Geminin becomes activated as an inhibitor of Cdt1/RLF-B following nuclear import

During late mitosis and early interphase, origins of replication become "licensed" for DNA replication by loading Mcm2-7 complexes [1-5]. Mcm2-7 complexes are removed from origins as replication forks initiate replication, thus preventing rereplication of DNA in a single cell cycle. Premature origin licensing is prevented in metaphase by the action of geminin, which binds and inhibits Cdt1/RLF-B, a protein that is required for the loading of Mcm2-7 [6-9]. Recombinant geminin that is added to Xenopus egg extracts is efficiently degraded upon exit from metaphase [10]. Here, we show that recombinant and endogenous forms of Xenopus geminin behave differently from one another, such that a significant proportion of endogenous geminin escapes proteolysis upon exit from metaphase. During late mitosis and early G1, the surviving population of endogenous geminin does not associate with Cdt1/RLF-B and does not inhibit licensing. Following nuclear assembly, geminin is imported into nuclei and becomes reactivated to bind Cdt1/RLF-B. This reactivated geminin provides the major nucleoplasmic inhibitor of origin relicensing during late interphase. Since the initiation of replication at licensed origins depends on nuclear assembly [11], our results suggest an elegant and novel mechanism for preventing rereplication of DNA in a single cell cycle.