FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.

Ribosomal RNA large subunit methyltransferase J (RrmJ), an Escherichia coli heat shock protein, is responsible for 2'-O-ribose methylation in 23S rRNA. In mammals, three close homologs of RrmJ have been identified and have been designated as FTSJ1, FTSJ2 and FTSJ3; however, little is known abou...

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Main Authors: Cheng-Wei Lai, Hsiao-Ling Chen, Ken-Yo Lin, Fang-Chueh Liu, Kowit-Yu Chong, Winston T K Cheng, Chuan-Mu Chen
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3942483?pdf=render
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spelling doaj-74eaf7f18d80453888016d5dda2129022020-11-25T02:06:26ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0193e9081810.1371/journal.pone.0090818FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.Cheng-Wei LaiHsiao-Ling ChenKen-Yo LinFang-Chueh LiuKowit-Yu ChongWinston T K ChengChuan-Mu ChenRibosomal RNA large subunit methyltransferase J (RrmJ), an Escherichia coli heat shock protein, is responsible for 2'-O-ribose methylation in 23S rRNA. In mammals, three close homologs of RrmJ have been identified and have been designated as FTSJ1, FTSJ2 and FTSJ3; however, little is known about these genes. In this study, we characterized the mammalian FTSJ2, which was the most related protein to RrmJ in a phylogenetic analysis that had similar amino acid sequence features and tertiary protein structures of RrmJ. FTSJ2 was first identified in this study as a nucleus encoded mitochondrial protein that preserves the heat shock protein character in mammals in which the mRNA expressions was increased in porcine lung tissues and A549 cells after heat shock treatment. In addition, a recent study in non-small cell lung cancer (NSCLC) suggested that the FTSJ2 gene is located in a novel oncogenic locus. However, our results demonstrate that the expression of FTSJ2 mRNA was decreased in the more invasive subline (CL1-5) of the lung adenocarcinoma cells (CL1) compared with the less invasive subline (CL1-0), and overexpression of FTSJ2 resulted in the inhibition of cell invasion and migration in the rhabdomyosarcoma cell (TE671). In conclusion, our findings indicate that mammalian FTSJ2 is a mitochondrial ortholog of E. coli RrmJ and conserves the heat shock protein properties. Moreover, FTSJ2 possesses suppressive effects on the invasion and migration of cancer cells.http://europepmc.org/articles/PMC3942483?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Cheng-Wei Lai
Hsiao-Ling Chen
Ken-Yo Lin
Fang-Chueh Liu
Kowit-Yu Chong
Winston T K Cheng
Chuan-Mu Chen
spellingShingle Cheng-Wei Lai
Hsiao-Ling Chen
Ken-Yo Lin
Fang-Chueh Liu
Kowit-Yu Chong
Winston T K Cheng
Chuan-Mu Chen
FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
PLoS ONE
author_facet Cheng-Wei Lai
Hsiao-Ling Chen
Ken-Yo Lin
Fang-Chueh Liu
Kowit-Yu Chong
Winston T K Cheng
Chuan-Mu Chen
author_sort Cheng-Wei Lai
title FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
title_short FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
title_full FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
title_fullStr FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
title_full_unstemmed FTSJ2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
title_sort ftsj2, a heat shock-inducible mitochondrial protein, suppresses cell invasion and migration.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Ribosomal RNA large subunit methyltransferase J (RrmJ), an Escherichia coli heat shock protein, is responsible for 2'-O-ribose methylation in 23S rRNA. In mammals, three close homologs of RrmJ have been identified and have been designated as FTSJ1, FTSJ2 and FTSJ3; however, little is known about these genes. In this study, we characterized the mammalian FTSJ2, which was the most related protein to RrmJ in a phylogenetic analysis that had similar amino acid sequence features and tertiary protein structures of RrmJ. FTSJ2 was first identified in this study as a nucleus encoded mitochondrial protein that preserves the heat shock protein character in mammals in which the mRNA expressions was increased in porcine lung tissues and A549 cells after heat shock treatment. In addition, a recent study in non-small cell lung cancer (NSCLC) suggested that the FTSJ2 gene is located in a novel oncogenic locus. However, our results demonstrate that the expression of FTSJ2 mRNA was decreased in the more invasive subline (CL1-5) of the lung adenocarcinoma cells (CL1) compared with the less invasive subline (CL1-0), and overexpression of FTSJ2 resulted in the inhibition of cell invasion and migration in the rhabdomyosarcoma cell (TE671). In conclusion, our findings indicate that mammalian FTSJ2 is a mitochondrial ortholog of E. coli RrmJ and conserves the heat shock protein properties. Moreover, FTSJ2 possesses suppressive effects on the invasion and migration of cancer cells.
url http://europepmc.org/articles/PMC3942483?pdf=render
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