Engineered SPIONs functionalized with endothelin a receptor antagonist ameliorate liver fibrosis by inhibiting hepatic stellate cell activation

Endothelin-1/endothelin A receptor (ET-1/ETAR) pathway plays an important role in the progression of liver fibrosis by activating hepatic stellate cells (HSCs) - a key cell type involved in the pathogenesis of liver fibrosis. Inactivating HSCs by blocking the ET-1/ETAR pathway using a selective ETAR...

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Bibliographic Details
Published in:Bioactive materials 2024-09, Vol.39, p.406-426
Main Authors: ten Hove, Marit, Smyris, Andreas, Booijink, Richell, Wachsmuth, Lydia, Hansen, Uwe, Alic, Lejla, Faber, Cornelius, Hӧltke, Carsten, Bansal, Ruchi
Format: Article
Language:English
Subjects:
Attenuation
Bioavailability
Biocompatibility
Body weight
Carbon tetrachloride
Cell activation
Cirrhosis
Collagen
Contractility
Effectiveness
Endothelin 1
Endothelin A receptor
Endothelin ETA receptors
Extracellular matrix
Fibrosis
Gene expression
Growth factors
Hepatic stellate cells
Hepatocytes
In vivo methods and tests
Kinases
Liver
Liver cancer
Liver cirrhosis
Liver fibrosis
Localization
Magnetic resonance imaging
Nanoparticles
Pathogenesis
Polyethylene glycol
Receptors
SPIONs
Stellate cells
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Summary:Endothelin-1/endothelin A receptor (ET-1/ETAR) pathway plays an important role in the progression of liver fibrosis by activating hepatic stellate cells (HSCs) - a key cell type involved in the pathogenesis of liver fibrosis. Inactivating HSCs by blocking the ET-1/ETAR pathway using a selective ETAR antagonist (ERA) represents a promising therapeutic approach for liver fibrosis. Unfortunately, small-molecule ERAs possess limited clinical potential due to poor bioavailability, short half-life, and rapid renal clearance. To improve the clinical applicability, we conjugated ERA to superparamagnetic iron-oxide nanoparticles (SPIONs) and investigated the therapeutic efficacy of ERA and ERA-SPIONs in vitro and in vivo and analyzed liver uptake by in vivo and ex vivo magnetic resonance imaging (MRI), HSCs-specific localization, and ET-1/ETAR-pathway antagonism in vivo. In murine and human liver fibrosis/cirrhosis, we observed overexpression of ET-1 and ETAR that correlated with HSC activation, and HSC-specific localization of ETAR. ERA and successfully synthesized ERA-SPIONs demonstrated significant attenuation in TGFβ-induced HSC activation, ECM production, migration, and contractility. In an acute CCl4-induced liver fibrosis mouse model, ERA-SPIONs exhibited higher liver uptake, HSC-specific localization, and ET-1/ETAR pathway antagonism. This resulted in significantly reduced liver-to-body weight ratio, plasma ALT levels, and α-SMA and collagen-I expression, indicating attenuation of liver fibrosis. In conclusion, our study demonstrates that the delivery of ERA using SPIONs enhances the therapeutic efficacy of ERA in vivo. This approach holds promise as a theranostic strategy for the MRI-based diagnosis and treatment of liver fibrosis. [Display omitted] •ET-1/ETAR pathway plays a key role in the activation of HSCs and liver fibrosis.•ETAR antagonists (ERAs) have shown to ameliorate liver fibrosis.•The clinical application of small-molecule ERAs is hindered due to short half-life.•Delivery of ERAs using SPIONs showed higher liver uptake and therapeutic efficacy.•We present versatile nano-theranostic for imaging and treatment of liver fibrosis.
ISSN:2452-199X
2097-1192
2452-199X
DOI:10.1016/j.bioactmat.2024.05.034