NIR is degraded by the anaphase-promoting complex proteasome pathway

Jeong Ho Myong; Kang Kook Min; Kim Yang-Hee; Han Jin Seung

doi:10.2298/ABS1404493J

Archives of Biological Sciences (Jan 2014)

NIR is degraded by the anaphase-promoting complex proteasome pathway

Jeong Ho Myong,
Kang Kook Min,
Kim Yang-Hee,
Han Jin Seung

Affiliations

Jeong Ho Myong: Inje University, Department of Biological Sciences, Gimhae, Gyeongnam, Republic of Korea
Kang Kook Min: Inje University, Department of Biological Sciences, Gimhae, Gyeongnam, Republic of Korea
Kim Yang-Hee: Sejong University, Department of Molecular Biology, Seoul, Republic of Korea
Han Jin Seung: Inje University, Department of Biological Sciences, Gimhae, Gyeongnam, Republic of Korea

DOI: https://doi.org/10.2298/ABS1404493J
Journal volume & issue: Vol. 66, no. 4
pp. 1493 – 1502

Abstract

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Novel INHAT Repressor (NIR) is a histone acetylation inhibitor that can directly bind histone complexes and the tumor suppressors p53 and p63. Because NIR is mainly localized in the nucleolus and disappears from the nucleolus upon RNase treatment, it is thought to bind RNA or ribonucleoproteins. When NIR moves to the cytoplasm, it is immediately degraded; this degradation was blocked by MG132, a proteasome inhibitor. Furthermore, the central domain of NIR specifically bound APC-CCdh1. These data show that the stability of NIR is governed by the ubiquitin/proteasome pathway.

Published in Archives of Biological Sciences

ISSN: 0354-4664 (Print); 1821-4339 (Online)
Publisher: University of Belgrade, University of Novi Sad
Country of publisher: Serbia
LCC subjects: Science: Biology (General)
Website: http://www.serbiosoc.org.rs/arch/index.php

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