Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells

Jennifer Y. Chen; Benjamin Newcomb; Chan Zhou; Joshua V. Pondick; Sarani Ghoshal; Samuel R. York; Daniel L. Motola; Nicolas Coant; Jae Kyo Yi; Cungui Mao; Kenneth K. Tanabe; Irina Bronova; Evgeny V. Berdyshev; Bryan C. Fuchs; Yusuf Hannun; Raymond T. Chung; Alan C. Mullen

doi:10.1038/srep44867

Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells

Jennifer Y. Chen
, Benjamin Newcomb
, Chan Zhou
, Joshua V. Pondick
, Sarani Ghoshal
, Samuel R. York
, Daniel L. Motola
, Nicolas Coant
, Jae Kyo Yi
, Cungui Mao
, Kenneth K. Tanabe
, Irina Bronova
, Evgeny V. Berdyshev
, Bryan C. Fuchs
, Yusuf Hannun
, Raymond T. Chung
, Alan C. Mullen

Massachusetts General Hospital
Stony Brook University
Harvard University
National Jewish Health

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

26 Scopus citations

Abstract

Activation of hepatic stellate cells (HSCs) in response to injury is a key step in hepatic fibrosis, and is characterized by trans-differentiation of quiescent HSCs to HSC myofibroblasts, which secrete extracellular matrix proteins responsible for the fibrotic scar. There are currently no therapies to directly inhibit hepatic fibrosis. We developed a small molecule screen to identify compounds that inactivate human HSC myofibroblasts through the quantification of lipid droplets. We screened 1600 compounds and identified 21 small molecules that induce HSC inactivation. Four hits were tricyclic antidepressants (TCAs), and they repressed expression of pro-fibrotic factors Alpha-Actin-2 (ACTA2) and Alpha-1 Type I Collagen (COL1A1) in HSCs. RNA sequencing implicated the sphingolipid pathway as a target of the TCAs. Indeed, TCA treatment of HSCs promoted accumulation of ceramide through inhibition of acid ceramidase (aCDase). Depletion of aCDase also promoted accumulation of ceramide and was associated with reduced COL1A1 expression. Treatment with B13, an inhibitor of aCDase, reproduced the antifibrotic phenotype as did the addition of exogenous ceramide. Our results show that detection of lipid droplets provides a robust readout to screen for regulators of hepatic fibrosis and have identified a novel antifibrotic role for ceramide.

Original language	English
Article number	44867
Journal	Scientific Reports
Volume	7
DOIs	https://doi.org/10.1038/srep44867
State	Published - Mar 21 2017

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Chen, J. Y., Newcomb, B., Zhou, C., Pondick, J. V., Ghoshal, S., York, S. R., Motola, D. L., Coant, N., Yi, J. K., Mao, C., Tanabe, K. K., Bronova, I., Berdyshev, E. V., Fuchs, B. C., Hannun, Y., Chung, R. T., & Mullen, A. C. (2017). Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells. Scientific Reports, 7, Article 44867. https://doi.org/10.1038/srep44867

@article{ae4fb1fbc3814999be4bf86b963819ad,

title = "Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells",

abstract = "Activation of hepatic stellate cells (HSCs) in response to injury is a key step in hepatic fibrosis, and is characterized by trans-differentiation of quiescent HSCs to HSC myofibroblasts, which secrete extracellular matrix proteins responsible for the fibrotic scar. There are currently no therapies to directly inhibit hepatic fibrosis. We developed a small molecule screen to identify compounds that inactivate human HSC myofibroblasts through the quantification of lipid droplets. We screened 1600 compounds and identified 21 small molecules that induce HSC inactivation. Four hits were tricyclic antidepressants (TCAs), and they repressed expression of pro-fibrotic factors Alpha-Actin-2 (ACTA2) and Alpha-1 Type I Collagen (COL1A1) in HSCs. RNA sequencing implicated the sphingolipid pathway as a target of the TCAs. Indeed, TCA treatment of HSCs promoted accumulation of ceramide through inhibition of acid ceramidase (aCDase). Depletion of aCDase also promoted accumulation of ceramide and was associated with reduced COL1A1 expression. Treatment with B13, an inhibitor of aCDase, reproduced the antifibrotic phenotype as did the addition of exogenous ceramide. Our results show that detection of lipid droplets provides a robust readout to screen for regulators of hepatic fibrosis and have identified a novel antifibrotic role for ceramide.",

author = "Chen, \{Jennifer Y.\} and Benjamin Newcomb and Chan Zhou and Pondick, \{Joshua V.\} and Sarani Ghoshal and York, \{Samuel R.\} and Motola, \{Daniel L.\} and Nicolas Coant and Yi, \{Jae Kyo\} and Cungui Mao and Tanabe, \{Kenneth K.\} and Irina Bronova and Berdyshev, \{Evgeny V.\} and Fuchs, \{Bryan C.\} and Yusuf Hannun and Chung, \{Raymond T.\} and Mullen, \{Alan C.\}",

note = "Publisher Copyright: {\textcopyright} 2017 The Author(s).",

year = "2017",

month = mar,

day = "21",

doi = "10.1038/srep44867",

language = "English",

volume = "7",

journal = "Scientific Reports",

issn = "2045-2322",

}

Chen, JY, Newcomb, B, Zhou, C, Pondick, JV, Ghoshal, S, York, SR, Motola, DL, Coant, N, Yi, JK, Mao, C, Tanabe, KK, Bronova, I, Berdyshev, EV, Fuchs, BC, Hannun, Y, Chung, RT & Mullen, AC 2017, 'Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells', Scientific Reports, vol. 7, 44867. https://doi.org/10.1038/srep44867

TY - JOUR

T1 - Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells

AU - Chen, Jennifer Y.

AU - Newcomb, Benjamin

AU - Zhou, Chan

AU - Pondick, Joshua V.

AU - Ghoshal, Sarani

AU - York, Samuel R.

AU - Motola, Daniel L.

AU - Coant, Nicolas

AU - Yi, Jae Kyo

AU - Mao, Cungui

AU - Tanabe, Kenneth K.

AU - Bronova, Irina

AU - Berdyshev, Evgeny V.

AU - Fuchs, Bryan C.

AU - Hannun, Yusuf

AU - Chung, Raymond T.

AU - Mullen, Alan C.

PY - 2017/3/21

Y1 - 2017/3/21

N2 - Activation of hepatic stellate cells (HSCs) in response to injury is a key step in hepatic fibrosis, and is characterized by trans-differentiation of quiescent HSCs to HSC myofibroblasts, which secrete extracellular matrix proteins responsible for the fibrotic scar. There are currently no therapies to directly inhibit hepatic fibrosis. We developed a small molecule screen to identify compounds that inactivate human HSC myofibroblasts through the quantification of lipid droplets. We screened 1600 compounds and identified 21 small molecules that induce HSC inactivation. Four hits were tricyclic antidepressants (TCAs), and they repressed expression of pro-fibrotic factors Alpha-Actin-2 (ACTA2) and Alpha-1 Type I Collagen (COL1A1) in HSCs. RNA sequencing implicated the sphingolipid pathway as a target of the TCAs. Indeed, TCA treatment of HSCs promoted accumulation of ceramide through inhibition of acid ceramidase (aCDase). Depletion of aCDase also promoted accumulation of ceramide and was associated with reduced COL1A1 expression. Treatment with B13, an inhibitor of aCDase, reproduced the antifibrotic phenotype as did the addition of exogenous ceramide. Our results show that detection of lipid droplets provides a robust readout to screen for regulators of hepatic fibrosis and have identified a novel antifibrotic role for ceramide.

AB - Activation of hepatic stellate cells (HSCs) in response to injury is a key step in hepatic fibrosis, and is characterized by trans-differentiation of quiescent HSCs to HSC myofibroblasts, which secrete extracellular matrix proteins responsible for the fibrotic scar. There are currently no therapies to directly inhibit hepatic fibrosis. We developed a small molecule screen to identify compounds that inactivate human HSC myofibroblasts through the quantification of lipid droplets. We screened 1600 compounds and identified 21 small molecules that induce HSC inactivation. Four hits were tricyclic antidepressants (TCAs), and they repressed expression of pro-fibrotic factors Alpha-Actin-2 (ACTA2) and Alpha-1 Type I Collagen (COL1A1) in HSCs. RNA sequencing implicated the sphingolipid pathway as a target of the TCAs. Indeed, TCA treatment of HSCs promoted accumulation of ceramide through inhibition of acid ceramidase (aCDase). Depletion of aCDase also promoted accumulation of ceramide and was associated with reduced COL1A1 expression. Treatment with B13, an inhibitor of aCDase, reproduced the antifibrotic phenotype as did the addition of exogenous ceramide. Our results show that detection of lipid droplets provides a robust readout to screen for regulators of hepatic fibrosis and have identified a novel antifibrotic role for ceramide.

UR - https://www.scopus.com/pages/publications/85015826040

U2 - 10.1038/srep44867

DO - 10.1038/srep44867

M3 - Article

C2 - 28322247

AN - SCOPUS:85015826040

SN - 2045-2322

VL - 7

JO - Scientific Reports

JF - Scientific Reports

M1 - 44867

ER -

Tricyclic Antidepressants Promote Ceramide Accumulation to Regulate Collagen Production in Human Hepatic Stellate Cells

Abstract

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