The ESCRT-III molecules regulate the apical targeting of bile salt export pump

The ESCRT-III molecules regulate the apical targeting of bile salt export pump

Abstract Background The bile salt export pump (BSEP) is a pivotal apical/canalicular bile salt transporter in hepatocytes that drives the bile flow. Defects in BSEP function and canalicular expression could lead to a spectrum of cholestatic liver diseases. One prominent manifestation of BSEP-associa...

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Main Authors: Shang-Hsin Wu, Mei-Hwei Chang, Ya-Hui Chen, Hui-Lin Wu, Huey-Huey Chua, Chin-Sung Chien, Yen-Hsuan Ni, Hui-Ling Chen, Huey-Ling Chen
Format: Article
Language:English
Published: BMC 2021-03-01
Series:Journal of Biomedical Science
Subjects:
Apical trafficking
Bile salt export pump
Cholestasis
CHMP5
ESCRT
Liver development
Online Access:https://doi.org/10.1186/s12929-020-00706-2
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spelling doaj-b09117dbbc004da487680ebecda8e9202021-03-11T11:57:38ZengBMCJournal of Biomedical Science1423-01272021-03-0128111810.1186/s12929-020-00706-2The ESCRT-III molecules regulate the apical targeting of bile salt export pumpShang-Hsin Wu0Mei-Hwei Chang1Ya-Hui Chen2Hui-Lin Wu3Huey-Huey Chua4Chin-Sung Chien5Yen-Hsuan Ni6Hui-Ling Chen7Huey-Ling Chen8Graduate Institute of Clinical Medicine, National Taiwan University College of MedicineGraduate Institute of Clinical Medicine, National Taiwan University College of MedicineDepartment of Pediatrics, National Taiwan University College of Medicine and National Taiwan University Children’s HospitalGraduate Institute of Clinical Medicine, National Taiwan University College of MedicineDepartment of Pediatrics, National Taiwan University College of Medicine and National Taiwan University Children’s HospitalGraduate Institute of Clinical Medicine, National Taiwan University College of MedicineDepartment of Pediatrics, National Taiwan University College of Medicine and National Taiwan University Children’s HospitalHepatitis Research Center, National Taiwan University HospitalDepartment of Pediatrics, National Taiwan University College of Medicine and National Taiwan University Children’s HospitalAbstract Background The bile salt export pump (BSEP) is a pivotal apical/canalicular bile salt transporter in hepatocytes that drives the bile flow. Defects in BSEP function and canalicular expression could lead to a spectrum of cholestatic liver diseases. One prominent manifestation of BSEP-associated cholestasis is the defective canalicular localization and cytoplasmic retention of BSEP. However, the etiology of impaired BSEP targeting to the canalicular membrane is not fully understood. Our goal was to discover what molecule could interact with BSEP and affect its post-Golgi sorting. Methods The human BSEP amino acids (a.a.) 491-630 was used as bait to screen a human fetal liver cDNA library through yeast two-hybrid system. We identified a BSEP-interacting candidate and showed the interaction and colocalization in the co-immunoprecipitation in hepatoma cell lines and histological staining in human liver samples. Temperature shift assays were used to study the post-Golgi trafficking of BSEP. We further determine the functional impacts of the BSEP-interacting candidate on BSEP in vitro. A hydrodynamically injected mouse model was established for in vivo characterizing the long-term impacts on BSEP. Results We identified that charged multivesicular body protein 5 (CHMP5), a molecule of the endosomal protein complex required for transport subcomplex-III (ESCRT-III), interacted and co-localized with BSEP in the subapical compartments (SACs) in developing human livers. Cholestatic BSEP mutations in the CHMP5-interaction region have defects in canalicular targeting and aberrant retention at the SACs. Post-Golgi delivery of BSEP and bile acid secretion were impaired in ESCRT-III perturbation or CHMP5-knockdown hepatic cellular and mouse models. This ESCRT-III-mediated BSEP sorting preceded Rab11A-regulated apical cycling of BSEP. Conclusions Our results showed the first example that ESCRT-III is essential for canalicular trafficking of apical membrane proteins, and provide new targets for therapeutic approaches in BSEP associated cholestasis.https://doi.org/10.1186/s12929-020-00706-2Apical traffickingBile salt export pumpCholestasisCHMP5ESCRTLiver development
collection DOAJ
language English
format Article
sources DOAJ
author Shang-Hsin Wu
Mei-Hwei Chang
Ya-Hui Chen
Hui-Lin Wu
Huey-Huey Chua
Chin-Sung Chien
Yen-Hsuan Ni
Hui-Ling Chen
Huey-Ling Chen
spellingShingle Shang-Hsin Wu
Mei-Hwei Chang
Ya-Hui Chen
Hui-Lin Wu
Huey-Huey Chua
Chin-Sung Chien
Yen-Hsuan Ni
Hui-Ling Chen
Huey-Ling Chen
The ESCRT-III molecules regulate the apical targeting of bile salt export pump
Journal of Biomedical Science
Apical trafficking
Bile salt export pump
Cholestasis
CHMP5
ESCRT
Liver development
author_facet Shang-Hsin Wu
Mei-Hwei Chang
Ya-Hui Chen
Hui-Lin Wu
Huey-Huey Chua
Chin-Sung Chien
Yen-Hsuan Ni
Hui-Ling Chen
Huey-Ling Chen
author_sort Shang-Hsin Wu
title The ESCRT-III molecules regulate the apical targeting of bile salt export pump
title_short The ESCRT-III molecules regulate the apical targeting of bile salt export pump
title_full The ESCRT-III molecules regulate the apical targeting of bile salt export pump
title_fullStr The ESCRT-III molecules regulate the apical targeting of bile salt export pump
title_full_unstemmed The ESCRT-III molecules regulate the apical targeting of bile salt export pump
title_sort escrt-iii molecules regulate the apical targeting of bile salt export pump
publisher BMC
series Journal of Biomedical Science
issn 1423-0127
publishDate 2021-03-01
description Abstract Background The bile salt export pump (BSEP) is a pivotal apical/canalicular bile salt transporter in hepatocytes that drives the bile flow. Defects in BSEP function and canalicular expression could lead to a spectrum of cholestatic liver diseases. One prominent manifestation of BSEP-associated cholestasis is the defective canalicular localization and cytoplasmic retention of BSEP. However, the etiology of impaired BSEP targeting to the canalicular membrane is not fully understood. Our goal was to discover what molecule could interact with BSEP and affect its post-Golgi sorting. Methods The human BSEP amino acids (a.a.) 491-630 was used as bait to screen a human fetal liver cDNA library through yeast two-hybrid system. We identified a BSEP-interacting candidate and showed the interaction and colocalization in the co-immunoprecipitation in hepatoma cell lines and histological staining in human liver samples. Temperature shift assays were used to study the post-Golgi trafficking of BSEP. We further determine the functional impacts of the BSEP-interacting candidate on BSEP in vitro. A hydrodynamically injected mouse model was established for in vivo characterizing the long-term impacts on BSEP. Results We identified that charged multivesicular body protein 5 (CHMP5), a molecule of the endosomal protein complex required for transport subcomplex-III (ESCRT-III), interacted and co-localized with BSEP in the subapical compartments (SACs) in developing human livers. Cholestatic BSEP mutations in the CHMP5-interaction region have defects in canalicular targeting and aberrant retention at the SACs. Post-Golgi delivery of BSEP and bile acid secretion were impaired in ESCRT-III perturbation or CHMP5-knockdown hepatic cellular and mouse models. This ESCRT-III-mediated BSEP sorting preceded Rab11A-regulated apical cycling of BSEP. Conclusions Our results showed the first example that ESCRT-III is essential for canalicular trafficking of apical membrane proteins, and provide new targets for therapeutic approaches in BSEP associated cholestasis.
topic Apical trafficking
Bile salt export pump
Cholestasis
CHMP5
ESCRT
Liver development
url https://doi.org/10.1186/s12929-020-00706-2
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