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黑色素瘤抗原-D2:一种在细胞周期和细胞应激后发生定位改变的核仁蛋白。

Melanoma antigen-D2: A nucleolar protein undergoing delocalization during cell cycle and after cellular stress.

作者信息

Pirlot Céline, Thiry Marc, Trussart Charlotte, Di Valentin Emmanuel, Piette Jacques, Habraken Yvette

机构信息

Laboratory of Virology and Immunology, GIGA-Signal Transduction, GIGA-B34, University of Liège, Liège, Belgium.

Unit of Cell and Tissue Biology, GIGA-Neurosciences, University of Liège, Liège, Belgium.

出版信息

Biochim Biophys Acta. 2016 Apr;1863(4):581-95. doi: 10.1016/j.bbamcr.2015.12.010. Epub 2015 Dec 17.

Abstract

Melanoma antigen D2 (MAGE-D2) is recognized as a cancer diagnostic marker; however, it has poorly characterized functions. Here, we established its intracellular localization and shuttling during cell cycle progression and in response to cellular stress. In normal conditions, MAGE-D2 is present in the cytoplasm, nucleoplasm, and nucleoli. Within the latter, MAGE-D2 is mostly found in the granular and the dense fibrillar components, and it interacts with nucleolin. Transfection of MAGE-D2 deletion mutants demonstrated that Δ203-254 leads to confinement of MAGE-D2 to the cytoplasm, while Δ248-254 prevents its accumulation in nucleoli but still allows its presence in the nucleoplasm. Consequently, this short sequence belongs to a nucleolar localization signal. MAGE-D2 deletion does not alter the nucleolar organization or rRNA levels. However, its intracellular localization varies with the cell cycle in a different kinetic than nucleolin. After genotoxic and nucleolar stresses, MAGE-D2 is excluded from nucleoli and concentrates in the nucleoplasm. We demonstrated that its camptothecin-related delocalization results from two distinct events: a rapid nucleolar release and a slower phospho-ERK-dependent cytoplasm to nucleoplasm translocation, which results from an increased flux from the cytoplasm to nucleoplasm. In conclusion, MAGE-D2 is a dynamic protein whose shuttling properties could suggest a role in cell cycle regulation.

摘要

黑色素瘤抗原D2(MAGE-D2)被认为是一种癌症诊断标志物;然而,其功能特性却鲜为人知。在此,我们确定了它在细胞周期进程中以及对细胞应激反应时的细胞内定位和穿梭情况。在正常条件下,MAGE-D2存在于细胞质、核质和核仁中。在核仁内,MAGE-D2主要存在于颗粒成分和致密纤维成分中,并且它与核仁素相互作用。MAGE-D2缺失突变体的转染表明,Δ203 - 254导致MAGE-D2局限于细胞质中,而Δ248 - 254阻止其在核仁中积累,但仍允许其存在于核质中。因此,这个短序列属于一个核仁定位信号。MAGE-D2的缺失不会改变核仁组织或rRNA水平。然而,其细胞内定位在细胞周期中的变化动力学与核仁素不同。在基因毒性和核仁应激后,MAGE-D2被排除在核仁之外并集中在核质中。我们证明其与喜树碱相关的重新定位是由两个不同的事件导致的:一个快速的核仁释放和一个较慢的磷酸化ERK依赖的从细胞质到核质的转运,这是由于从细胞质到核质的通量增加所致。总之,MAGE-D2是一种动态蛋白,其穿梭特性可能表明它在细胞周期调控中发挥作用。

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