Simian virus 40 DNA replication in vitro: identification of multiple stages of initiation.

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Mol Cell Biol. 1989 September; 9(9): 3839-3849

Simian virus 40 DNA replication in vitro: identification of multiple stages of initiation.

T Tsurimoto, M P Fairman and B Stillman

Cold Spring Harbor Laboratory, New York 11724.

ABSTRACT

A cell-free DNA replication system dependent upon five purifiedcellular proteins, one crude cellular fraction, and the simianvirus 40 (SV40)-encoded large tumor antigen (T antigen) initiatedand completed replication of plasmids containing the SV40 originsequence. DNA synthesis initiated at or near the origin sequenceafter a time lag of approximately 10 min and then proceededbidirectionally from the origin to yield covalently closed,monomer daughter molecules. The time lag could be completelyeliminated by a preincubation of SV40 ori DNA in the presenceof T antigen, a eucaryotic single-stranded DNA-binding protein(replication factor A [RF-A]), and topoisomerases I and II.In contrast, if T antigen and the template DNA were incubatedalone, the time lag was only partially decreased. Kinetic analysesof origin recognition by T antigen, origin unwinding, and DNAsynthesis suggest that the time lag in replication was due tothe formation of a complex between T antigen and DNA calledthe T complex, followed by formation of a second complex calledthe unwound complex. Formation of the unwound complex requiredRF-A. When origin unwinding was coupled to DNA replication bythe addition of a partially purified cellular fraction (IIA),DNA synthesis initiated at the ori sequence, but the templateDNA was not completely replicated. Complete DNA replicationin this system required the proliferating-cell nuclear antigenand another cellular replication factor, RF-C, during the elongationstage. In a less fractionated system, another cellular fraction,SSI, was previously shown to be necessary for reconstitutionof DNA replication. The SSI fraction was required in the lesspurified system to antagonize the inhibitory action of anothercellular protein(s). This inhibitor specifically blocked theearliest stage of DNA replication, but not the later stages.The implications of these results for the mechanisms of initiationand elongation of DNA replication are discussed.

Mol Cell Biol. 1989 September; 9(9): 3839-3849

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