4.8 Article

iRGD-Liposomes Enhance Tumor Delivery and Therapeutic Efficacy of Antisense Oligonucleotide Drugs against Primary Prostate Cancer and Bone Metastasis

ADVANCED FUNCTIONAL MATERIALS (2021)

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Journal

ADVANCED FUNCTIONAL MATERIALS
Volume 31, Issue 24, Pages -

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/adfm.202100478

Keywords

antisense oligonucleotides; bone metastasis; cancer therapies; iRGD‐ liposomes; primary prostate cancer

Categories

Chemistry, Multidisciplinary Chemistry, Physical Nanoscience & Nanotechnology Materials Science, Multidisciplinary Physics, Applied Physics, Condensed Matter

Funding

  1. National Institute of Health [R01CA214550, R01GM133885, R21EB022652]
  2. State of Minnesota [19.08]
  3. National Science Foundation through the National Nanotechnology Coordinated Infrastructure (NNCI) [ECCS-2025124]

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The study demonstrates that using iRGD-liposomes as carriers for ASOs in tumor treatment can enhance drug accumulation in tumor tissue and effectively suppress tumor growth without increasing accumulation or toxicity in healthy organs.
Nucleotide-based drugs, such as antisense oligonucleotides (ASOs), have unique advantages in treating human diseases as they provide virtually unlimited ability to target any gene. However, their clinical translation faces many challenges, one of which is poor delivery to the target tissue in vivo. This problem is particularly evident in solid tumors. Here, liposomes are functionalized with a tumor-homing and -penetrating peptide, iRGD, as a carrier of an ASO against androgen receptor (AR) for prostate cancer treatment. The iRGD-liposomes exhibit a high loading efficiency of AR-ASO, and an efficient knockdown of AR gene products is achieved in vitro, including AR splice variants. In vivo, iRGD-liposomes significantly increase AR-ASO accumulation in the tumor tissue and decrease AR expression relative to free ASOs in prostate tumors established as subcutaneous xenografts. Similar results are obtained with intra-tibial xenografts modeling metastasis to bones, the predominant site of metastasis for prostate cancer. In treatment studies, iRGD-liposomes markedly improve the AR-ASO efficacy in suppressing the growth of both subcutaneous xenografts and intra-tibial xenografts. The inhibitory effect on tumor growth is also significantly prolonged by the delivery of the AR-ASO in the iRGD-liposomes. Meanwhile, iRGD-liposomes does not increase ASO accumulation or toxicity in healthy organs. Overall, a delivery system that can significantly increase ASO accumulation and efficacy in solid tumors is provided here. These benefits are achieved without significant side effects, providing a way to increase the antitumor efficacy of ASOs.

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