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Functional domains of the Xenopus replication licensing factor Cdt1

机译:Xenopus复制许可因子Cdt1的功能域

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摘要

During late mitosis and early G1, replication origins are licensed for subsequent replication by loading heterohexamers of the mini-chromosome maintenance proteins (Mcm2-7). To prevent re-replication of DNA, the licensing system is down-regulated at other cell cycle stages. A small protein called geminin plays an important role in this down-regulation by binding and inhibiting the Cdt1 component of the licensing system. We examine here the organization of Xenopus Cdt1, delimiting regions of Cdt1 required for licensing and regions required for geminin interaction. The C-terminal 377 residues of Cdt1 are required for licensing and the extreme C-terminus contains a domain that interacts with an Mcm(2,4,6,7) complex. Two regions of Cdt1 interact with geminin: one at the N-terminus, and one in the centre of the protein. Only the central region binds geminin tightly enough to successfully compete with full-length Cdt1 for geminin binding. This interaction requires a predicted coiled-coil domain that is conserved amongst metazoan Cdt1 homologues. Geminin forms a homodimer, with each dimer binding one molecule of Cdt1. Separation of the domains necessary for licensing activity from domains required for a strong interaction with geminin generated a construct, whose licensing activity was partially insensitive to geminin inhibition.
机译:在有丝分裂晚期和G1早期,通过加载微型染色体维持蛋白(Mcm2-7)的异六聚体,复制起点可用于随后的复制。为防止DNA复制,在其他细胞周期阶段下调了许可系统。一种称为geminin的小蛋白通过结合和抑制许可系统的Cdt1成分在这种下调中起重要作用。我们在这里检查非洲爪蟾Cdt1的组织,划定了许可所需的Cdt1区域和geminin相互作用所需的区域。 Cdt1的C端377个残基是获得许可所必需的,并且极端C端包含一个与Mcm(2,4,6,7)复合体相互作用的域。 Cdt1的两个区域与geminin相互作用:一个位于N末端,一个位于蛋白质中心。只有中央区域足够紧密地结合geminin,以成功与全长Cdt1竞争geminin结合。这种相互作用需要在后生动物Cdt1同源物中保守的预计卷曲螺旋结构域。 Geminin形成同型二聚体,每个二聚体结合一个Cdt1分子。将许可活动所必需的域与与geminin强烈相互作用所需的域分开,可生成一种构建体,该构建体的许可活动对geminin抑制不敏感。

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