Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions

The BCNT (Bucentaur) superfamily is classified by an uncharacteristic conserved sequence of ∼80 amino acids (aa) at the C-terminus, BCNT-C (the conserved C-terminal region of Bcnt/Cfdp1). Whereas the yeast Swc5 and Drosophila Yeti homologues play crucial roles in chromatin remodelling organization,...

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Autores principales: Iwashita, Shintaro, Suzuki, Takehiro, Yasuda, Takeshi, Nakashima, Kentaro, Sakamoto, Taiichi, Kohno, Toshiyuki, Takahashi, Ichiro, Kobayashi, Takayasu, Ohno-Iwashita, Yoshiko, Imajoh-Ohmi, Shinobu, Song, Si-Young, Dohmae, Naoshi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Portland Press Ltd. 2015
Materias:
Original Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4613681/
https://www.ncbi.nlm.nih.gov/pubmed/26182435
http://dx.doi.org/10.1042/BSR20150111
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author Iwashita, Shintaro
Suzuki, Takehiro
Yasuda, Takeshi
Nakashima, Kentaro
Sakamoto, Taiichi
Kohno, Toshiyuki
Takahashi, Ichiro
Kobayashi, Takayasu
Ohno-Iwashita, Yoshiko
Imajoh-Ohmi, Shinobu
Song, Si-Young
Dohmae, Naoshi
author_facet Iwashita, Shintaro
Suzuki, Takehiro
Yasuda, Takeshi
Nakashima, Kentaro
Sakamoto, Taiichi
Kohno, Toshiyuki
Takahashi, Ichiro
Kobayashi, Takayasu
Ohno-Iwashita, Yoshiko
Imajoh-Ohmi, Shinobu
Song, Si-Young
Dohmae, Naoshi
author_sort Iwashita, Shintaro
collection PubMed
description The BCNT (Bucentaur) superfamily is classified by an uncharacteristic conserved sequence of ∼80 amino acids (aa) at the C-terminus, BCNT-C (the conserved C-terminal region of Bcnt/Cfdp1). Whereas the yeast Swc5 and Drosophila Yeti homologues play crucial roles in chromatin remodelling organization, mammalian Bcnt/Cfdp1 (craniofacial developmental protein 1) remains poorly understood. The protein, which lacks cysteine, is largely disordered and comprises an acidic N-terminal region, a lysine/glutamic acid/proline-rich 40 aa sequence and BCNT-C. It shows complex mobility on SDS/PAGE at ∼50 kDa, whereas its calculated molecular mass is ∼33 kDa. To characterize this mobility discrepancy and the effects of post-translational modifications (PTMs), we expressed various deleted His–Bcnt in E. coli and HEK cells and found that an acidic stretch in the N-terminal region is a main cause of the gel shift. Exogenous BCNT/CFDP1 constitutively expressed in HEK clones appears as a doublet at 49 and 47 kDa, slower than the protein expressed in Escherichia coli but faster than the endogenous protein on SDS/PAGE. Among seven in vivo phosphorylation sites, Ser(250), which resides in a region between disordered and ordered regions in BCNT-C, is heavily phosphorylated and detected predominantly in the 49 kDa band. Together with experiments involving treatment with phosphatases and Ser(250) substitutions, the results indicate that the complex behaviour of Bcnt/Cfdp1 on SDS/PAGE is caused mainly by an acidic stretch in the N-terminal region and Ser(250) phosphorylation in BCNT-C. Furthermore, Bcnt/Cfdp1 is acetylated in vitro by CREB-binding protein (CBP) and four lysine residues including Lys(268) in BCNT-C are also acetylated in vivo, revealing a protein regulated at multiple levels.
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spelling pubmed-46136812015-11-02 Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions Iwashita, Shintaro Suzuki, Takehiro Yasuda, Takeshi Nakashima, Kentaro Sakamoto, Taiichi Kohno, Toshiyuki Takahashi, Ichiro Kobayashi, Takayasu Ohno-Iwashita, Yoshiko Imajoh-Ohmi, Shinobu Song, Si-Young Dohmae, Naoshi Biosci Rep Original Papers The BCNT (Bucentaur) superfamily is classified by an uncharacteristic conserved sequence of ∼80 amino acids (aa) at the C-terminus, BCNT-C (the conserved C-terminal region of Bcnt/Cfdp1). Whereas the yeast Swc5 and Drosophila Yeti homologues play crucial roles in chromatin remodelling organization, mammalian Bcnt/Cfdp1 (craniofacial developmental protein 1) remains poorly understood. The protein, which lacks cysteine, is largely disordered and comprises an acidic N-terminal region, a lysine/glutamic acid/proline-rich 40 aa sequence and BCNT-C. It shows complex mobility on SDS/PAGE at ∼50 kDa, whereas its calculated molecular mass is ∼33 kDa. To characterize this mobility discrepancy and the effects of post-translational modifications (PTMs), we expressed various deleted His–Bcnt in E. coli and HEK cells and found that an acidic stretch in the N-terminal region is a main cause of the gel shift. Exogenous BCNT/CFDP1 constitutively expressed in HEK clones appears as a doublet at 49 and 47 kDa, slower than the protein expressed in Escherichia coli but faster than the endogenous protein on SDS/PAGE. Among seven in vivo phosphorylation sites, Ser(250), which resides in a region between disordered and ordered regions in BCNT-C, is heavily phosphorylated and detected predominantly in the 49 kDa band. Together with experiments involving treatment with phosphatases and Ser(250) substitutions, the results indicate that the complex behaviour of Bcnt/Cfdp1 on SDS/PAGE is caused mainly by an acidic stretch in the N-terminal region and Ser(250) phosphorylation in BCNT-C. Furthermore, Bcnt/Cfdp1 is acetylated in vitro by CREB-binding protein (CBP) and four lysine residues including Lys(268) in BCNT-C are also acetylated in vivo, revealing a protein regulated at multiple levels. Portland Press Ltd. 2015-07-14 /pmc/articles/PMC4613681/ /pubmed/26182435 http://dx.doi.org/10.1042/BSR20150111 Text en © 2015 Authors http://creativecommons.org/licenses/by/3.0/ This is an open access article published by Portland Press Limited and distributed under the Creative Commons Attribution Licence 3.0 (http://creativecommons.org/licenses/by/3.0/) .
spellingShingle Original Papers
Iwashita, Shintaro
Suzuki, Takehiro
Yasuda, Takeshi
Nakashima, Kentaro
Sakamoto, Taiichi
Kohno, Toshiyuki
Takahashi, Ichiro
Kobayashi, Takayasu
Ohno-Iwashita, Yoshiko
Imajoh-Ohmi, Shinobu
Song, Si-Young
Dohmae, Naoshi
Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title_full Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title_fullStr Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title_full_unstemmed Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title_short Mammalian Bcnt/Cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered N-terminal and Ser(250) phosphorylation in the conserved C-terminal regions
title_sort mammalian bcnt/cfdp1, a potential epigenetic factor characterized by an acidic stretch in the disordered n-terminal and ser(250) phosphorylation in the conserved c-terminal regions
topic Original Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4613681/
https://www.ncbi.nlm.nih.gov/pubmed/26182435
http://dx.doi.org/10.1042/BSR20150111
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