March 3, 2026Open Access

Exosomes displaying native EGF enhance doxorubicin’s therapeutic efficacy and reduce cardiotoxicity

Key Points

Enhanced therapeutic efficacy of doxorubicin was observed with exosomes displaying native EGF, improving drug response.
Cardiotoxicity was significantly reduced in the presence of EGF-exosomes, potentially protecting heart health during cancer therapy.

Structured PICO

Does EGF-Exo-DOX improve anti-tumor efficacy and reduce cardiotoxicity compared to Lipo-DOX in EGFR-overexpressing tumor models?

Population

In vitro and in vivo models of EGFR-overexpressing tumors

Intervention

EGF-Exo-DOX (tumor-derived exosomes engineered with EGF on their surface loaded with doxorubicin)

Comparator

Lipo-DOX (liposomal doxorubicin)

Outcome

Anti-tumor efficacy and tumor accumulation relative to the heartsurrogate

Engineered exosomes displaying EGF offer a promising targeted delivery platform for doxorubicin, potentially enhancing anti-tumor efficacy while minimizing cardiotoxicity in EGFR-overexpressing tumors.

Abstract

Our findings demonstrate that tumor-derived exosomes engineered with EGF on their surface enable targeted drug delivery to tumors with high EGFR expression. Although the exosomes modestly increase cell proliferation in vitro, the EGF-Exo-DOX formulation exhibits enhanced tumor accumulation relative to the heart, minimal cardiac uptake, and shows no tumorigenic effects in vivo. Compared to Lipo-DOX, a widely used clinical formulation of liposomal DOX in China, EGF-Exo-DOX demonstrates superior cellular uptake, greater induction of tumor cell apoptosis, and improved anti-tumor efficacy. These results highlight the potential of engineered exosomes as a targeted drug delivery platform for patients with EGFR-overexpressing tumors.

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