Histone deacetylase inhibition prevents cell death induced by loss of tricellular tight junction proteins in temperature-sensitive mouse cochlear cells.

Kenichi Takano,Takashi Kojima,Shin Kikuchi,Tetsuo Himi,Yakuto Kaneko,Takayuki Kohno,Takuya Kakuki,Bin He

doi:10.1371/journal.pone.0182291

Kenichi Takano, Takashi Kojima + Show 6 more

Open Access

https://doi.org/10.1371/journal.pone.0182291

Copy DOI

Journal: PloS one	Publication Date: Aug 2, 2017
Citations: 7	License type: CC BY 4.0

Affiliation: Sapporo Medical University

Abstract

Tricellular tight junctions (tTJs) are specialized structures that occur where the corners of three cells meet to seal adjacent intercellular space. The molecular components of tTJs include tricellulin (TRIC) and lipolysis-stimulated lipoprotein receptor (LSR) which recruits TRIC, are required for normal hearing. Although loss of TRIC causes hearing loss with degeneration of cochlear cells, the detailed mechanisms remains unclear. In the present study, by using temperature-sensitive mouse cochlear cells, US/VOT-E36 cell line, we investigated the changes of TRIC and LSR during cochlear cell differentiation and the effects of histone deacetylase (HDAC) inhibitors against cell degeneration induced by loss of TRIC and LSR. During cell differentiation induced by the temperature change, expression of TRIC and LSR were clearly induced. Treatment with metformin enhanced expression TRIC and LSR via AMPK during cell differentiation. Loss of TRIC and LSR by the siRNAs induced cell death in differentiated cells. Treatment with HDAC inhibitors trichostatin A and HDAC6 inhibitor prevented the cell death induced by loss of TRIC and LSR. Collectively, these findings suggest that both tTJ proteins TRIC and LSR have crucial roles for the differentiated cochlear cell survival, and that HDAC inhibitors may be potential therapeutic agents to prevent hearing loss.

Highlights

The tight junctions (TJs) between epithelial cells are necessary to maintain cell polarity and the transepithelial barrier, and regulate the flow of solutes through paracellular spaces [1, 2]
Few TRIC molecules and LSRs were observed in the cytoplasm of undifferentiated cochlear cells; abundant TRIC molecules and LSRs were observed on the membrane and in the cytoplasm in differentiated counterparts (Fig 1A)
We found that knockdown of TRIC and LSR led to cochlear cell death via apoptosis and necrosis, which could be mitigated by treatment with either Trichostatin A (TSA) and iHDAC6

Summary

Introduction

The tight junctions (TJs) between epithelial cells are necessary to maintain cell polarity and the transepithelial barrier, and regulate the flow of solutes through paracellular spaces [1, 2]. TJs between epithelial cell that line the cochlear duct (or scala media) function to compartmentalize endolymph and perilymph [3]. Histone deacetylase inhibition prevents cochlear cell death induced by loss of tricellular tight junction

Methods

Results

Discussion

Conclusion