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Reexamining the effects of drug loading on the in vivo performance of PEGylated liposomal doxorubicin. | LitMetric

Reexamining the effects of drug loading on the in vivo performance of PEGylated liposomal doxorubicin.

Acta Pharmacol Sin

Department of Pharmacology, School of Basic Medical Sciences & Department of Pharmacy, Shanghai Pudong Hospital & State Key Laboratory of Molecular Engineering of Polymers, Fudan University, Shanghai, 200032, China.

Published: March 2024

AI Article Synopsis

  • Researchers aim to achieve higher drug loading in nanoscale delivery systems, but the effects on the body are often overlooked.
  • In this study, the performance of PEGylated liposomal doxorubicin (PLD) was evaluated by comparing high drug loading (H-Dox) and low drug loading (L-Dox) formulations in animal tests.
  • The findings suggested that lower drug loading did not significantly affect the essential properties of PLDs, and it may even reduce unwanted side effects by improving the delivery and circulation of the drug in the body, highlighting the need for further investigation of each delivery platform.

Article Abstract

Higher drug loading employed in nanoscale delivery platforms is a goal that researchers have long sought after. But such viewpoint remains controversial because the impacts that nanocarriers bring about on bodies have been seriously overlooked. In the present study we investigated the effects of drug loading on the in vivo performance of PEGylated liposomal doxorubicin (PLD). We prepared PLDs with two different drug loading rates: high drug loading rate, H-Dox, 12.9% w/w Dox/HSPC; low drug loading rate, L-Dox, 2.4% w/w Dox/HSPC (L-Dox had about 5 folds drug carriers of H-Dox at the same Dox dose). The pharmaceutical properties and biological effects of H-Dox and L-Dox were compared in mice, rats or 4T1 subcutaneous tumor-bearing mice. We showed that the lowering of doxorubicin loading did not cause substantial shifts to the pharmaceutical properties of PLDs such as in vitro and in vivo stability (stable), anti-tumor effect (equivalent effective), as well as tissue and cellular distribution. Moreover, it was even more beneficial for mitigating the undesired biological effects caused by PLDs, through prolonging blood circulation and alleviating cutaneous accumulation in the presence of pre-existing anti-PEG Abs due to less opsonins (e.g. IgM and C3) deposition on per particle. Our results warn that the effects of drug loading would be much more convoluted than expected due to the complex intermediation between nanocarriers and bodies, urging independent investigation for each individual delivery platform to facilitate clinical translation and application.

Download full-text PDF

Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10834505PMC
http://dx.doi.org/10.1038/s41401-023-01169-5DOI Listing

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