Functional Analysis of Human Hepatocytes Isolated From Chimeric Mouse Liver

Porphyrinogenic compounds are known to induce porphyria-mediated hepatocellular injury and subsequent regenerative proliferation in rodents, ultimately leading to hepatocellular tumor induction. However, an appropriate in vivo experimental model to evaluate an effect of porphyrinogenic compounds on human liver has not been fully established. Recently, the chimeric mouse with humanized liver (PXB mice) became widely used as a humanized model in which human hepatocytes are transplanted. In the present study, we examined the utility of PXB mice as an in vivo experimental model to evaluate the key events of the porphyria-mediated cytotoxicity mode of action (MOA) in humans. The treatment of PXB mice with 5-aminolevulinic acid, a representative porphyrinogenic compound, for 28 days caused protoporphyrin IX accumulation, followed by hepatocyte necrosis, increased mitosis, and an increase in replicative DNA synthesis in human hepatocytes, indicative of cellular injury and regenerative proliferation, similar to findings in patients with porphyria or experimental porphyria models and corresponding to the key events of the MOA for porphyria-mediated hepatocellular carcinogenesis. We conclude that the PXB mouse is a useful model to evaluate the key events of the porphyria-mediated cytotoxicity MOA in humans and suggest the utility of PXB mice for clarifying the human relevancy of findings in mice.

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Repopulation of mouse liver with human hepatocytes and in vivo infection with hepatitis B virus

Hepatology ◽

10.1053/jhep.2001.23314 ◽

2001 ◽

Vol 33 (4) ◽

pp. 981-988 ◽

Cited By ~ 275

Author(s):

M Dandri

Keyword(s):

Hepatitis B Virus ◽

Hepatitis B ◽

Mouse Liver ◽

Human Hepatocytes ◽

B Virus

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Comparison of the Hepatic Effects of Phenobarbital in Chimeric Mice Containing Either Rat or Human Hepatocytes With Humanized Constitutive Androstane Receptor and Pregnane X Receptor Mice

Toxicological Sciences ◽

10.1093/toxsci/kfaa125 ◽

2020 ◽

Vol 177 (2) ◽

pp. 362-376

Author(s):

Tomoya Yamada ◽

Ayako Ohara ◽

Naoya Ozawa ◽

Keiko Maeda ◽

Miwa Kondo ◽

...

Keyword(s):

Gene Expression ◽

Liver Tumor ◽

Constitutive Androstane Receptor ◽

Pregnane X Receptor ◽

Rat Hepatocytes ◽

Global Gene Expression ◽

Human Hepatocytes ◽

Chimeric Mouse ◽

Chimeric Mice ◽

Wild Type

Abstract Using a chimeric mouse humanized liver model, we provided evidence that human hepatocytes are refractory to the mitogenic effects of rodent constitutive androstane receptor (CAR) activators. To evaluate the functional reliability of this model, the present study examined mitogenic responses to phenobarbital (PB) in chimeric mice transplanted with rat hepatocytes, because rats are responsive to CAR activators. Treatment with 1000 ppm PB for 7 days significantly increased replicative DNA synthesis (RDS) in rat hepatocytes of the chimeric mice, demonstrating that the transplanted hepatocyte model is functionally reliable for cell proliferation analysis. Treatment of humanized CAR and pregnane X receptor (PXR) mice (hCAR/hPXR mice) with 1000 ppm PB for 7 days significantly increased hepatocyte RDS together with increases in several mitogenic genes. Global gene expression analysis was performed with liver samples from this and from previous studies focusing on PB-induced Wnt/β-catenin signaling and showed that altered genes in hCAR/hPXR mice clustered most closely with liver tumor samples from a diethylnitrosamine/PB initiation/promotion study than with wild-type mice. However, different gene clusters were observed for chimeric mice with human hepatocytes for Wnt/β-catenin signaling when compared with those of hCAR/hPXR mice, wild-type mice, and liver tumor samples. The results of this study demonstrate clear differences in the effects of PB on hepatocyte RDS and global gene expression between human hepatocytes of chimeric mice and hCAR/hPXR mice, suggesting that the chimeric mouse model is relevant to humans for studies on the hepatic effects of rodent CAR activators whereas the hCAR/hPXR mouse is not.

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Pharmacological activation of AMPK suppresses inflammatory response evoked by IL-6 signalling in mouse liver and in human hepatocytes

Molecular and Cellular Endocrinology ◽

10.1016/j.mce.2013.05.013 ◽

2013 ◽

Vol 375 (1-2) ◽

pp. 68-78 ◽

Cited By ~ 22

Author(s):

Annika Nerstedt ◽

Emmelie Cansby ◽

Manoj Amrutkar ◽

Ulf Smith ◽

Margit Mahlapuu

Keyword(s):

Inflammatory Response ◽

Mouse Liver ◽

Human Hepatocytes

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Plasma mannose-binding lectin is stimulated by PPARα in humans

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00299.2011 ◽

2012 ◽

Vol 302 (5) ◽

pp. E595-E602 ◽

Cited By ~ 16

Author(s):

Maryam Rakhshandehroo ◽

Rinke Stienstra ◽

Nicole J. de Wit ◽

Marjolijn C. E. Bragt ◽

Martin Haluzik ◽

...

Keyword(s):

Innate Immunity ◽

Lipid Metabolism ◽

Mouse Liver ◽

Human Hepatocytes ◽

Primary Mouse Hepatocytes ◽

Primary Mouse ◽

Mannose Binding ◽

Mouse Hepatocytes ◽

Binding Lectin ◽

Pparα Agonist

The peroxisome proliferator activated receptor-α (PPARα) is a major transcriptional regulator of lipid metabolism in liver and represents the molecular target for hypolipidemic fibrate drugs. Effects of PPARα on lipid metabolism are partially mediated by circulating proteins such as FGF21 and ANGPTL4. The present study was undertaken to screen for and identify circulating proteins produced by human liver that are under the control of PPARα. Toward that aim, primary human hepatocytes were treated with the synthetic PPARα agonist Wy-14643 and whole genome expression data selected for secreted proteins. Expression of FGF21, ANGPTL4, and mannose-binding lectin (MBL), a soluble mediator of innate immunity and primary component of the lectin branch of the complement system, was markedly upregulated by Wy-14643 in primary human hepatocytes. Mice express two MBL isomers, Mbl1 and Mbl2. Mbl1 mRNA was weakly induced by Wy-14643 in primary mouse hepatocytes and remained unaltered by Wy-14643 in mouse liver. Mbl2 mRNA was unchanged by Wy-14643 in primary mouse hepatocytes and was strongly reduced by Wy-14643 in mouse liver. Remarkably, plasma Mbl1 levels were increased by chronic PPARα activation in lean and obese mice. Importantly, in two independent clinical trials, treatment with the PPARα agonist fenofibrate at 200 mg/day for 6 wk and 3 mo increased plasma MBL levels by 73 ( P = 0.0016) and 86% ( P = 0.017), respectively. It is concluded that hepatocyte gene expression and plasma levels of MBL are stimulated by PPARα and fenofibrate in humans, linking PPARα to regulation of innate immunity and complement activation in humans and suggesting a possible role of MBL in lipid metabolism.

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