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Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System
Acute liver failure has a high mortality unless patients receive a liver transplant; however, there are insufficient donor organs to meet the clinical need. The liver may rapidly recover from acute injury by hepatic cell regeneration given time. A bioartificial liver machine can provide temporary li...
Autores principales: | , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
Mary Ann Liebert, Inc.
2013
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3569957/ https://www.ncbi.nlm.nih.gov/pubmed/23514704 http://dx.doi.org/10.1089/biores.2012.0286 |
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author | Erro, Eloy Bundy, James Massie, Isobel Chalmers, Sherri-Ann Gautier, Aude Gerontas, Spyridon Hoare, Mike Sharratt, Peter Choudhury, Sarah Lubowiecki, Marcin Llewellyn, Ian Legallais, Cécile Fuller, Barry Hodgson, Humphrey Selden, Clare |
author_facet | Erro, Eloy Bundy, James Massie, Isobel Chalmers, Sherri-Ann Gautier, Aude Gerontas, Spyridon Hoare, Mike Sharratt, Peter Choudhury, Sarah Lubowiecki, Marcin Llewellyn, Ian Legallais, Cécile Fuller, Barry Hodgson, Humphrey Selden, Clare |
author_sort | Erro, Eloy |
collection | PubMed |
description | Acute liver failure has a high mortality unless patients receive a liver transplant; however, there are insufficient donor organs to meet the clinical need. The liver may rapidly recover from acute injury by hepatic cell regeneration given time. A bioartificial liver machine can provide temporary liver support to enable such regeneration to occur. We developed a bioartificial liver machine using human-derived liver cells encapsulated in alginate, cultured in a fluidized bed bioreactor to a level of function suitable for clinical use (performance competence). HepG2 cells were encapsulated in alginate using a JetCutter to produce ∼500 μm spherical beads containing cells at ∼1.75 million cells/mL beads. Within the beads, encapsulated cells proliferated to form compact cell spheroids (AELS) with good cell-to-cell contact and cell function, that were analyzed functionally and by gene expression at mRNA and protein levels. We established a methodology to enable a ∼34-fold increase in cell density within the AELS over 11–13 days, maintaining cell viability. Optimized nutrient and oxygen provision were numerically modeled and tested experimentally, achieving a cell density at harvest of >45 million cells/mL beads; >5×10(10) cells were produced in 1100 mL of beads. This process is scalable to human size ([0.7–1]×10(11)). A short-term storage protocol at ambient temperature was established, enabling transport from laboratory to bedside over 48 h, appropriate for clinical translation of a manufactured bioartificial liver machine. |
format | Online Article Text |
id | pubmed-3569957 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2013 |
publisher | Mary Ann Liebert, Inc. |
record_format | MEDLINE/PubMed |
spelling | pubmed-35699572013-03-20 Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System Erro, Eloy Bundy, James Massie, Isobel Chalmers, Sherri-Ann Gautier, Aude Gerontas, Spyridon Hoare, Mike Sharratt, Peter Choudhury, Sarah Lubowiecki, Marcin Llewellyn, Ian Legallais, Cécile Fuller, Barry Hodgson, Humphrey Selden, Clare Biores Open Access Original Research Articles Acute liver failure has a high mortality unless patients receive a liver transplant; however, there are insufficient donor organs to meet the clinical need. The liver may rapidly recover from acute injury by hepatic cell regeneration given time. A bioartificial liver machine can provide temporary liver support to enable such regeneration to occur. We developed a bioartificial liver machine using human-derived liver cells encapsulated in alginate, cultured in a fluidized bed bioreactor to a level of function suitable for clinical use (performance competence). HepG2 cells were encapsulated in alginate using a JetCutter to produce ∼500 μm spherical beads containing cells at ∼1.75 million cells/mL beads. Within the beads, encapsulated cells proliferated to form compact cell spheroids (AELS) with good cell-to-cell contact and cell function, that were analyzed functionally and by gene expression at mRNA and protein levels. We established a methodology to enable a ∼34-fold increase in cell density within the AELS over 11–13 days, maintaining cell viability. Optimized nutrient and oxygen provision were numerically modeled and tested experimentally, achieving a cell density at harvest of >45 million cells/mL beads; >5×10(10) cells were produced in 1100 mL of beads. This process is scalable to human size ([0.7–1]×10(11)). A short-term storage protocol at ambient temperature was established, enabling transport from laboratory to bedside over 48 h, appropriate for clinical translation of a manufactured bioartificial liver machine. Mary Ann Liebert, Inc. 2013-02 /pmc/articles/PMC3569957/ /pubmed/23514704 http://dx.doi.org/10.1089/biores.2012.0286 Text en Copyright 2013, Mary Ann Liebert, Inc. |
spellingShingle | Original Research Articles Erro, Eloy Bundy, James Massie, Isobel Chalmers, Sherri-Ann Gautier, Aude Gerontas, Spyridon Hoare, Mike Sharratt, Peter Choudhury, Sarah Lubowiecki, Marcin Llewellyn, Ian Legallais, Cécile Fuller, Barry Hodgson, Humphrey Selden, Clare Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title | Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title_full | Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title_fullStr | Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title_full_unstemmed | Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title_short | Bioengineering the Liver: Scale-Up and Cool Chain Delivery of the Liver Cell Biomass for Clinical Targeting in a Bioartificial Liver Support System |
title_sort | bioengineering the liver: scale-up and cool chain delivery of the liver cell biomass for clinical targeting in a bioartificial liver support system |
topic | Original Research Articles |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3569957/ https://www.ncbi.nlm.nih.gov/pubmed/23514704 http://dx.doi.org/10.1089/biores.2012.0286 |
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