4.5 Article

Cationic lipid-based formulations for encapsulation and delivery of anti-EFG1 2′ OMethylRNA oligomer

MEDICAL MYCOLOGY (2022)

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Journal

MEDICAL MYCOLOGY
Volume 60, Issue 5, Pages -

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/mmy/myac030

Keywords

Candida albicans; filamentation; nucleic acid mimics; non-viral vectors; lipoplexes carriers

Categories

Infectious Diseases Mycology Veterinary Sciences

Funding

  1. Portuguese Foundation for Science and Technology (FCT) [UIDB/04469/2020]
  2. European Regional Development Fund [NORTE-01-0145-FEDER-000004, SFRH/BD/121417/2016]
  3. Projetos de InvestigacAo Cientifica e Desenvolvimento Tecnologico (ICDT) [02/SAICT/2017, POCI-01-0145-FEDER-028893]
  4. Microfluidic Layer-by-layer Assembly of Cationic Liposome-Nucleic Acid Nanoparticles for Gene Delivery project [032520]
  5. FCT
  6. ERDF
  7. Fundação para a Ciência e a Tecnologia [SFRH/BD/121417/2016] Funding Source: FCT

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This study aimed to investigate the complexation of cationic liposomes with anti-EFG1 2 ' OMe oligomers and evaluate its efficacy in controlling Candida albicans filamentation in vitro and in vivo using a Galleria mellonella model. The results showed that DOTAP-based lipoplexes were able to release the anti-EFG1 2 ' OMe oligomers and inhibit C. albicans filamentation. In vivo, the DOTAP/DOPC 80/20 rho(chg )= 3 formulation was the most effective, enhancing the G. mellonella survival.
The effective protection and delivery of antisense oligomers to its site of action is a challenge without an optimal strategy. Some of the most promising approaches encompass the complexation of nucleic acids, which are anionic, with liposomes of fixed or ionizable cationic charge. Thus, the main purpose of this work was to study the complexation of cationic liposomes with anti-EFG1 2 ' OMe oligomers and evaluate the complex efficacy to control Candida albicans filamentation in vitro and in vivo using a Galleria mellonella model. To accomplish this, cationic dioleoyl-trimethylammoniumpropane (DOTAP) was mixed with three different neutral lipids dioleoyl-phosphocholine (DOPC), dioleoyl-phosphatidylethanolamine (DOPE) and monoolein (MO) and used as delivery vectors. Fluorescence Cross Correlation Spectroscopy measurements revealed a high association between antisense oligomers (ASO) and cationic liposomes confirming the formation of lipoplexes. In vitro, all cationic liposome-ASO complexes were able to release the anti-EFG1 2 ' OMe oligomers and consequently inhibit C. albicans filamentation up to 60% after 72 h. In vivo, from all formulations the DOTAP/DOPC 80/20 rho(chg )= 3 formulation proved to be the most effective, enhancing the G. mellonella survival by 40% within 48 h and by 25% after 72 h of infection. In this sense, our findings show that DOTAP-based lipoplexes are very good candidates for nano-carriers of anti-EFG1 2 ' OMe oligomers.

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