Detail publikace

Passive diffusion vs. active pH-dependent encapsulation of tyrosine kinase inhibitors vandetanib and lenvatinib into folate-targeted ferritin delivery system

ŠKUBALOVÁ, Z. REX, S. SÚKUPOVÁ, M. ZAHÁLKA, M. SKLÁDAL, P. PŘIBYL, J. MICHÁLKOVÁ, H. WEERASEKERA, A. ADAM, V. HEGER, Z.

Originální název

Passive diffusion vs. active pH-dependent encapsulation of tyrosine kinase inhibitors vandetanib and lenvatinib into folate-targeted ferritin delivery system

Typ

článek v časopise ve Web of Science, Jimp

Jazyk

angličtina

Originální abstrakt

Introduction: The present study reports on examination of the effects of encapsulating the tyrosine kinase inhibitors (TKIs) vandetanib and lenvatinib into a biomacromolecular ferritin-based delivery system. Methods: The encapsulation of TKIs was performed via two strategies: i) using an active reversible pH-dependent reassembly of ferritin's quaternary structure and ii) passive loading of hydrophobic TKIs through the hydrophobic channels at the junctions of ferritin subunits. After encapsulation, ferritins were surface-functionalized with folic acid promoting active-targeting capabilities. Results: The physico-chemical and nanomechanical analyses revealed that despite the comparable encapsulation efficiencies of both protocols, the active loading affects stability and rigidity of ferritins, plausibly due to their imperfect reassembly. Biological experiments with hormone-responsive breast cancer cells (T47-D and MCF-7) confirmed the cytotoxicity of encapsulated and folate-targeted TKIs to folate-receptor positive cancer cells, but only limited cytotoxic effects to healthy breast epithelium. Importantly, the long-term cytotoxic experiments revealed that compared to the pH-dependent encapsulation, the passively-loaded TKIs exert markedly higher anticancer activity, most likely due to undesired influence of harsh acidic environment used for the pH-dependent encapsulation on the TKIs' structural and functional properties. Conclusion: Since the passive loading does not require a reassembly step for which acids are needed, the presented investigation serves as a solid basis for future studies focused on encapsulation of small hydrophobic molecules.

Klíčová slova

drug delivery; nanomedicine; lenvatinib; vandetanib

Autoři

ŠKUBALOVÁ, Z.; REX, S.; SÚKUPOVÁ, M.; ZAHÁLKA, M.; SKLÁDAL, P.; PŘIBYL, J.; MICHÁLKOVÁ, H.; WEERASEKERA, A.; ADAM, V.; HEGER, Z.

Vydáno

2. 2. 2021

Nakladatel

Dove Medical Press

ISSN

1178-2013

Periodikum

International Journal of Nanomedicine

Ročník

16

Číslo

1

Stát

Nový Zéland

Strany od

1

Strany do

14

Strany počet

14

URL

https://www.dovepress.com/passive-diffusion-vs-active-ph-dependent-encapsulation-of-tyrosine-kin-peer-reviewed-article-IJN

Plný text v Digitální knihovně

http://hdl.handle.net/11012/196711

BibTex

@article{BUT168946,
  author="Zuzana {Škubalová} and Simona {Rex} and Martina {Súkupová} and Martin {Zahálka} and Petr {Skládal} and Jan {Přibyl} and Hana {Michálková} and Akila {Weerasekera} and Vojtěch {Adam} and Zbyněk {Heger}",
  title="Passive diffusion vs. active pH-dependent encapsulation of tyrosine kinase inhibitors vandetanib and lenvatinib into folate-targeted ferritin delivery system",
  journal="International Journal of Nanomedicine",
  year="2021",
  volume="16",
  number="1",
  pages="1--14",
  doi="10.2147/IJN.S275808",
  issn="1178-2013",
  url="https://www.dovepress.com/passive-diffusion-vs-active-ph-dependent-encapsulation-of-tyrosine-kin-peer-reviewed-article-IJN"
}