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核定位信号的比较诱变揭示了中性和酸性氨基酸的重要性。

Comparative mutagenesis of nuclear localization signals reveals the importance of neutral and acidic amino acids.

作者信息

Makkerh J P, Dingwall C, Laskey R A

机构信息

Wellcome/CRC Institute, Tennis Court Road, Cambridge CB2 1QR UK.

出版信息

Curr Biol. 1996 Aug 1;6(8):1025-7. doi: 10.1016/s0960-9822(02)00648-6.

DOI:10.1016/s0960-9822(02)00648-6
PMID:8805337
Abstract

Nuclear proteins contain information within their primary structures which causes them to accumulate selectively in the nucleus [1,2] by associating with the cytosolic receptor importin [3]. The alpha subunit of importin binds the nuclear localization signal (NLS), and the beta subunit docks at the nuclear pore complex. The NLS of the simian virus 40 large T-antigen (SV40 T-ag) is a single cluster of basic amino acids (PKKKRKV132; single-letter code, the basic amino acids are shown in bold; [4,5]), whereas the NLS of nucleoplasmin is bipartite. The nucleoplasmin NLS requires two essential clusters of basic amino acids, separated by a mutation-tolerant spacer (KRPAATKKAGQAKKKK171; [6] [7]). A SwissProt database search shows that more than 50% of nuclear proteins contain a match to this consensus, and many NLSs have since been found to conform to this type of motif in yeast, plants and animals [8-10]. A different NLS (PAAKRVKLD) has been reported in the oncoprotein c-Myc, but it has received little attention because, unlike other known NLSs, only three of nine residues are basic [11], and one residue is even acidic. Here, we report that constructs containing an inactive basic cluster downstream of the bipartite signal of nucleoplasmin can be directed to the nucleus by flanking them with specific neutral and acidic residues taken from the signal reported for c-Myc. Nuclear targeting by the single cluster KKKK is dependent on it being preceded by PAA and is stimulated if it is followed by the dipeptide LD. The relative positions of these elements are crucial to the function of these NLSs. All regions of the unconventional signal of c-Myc are functionally important. Contrary to conventional views, neutral and even acidic amino acids can play crucial roles in NLSs.

摘要

核蛋白在其一级结构中包含一些信息,这些信息使其通过与胞质受体输入蛋白结合而选择性地在细胞核中积累[1,2]。输入蛋白的α亚基结合核定位信号(NLS),β亚基停靠在核孔复合体上。猿猴病毒40大T抗原(SV40 T-ag)的NLS是一组单一的碱性氨基酸(PKKKRKV132;单字母编码,碱性氨基酸用粗体显示;[4,5]),而核质蛋白的NLS是双分的。核质蛋白NLS需要两个必需的碱性氨基酸簇,中间由一个耐受突变的间隔区隔开(KRPAATKKAGQAKKKK171;[6][7])。瑞士蛋白质数据库搜索显示,超过50%的核蛋白与这个共有序列匹配,此后在酵母、植物和动物中发现许多NLS符合这种基序类型[8-10]。在癌蛋白c-Myc中报道了一种不同的NLS(PAAKRVKLD),但它很少受到关注,因为与其他已知的NLS不同,九个残基中只有三个是碱性的[11],而且有一个残基甚至是酸性的。在这里,我们报告说,在核质蛋白双分信号下游含有无活性碱性簇的构建体,可以通过在其两侧加上取自c-Myc报道信号的特定中性和酸性残基而被导向细胞核。单簇KKKK的核靶向依赖于其前面有PAA,如果后面有二肽LD则会被刺激。这些元件的相对位置对这些NLS的功能至关重要。c-Myc非常规信号的所有区域在功能上都很重要。与传统观点相反,中性甚至酸性氨基酸在NLS中可以发挥关键作用。

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