Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats

Hepatocyte transplantation is an attractive alternative to liver transplantation. Thus far, however, extensive liver repopulation by adult hepatocytes has required ongoing genetic, physical, or chemical injury to host liver. We hypothesized that providing a regulated proliferative and/or survival ad...

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Autores principales: Peterson, Esther A., Polgar, Zsuzsanna, Devakanmalai, Gnanapackiam S., Li, Yanfeng, Jaber, Fadi L., Zhang, Wei, Wang, Xia, Iqbal, Niloy J., Murray, John W., Roy‐Chowdhury, Namita, Quispe‐Tintaya, Wilber, Maslov, Alexander Y., Tchaikovskaya, Tatyana L., Sharma, Yogeshwar, Rogler, Leslie E., Gupta, Sanjeev, Zhu, Liang, Roy‐Chowdhury, Jayanta, Shafritz, David A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2018
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6312667/
https://www.ncbi.nlm.nih.gov/pubmed/30620000
http://dx.doi.org/10.1002/hep4.1278
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author Peterson, Esther A.
Polgar, Zsuzsanna
Devakanmalai, Gnanapackiam S.
Li, Yanfeng
Jaber, Fadi L.
Zhang, Wei
Wang, Xia
Iqbal, Niloy J.
Murray, John W.
Roy‐Chowdhury, Namita
Quispe‐Tintaya, Wilber
Maslov, Alexander Y.
Tchaikovskaya, Tatyana L.
Sharma, Yogeshwar
Rogler, Leslie E.
Gupta, Sanjeev
Zhu, Liang
Roy‐Chowdhury, Jayanta
Shafritz, David A.
author_facet Peterson, Esther A.
Polgar, Zsuzsanna
Devakanmalai, Gnanapackiam S.
Li, Yanfeng
Jaber, Fadi L.
Zhang, Wei
Wang, Xia
Iqbal, Niloy J.
Murray, John W.
Roy‐Chowdhury, Namita
Quispe‐Tintaya, Wilber
Maslov, Alexander Y.
Tchaikovskaya, Tatyana L.
Sharma, Yogeshwar
Rogler, Leslie E.
Gupta, Sanjeev
Zhu, Liang
Roy‐Chowdhury, Jayanta
Shafritz, David A.
author_sort Peterson, Esther A.
collection PubMed
description Hepatocyte transplantation is an attractive alternative to liver transplantation. Thus far, however, extensive liver repopulation by adult hepatocytes has required ongoing genetic, physical, or chemical injury to host liver. We hypothesized that providing a regulated proliferative and/or survival advantage to transplanted hepatocytes should enable repopulation in a normal liver microenvironment. Here, we repopulated livers of DPPIV(−) (dipeptidyl peptidase‐4) rats and Ugt1a1 (uridinediphosphoglucuronate glucuronosyltransferase 1a1)‐deficient Gunn rats (model of Crigler‐Najjar syndrome type 1), both models without underlying liver injury, for up to 1 year by transplanting lenti‐hYAP‐ERT2 (mutated estrogen receptor ligand‐binding domain 2)‐transduced hepatocytes (YAP‐Hc). Yap (yes‐associated protein) nuclear translocation/function in YAP‐Hc was regulated by tamoxifen. Repopulating YAP‐Hc and host hepatocytes were fluorescence‐activated cell sorting–purified and their transcriptomic profiles compared by RNAseq. After 1 year of liver repopulation, YAP‐Hc clusters exhibited normal morphology, integration into hepatic plates and hepatocyte‐specific gene expression, without dysplasia, dedifferentiation, or tumorigenesis. RNAseq analysis showed up‐regulation of 145 genes promoting cell proliferation and 305 genes suppressing apoptosis, including hepatocyte growth factor and connective tissue growth factor among the top 30 in each category and provided insight into the mechanism of cell competition that enabled replacement of host hepatocytes by YAP‐Hc. In Gunn rats transplanted with YAP‐Hc+tamoxifen, there was a 65%‐81% decline in serum bilirubin over 6 months versus 8%‐20% with control‐Hc, representing a 3‐4‐fold increase in therapeutic response. This correlated with liver repopulation as demonstrated by the presence of Ugt1a1‐positive hepatocyte clusters in livers and western blot analysis of tissue homogenates. Conclusion: Tamoxifen‐regulated nuclear translocation/function of hYAP‐ERT2 enabled long‐term repopulation of DPPIV(−/−) and Gunn rat livers by hYAP‐ERT2‐transduced hepatocytes without tumorigenesis. This cell transplantation strategy may offer a potential therapy for most of the inherited monogenic liver diseases that do not exhibit liver injury.
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spelling pubmed-63126672019-01-07 Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats Peterson, Esther A. Polgar, Zsuzsanna Devakanmalai, Gnanapackiam S. Li, Yanfeng Jaber, Fadi L. Zhang, Wei Wang, Xia Iqbal, Niloy J. Murray, John W. Roy‐Chowdhury, Namita Quispe‐Tintaya, Wilber Maslov, Alexander Y. Tchaikovskaya, Tatyana L. Sharma, Yogeshwar Rogler, Leslie E. Gupta, Sanjeev Zhu, Liang Roy‐Chowdhury, Jayanta Shafritz, David A. Hepatol Commun Original Articles Hepatocyte transplantation is an attractive alternative to liver transplantation. Thus far, however, extensive liver repopulation by adult hepatocytes has required ongoing genetic, physical, or chemical injury to host liver. We hypothesized that providing a regulated proliferative and/or survival advantage to transplanted hepatocytes should enable repopulation in a normal liver microenvironment. Here, we repopulated livers of DPPIV(−) (dipeptidyl peptidase‐4) rats and Ugt1a1 (uridinediphosphoglucuronate glucuronosyltransferase 1a1)‐deficient Gunn rats (model of Crigler‐Najjar syndrome type 1), both models without underlying liver injury, for up to 1 year by transplanting lenti‐hYAP‐ERT2 (mutated estrogen receptor ligand‐binding domain 2)‐transduced hepatocytes (YAP‐Hc). Yap (yes‐associated protein) nuclear translocation/function in YAP‐Hc was regulated by tamoxifen. Repopulating YAP‐Hc and host hepatocytes were fluorescence‐activated cell sorting–purified and their transcriptomic profiles compared by RNAseq. After 1 year of liver repopulation, YAP‐Hc clusters exhibited normal morphology, integration into hepatic plates and hepatocyte‐specific gene expression, without dysplasia, dedifferentiation, or tumorigenesis. RNAseq analysis showed up‐regulation of 145 genes promoting cell proliferation and 305 genes suppressing apoptosis, including hepatocyte growth factor and connective tissue growth factor among the top 30 in each category and provided insight into the mechanism of cell competition that enabled replacement of host hepatocytes by YAP‐Hc. In Gunn rats transplanted with YAP‐Hc+tamoxifen, there was a 65%‐81% decline in serum bilirubin over 6 months versus 8%‐20% with control‐Hc, representing a 3‐4‐fold increase in therapeutic response. This correlated with liver repopulation as demonstrated by the presence of Ugt1a1‐positive hepatocyte clusters in livers and western blot analysis of tissue homogenates. Conclusion: Tamoxifen‐regulated nuclear translocation/function of hYAP‐ERT2 enabled long‐term repopulation of DPPIV(−/−) and Gunn rat livers by hYAP‐ERT2‐transduced hepatocytes without tumorigenesis. This cell transplantation strategy may offer a potential therapy for most of the inherited monogenic liver diseases that do not exhibit liver injury. John Wiley and Sons Inc. 2018-11-20 /pmc/articles/PMC6312667/ /pubmed/30620000 http://dx.doi.org/10.1002/hep4.1278 Text en © 2018 The Authors. Hepatology Communications published by Wiley Periodicals, Inc., on behalf of the American Association for the Study of Liver Diseases. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Original Articles
Peterson, Esther A.
Polgar, Zsuzsanna
Devakanmalai, Gnanapackiam S.
Li, Yanfeng
Jaber, Fadi L.
Zhang, Wei
Wang, Xia
Iqbal, Niloy J.
Murray, John W.
Roy‐Chowdhury, Namita
Quispe‐Tintaya, Wilber
Maslov, Alexander Y.
Tchaikovskaya, Tatyana L.
Sharma, Yogeshwar
Rogler, Leslie E.
Gupta, Sanjeev
Zhu, Liang
Roy‐Chowdhury, Jayanta
Shafritz, David A.
Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title_full Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title_fullStr Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title_full_unstemmed Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title_short Genes and Pathways Promoting Long‐Term Liver Repopulation by Ex Vivo hYAP‐ERT2 Transduced Hepatocytes and Treatment of Jaundice in Gunn Rats
title_sort genes and pathways promoting long‐term liver repopulation by ex vivo hyap‐ert2 transduced hepatocytes and treatment of jaundice in gunn rats
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6312667/
https://www.ncbi.nlm.nih.gov/pubmed/30620000
http://dx.doi.org/10.1002/hep4.1278
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