What question did this study set out to answer?

The objective is to assess the efficacy of Her2-targeted lipid nanoparticles delivering p53 mRNA in overcoming radioresistance in p53-deficient ovarian cancer.

April 19, 2026

Abstract LB456: Her2-targeted p53 mRNA-LNP platform: A novel strategy for overcoming radioresistance in p53-deficient ovarian cancer

Puntos clave

The objective is to assess the efficacy of Her2-targeted lipid nanoparticles delivering p53 mRNA in overcoming radioresistance in p53-deficient ovarian cancer.
Utilized p53-null, Her2-overexpressing SKOV3 cells and xenografts for in vitro and in vivo studies.
Administered 0.5 mg/kg of LNPs before and after local tumor irradiation (4 or 8 Gy).
Evaluated apoptosis levels and cytotoxicity outcomes comparing targeted mRNA platform and controls.
p53@HER-LNPs restored p53 expression and induced significant apoptosis in cancer cells.
Combination of p53 mRNA and radiotherapy significantly increased DNA damage-induced cytotoxicity.
In vivo studies showed superior tumor growth inhibition using p53@HER-LNPs compared to controls, demonstrating enhanced radiosensitivity.

Resumen

Abstract Extending our previous findings on Her2-targeted lipid nanoparticles (LNPs) for p53 mRNA delivery, this study evaluates this platform’s potential as a radiosensitizer to counteract p53-deficiency-mediated radioresistance. p53 or firefly luciferase (Fluc, non-therapeutic control) mRNA was encapsulated in LNPs functionalized with Her2-specific antibodies (p53@HER-LNP or Fluc@HER-LNP). Utilizing p53-null, Her2-overexpressing SKOV3 cells and xenografts, we assessed synergistic efficacy of radiotherapy (RT) and the targeted mRNA platform. For in vivo validation, 0. 5 mg/kg of LNPs were administered intravenously one day prior to and one day after local tumor irradiation (4 or 8 Gy). The p53@HER-LNPs effectively restored p53 expression, eliciting robust apoptosis. When integrated with RT, this targeted nanotherapeutic significantly potentiated DNA damage-induced cytotoxicity and attenuated clonogenic survival compared to RT alone or Fluc-loaded controls. Notably, in vitro scheduling analysis identified that p53 mRNA administration subsequent to RT (post-RT) exerted a more pronounced synergistic effect than pre-RT treatment. These results were recapitulated in vivo, where the p53@HER-LNP + RT cohort exhibited superior tumor growth inhibition and enhanced radiosensitivity compared to both RT alone and the Fluc@HER-LNP control group. Consequently, targeted p53 restoration via antibody-conjugated LNPs represents a robust strategy for maximizing RT efficacy, offering a rational framework for optimized clinical scheduling in Her2-positive, radioresistant malignancies. Citation Format: Sung Eun Lee, Arang Son, Yeeun Kim, Ji Won Lee, Heewon Song, Changhoon Choi, Dongryul Oh, Dae-Hyuk Kweon. Her2-targeted p53 mRNA-LNP platform: A novel strategy for overcoming radioresistance in p53-deficient ovarian cancer abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 2 (Late-Breaking, Clinical Trial, and Invited Abstracts) ; 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86 (8Suppl): Abstract nr LB456.

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Abstract LB456: Her2-targeted p53 mRNA-LNP platform: A novel strategy for overcoming radioresistance in p53-deficient ovarian cancer

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