Literature DB >> 30272645

A Familial Hypercholesterolemia Human Liver Chimeric Mouse Model Using Induced Pluripotent Stem Cell-derived Hepatocytes.

Jiayin Yang1, Lai-Yung Wong2, Xiao-Yu Tian3, Rui Wei4, Wing-Hon Lai2, Ka-Wing Au2, Zhiwei Luo5, Carl Ward5, Wai-In Ho2, David P Ibañez5, Hao Liu5, Xichen Bao5, Baoming Qin5, Yu Huang3, Miguel A Esteban6, Hung-Fat Tse7.   

Abstract

Familial hypercholesterolemia (FH) is mostly caused by low-density lipoprotein receptor (LDLR) mutations and results in an increased risk of early-onset cardiovascular disease due to marked elevation of LDL cholesterol (LDL-C) in blood. Statins are the first line of lipid-lowering drugs for treating FH and other types of hypercholesterolemia, but new approaches are emerging, in particular PCSK9 antibodies, which are now being tested in clinical trials. To explore novel therapeutic approaches for FH, either new drugs or new formulations, we need appropriate in vivo models. However, differences in the lipid metabolic profiles compared to humans are a key problem of the available animal models of FH. To address this issue, we have generated a human liver chimeric mouse model using FH induced pluripotent stem cell (iPSC)-derived hepatocytes (iHeps). We used Ldlr-/-/Rag2-/-/Il2rg-/- (LRG) mice to avoid immune rejection of transplanted human cells and to assess the effect of LDLR-deficient iHeps in an LDLR null background. Transplanted FH iHeps could repopulate 5-10% of the LRG mouse liver based on human albumin staining. Moreover, the engrafted iHeps responded to lipid-lowering drugs and recapitulated clinical observations of increased efficacy of PCSK9 antibodies compared to statins. Our human liver chimeric model could thus be useful for preclinical testing of new therapies to FH. Using the same protocol, similar human liver chimeric mice for other FH genetic variants, or mutations corresponding to other inherited liver diseases, may also be generated.

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Year:  2018        PMID: 30272645      PMCID: PMC6235199          DOI: 10.3791/57556

Source DB:  PubMed          Journal:  J Vis Exp        ISSN: 1940-087X            Impact factor:   1.355


  19 in total

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10.  Generation of Human Liver Chimeric Mice with Hepatocytes from Familial Hypercholesterolemia Induced Pluripotent Stem Cells.

Authors:  Jiayin Yang; Yu Wang; Ting Zhou; Lai-Yung Wong; Xiao-Yu Tian; Xueyu Hong; Wing-Hon Lai; Ka-Wing Au; Rui Wei; Yuqing Liu; Lai-Hung Cheng; Guichan Liang; Zhijian Huang; Wenxia Fan; Ping Zhao; Xiwei Wang; David P Ibañez; Zhiwei Luo; Yingying Li; Xiaofen Zhong; Shuhan Chen; Dongye Wang; Li Li; Liangxue Lai; Baoming Qin; Xichen Bao; Andrew P Hutchins; Chung-Wah Siu; Yu Huang; Miguel A Esteban; Hung-Fat Tse
Journal:  Stem Cell Reports       Date:  2017-03-02       Impact factor: 7.765

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  3 in total

1.  CRISPR-targeted genome editing of human induced pluripotent stem cell-derived hepatocytes for the treatment of Wilson's disease.

Authors:  Rui Wei; Jiayin Yang; Chi-Wa Cheng; Wai-In Ho; Na Li; Yang Hu; Xueyu Hong; Jian Fu; Bo Yang; Yuqing Liu; Lixiang Jiang; Wing-Hon Lai; Ka-Wing Au; Wai-Ling Tsang; Yiu-Lam Tse; Kwong-Man Ng; Miguel A Esteban; Hung-Fat Tse
Journal:  JHEP Rep       Date:  2021-10-30

Review 2.  Advancements in Disease Modeling and Drug Discovery Using iPSC-Derived Hepatocyte-like Cells.

Authors:  Josef Blaszkiewicz; Stephen A Duncan
Journal:  Genes (Basel)       Date:  2022-03-24       Impact factor: 4.141

Review 3.  Induced pluripotent stem cells for the treatment of liver diseases: challenges and perspectives from a clinical viewpoint.

Authors:  Eugenia Pareja; M José Gómez-Lechón; Laia Tolosa
Journal:  Ann Transl Med       Date:  2020-04
  3 in total

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