AI Article Synopsis

  • * The development of targeted liposomes for cancer therapy has faced challenges, but a new type called Super Stealth Immunoliposomes (SSIL2) shows promise by stabilizing the protective polymer layer and effectively targeting cancer cells.
  • * Experimental results indicate that SSIL2 outperforms traditional stealth liposomes and stealth immunoliposomes in both safety and anticancer efficacy during tests in cell cultures, zebrafish larvae, and rodent models, marking progress in targeted cancer treatment.

Article Abstract

Liposomes play an important role in the field of drug delivery by virtue of their biocompatibility and versatility as carriers. Stealth liposomes, obtained by surface decoration with hydrophilic polyethylene glycol (PEG) molecules, represent an important turning point in liposome technology, leading to significant improvements in the pharmacokinetic profile compared to naked liposomes. Nevertheless, the generation of effective targeted liposomes-a central issue for cancer therapy-has faced several difficulties and clinical phase failures. Active targeting remains a challenge for liposomes. In this direction, a new Super Stealth Immunoliposomes (SSIL2) composed of a PEG-bi-phospholipids derivative is designed that stabilizes the polymer shielding over the liposomes. Furthermore, its counterpart, conjugated to the fragment antigen-binding of trastuzumab (Fab' -PEG-bi-phospholipids), is firmly anchored on the liposomes surface and correctly orients outward the targeting moiety. Throughout this study, the performances of SSIL2 are evaluated and compared to classic stealth liposomes and stealth immunoliposomes in vitro in a panel of cell lines and in vivo studies in zebrafish larvae and rodent models. Overall, SSIL2 shows superior in vitro and in vivo outcomes, both in terms of safety and anticancer efficacy, thus representing a step forward in targeted cancer therapy, and valuable for future development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11469322PMC
http://dx.doi.org/10.1002/adhm.202301650DOI Listing

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