Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway

Cancer cells are characterized by malignant proliferation and aberrant metabolism and are thereby liable to the depletion of nutrients and accumulation of metabolic waste. To maintain cellular homeostasis, cancer cells are prone to upregulating the canonical autophagy pathway. Here, we identified pa...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Kun, Gong, Qing, Zhan, Yujuan, Chen, Bonan, Yin, Ting, Lu, Yuhua, Zhang, Yilin, Wang, Huiqi, Ke, Junzi, Du, Biaoyan, Liu, Xiaodong, Xiao, Jianyong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6987457/
https://www.ncbi.nlm.nih.gov/pubmed/32039209
http://dx.doi.org/10.3389/fcell.2019.00397
_version_ 1783492145401823232
author Wang, Kun
Gong, Qing
Zhan, Yujuan
Chen, Bonan
Yin, Ting
Lu, Yuhua
Zhang, Yilin
Wang, Huiqi
Ke, Junzi
Du, Biaoyan
Liu, Xiaodong
Xiao, Jianyong
author_facet Wang, Kun
Gong, Qing
Zhan, Yujuan
Chen, Bonan
Yin, Ting
Lu, Yuhua
Zhang, Yilin
Wang, Huiqi
Ke, Junzi
Du, Biaoyan
Liu, Xiaodong
Xiao, Jianyong
author_sort Wang, Kun
collection PubMed
description Cancer cells are characterized by malignant proliferation and aberrant metabolism and are thereby liable to the depletion of nutrients and accumulation of metabolic waste. To maintain cellular homeostasis, cancer cells are prone to upregulating the canonical autophagy pathway. Here, we identified paroxetine hydrochloride (Paxil) as a late autophagy inhibitor and investigated its killing effect on lung cancer cells and with a xenograft mouse model in vivo. Upregulated LC3-II and p62 expression indicated that Paxil inhibited autophagy. Acid-sensitive dyes (e.g., LysoTracker and AO staining) indicated reduced lysosomal acidity following Paxil treatment; consequently, the maturation of the pH-dependent hydroxylases (e.g., cathepsin B and D) substantially declined. Paxil also induced the fragmentation of mitochondria and further intensified ROS overproduction. Since the autophagy pathway was blocked, ROS rapidly accumulated, which activated JNK and p38 kinase. Such activity promoted the localization of Bax, which led to increased mitochondrial outer membrane permeability. The release of Cytochrome c with the loss of the membrane potential triggered a caspase cascade, ultimately leading to apoptosis. In contrast, the clearance of ROS by its scavenger, NAC, rescued Paxil-induced apoptosis accompanied by reduced p38 and JNK activation. Thus, Paxil blocked the autophagic flux and induced the mitochondria-dependent apoptosis via the ROS-MAPK pathway.
format Online
Article
Text
id pubmed-6987457
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-69874572020-02-07 Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway Wang, Kun Gong, Qing Zhan, Yujuan Chen, Bonan Yin, Ting Lu, Yuhua Zhang, Yilin Wang, Huiqi Ke, Junzi Du, Biaoyan Liu, Xiaodong Xiao, Jianyong Front Cell Dev Biol Cell and Developmental Biology Cancer cells are characterized by malignant proliferation and aberrant metabolism and are thereby liable to the depletion of nutrients and accumulation of metabolic waste. To maintain cellular homeostasis, cancer cells are prone to upregulating the canonical autophagy pathway. Here, we identified paroxetine hydrochloride (Paxil) as a late autophagy inhibitor and investigated its killing effect on lung cancer cells and with a xenograft mouse model in vivo. Upregulated LC3-II and p62 expression indicated that Paxil inhibited autophagy. Acid-sensitive dyes (e.g., LysoTracker and AO staining) indicated reduced lysosomal acidity following Paxil treatment; consequently, the maturation of the pH-dependent hydroxylases (e.g., cathepsin B and D) substantially declined. Paxil also induced the fragmentation of mitochondria and further intensified ROS overproduction. Since the autophagy pathway was blocked, ROS rapidly accumulated, which activated JNK and p38 kinase. Such activity promoted the localization of Bax, which led to increased mitochondrial outer membrane permeability. The release of Cytochrome c with the loss of the membrane potential triggered a caspase cascade, ultimately leading to apoptosis. In contrast, the clearance of ROS by its scavenger, NAC, rescued Paxil-induced apoptosis accompanied by reduced p38 and JNK activation. Thus, Paxil blocked the autophagic flux and induced the mitochondria-dependent apoptosis via the ROS-MAPK pathway. Frontiers Media S.A. 2020-01-22 /pmc/articles/PMC6987457/ /pubmed/32039209 http://dx.doi.org/10.3389/fcell.2019.00397 Text en Copyright © 2020 Wang, Gong, Zhan, Chen, Yin, Lu, Zhang, Wang, Ke, Du, Liu and Xiao. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cell and Developmental Biology
Wang, Kun
Gong, Qing
Zhan, Yujuan
Chen, Bonan
Yin, Ting
Lu, Yuhua
Zhang, Yilin
Wang, Huiqi
Ke, Junzi
Du, Biaoyan
Liu, Xiaodong
Xiao, Jianyong
Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title_full Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title_fullStr Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title_full_unstemmed Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title_short Blockage of Autophagic Flux and Induction of Mitochondria Fragmentation by Paroxetine Hydrochloride in Lung Cancer Cells Promotes Apoptosis via the ROS-MAPK Pathway
title_sort blockage of autophagic flux and induction of mitochondria fragmentation by paroxetine hydrochloride in lung cancer cells promotes apoptosis via the ros-mapk pathway
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6987457/
https://www.ncbi.nlm.nih.gov/pubmed/32039209
http://dx.doi.org/10.3389/fcell.2019.00397
work_keys_str_mv AT wangkun blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT gongqing blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT zhanyujuan blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT chenbonan blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT yinting blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT luyuhua blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT zhangyilin blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT wanghuiqi blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT kejunzi blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT dubiaoyan blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT liuxiaodong blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway
AT xiaojianyong blockageofautophagicfluxandinductionofmitochondriafragmentationbyparoxetinehydrochlorideinlungcancercellspromotesapoptosisviatherosmapkpathway

Ejemplares similares