomal Disorders: a New Type of Drug Interaction?

Rachel L Manthe, Jeffrey A Rappaport, Yan Long, Melani Solomon, Vinay Veluvolu, Michael Hildreth, Dencho Gugutkov, Juan Marugan, Wei Zheng and Silvia Muro
Journal of Pharmacology and Experimental Therapeutics May 17, 2019, jpet.119.257345; DOI: https://doi.org/10.1124/jpet.119.257345

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Research ArticleSpecial Section Articles

δ-Tocopherol Effect on Endocytosis and its Combination with Enzyme Replacement Therapy for Lysosomal Disorders: a New Type of Drug Interaction?

Rachel L Manthe, Jeffrey A Rappaport, Yan Long, Melani Solomon, Vinay Veluvolu, Michael Hildreth, Dencho Gugutkov, Juan Marugan, Wei Zheng and Silvia Muro
Journal of Pharmacology and Experimental Therapeutics May 17, 2019, jpet.119.257345; DOI: https://doi.org/10.1124/jpet.119.257345
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