Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein

Elke Prade; Moritz Tobiasch; Ivana Hitkova; Isabell Schäffer; Fan Lian; Xiangbin Xing; Marc Tänzer; Sandra Rauser; Axel Walch; Marcus Feith; Stefan Post; Christoph Röcken; Roland M. Schmid; Matthias P.A. Ebert; Elke Burgermeister

doi:10.1210/me.2011-1140

Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein

Elke Prade
, Moritz Tobiasch
, Ivana Hitkova
, Isabell Schäffer
, Fan Lian
, Xiangbin Xing
, Marc Tänzer
, Sandra Rauser
, Axel Walch
, Marcus Feith
, Stefan Post
, Christoph Röcken
, Roland M. Schmid
, Matthias P.A. Ebert
, Elke Burgermeister

Department of Surgery

Technical University of Munich
Universitätsmedizin Mannheim
The First Affiliated Hospital of Sun Yat-sen University
München GmbH
Christian-Albrechts-University of Kiel

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

10 Scopus citations

Abstract

Bile acids are synthesized from cholesterol and are major risk factors for Barrett adenocarcinoma (BAC) of the esophagus. Caveolin-1 (Cav1), a scaffold protein of membrane caveolae, is transcriptionally regulated by cholesterol via sterol-responsive element-binding protein-1 (SREBP1). Cav1 protects squamous epithelia by controlling cell growth and stabilizing cell junctions and matrix adhesion. Cav1 is frequently down-regulated in human cancers; however, the molecular mechanisms that lead to this event are unknown.Weshow that the basal layer of the nonneoplastic human esophageal squamous epithelium expressed Cav1 mainly at intercellular junctions. In contrast, Cav1 was lost in 95% of tissue specimens from BAC patients (n100). A strong cytoplasmic expression of Cav1 correlated with poor survival in a small subgroup (n5) ofBACpatients, and stable expression of an oncogenic Cav1 variant (Cav1-P132L) in the human BAC cell line OE19 promoted proliferation. Cav1 was also detectable in immortalizedhumansquamous epithelial, Barrett esophagus (CPC), and squamous cell carcinoma cells (OE21), but was low in BAC cell lines (OE19, OE33). Mechanistically, bile acids down-regulated Cav1 expression by inhibition of the proteolytic cleavage of 125-kDa pre-SREBP1 from the endoplasmic reticulum/Golgi apparatus and nuclear translocation of active 68-kDa SREBP1. This block in SREBP1's posttranslational processing impaired transcriptional activation of SREBP1 response elements in the proximal human Cav1 promoter. Cav1 was also down-regulated in esophagi from C57BL/6 mice on a diet enriched with 1% (wt/wt) chenodeoxycholic acid. Mice deficient for Cav1 or the nuclear bile acid receptor farnesoid X receptor showed hyperplasia and hyperkeratosis of the basal cell layer of esophageal epithelia, respectively. These data indicate that bile acid-mediated down-regulation of Cav1 marks early changes in the squamous epithelium, which may contribute to onset of Barrett esophagus metaplasia and progression to BAC.

Original language	English
Pages (from-to)	819-832
Number of pages	14
Journal	Molecular Endocrinology
Volume	26
Issue number	5
DOIs	https://doi.org/10.1210/me.2011-1140
State	Published - May 2012

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10.1210/me.2011-1140

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Prade, E., Tobiasch, M., Hitkova, I., Schäffer, I., Lian, F., Xing, X., Tänzer, M., Rauser, S., Walch, A., Feith, M., Post, S., Röcken, C., Schmid, R. M., Ebert, M. P. A., & Burgermeister, E. (2012). Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein. Molecular Endocrinology, 26(5), 819-832. https://doi.org/10.1210/me.2011-1140

@article{6b18934253444feab6381e1c9a9f077f,

title = "Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein",

abstract = "Bile acids are synthesized from cholesterol and are major risk factors for Barrett adenocarcinoma (BAC) of the esophagus. Caveolin-1 (Cav1), a scaffold protein of membrane caveolae, is transcriptionally regulated by cholesterol via sterol-responsive element-binding protein-1 (SREBP1). Cav1 protects squamous epithelia by controlling cell growth and stabilizing cell junctions and matrix adhesion. Cav1 is frequently down-regulated in human cancers; however, the molecular mechanisms that lead to this event are unknown.Weshow that the basal layer of the nonneoplastic human esophageal squamous epithelium expressed Cav1 mainly at intercellular junctions. In contrast, Cav1 was lost in 95\% of tissue specimens from BAC patients (n100). A strong cytoplasmic expression of Cav1 correlated with poor survival in a small subgroup (n5) ofBACpatients, and stable expression of an oncogenic Cav1 variant (Cav1-P132L) in the human BAC cell line OE19 promoted proliferation. Cav1 was also detectable in immortalizedhumansquamous epithelial, Barrett esophagus (CPC), and squamous cell carcinoma cells (OE21), but was low in BAC cell lines (OE19, OE33). Mechanistically, bile acids down-regulated Cav1 expression by inhibition of the proteolytic cleavage of 125-kDa pre-SREBP1 from the endoplasmic reticulum/Golgi apparatus and nuclear translocation of active 68-kDa SREBP1. This block in SREBP1's posttranslational processing impaired transcriptional activation of SREBP1 response elements in the proximal human Cav1 promoter. Cav1 was also down-regulated in esophagi from C57BL/6 mice on a diet enriched with 1\% (wt/wt) chenodeoxycholic acid. Mice deficient for Cav1 or the nuclear bile acid receptor farnesoid X receptor showed hyperplasia and hyperkeratosis of the basal cell layer of esophageal epithelia, respectively. These data indicate that bile acid-mediated down-regulation of Cav1 marks early changes in the squamous epithelium, which may contribute to onset of Barrett esophagus metaplasia and progression to BAC.",

author = "Elke Prade and Moritz Tobiasch and Ivana Hitkova and Isabell Sch{\"a}ffer and Fan Lian and Xiangbin Xing and Marc T{\"a}nzer and Sandra Rauser and Axel Walch and Marcus Feith and Stefan Post and Christoph R{\"o}cken and Schmid, \{Roland M.\} and Ebert, \{Matthias P.A.\} and Elke Burgermeister",

year = "2012",

month = may,

doi = "10.1210/me.2011-1140",

language = "English",

volume = "26",

pages = "819--832",

journal = "Molecular Endocrinology",

issn = "0888-8809",

publisher = "The Endocrine Society",

number = "5",

}

Prade, E, Tobiasch, M, Hitkova, I, Schäffer, I, Lian, F, Xing, X, Tänzer, M, Rauser, S, Walch, A, Feith, M, Post, S, Röcken, C, Schmid, RM, Ebert, MPA & Burgermeister, E 2012, 'Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein', Molecular Endocrinology, vol. 26, no. 5, pp. 819-832. https://doi.org/10.1210/me.2011-1140

TY - JOUR

T1 - Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein

AU - Prade, Elke

AU - Tobiasch, Moritz

AU - Hitkova, Ivana

AU - Schäffer, Isabell

AU - Lian, Fan

AU - Xing, Xiangbin

AU - Tänzer, Marc

AU - Rauser, Sandra

AU - Walch, Axel

AU - Feith, Marcus

AU - Post, Stefan

AU - Röcken, Christoph

AU - Schmid, Roland M.

AU - Ebert, Matthias P.A.

AU - Burgermeister, Elke

PY - 2012/5

Y1 - 2012/5

N2 - Bile acids are synthesized from cholesterol and are major risk factors for Barrett adenocarcinoma (BAC) of the esophagus. Caveolin-1 (Cav1), a scaffold protein of membrane caveolae, is transcriptionally regulated by cholesterol via sterol-responsive element-binding protein-1 (SREBP1). Cav1 protects squamous epithelia by controlling cell growth and stabilizing cell junctions and matrix adhesion. Cav1 is frequently down-regulated in human cancers; however, the molecular mechanisms that lead to this event are unknown.Weshow that the basal layer of the nonneoplastic human esophageal squamous epithelium expressed Cav1 mainly at intercellular junctions. In contrast, Cav1 was lost in 95% of tissue specimens from BAC patients (n100). A strong cytoplasmic expression of Cav1 correlated with poor survival in a small subgroup (n5) ofBACpatients, and stable expression of an oncogenic Cav1 variant (Cav1-P132L) in the human BAC cell line OE19 promoted proliferation. Cav1 was also detectable in immortalizedhumansquamous epithelial, Barrett esophagus (CPC), and squamous cell carcinoma cells (OE21), but was low in BAC cell lines (OE19, OE33). Mechanistically, bile acids down-regulated Cav1 expression by inhibition of the proteolytic cleavage of 125-kDa pre-SREBP1 from the endoplasmic reticulum/Golgi apparatus and nuclear translocation of active 68-kDa SREBP1. This block in SREBP1's posttranslational processing impaired transcriptional activation of SREBP1 response elements in the proximal human Cav1 promoter. Cav1 was also down-regulated in esophagi from C57BL/6 mice on a diet enriched with 1% (wt/wt) chenodeoxycholic acid. Mice deficient for Cav1 or the nuclear bile acid receptor farnesoid X receptor showed hyperplasia and hyperkeratosis of the basal cell layer of esophageal epithelia, respectively. These data indicate that bile acid-mediated down-regulation of Cav1 marks early changes in the squamous epithelium, which may contribute to onset of Barrett esophagus metaplasia and progression to BAC.

AB - Bile acids are synthesized from cholesterol and are major risk factors for Barrett adenocarcinoma (BAC) of the esophagus. Caveolin-1 (Cav1), a scaffold protein of membrane caveolae, is transcriptionally regulated by cholesterol via sterol-responsive element-binding protein-1 (SREBP1). Cav1 protects squamous epithelia by controlling cell growth and stabilizing cell junctions and matrix adhesion. Cav1 is frequently down-regulated in human cancers; however, the molecular mechanisms that lead to this event are unknown.Weshow that the basal layer of the nonneoplastic human esophageal squamous epithelium expressed Cav1 mainly at intercellular junctions. In contrast, Cav1 was lost in 95% of tissue specimens from BAC patients (n100). A strong cytoplasmic expression of Cav1 correlated with poor survival in a small subgroup (n5) ofBACpatients, and stable expression of an oncogenic Cav1 variant (Cav1-P132L) in the human BAC cell line OE19 promoted proliferation. Cav1 was also detectable in immortalizedhumansquamous epithelial, Barrett esophagus (CPC), and squamous cell carcinoma cells (OE21), but was low in BAC cell lines (OE19, OE33). Mechanistically, bile acids down-regulated Cav1 expression by inhibition of the proteolytic cleavage of 125-kDa pre-SREBP1 from the endoplasmic reticulum/Golgi apparatus and nuclear translocation of active 68-kDa SREBP1. This block in SREBP1's posttranslational processing impaired transcriptional activation of SREBP1 response elements in the proximal human Cav1 promoter. Cav1 was also down-regulated in esophagi from C57BL/6 mice on a diet enriched with 1% (wt/wt) chenodeoxycholic acid. Mice deficient for Cav1 or the nuclear bile acid receptor farnesoid X receptor showed hyperplasia and hyperkeratosis of the basal cell layer of esophageal epithelia, respectively. These data indicate that bile acid-mediated down-regulation of Cav1 marks early changes in the squamous epithelium, which may contribute to onset of Barrett esophagus metaplasia and progression to BAC.

UR - https://www.scopus.com/pages/publications/84860340369

U2 - 10.1210/me.2011-1140

DO - 10.1210/me.2011-1140

M3 - Article

C2 - 22474125

AN - SCOPUS:84860340369

SN - 0888-8809

VL - 26

SP - 819

EP - 832

JO - Molecular Endocrinology

JF - Molecular Endocrinology

IS - 5

ER -

Bile acids down-regulate caveolin-1 in esophageal epithelial cells through sterol responsive element-binding protein

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