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A novel microscopy-based assay identifies extended synaptotagmin-1 (ESYT1) as a positive regulator of anoctamin 1 traffic
Authors:Joana R. Lérias  Madalena C. Pinto  Hugo M. Botelho  Nikhil T. Awatade  Margarida C. Quaresma  Iris A.L. Silva  Podchanart Wanitchakool  Rainer Schreiber  Rainer Pepperkok  Karl Kunzelmann  Margarida D. Amaral
Affiliation:1. University of Lisboa, Faculty of Sciences, BioISI - Biosystems & Integrative Sciences Institute, Campo Grande, C8, 1749-016 Lisboa, Portugal;2. Department of Physiology, University of Regensburg, Universitätsstrasse 31, 93053 Regensburg, Germany;3. Cell Biology and Biophysics Unit and Advanced Light Microscopy Facility, European Molecular Biology Laboratory (EMBL), Meyerhofstraße 1, 69117 Heidelberg, Germany
Abstract:An attractive possibility to treat Cystic Fibrosis (CF), a severe condition caused by dysfunctional CFTR, an epithelial anion channel, is through the activation of alternative (non-CFTR) anion channels. Anoctamin 1 (ANO1) was demonstrated to be a Ca2+-activated chloride channel (CaCC) and thus of high potential to replace CFTR. Despite that ANO1 is expressed in human lung CF tissue, it is present at the cell surface at very low levels. In addition, little is known about regulation of ANO1 traffic, namely which factors promote its plasma membrane (PM) localization.Here, we generated a novel cellular model, expressing an inducible 3HA-ANO1-eGFP construct, and validated its usage as a microscopy tool to monitor for ANO1 traffic.We demonstrate the robustness and specificity of this cell-based assay, by the identification of siRNAs acting both as ANO1 traffic enhancer and inhibitor, targeting respectively COPB1 and ESYT1 (extended synaptotagmin-1), the latter involved in coupling of the endoplasmic reticulum to the PM at specific microdomains. We further show that knockdown of ESYT1 (and family members ESYT2 and ESYT3) significantly decreased ANO1 current density.This ANO1 cell-based assay constitutes an important tool to be further used in high-throughput screens and drug discovery of high relevance for CF and cancer.
Keywords:ANO  Anoctamin  BSA  bovine serum albumin  CaCC  CF  cystic fibrosis  CFBE  cystic fibrosis bronchial epithelial (cells)  CFTR  cystic fibrosis transmembrane conductance regulator  Dox  doxycycline  ER  endoplasmic reticulum  EGFR  epidermal growth factor receptor  ERQC  ER quality control  ESYT1  extended synaptotagmin-1  HA  hemagglutinin  HTS  high throughput screening  SC  short circuit current  PBS  phosphate buffered saline  PFA  paraformaldehyde  PM  plasma membrane  TEER  transepithelial resistance  Vte  transepithelial voltage  WB  Western blot  Intracellular traffic  Endoplasmic reticulum  Calcium-activated chloride channels  Cystic fibrosis  Automated fluorescence microscopy
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