Artikel

Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation

02.09.2025

Von Wiley-VCH zur Verfügung gestellt

This work designs an HA-GO nanocarrier co-loaded with DOX, MDR1 ASO, and MiR-489 for targeted cancer therapy. MDR1 ASO inhibits P-gp expression, MiR-489 suppresses Smad3 signaling, and DOX damages DNA. The synergistic gene and chemotherapy overcome multidrug resistance, increase drug accumulation, and induce potent cancer cell apoptosis.


Abstract

Multidrug resistance (MDR) significantly limits breast cancer chemotherapy effectiveness. Here, we engineered a hyaluronic acid–functionalized graphene oxide (HA-GO) nanocarrier for co-delivery of microRNA-489 and MDR1 antisense oligonucleotide (ASO, MB1) alongside doxorubicin (DOX). Among various nucleic acid ratios, a MiR-489:MDR1 ASO ratio of 2:1 exhibited the most potent enhancement of DOX sensitivity in MCF-7/ADM cells. This co-delivery system synergistically reduced drug resistance, increased intracellular DOX accumulation, and amplified cytotoxicity. These results highlight the optimized HA-GO platform as a promising strategy to overcome MDR in breast cancer therapy.

Verwandte Artikel
Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation
In Kürze
Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation
Ehrungen, Karriere
Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation
Aus den Fachgruppen
Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation
EuChemS Policy Workshop „PFAS”
Enhancement of Doxorubicin Efficacy in Drug‐Resistant Breast Cancer Cells Through Nucleic Acid Modulation
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