AI Article Synopsis

  • The study focused on creating calixarene-based liposomes and characterizing them using various techniques, employing four different amphiphilic calixarenes with varying hydrophobic chain lengths and polar groups.
  • The liposomes were formed using one calixarene and DOPE phospholipid, followed by cytotoxicity assessments across different cell lines.
  • The least toxic calixarene (TEAC) was successfully utilized to deliver nucleic acids and the cancer drug doxorubicin, showing improved transfection efficiency with extra DOPE and demonstrating high encapsulation and controlled release of the drug.

Article Abstract

The formation of calixarene-based liposomes was investigated, and the characterization of these nanostructures was carried out using several techniques. Four amphiphilic calixarenes were used. The length of the hydrophobic chains attached to the lower rim as well as the nature of the polar group present in the upper rim of the calixarenes were varied. The lipid bilayer was formed with one calixarene and with the phospholipid 1,2-dioleoyl-sn-glycero-3-phosphoethanolamine, DOPE. The cytotoxicity of the liposomes for various cell lines was also studied. From the results obtained, the liposomes formed with the least cytotoxic calixarene, (TEAC), were used as nanocarriers of both nucleic acids and the antineoplastic drug doxorubicin, DOX. Results showed that (TEAC)/DOPE/p-EGFP-C1 lipoplexes, of a given composition, can transfect the genetic material, although the transfection efficiency substantially increases in the presence of an additional amount of DOPE as coadjuvant. On the other hand, the (TEAC)/DOPE liposomes present a high doxorubicin encapsulation efficiency, and a slow controlled release, which could diminish the side effects of the drug.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8398082PMC
http://dx.doi.org/10.3390/pharmaceutics13081250DOI Listing

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