Modulation of hepatocyte phenotype in vitro via chemomechanical tuning of polyelectrolyte multilayers

Alice A. Chen; Salman R. Khetani; Sunyoung Lee; Sangeeta N. Bhatia; Krystyn J. Van Vliet

doi:10.1016/j.biomaterials.2008.10.055

Modulation of hepatocyte phenotype in vitro via chemomechanical tuning of polyelectrolyte multilayers

Alice A. Chen, Salman R. Khetani, Sunyoung Lee, Sangeeta N. Bhatia, Krystyn J. Van Vliet

Research output: Contribution to journal › Article › peer-review

79 Scopus citations

Abstract

It is increasingly appreciated that since cell and tissue functions are regulated by chemomechanical stimuli, precise control over such stimuli will improve the functionality of tissue models. However, due to the inherent difficulty in decoupling these cues as presented by extracellular materials, few studies have explored the independent modulation of biochemical and mechanical stimuli towards the manipulation of sustained cellular processes. Here, we demonstrate that both mechanical compliance and ligand presentation of synthetic, weak polyelectrolyte multilayers (PEMs) can be tuned independently to influence the adhesion and liver-specific functions of primary rat hepatocytes over extended in vitro culture (two weeks). These synthetic PEMs exhibited elastic moduli E ranging over 200 kPa < E < 142 MPa, as much as one thousand-fold more compliant than tissue-culture polystyrene (E ∼ 2.5 GPa). The most compliant of these PEM substrata promoted hepatocyte adhesion and spheroidal morphology. Subsequent modification of PEMs with type I collagen and the proteoglycan decorin did not alter substrata compliance, but enhanced the retention of spheroids on surfaces and stabilized hepatic functions (albumin and urea secretion, CYP450 detoxification activity). Decorin exhibited unique compliance-mediated effects on hepatic functions, down-regulating the hepatocyte phenotype when presented on highly compliant substrata while up-regulating hepatocyte functions when presented on increasingly stiffer substrata. These results show that phenotypic functions of liver models can be modulated by leveraging synthetic polymers to study and optimize the interplay of biochemical and mechanical cues at the cell-material interface. More broadly, these results suggest an enabling approach for the systematic design of functional tissue models applied to drug screening, cell-based therapies and fundamental studies in development, physiology and disease.

Original language	English (US)
Pages (from-to)	1113-1120
Number of pages	8
Journal	Biomaterials
Volume	30
Issue number	6
DOIs	https://doi.org/10.1016/j.biomaterials.2008.10.055
State	Published - Feb 2009
Externally published	Yes

Keywords

Chemomechanics
Compliance
Hepatocyte
Polyelectrolyte multilayers
Surface modification

ASJC Scopus subject areas

Bioengineering
Ceramics and Composites
Biophysics
Biomaterials
Mechanics of Materials

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10.1016/j.biomaterials.2008.10.055

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title = "Modulation of hepatocyte phenotype in vitro via chemomechanical tuning of polyelectrolyte multilayers",

abstract = "It is increasingly appreciated that since cell and tissue functions are regulated by chemomechanical stimuli, precise control over such stimuli will improve the functionality of tissue models. However, due to the inherent difficulty in decoupling these cues as presented by extracellular materials, few studies have explored the independent modulation of biochemical and mechanical stimuli towards the manipulation of sustained cellular processes. Here, we demonstrate that both mechanical compliance and ligand presentation of synthetic, weak polyelectrolyte multilayers (PEMs) can be tuned independently to influence the adhesion and liver-specific functions of primary rat hepatocytes over extended in vitro culture (two weeks). These synthetic PEMs exhibited elastic moduli E ranging over 200 kPa < E < 142 MPa, as much as one thousand-fold more compliant than tissue-culture polystyrene (E ∼ 2.5 GPa). The most compliant of these PEM substrata promoted hepatocyte adhesion and spheroidal morphology. Subsequent modification of PEMs with type I collagen and the proteoglycan decorin did not alter substrata compliance, but enhanced the retention of spheroids on surfaces and stabilized hepatic functions (albumin and urea secretion, CYP450 detoxification activity). Decorin exhibited unique compliance-mediated effects on hepatic functions, down-regulating the hepatocyte phenotype when presented on highly compliant substrata while up-regulating hepatocyte functions when presented on increasingly stiffer substrata. These results show that phenotypic functions of liver models can be modulated by leveraging synthetic polymers to study and optimize the interplay of biochemical and mechanical cues at the cell-material interface. More broadly, these results suggest an enabling approach for the systematic design of functional tissue models applied to drug screening, cell-based therapies and fundamental studies in development, physiology and disease.",

keywords = "Chemomechanics, Compliance, Hepatocyte, Polyelectrolyte multilayers, Surface modification",

author = "Chen, {Alice A.} and Khetani, {Salman R.} and Sunyoung Lee and Bhatia, {Sangeeta N.} and {Van Vliet}, {Krystyn J.}",

note = "Funding Information: We gratefully acknowledge K. Hudson, M. Akiyama and S. Katz for rat hepatocyte isolations and media preparation, Y. Li for generation of recombinant protein and assistance with cell culture, S. Kambhampati and E. Liu for assistance with biochemical assays, and J.M. Maloney and J.M. Milwid for assistance with PEM substrata assembly. Funding was provided by the NSF Graduate Research Fellowship (A.A.C.), NSF CAREER Awards (K.J.V.V. and S.N.B.), Arnold & Mabel Beckman Foundation Young Investigator Award (K.J.V.V.), NIH NIDDK (S.N.B.), and the David and Lucile Packard Foundation (S.N.B.). K.J.V.V. and S.L. acknowledge use of shared experimental facilities in the NSF MRSEC Center for Materials Science and Engineering (award number DMR 02-13282). ",

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doi = "10.1016/j.biomaterials.2008.10.055",

language = "English (US)",

volume = "30",

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journal = "Biomaterials",

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AU - Khetani, Salman R.

AU - Lee, Sunyoung

AU - Bhatia, Sangeeta N.

AU - Van Vliet, Krystyn J.

N1 - Funding Information: We gratefully acknowledge K. Hudson, M. Akiyama and S. Katz for rat hepatocyte isolations and media preparation, Y. Li for generation of recombinant protein and assistance with cell culture, S. Kambhampati and E. Liu for assistance with biochemical assays, and J.M. Maloney and J.M. Milwid for assistance with PEM substrata assembly. Funding was provided by the NSF Graduate Research Fellowship (A.A.C.), NSF CAREER Awards (K.J.V.V. and S.N.B.), Arnold & Mabel Beckman Foundation Young Investigator Award (K.J.V.V.), NIH NIDDK (S.N.B.), and the David and Lucile Packard Foundation (S.N.B.). K.J.V.V. and S.L. acknowledge use of shared experimental facilities in the NSF MRSEC Center for Materials Science and Engineering (award number DMR 02-13282).

PY - 2009/2

Y1 - 2009/2

N2 - It is increasingly appreciated that since cell and tissue functions are regulated by chemomechanical stimuli, precise control over such stimuli will improve the functionality of tissue models. However, due to the inherent difficulty in decoupling these cues as presented by extracellular materials, few studies have explored the independent modulation of biochemical and mechanical stimuli towards the manipulation of sustained cellular processes. Here, we demonstrate that both mechanical compliance and ligand presentation of synthetic, weak polyelectrolyte multilayers (PEMs) can be tuned independently to influence the adhesion and liver-specific functions of primary rat hepatocytes over extended in vitro culture (two weeks). These synthetic PEMs exhibited elastic moduli E ranging over 200 kPa < E < 142 MPa, as much as one thousand-fold more compliant than tissue-culture polystyrene (E ∼ 2.5 GPa). The most compliant of these PEM substrata promoted hepatocyte adhesion and spheroidal morphology. Subsequent modification of PEMs with type I collagen and the proteoglycan decorin did not alter substrata compliance, but enhanced the retention of spheroids on surfaces and stabilized hepatic functions (albumin and urea secretion, CYP450 detoxification activity). Decorin exhibited unique compliance-mediated effects on hepatic functions, down-regulating the hepatocyte phenotype when presented on highly compliant substrata while up-regulating hepatocyte functions when presented on increasingly stiffer substrata. These results show that phenotypic functions of liver models can be modulated by leveraging synthetic polymers to study and optimize the interplay of biochemical and mechanical cues at the cell-material interface. More broadly, these results suggest an enabling approach for the systematic design of functional tissue models applied to drug screening, cell-based therapies and fundamental studies in development, physiology and disease.

AB - It is increasingly appreciated that since cell and tissue functions are regulated by chemomechanical stimuli, precise control over such stimuli will improve the functionality of tissue models. However, due to the inherent difficulty in decoupling these cues as presented by extracellular materials, few studies have explored the independent modulation of biochemical and mechanical stimuli towards the manipulation of sustained cellular processes. Here, we demonstrate that both mechanical compliance and ligand presentation of synthetic, weak polyelectrolyte multilayers (PEMs) can be tuned independently to influence the adhesion and liver-specific functions of primary rat hepatocytes over extended in vitro culture (two weeks). These synthetic PEMs exhibited elastic moduli E ranging over 200 kPa < E < 142 MPa, as much as one thousand-fold more compliant than tissue-culture polystyrene (E ∼ 2.5 GPa). The most compliant of these PEM substrata promoted hepatocyte adhesion and spheroidal morphology. Subsequent modification of PEMs with type I collagen and the proteoglycan decorin did not alter substrata compliance, but enhanced the retention of spheroids on surfaces and stabilized hepatic functions (albumin and urea secretion, CYP450 detoxification activity). Decorin exhibited unique compliance-mediated effects on hepatic functions, down-regulating the hepatocyte phenotype when presented on highly compliant substrata while up-regulating hepatocyte functions when presented on increasingly stiffer substrata. These results show that phenotypic functions of liver models can be modulated by leveraging synthetic polymers to study and optimize the interplay of biochemical and mechanical cues at the cell-material interface. More broadly, these results suggest an enabling approach for the systematic design of functional tissue models applied to drug screening, cell-based therapies and fundamental studies in development, physiology and disease.

KW - Chemomechanics

KW - Compliance

KW - Hepatocyte

KW - Polyelectrolyte multilayers

KW - Surface modification

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ER -

Modulation of hepatocyte phenotype in vitro via chemomechanical tuning of polyelectrolyte multilayers

Abstract

Keywords

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