Literature DB >> 24844924

Etanercept blocks inflammatory responses orchestrated by TNF-α to promote transplanted cell engraftment and proliferation in rat liver.

Preeti Viswanathan1, Sorabh Kapoor, Vinay Kumaran, Brigid Joseph, Sanjeev Gupta.   

Abstract

UNLABELLED: Engraftment of transplanted cells is critical for liver-directed cell therapy, but most transplanted cells are rapidly cleared from liver sinusoids by proinflammatory cytokines/chemokines/receptors after activation of neutrophils or Kupffer cells (KCs). To define whether tumor necrosis factor alpha (TNF-α) served roles in cell-transplantation-induced hepatic inflammation, we used the TNF-α antagonist, etanercept (ETN), for studies in syngeneic rat hepatocyte transplantation systems. After cell transplantation, multiple cytokines/chemokines/receptors were overexpressed, whereas ETN before cell transplantation essentially normalized these responses. Moreover, ETN down-regulated cell-transplantation-induced intrahepatic release of secretory cytokines, such as high-mobility group box 1. These effects of ETN decreased cell-transplantation-induced activation of neutrophils, but not of KCs. Transplanted cell engraftment improved by several-fold in ETN-treated animals. These gains in cell engraftment were repeatedly realized after pretreatment of animals with ETN before multiple cell transplantation sessions. Transplanted cell numbers did not change over time, indicating absence of cell proliferation after ETN alone. By contrast, in animals preconditioned with retrorsine and partial hepatectomy, cell transplantation after ETN pretreatment significantly accelerated liver repopulation, compared to control rats.
CONCLUSION: TNF-α plays a major role in orchestrating cell-transplantation-induced inflammation through regulation of multiple cytokines/chemokines/receptor expression. Because TNF-α antagonism by ETN decreased transplanted cell clearance, improved cell engraftment, and accelerated liver repopulation, this pharmacological approach to control hepatic inflammation will help optimize clinical strategies for liver cell therapy.
© 2014 by the American Association for the Study of Liver Diseases.

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Year:  2014        PMID: 24844924      PMCID: PMC4176524          DOI: 10.1002/hep.27232

Source DB:  PubMed          Journal:  Hepatology        ISSN: 0270-9139            Impact factor:   17.425


  42 in total

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3.  Hepatocyte transplantation activates hepatic stellate cells with beneficial modulation of cell engraftment in the rat.

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Journal:  Hepatology       Date:  2005-11       Impact factor: 17.425

4.  Cholinergic agonists inhibit HMGB1 release and improve survival in experimental sepsis.

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Journal:  Nat Med       Date:  2004-10-24       Impact factor: 53.440

5.  Monocrotaline promotes transplanted cell engraftment and advances liver repopulation in rats via liver conditioning.

Authors:  Brigid Joseph; Vinay Kumaran; Ekaterine Berishvili; Kuldeep K Bhargava; Christopher J Palestro; Sanjeev Gupta
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6.  Generation of Th1 and Th2 chemokines by human eosinophils: evidence for a critical role of TNF-alpha.

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7.  Selective local PMN recruitment by CXCL1 or CXCL2/3 injection does not cause inflammatory pain.

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10.  Immunomodulatory effects of etanercept in a model of brain injury act through attenuation of the acute-phase response.

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Review 3.  Immunological aspects of liver cell transplantation.

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4.  Replicative stress and alterations in cell cycle checkpoint controls following acetaminophen hepatotoxicity restrict liver regeneration.

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5.  Demonstrating Potential of Cell Therapy for Wilson's Disease with the Long-Evans Cinnamon Rat Model.

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6.  Decellularized human placenta supports hepatic tissue and allows rescue in acute liver failure.

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Review 7.  Cell therapy in chronic liver disease.

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8.  Thalidomide promotes transplanted cell engraftment in the rat liver by modulating inflammation and endothelial integrity.

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9.  A genetic screen reveals Foxa3 and TNFR1 as key regulators of liver repopulation.

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10.  Kupffer Cell Transplantation in Mice for Elucidating Monocyte/Macrophage Biology and for Potential in Cell or Gene Therapy.

Authors:  Simone Merlin; Kuldeep K Bhargava; Gabriella Ranaldo; Diego Zanolini; Christopher J Palestro; Laura Santambrogio; Maria Prat; Antonia Follenzi; Sanjeev Gupta
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