High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles

While NF90 has been known to participate in transcription, translation and microRNA biogenesis, physiological functions of this protein still remain unclear. To uncover this, we generated transgenic (Tg) mice using NF90 cDNA under the control of β-actin promoter. The NF90 Tg mice exhibited a reducti...

Descripción completa

Detalles Bibliográficos
Autores principales: Higuchi, Takuma, Sakamoto, Shuji, Kakinuma, Yoshihiko, Kai, Shoko, Yagyu, Ken-ichi, Todaka, Hiroshi, Chi, Eunsup, Okada, Shoshiro, Ujihara, Takako, Morisawa, Keiko, Ono, Masafumi, Sugiyama, Yasunori, Ishida, Waka, Fukushima, Atsuki, Tsuda, Masayuki, Agata, Yasutoshi, Taniguchi, Taketoshi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3422296/
https://www.ncbi.nlm.nih.gov/pubmed/22912857
http://dx.doi.org/10.1371/journal.pone.0043340
_version_ 1782241031054426112
author Higuchi, Takuma
Sakamoto, Shuji
Kakinuma, Yoshihiko
Kai, Shoko
Yagyu, Ken-ichi
Todaka, Hiroshi
Chi, Eunsup
Okada, Shoshiro
Ujihara, Takako
Morisawa, Keiko
Ono, Masafumi
Sugiyama, Yasunori
Ishida, Waka
Fukushima, Atsuki
Tsuda, Masayuki
Agata, Yasutoshi
Taniguchi, Taketoshi
author_facet Higuchi, Takuma
Sakamoto, Shuji
Kakinuma, Yoshihiko
Kai, Shoko
Yagyu, Ken-ichi
Todaka, Hiroshi
Chi, Eunsup
Okada, Shoshiro
Ujihara, Takako
Morisawa, Keiko
Ono, Masafumi
Sugiyama, Yasunori
Ishida, Waka
Fukushima, Atsuki
Tsuda, Masayuki
Agata, Yasutoshi
Taniguchi, Taketoshi
author_sort Higuchi, Takuma
collection PubMed
description While NF90 has been known to participate in transcription, translation and microRNA biogenesis, physiological functions of this protein still remain unclear. To uncover this, we generated transgenic (Tg) mice using NF90 cDNA under the control of β-actin promoter. The NF90 Tg mice exhibited a reduction in body weight compared with wild-type mice, and a robust expression of NF90 was detected in skeletal muscle, heart and eye of the Tg mice. To evaluate the NF90 overexpression-induced physiological changes in the tissues, we performed a number of analyses including CT-analysis and hemodynamic test, revealing that the NF90 Tg mice developed skeletal muscular atrophy and heart failure. To explore causes of the abnormalities in the NF90 Tg mice, we performed histological and biochemical analyses for the skeletal and cardiac muscles of the Tg mice. Surprisingly, these analyses demonstrated that mitochondria in those muscular tissues of the Tg mice were degenerated by autophagy. To gain further insight into the cause for the mitochondrial degeneration, we identified NF90-associated factors by peptide mass fingerprinting. Of note, approximately half of the NF90-associated complexes were ribosome-related proteins. Interestingly, protein synthesis rate was significantly suppressed by high-expression of NF90. These observations suggest that NF90 would negatively regulate the function of ribosome via its interaction with the factors involved in the ribosome function. Furthermore, we found that the translations or protein stabilities of PGC-1 and NRF-1, which are critical transcription factors for expression of mitochondrial genes, were significantly depressed in the skeletal muscles of the NF90 Tg mice. Taken together, these findings suggest that the mitochondrial degeneration engaged in the skeletal muscle atrophy and the heart failure in the NF90 Tg mice may be caused by NF90-induced posttranscriptional repression of transcription factors such as PGC-1 and NRF-1 for regulating nuclear-encoded genes relevant to mitochondrial function.
format Online
Article
Text
id pubmed-3422296
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-34222962012-08-21 High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles Higuchi, Takuma Sakamoto, Shuji Kakinuma, Yoshihiko Kai, Shoko Yagyu, Ken-ichi Todaka, Hiroshi Chi, Eunsup Okada, Shoshiro Ujihara, Takako Morisawa, Keiko Ono, Masafumi Sugiyama, Yasunori Ishida, Waka Fukushima, Atsuki Tsuda, Masayuki Agata, Yasutoshi Taniguchi, Taketoshi PLoS One Research Article While NF90 has been known to participate in transcription, translation and microRNA biogenesis, physiological functions of this protein still remain unclear. To uncover this, we generated transgenic (Tg) mice using NF90 cDNA under the control of β-actin promoter. The NF90 Tg mice exhibited a reduction in body weight compared with wild-type mice, and a robust expression of NF90 was detected in skeletal muscle, heart and eye of the Tg mice. To evaluate the NF90 overexpression-induced physiological changes in the tissues, we performed a number of analyses including CT-analysis and hemodynamic test, revealing that the NF90 Tg mice developed skeletal muscular atrophy and heart failure. To explore causes of the abnormalities in the NF90 Tg mice, we performed histological and biochemical analyses for the skeletal and cardiac muscles of the Tg mice. Surprisingly, these analyses demonstrated that mitochondria in those muscular tissues of the Tg mice were degenerated by autophagy. To gain further insight into the cause for the mitochondrial degeneration, we identified NF90-associated factors by peptide mass fingerprinting. Of note, approximately half of the NF90-associated complexes were ribosome-related proteins. Interestingly, protein synthesis rate was significantly suppressed by high-expression of NF90. These observations suggest that NF90 would negatively regulate the function of ribosome via its interaction with the factors involved in the ribosome function. Furthermore, we found that the translations or protein stabilities of PGC-1 and NRF-1, which are critical transcription factors for expression of mitochondrial genes, were significantly depressed in the skeletal muscles of the NF90 Tg mice. Taken together, these findings suggest that the mitochondrial degeneration engaged in the skeletal muscle atrophy and the heart failure in the NF90 Tg mice may be caused by NF90-induced posttranscriptional repression of transcription factors such as PGC-1 and NRF-1 for regulating nuclear-encoded genes relevant to mitochondrial function. Public Library of Science 2012-08-17 /pmc/articles/PMC3422296/ /pubmed/22912857 http://dx.doi.org/10.1371/journal.pone.0043340 Text en © 2012 Higuchi et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Higuchi, Takuma
Sakamoto, Shuji
Kakinuma, Yoshihiko
Kai, Shoko
Yagyu, Ken-ichi
Todaka, Hiroshi
Chi, Eunsup
Okada, Shoshiro
Ujihara, Takako
Morisawa, Keiko
Ono, Masafumi
Sugiyama, Yasunori
Ishida, Waka
Fukushima, Atsuki
Tsuda, Masayuki
Agata, Yasutoshi
Taniguchi, Taketoshi
High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title_full High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title_fullStr High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title_full_unstemmed High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title_short High Expression of Nuclear Factor 90 (NF90) Leads to Mitochondrial Degradation in Skeletal and Cardiac Muscles
title_sort high expression of nuclear factor 90 (nf90) leads to mitochondrial degradation in skeletal and cardiac muscles
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3422296/
https://www.ncbi.nlm.nih.gov/pubmed/22912857
http://dx.doi.org/10.1371/journal.pone.0043340
work_keys_str_mv AT higuchitakuma highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT sakamotoshuji highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT kakinumayoshihiko highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT kaishoko highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT yagyukenichi highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT todakahiroshi highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT chieunsup highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT okadashoshiro highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT ujiharatakako highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT morisawakeiko highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT onomasafumi highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT sugiyamayasunori highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT ishidawaka highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT fukushimaatsuki highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT tsudamasayuki highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT agatayasutoshi highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles
AT taniguchitaketoshi highexpressionofnuclearfactor90nf90leadstomitochondrialdegradationinskeletalandcardiacmuscles

Ejemplares similares