Spike structure of gold nanobranches induces hepatotoxicity in mouse hepatocyte organoid models.

J Nanobiotechnology

Institute for Smart Biomedical Materials, School of Materials Science & Engineering, Zhejiang Sci-Tech University, Hangzhou, 310000, PR China.

Published: March 2024

AI Article Synopsis

  • Gold nanoparticles (GNPs) are promising for biomedical use, but their potential liver toxicity poses significant challenges for clinical application.
  • To study this toxicity, researchers used hepatocyte organoid models to compare the effects of two GNP shapes: spiny gold nanobranches (GNBs) and gold nanospheres (GNSs).
  • The findings revealed that GNBs caused more harm to liver cells than GNSs, as they led to mitochondrial damage and metabolic issues, suggesting that Hep-orgs are effective for studying how GNPs interact with liver cells in a more realistic environment.

Article Abstract

Background: Gold nanoparticles (GNPs) have been extensively recognized as an active candidate for a large variety of biomedical applications. However, the clinical conversion of specific types of GNPs has been hindered due to their potential liver toxicity. The origin of their hepatotoxicity and the underlying key factors are still ambiguous. Because the size, shape, and surfactant of GNPs all affect their properties and cytotoxicity. An effective and sensitive platform that can provide deep insights into the cause of GNPs' hepatotoxicity in vitro is therefore highly desired.

Methods: Here, hepatocyte organoid models (Hep-orgs) were constructed to evaluate the shape-dependent hepatotoxicity of GNPs. Two types of GNPs with different nanomorphology, gold nanospheres (GNSs) and spiny gold nanobranches (GNBs), were synthesized as the representative samples. Their shape-dependent effects on mice Hep-orgs' morphology, cellular cytoskeletal structure, mitochondrial structure, oxidative stress, and metabolism were carefully investigated.

Results: The results showed that GNBs with higher spikiness and tip curvature exhibited more significant cytotoxicity compared to the rounded GNSs. The spike structure of GNBs leads to a mitochondrial damage, oxidative stress, and metabolic disorder in Hep-orgs. Meanwhile, similar trends can be observed in HepG2 cells and mice models, demonstrating the reliability of the Hep-orgs.

Conclusions: Hep-orgs can serve as an effective platform for exploring the interactions between GNPs and liver cells in a 3D perspective, filling the gap between 2D cell models and animal models. This work further revealed that organoids can be used as an indispensable tool to rapidly screen and explore the toxic mechanism of nanomaterials before considering their biomedical functionalities.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10913213PMC
http://dx.doi.org/10.1186/s12951-024-02363-1DOI Listing

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