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Katanin-p80 Gene Promoter Characterization and Regulation via Elk1

Katanin is an ATPase family member protein that participates in microtubule severing. It has heterodimeric structure consisting of 60 kDa (katanin-p60) and 80 kDa (katanin-p80) subunits encoded by KATNA1 and KATNB1 genes, respectively. Katanin-p60 has the enzymatic activity for microtubule severing,...

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Autores principales: Selçuk, Ece, Kırımtay, Koray, Canbaz, Derya, Cesur, Güher Işık, Korulu, Sirin, Karabay, Arzu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3722181/
https://www.ncbi.nlm.nih.gov/pubmed/23894477
http://dx.doi.org/10.1371/journal.pone.0069423
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author Selçuk, Ece
Kırımtay, Koray
Canbaz, Derya
Cesur, Güher Işık
Korulu, Sirin
Karabay, Arzu
author_facet Selçuk, Ece
Kırımtay, Koray
Canbaz, Derya
Cesur, Güher Işık
Korulu, Sirin
Karabay, Arzu
author_sort Selçuk, Ece
collection PubMed
description Katanin is an ATPase family member protein that participates in microtubule severing. It has heterodimeric structure consisting of 60 kDa (katanin-p60) and 80 kDa (katanin-p80) subunits encoded by KATNA1 and KATNB1 genes, respectively. Katanin-p60 has the enzymatic activity for microtubule severing, whereas katanin-p80 consists of multiple domains with different functions such as targeting katanin-p60 to the centrosome, augmenting microtubule severing by katanin-p60, and even suppressing microtubule severing. Despite the various important functions of katanin-p80, its transcriptional regulation has not been studied yet. Elk1 transcription factor has been shown to interact with microtubules and regulate the transcription of another microtubule severing protein, spastin. In spite of katanin’s importance, and structural and functional similarities to spastin, there is no study on the transcriptional regulation of katanin yet. In this study, we aimed to characterize KATNB1 promoter and analyze the effects of Elk1 on katanin-p80 expression. We identified a 518- bp TATA-less promoter including a critical CpG island and GC boxes as an optimal promoter, and sequential deletion of CpG island and the GC elements gradually decreased the KATNB1 promoter activity. In addition, we showed Elk1 binding on the KATNB1 promoter by EMSA. We found that Elk1 activated KATNB1 promoter, and increased both mRNA and protein levels of katanin-p80 in SH-SY5Y cells. On the other hand, KCl treatment increasing SUMOylation decreased KATNB1 promoter activity. Since microtubule severing is an important cellular mechanism of which malfunctions result in serious diseases such as spastic paraplegia, Alzheimer’s disease and cell cycle related disorders, identification of KATNB1 transcriptional regulation is crucial in understanding the coordination of microtubule severing activity by different proteins in the cells.
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spelling pubmed-37221812013-07-26 Katanin-p80 Gene Promoter Characterization and Regulation via Elk1 Selçuk, Ece Kırımtay, Koray Canbaz, Derya Cesur, Güher Işık Korulu, Sirin Karabay, Arzu PLoS One Research Article Katanin is an ATPase family member protein that participates in microtubule severing. It has heterodimeric structure consisting of 60 kDa (katanin-p60) and 80 kDa (katanin-p80) subunits encoded by KATNA1 and KATNB1 genes, respectively. Katanin-p60 has the enzymatic activity for microtubule severing, whereas katanin-p80 consists of multiple domains with different functions such as targeting katanin-p60 to the centrosome, augmenting microtubule severing by katanin-p60, and even suppressing microtubule severing. Despite the various important functions of katanin-p80, its transcriptional regulation has not been studied yet. Elk1 transcription factor has been shown to interact with microtubules and regulate the transcription of another microtubule severing protein, spastin. In spite of katanin’s importance, and structural and functional similarities to spastin, there is no study on the transcriptional regulation of katanin yet. In this study, we aimed to characterize KATNB1 promoter and analyze the effects of Elk1 on katanin-p80 expression. We identified a 518- bp TATA-less promoter including a critical CpG island and GC boxes as an optimal promoter, and sequential deletion of CpG island and the GC elements gradually decreased the KATNB1 promoter activity. In addition, we showed Elk1 binding on the KATNB1 promoter by EMSA. We found that Elk1 activated KATNB1 promoter, and increased both mRNA and protein levels of katanin-p80 in SH-SY5Y cells. On the other hand, KCl treatment increasing SUMOylation decreased KATNB1 promoter activity. Since microtubule severing is an important cellular mechanism of which malfunctions result in serious diseases such as spastic paraplegia, Alzheimer’s disease and cell cycle related disorders, identification of KATNB1 transcriptional regulation is crucial in understanding the coordination of microtubule severing activity by different proteins in the cells. Public Library of Science 2013-07-24 /pmc/articles/PMC3722181/ /pubmed/23894477 http://dx.doi.org/10.1371/journal.pone.0069423 Text en © 2013 Selçuk 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
Selçuk, Ece
Kırımtay, Koray
Canbaz, Derya
Cesur, Güher Işık
Korulu, Sirin
Karabay, Arzu
Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title_full Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title_fullStr Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title_full_unstemmed Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title_short Katanin-p80 Gene Promoter Characterization and Regulation via Elk1
title_sort katanin-p80 gene promoter characterization and regulation via elk1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3722181/
https://www.ncbi.nlm.nih.gov/pubmed/23894477
http://dx.doi.org/10.1371/journal.pone.0069423
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