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Strategic Nanosuspension of Darolutamide for Enhanced Dissolution, Bioavailability, and Potentiated Prostate Cancer Treatment: Insights from Multiscale Computational Modeling.

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ACS applied bio materials 📖 저널 OA 15.6% 2022: 1/1 OA 2024: 1/4 OA 2025: 1/16 OA 2026: 7/43 OA 2022~2026 2025 Vol.8(11) p. 10112-10136
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Pardhi E, Khemchandani R, Pawar A, Kharwar A, Samanthula G, Dandekar M

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Darolutamide (DA), a nonsteroidal antiandrogen, demonstrates significant potential as a targeted therapeutic agent for prostate cancer; however, its clinical application is limited due to its poor aqu

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APA Pardhi E, Khemchandani R, et al. (2025). Strategic Nanosuspension of Darolutamide for Enhanced Dissolution, Bioavailability, and Potentiated Prostate Cancer Treatment: Insights from Multiscale Computational Modeling.. ACS applied bio materials, 8(11), 10112-10136. https://doi.org/10.1021/acsabm.5c01473
MLA Pardhi E, et al.. "Strategic Nanosuspension of Darolutamide for Enhanced Dissolution, Bioavailability, and Potentiated Prostate Cancer Treatment: Insights from Multiscale Computational Modeling.." ACS applied bio materials, vol. 8, no. 11, 2025, pp. 10112-10136.
PMID 41121753 ↗

Abstract

Darolutamide (DA), a nonsteroidal antiandrogen, demonstrates significant potential as a targeted therapeutic agent for prostate cancer; however, its clinical application is limited due to its poor aqueous solubility and low oral bioavailability. To overcome these limitations, we developed a nanosuspension-based formulation (DA-NS) with a mean particle size (PS) of 143.36 ± 5.24 nm, which, upon lyophilization, yielded nanocrystals (DA-NC) with a mean PS of 156.26 ± 7.58 nm, aimed at enhancing the solubility and dissolution rate. Molecular dynamics simulations provided mechanistic insights into the stabilization and formation of DA-NS at the atomic level. In vitro studies demonstrated superior antitumor activity of DA-NC in PC3 prostate cancer cells, characterized by enhanced cellular internalization, nuclear condensation, and apoptotic morphology under fluorescence microscopy. Mechanistic investigations further validated its pro-apoptotic action via elevated reactive oxygen species generation and induction of DNA damage. Western blot analysis confirmed the molecular signature of apoptosis, showing downregulation of antiapoptotic Bcl-2 and upregulation of caspase-3. Pharmacokinetic evaluation revealed a 5.81-fold increase in and a 3.33-fold enhancement in AUC over pure DA, confirming a significant improvement in oral bioavailability ( < 0.0001). Importantly, DA-NC exhibited a favorable safety profile, underscoring its potential as a biocompatible and efficacious oral therapeutic strategy for advanced prostate cancer.

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