Saponin Gallate-Loaded Gd-Doped Zinc–Gallium Layered Double Hydroxides (Zn/Ga@Gd-LDH) Nanocarrier for Attenuating NF-κB-Mediated Inflammation (2025)

    Biological and Medical Applications of Materials and Interfaces

    • Momna Aslam

      Momna Aslam

      Department of Biochemistry, Bahauddin Zakariya University, Multan 60800, Pakistan

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    • Batool Fatima*

      Batool Fatima

      Department of Biochemistry, Bahauddin Zakariya University, Multan 60800, Pakistan

      *Email: [emailprotected]

      More by Batool Fatima

    • Rafia Batool

      Rafia Batool

      Department of Biochemistry, Bahauddin Zakariya University, Multan 60800, Pakistan

      More by Rafia Batool

    • Muhammad Imran

      Muhammad Imran

      Institute of Chemical Sciences, University of Peshawar, Peshawar 25120, Pakistan

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    • Dilshad Hussain

      Dilshad Hussain

      HEJ Research Institute of Chemistry, International Center for Chemical and Biological Sciences, University of Karachi, Karachi 75270, Pakistan

    • Muhammad Najam-ul-Haq

      Muhammad Najam-ul-Haq

      Institute of Chemical Sciences, Bahauddin Zakariya University, Multan 60800, Pakistan

      More by Muhammad Najam-ul-Haq

    • Rubaida Mehmood

      Rubaida Mehmood

      MINAR Cancer Hospital Multan, Multan 60000, Pakistan

      More by Rubaida Mehmood

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    ACS Applied Materials & Interfaces

    Cite this: ACS Appl. Mater. Interfaces 2025, XXXX, XXX, XXX-XXX

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    https://pubs.acs.org/doi/10.1021/acsami.5c00453

    Published April 24, 2025

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    Saponin Gallate-Loaded Gd-Doped Zinc–Gallium Layered Double Hydroxides (Zn/Ga@Gd-LDH) Nanocarrier for Attenuating NF-κB-Mediated Inflammation (5)

    This work describes a drug delivery system (DDS) based on the therapeutic anti-inflammatory efficacy of saponin gallate (SG), a combination of gallic acid and saponin, chemically conjugated via an ester linkage. This formulation was loaded onto a biocompatible gadolinium-doped zinc–gallium-layered double hydroxide (Zn/Ga@Gd-LDH) nanocarrier. FT-IR, XRD, SEM, and HPLC were used to characterize the synthesized materials. UV–visible spectroscopy was employed to investigate the drug release from SG-Zn/Ga@Gd-LDH at an optimized temperature (45 °C) and pH (5). The kinetic release behavior of SG-Zn/Ga@Gd-LDH nanoparticles suggested that the first-order kinetic model was the most appropriate for the release profile. The regression value (R2) of 0.96614 indicated an optimal and controlled release for therapeutic effectiveness and minimal adverse effects over 54 h. The in vitro and in vivo models confirmed that drug-loaded nanocarriers exhibited antioxidant, anti-inflammatory, and anticancer properties. Western blotting analysis suggested that SG-Zn/Ga@Gd-LDH abrogates the anti-inflammatory properties by halting the phosphorylation of pro-inflammatory proteins p-p65 and decreasing CRP levels involved in the NF-κB pathway. SG-Zn/Ga@Gd-LDH exhibited an anti-inflammatory effect by reducing the secretion of proinflammatory cytokines. SG-Zn/Ga@Gd-LDH treatment against an acute CCl4-induced liver injury model showed anti-inflammatory potential in histological parameters’ study. Radiolabeling of the drug saponin gallate with 99mTc was carried out to determine its in vivo biodistribution. The chromatographic results indicated promising radiolabeling of up to 90% percentages. SPECT-CT imaging and ex vivo gamma counting in Wistar rats revealed different clearance rates of nanoparticles, aiding in the evaluation of the drug delivery nanosystem. The designed system also demonstrated antioxidant potential due to the SG compound having IC50 127.45 μg/mL free radical scavenging activity. Ga@Gd-LDH showed a tumor-suppressing ability of 79.89 ± 3.91% for viable cells against breast cancer MCF-7 cells. The developed formulation could thus be a conducive strategy against inflammatory diseases.

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    • Drug release
    • Inflammation
    • Nanocarriers
    • Peptides and proteins
    • Rodent models

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    ACS Applied Materials & Interfaces

    Cite this: ACS Appl. Mater. Interfaces 2025, XXXX, XXX, XXX-XXX

    Click to copy citationCitation copied!

    Published April 24, 2025

    Publication History

    • Received

    • Accepted

    • Revised

    • Published

      online

    © 2025 American Chemical Society

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