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早幼粒细胞白血病(PML)环指结构域的表面残基突变会改变与核基质相关的PML小体的形成。

Surface residue mutations of the PML RING finger domain alter the formation of nuclear matrix-associated PML bodies.

作者信息

Boddy M N, Duprez E, Borden K L, Freemont P S

机构信息

The Scripps Research Institute, Department of Molecular Biology, La Jolla, CA 92037, USA.

出版信息

J Cell Sci. 1997 Sep;110 ( Pt 18):2197-205. doi: 10.1242/jcs.110.18.2197.

Abstract

The human protein PML, was first identified as part of a fusion protein with retinoic acid receptor alpha as found in the chromosomal translocation which gives rise to acute promyelocytic leukaemia. PML is normally localised to large matrix-associated nuclear domains (known as ND10, Kr bodies, PODS or PML NBs) which comprise several multi-protein complexes. Within the PML protein, there are a number of identified zinc-binding domains, one of which called the RING finger is found in a large family of diverse and unrelated proteins. Here, we report the effect of site-directed mutations within the context of the whole PML protein, of amino acids found on the surface of the PML RING finger domain and PML NB formation in vivo. Mutations of a small region of the RING finger domain surface affect the size and numbers of PML NBs in a mouse fibroblast expression assay, resulting in fewer but larger exogenous PML NBs. Mutations of other surface RING residues, however, do not affect exogenous PML NB formation. Furthermore, all of the PML RING mutants co-localise to both endogenous and exogenous wild-type PML NBs. These data identify a specific region of the PML RING finger domain which is directly involved in correct PML NB formation. They also provide evidence to suggest that the PML RING finger is involved in mediating PML-PML oligomeric interactions, as part of a mechanism leading to the assembly of the PML NB complex.

摘要

人类蛋白质PML最初被鉴定为一种融合蛋白的一部分,该融合蛋白与视黄酸受体α相关,在导致急性早幼粒细胞白血病的染色体易位中被发现。PML通常定位于与基质相关的大型核结构域(称为ND10、Kr小体、POD或PML核小体),这些结构域由几种多蛋白复合物组成。在PML蛋白中,有许多已确定的锌结合结构域,其中一个称为RING指结构域,存在于一大类不同且不相关的蛋白质中。在此,我们报告了在整个PML蛋白背景下,PML RING指结构域表面氨基酸的定点突变对体内PML核小体形成的影响。在小鼠成纤维细胞表达试验中,RING指结构域表面一小区域的突变会影响PML核小体的大小和数量,导致外源PML核小体数量减少但体积增大。然而,其他表面RING残基的突变并不影响外源PML核小体的形成。此外,所有PML RING突变体都与内源性和外源性野生型PML核小体共定位。这些数据确定了PML RING指结构域中一个直接参与正确PML核小体形成的特定区域。它们还提供证据表明,PML RING指结构域参与介导PML - PML寡聚相互作用,作为导致PML核小体复合物组装机制的一部分。

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