分支点序列结合蛋白的KH结构域决定了对前体mRNA分支点序列的特异性。
The KH domain of the branchpoint sequence binding protein determines specificity for the pre-mRNA branchpoint sequence.
作者信息
Berglund J A, Fleming M L, Rosbash M
机构信息
Howard Hughes Medical Institute, Department of Biochemistry, Brandeis University, Waltham, Massachusetts 02254, USA.
出版信息
RNA. 1998 Aug;4(8):998-1006. doi: 10.1017/s1355838298980499.
Abstract
The yeast and mammalian branchpoint sequence binding proteins (BBP and mBBP/SF1) contain both KH domain and Zn knuckle RNA-binding motifs. The single KH domain of these proteins is sufficient for specific recognition of the pre-mRNA branchpoint sequence (BPS). However, an interaction is only apparent if one or more accessory modules are present to increase binding affinity. The Zn knuckles of BBP/mBBP can be replaced by an RNA-binding peptide derived from the HIV-1 nucleocapsid protein or by an arginine-serine (RS)7 peptide, without loss of specificity. Only the seven-nucleotide branchpoint sequence and two nucleotides to either side are necessary for RNA binding to the chimeric proteins. Therefore, we propose that all three of these accessory RNA-binding modules bind the phosphate backbone, whereas the KH domain interacts specifically with the bases of the BPS. Proteins and protein complexes with multiple RNA-binding motifs are frequent, suggesting that an intimate collaboration between two or more motifs will be a general theme in RNA-protein interactions.
摘要
酵母和哺乳动物的分支点序列结合蛋白(BBP和mBBP/SF1)都含有KH结构域和锌指RNA结合基序。这些蛋白质的单个KH结构域足以特异性识别前体mRNA分支点序列(BPS)。然而,只有当存在一个或多个辅助模块以增加结合亲和力时,相互作用才会明显。BBP/mBBP的锌指可以被源自HIV-1核衣壳蛋白的RNA结合肽或精氨酸-丝氨酸(RS)7肽取代,而不会丧失特异性。RNA与嵌合蛋白结合仅需要七核苷酸的分支点序列及其两侧的两个核苷酸。因此,我们提出所有这三个辅助RNA结合模块都与磷酸骨架结合,而KH结构域则与BPS的碱基特异性相互作用。具有多个RNA结合基序的蛋白质和蛋白质复合物很常见,这表明两个或更多基序之间的密切协作将是RNA-蛋白质相互作用中的一个普遍主题。
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