Chimeric TK-NOG Mice: A Predictive Model for Cholestatic Human Liver Toxicity

Xu, Dan; Wu, Manhong; Nishimura, Shigehiro; Nishimura, Toshihiko; Michie, Sara A.; Zheng, Ming; Yang, Zhen; Yates, Alexander John; Day, Jeffrey S.; Hillgren, Kathleen M.; Takeda, Saori; Guan, Yuan; Guo, Yingying; Peltz, Gary

doi:10.1124/jpet.114.220798

Cited by 44 publications

(31 citation statements)

References 30 publications

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“…For human drug metabolism, the model facilitates the administration of metabolites that are identified as culprits of toxicity/activity, as required in new drugdiscovery processes. The preparation serves as useful preclinical tools for drug-drug interactions (Jaiswal et al, 2014), and for drug-induced liver injury (DILI) studies on troglitazone (Barnes et al, 2014;Samuelsson et al, 2014), bosentin (Xu et al, 2015), and fialuridine (Xu et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

Functional Integrity of the Chimeric (Humanized) Mouse Liver: Enzyme Zonation, Physiologic Spaces, and Hepatic Enzymes and Transporters

Chow

Wang

Quach

et al. 2016

Drug Metabolism and Disposition

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Chimeric mouse liver models are useful in vivo tools for human drug metabolism studies; however, liver integrity and the microcirculation remain largely uninvestigated. Hence, we conducted liver perfusion studies to examine these attributes in FRGN [Fah(2/2), Rag2(2/2), and Il2rg(2/2), NOD strain] livers (control) and chimeric livers repopulated with mouse (mFRGN) or human (hFRGN) hepatocytes. In single-pass perfusion studies (2.5 ml/min), outflow dilution profiles of noneliminated reference indicators ( 51 Cr-RBC, 125 I-albumin, 14 C-sucrose, and 3 H-water) revealed preservation of flow-limited distribution and reduced water and albumin spaces in hFRGN livers compared with FRGN livers, a view supported microscopically by tightly packed sinusoids. With prograde and retrograde perfusion of harmol (50 mM) in FRGN livers, an anterior sulfation (Sult1a1) over the posterior distribution of glucuronidation (Ugt1a1) activity was preserved, evidenced by the 42% lower sulfation-to-glucuronidation ratio (HS/HG) and 14% higher harmol extraction ratio (E) upon switching from prograde to retrograde flow. By contrast, zonation was lost in mFRGN and hFRGN livers, with HS/HG and E for both flows remaining unchanged. Remnant mouse genes persisted in hFRGN livers (10%-300% those of FRGN). When hFRGN livers were compared with human liver tissue, higher UGT1A1 and MRP2, lower MRP3, and unchanged SULT1A1 and MRP4 mRNA expression were observed. Total Sult1a1/SULT1A1 protein expression in hFRGN livers was higher than that of FRGN livers, consistent with higher harmol sulfate formation. The composite data on humanized livers suggest a loss of zonation, lack of complete liver humanization, and persistence of murine hepatocyte activities leading to higher sulfation.

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Section: Discussionmentioning

confidence: 99%

Functional Integrity of the Chimeric (Humanized) Mouse Liver: Enzyme Zonation, Physiologic Spaces, and Hepatic Enzymes and Transporters

Chow

Wang

Quach

et al. 2016

Drug Metabolism and Disposition

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“…The toxicity of Furosemide is reduced in the TK-NOG mice, similar to what is seen in humans (87). Human liver chimeric TK-NOG mice have also been used to model cholestatic liver toxicity induced by bosentan, which is not seen in control mice (89). Finally, Fah null Rag2 null IL2rg null mice were engrafted with hepatocytes obtained from a donor with familial hypercholesterolaemia.…”

Section: Human-murine Liver Chimeric Mouse Models For the Study Of LImentioning

confidence: 99%

“…The mice developed hypercholesterolaemia and human cholesteryl ester transfer protein as well as apolipoprotein A, which are not found in normal mice, were present in the serum. Replacement of the low-density lipoprotein receptor by AAV9-based gene therapy restored normal lipoprotein profiles, showing that this model could also be used to test gene therapy treatments for this disease (89). …”

Section: Human-murine Liver Chimeric Mouse Models For the Study Of LImentioning

confidence: 99%

Humanized Mouse Models of Clinical Disease

Walsh

Kenney

Jangalwe

et al. 2017

Annu. Rev. Pathol. Mech. Dis.

442

384

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Immunodeficient mice engrafted with functional human cells and tissues, i.e., “humanized mice”, have become increasingly important as small pre-clinical animal models for the study of human diseases. Since the description of immunodeficient mice bearing mutations in the IL2 receptor common gamma chain (IL2rgnull) in the early 2000’s, investigators have been able to engraft murine recipients with human hematopoietic stem cells that develop into functional human immune systems. These mice can also be engrafted with human tissues such as islets, liver, skin, and most solid and hematologic cancers. Humanized mice are permitting significant progress in studies of human infectious disease, cancer, regenerative medicine, graft versus host disease, allergies, and immunity. Ultimately, use of humanized mice may lead to the implementation of truly “personalized” medicine in the clinic. This review discusses recent progress in the development and use of humanized mice, and highlights their utility for the study of human diseases.

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“…These mice respond to selective induction of ligands for humanspecific nuclear receptors (Katoh et al, 2005a;Emoto et al, 2008;Sanoh and Ohta, 2014). In addition, h-chimeric liver mouse models have been used to study preclinical drugdrug interactions (Jaiswal et al, 2014) and drug-induced liver injury stemming from troglitazone (Barnes et al, 2014;Samuelsson et al, 2014), bosentan (Xu et al, 2015), and fialuridine (Xu et al, 2014), and have provided an essential in vivo safety testing tool for potential human toxic metabolites (Strom et al, 2010;Cohen, 2014;Kitamura and Sugihara, 2014;Xu et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Disrupted Murine Gut–to–Human Liver Signaling Alters Bile Acid Homeostasis in Humanized Mouse Liver Models

Chow

Quach

Zhang

et al. 2016

J Pharmacol Exp Ther

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The humanized liver mouse model is being exploited increasingly for human drug metabolism studies. However, its model stability, intercommunication between human hepatocytes and mouse nonparenchymal cells in liver and murine intestine, and changes in extrahepatic transporter and enzyme expressions have not been investigated. We examined these issues in FRGN [fumarylacetoacetate hydrolase (Fah2/2), recombination activating gene 2 (Rag22/2), and interleukin 2 receptor subunit gamma (IL-2rg 2/2) triple knockout] on nonobese diabetic (NOD) background] and chimeric mice: mFRGN and hFRGN (repopulated with mouse or human hepatocytes, respectively). hFRGN mice showed markedly higher levels of liver cholesterol, biliary bilirubin, and bile acids (liver, bile, and plasma; mainly human forms, but also murine bile acids) but lower transforming growth factor beta receptor 2 (TGFBR2) mRNA expression levels (10%) in human hepatocytes and other proliferative markers in mouse nonparenchymal cells (Tgf-b1) and cholangiocytes [plasma membrane-bound, G protein-coupled receptor for bile acids (Tgr5)], suggestive of irregular regeneration processes in hFRGN livers. Changes in gene expression in murine intestine, kidney, and brain of hFRGN mice, in particular, induction of intestinal farnesoid X receptor (Fxr) genes: fibroblast growth factor 15 (Fgf15), mouse ileal bile acid binding protein (Ibabp), small heterodimer partner (Shp), and the organic solute transporter alpha (Osta), were observed. Proteomics revealed persistence of remnant murine proteins (cyotchrome P450 7a-hydroxylase (Cyp7a1) and other enzymes and transporters) in hFRGN livers and suggest the likelihood of mouse activity. When compared with normal human liver tissue, hFRGN livers showed lower SHP mRNA and higher CYP7A1 (300%) protein expression, consequences of tb-and ta-muricholic acid-mediated inhibition of the FXR-SHP cascade and miscommunication between intestinal Fgf15 and human liver fibroblast growth factor receptor 4 (FGFR4), as confirmed by the unchanged hepatic pERK/total ERK ratio. Dysregulation of hepatocyte proliferation and bile acid homeostasis in hFRGN livers led to hepatotoxicity, gallbladder distension, liver deformity, and other extrahepatic changes, making questionable the use of the preparation for drug metabolism studies.

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Chimeric TK-NOG Mice: A Predictive Model for Cholestatic Human Liver Toxicity

Cited by 44 publications

References 30 publications

Functional Integrity of the Chimeric (Humanized) Mouse Liver: Enzyme Zonation, Physiologic Spaces, and Hepatic Enzymes and Transporters

Functional Integrity of the Chimeric (Humanized) Mouse Liver: Enzyme Zonation, Physiologic Spaces, and Hepatic Enzymes and Transporters

Humanized Mouse Models of Clinical Disease

Disrupted Murine Gut–to–Human Liver Signaling Alters Bile Acid Homeostasis in Humanized Mouse Liver Models

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