Pregnane X receptor activation potentiates ritonavir hepatotoxicity
Amina I. Shehu, … , Frank J. Gonzalez, Xiaochao Ma
Amina I. Shehu, … , Frank J. Gonzalez, Xiaochao Ma
Published July 1, 2019; First published April 30, 2019
Citation Information: J Clin Invest. 2019;129(7):2898-2903. https://doi.org/10.1172/JCI128274.
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Categories: Concise Communication AIDS/HIV Hepatology

Pregnane X receptor activation potentiates ritonavir hepatotoxicity

Abstract

Ritonavir (RTV) is on the World Health Organization’s list of essential medicines for antiretroviral therapy, but can cause hepatotoxicity by unknown mechanisms. Multiple clinical studies found that hepatotoxicity occurred in 100% of participants who were pretreated with rifampicin or efavirenz followed by RTV-containing regimens. Both rifampicin and efavirenz are activators of the pregnane X receptor (PXR), a transcription factor with marked interspecies differences in ligand-dependent activation. Using PXR-humanized mouse models, we recapitulated the RTV hepatotoxicity observed in the clinic. PXR was found to modulate RTV hepatotoxicity through CYP3A4-dependent pathways involved in RTV bioactivation, oxidative stress, and endoplasmic reticulum stress. In summary, the current work demonstrated the essential roles of human PXR and CYP3A4 in RTV hepatotoxicity, which can be applied to guide the safe use of RTV-containing regimens in the clinic.

Authors

Amina I. Shehu, Jie Lu, Pengcheng Wang, Junjie Zhu, Yue Wang, Da Yang, Deborah McMahon, Wen Xie, Frank J. Gonzalez, Xiaochao Ma

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Figure 2

Role of CYP3A4 in the hepatotoxicity caused by pretreatment with RIF followed by RTV.

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Role of CYP3A4 in the hepatotoxicity caused by pretreatment with RIF fol...
hPXR/CYP3A4 and hPXR/Cyp3a-null mice were pretreated with RIF for 7 days followed by RTV. (A) Genotyping results of hPXR/Cyp3a-null mice, which are positive for human PXR, but negative for human CYP3A4. (B) Expression of CYP3A4 in the liver of hPXR/CYP3A4 and hPXR/Cyp3a-null mice pretreated with or without PXR ligand RIF for 7 days. Gapdh was used as a loading control. (C and D) Activities of ALT and AST in the serum. All data are shown as mean ± SEM. (n = 3-4). Statistical significance was determined by 2-way ANOVA with Tukey’s post hoc test. ****P < 0.0001. (E and F) Histological analysis of liver samples from control and RIF+RTV groups of hPXR/CYP3A4 and hPXR/Cyp3a-null mice. H&E staining. CV, central vein; ψ indicates hepatocyte degeneration. Original magnification: ×400.