Improving selective targeting to cancer-associated fibroblasts by modifying liposomes with arginine based materials

A library of arginine-like surface modifiers was tested to improve the targetability of DOPE:DOPC liposomes towards myofibroblasts in a tumour microenvironment. Liposomes were characterised using zeta potential and dynamic light scattering. Cell viability remained unchanged for all liposomes. Liposo...

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Bibliographic Details
Published inJournal of drug targeting Vol. 30; no. 1; pp. 94 - 107
Main Authors Rehman, Tanzeel Ur, Bratlie, Kaitlin M.
Format Journal Article
LanguageEnglish
Published England Taylor & Francis 02.01.2022
Subjects
arginine
bioconjugation
cancer-associated fibroblasts
Liposomes
selective targeting
targeted drug delivery
bioconjugation
cancer-associated fibroblasts
arginine
IC50
targeted drug delivery
Liposomes
selective targeting
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Summary:A library of arginine-like surface modifiers was tested to improve the targetability of DOPE:DOPC liposomes towards myofibroblasts in a tumour microenvironment. Liposomes were characterised using zeta potential and dynamic light scattering. Cell viability remained unchanged for all liposomes. Liposomes were encapsulated using doxorubicin (DOX) with an encapsulation efficiency >94%. The toxicity of DOX-loaded liposomes was calculated via half-maximal inhibitory concentration (IC 50 ) for fibroblasts and myofibroblasts. These liposomes resulted in significantly lower IC 50 -values for myofibroblasts compared to fibroblasts, making them more toxic towards the myofibroblasts. Furthermore, a significant increase in cell internalisation was observed for myofibroblasts compared to fibroblasts, using fluorescein-loaded liposomes. Most importantly, a novel regression model was constructed to predict the IC 50 -values for different modifications using their physicochemical properties. Fourteen modifications (A-N) were used to train and validate this model; subsequently, this regression model predicted IC 50 -values for three new modifications (O, P and Q) for both fibroblasts and myofibroblasts. Predicted and measured IC 50 -values showed no significant difference for fibroblasts. For myofibroblasts, modification O showed no significant difference. This study demonstrates that the tested surface modifications can improve targeting to myofibroblasts in the presence of fibroblasts and hence are suitable drug delivery vehicles for myofibroblasts in a tumour microenvironment.
ISSN:1061-186X
1029-2330
DOI:10.1080/1061186X.2021.1941059