BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways

Dysregulation of the circadian timing system (CTS) frequently appears during colorectal cancer (CRC) progression. In order to better understand the role of the circadian clock in CRC progression, this study evaluated in vitro how knockdown of a core circadian protein BMAL1 (BMAL1-KD) influenced the...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhang, Yuan, Devocelle, Aurore, Souza, Lucas, Foudi, Adlen, Tenreira Bento, Sabrina, Desterke, Christophe, Sherrard, Rachel, Ballesta, Annabelle, Adam, Rene, Giron-Michel, Julien, Chang, Yunhua
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2020
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7244025/
https://www.ncbi.nlm.nih.gov/pubmed/32388500
http://dx.doi.org/10.18632/aging.103124
_version_ 1783537498852425728
author Zhang, Yuan
Devocelle, Aurore
Souza, Lucas
Foudi, Adlen
Tenreira Bento, Sabrina
Desterke, Christophe
Sherrard, Rachel
Ballesta, Annabelle
Adam, Rene
Giron-Michel, Julien
Chang, Yunhua
author_facet Zhang, Yuan
Devocelle, Aurore
Souza, Lucas
Foudi, Adlen
Tenreira Bento, Sabrina
Desterke, Christophe
Sherrard, Rachel
Ballesta, Annabelle
Adam, Rene
Giron-Michel, Julien
Chang, Yunhua
author_sort Zhang, Yuan
collection PubMed
description Dysregulation of the circadian timing system (CTS) frequently appears during colorectal cancer (CRC) progression. In order to better understand the role of the circadian clock in CRC progression, this study evaluated in vitro how knockdown of a core circadian protein BMAL1 (BMAL1-KD) influenced the behavior of two primary human CRC cell lines (HCT116 and SW480) and a metastatic CRC cell line (SW620). Unexpectedly, BMAL1-KD induced CRC cell-type specific responses rather than the same phenomenon throughout. First, BMAL1-KD increased AKT/mTOR activation in each CRC cell line, but to different extents. Second, BMAL1-KD-induced P53 activation varied with cell context. In a wild type P53 background, HCT116 BMAL1-KD cells quickly underwent apoptosis after shBMAL1 lentivirus transduction, while surviving cells showed less P53 but increased AKT/mTOR activation, which ultimately caused higher proliferation. In the presence of a partially functional mutant P53, SW480 BMAL1-KD cells showed moderate P53 and mTOR activation simultaneously with cell senescence. With a moderate increased AKT but unchanged mutant P53 activation, SW620 BMAL1-KD cells grew faster. Thus, under different CRC cellular pathological contexts, BMAL1 knockdown induced relatively equal effects on AKT/mTOR activation but different effects on P53 activation, which finally triggered different CRC cell fates.
format Online
Article
Text
id pubmed-7244025
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Impact Journals
record_format MEDLINE/PubMed
spelling pubmed-72440252020-06-03 BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways Zhang, Yuan Devocelle, Aurore Souza, Lucas Foudi, Adlen Tenreira Bento, Sabrina Desterke, Christophe Sherrard, Rachel Ballesta, Annabelle Adam, Rene Giron-Michel, Julien Chang, Yunhua Aging (Albany NY) Research Paper Dysregulation of the circadian timing system (CTS) frequently appears during colorectal cancer (CRC) progression. In order to better understand the role of the circadian clock in CRC progression, this study evaluated in vitro how knockdown of a core circadian protein BMAL1 (BMAL1-KD) influenced the behavior of two primary human CRC cell lines (HCT116 and SW480) and a metastatic CRC cell line (SW620). Unexpectedly, BMAL1-KD induced CRC cell-type specific responses rather than the same phenomenon throughout. First, BMAL1-KD increased AKT/mTOR activation in each CRC cell line, but to different extents. Second, BMAL1-KD-induced P53 activation varied with cell context. In a wild type P53 background, HCT116 BMAL1-KD cells quickly underwent apoptosis after shBMAL1 lentivirus transduction, while surviving cells showed less P53 but increased AKT/mTOR activation, which ultimately caused higher proliferation. In the presence of a partially functional mutant P53, SW480 BMAL1-KD cells showed moderate P53 and mTOR activation simultaneously with cell senescence. With a moderate increased AKT but unchanged mutant P53 activation, SW620 BMAL1-KD cells grew faster. Thus, under different CRC cellular pathological contexts, BMAL1 knockdown induced relatively equal effects on AKT/mTOR activation but different effects on P53 activation, which finally triggered different CRC cell fates. Impact Journals 2020-05-10 /pmc/articles/PMC7244025/ /pubmed/32388500 http://dx.doi.org/10.18632/aging.103124 Text en Copyright © 2020 Zhang et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Zhang, Yuan
Devocelle, Aurore
Souza, Lucas
Foudi, Adlen
Tenreira Bento, Sabrina
Desterke, Christophe
Sherrard, Rachel
Ballesta, Annabelle
Adam, Rene
Giron-Michel, Julien
Chang, Yunhua
BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title_full BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title_fullStr BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title_full_unstemmed BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title_short BMAL1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between AKT/mTOR and P53/P21 pathways
title_sort bmal1 knockdown triggers different colon carcinoma cell fates by altering the delicate equilibrium between akt/mtor and p53/p21 pathways
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7244025/
https://www.ncbi.nlm.nih.gov/pubmed/32388500
http://dx.doi.org/10.18632/aging.103124
work_keys_str_mv AT zhangyuan bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT devocelleaurore bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT souzalucas bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT foudiadlen bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT tenreirabentosabrina bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT desterkechristophe bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT sherrardrachel bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT ballestaannabelle bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT adamrene bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT gironmicheljulien bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways
AT changyunhua bmal1knockdowntriggersdifferentcoloncarcinomacellfatesbyalteringthedelicateequilibriumbetweenaktmtorandp53p21pathways

Ejemplares similares