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Dynamic DNA Helicase-DNA Polymerase Interactions Assure Processive Replication Fork Movement

Authors :
Hamdan, Samir M.
Johnson, Donald E.
Tanner, Nathan A.
Lee, Jong-Bong
Qimron, Udi
Tabor, Stanley
Oijen, Antoine M. van
Richardson, Charles C.
Hamdan, Samir M.
Johnson, Donald E.
Tanner, Nathan A.
Lee, Jong-Bong
Qimron, Udi
Tabor, Stanley
Oijen, Antoine M. van
Richardson, Charles C.
Source :
Hamdan , S M , Johnson , D E , Tanner , N A , Lee , J-B , Qimron , U , Tabor , S , Oijen , A M V & Richardson , C C 2007 , ' Dynamic DNA Helicase-DNA Polymerase Interactions Assure Processive Replication Fork Movement ' Molecular Cell , vol 27 , no. 4 , pp. 539-549 . DOI: 10.1016/j.molcel.2007.06.020
Publication Year :
2007

Abstract

A single copy of bacteriophage T7 DNA polymerase and DNA helicase advance the replication fork with a processivity greater than 17,000 nucleotides. Nonetheless, the polymerase transiently dissociates from the DNA without leaving the replisome. Ensemble and single-molecule techniques demonstrate that this dynamic processivity is made possible by two modes of DNA polymerase-helicase interaction. During DNA synthesis the polymerase and the helicase interact at a high-affinity site. In this polymerizing mode, the polymerase dissociates from the DNA approximately every 5000 bases. The polymerase, however, remains bound to the helicase via an electrostatic binding mode that involves the acidic C-terminal tail of the helicase and a basic region in the polymerase to which the processivity factor also binds. The polymerase transfers via the electrostatic interaction around the hexameric helicase in search of the primer-template.

Details

Database :
OAIster
Journal :
Hamdan , S M , Johnson , D E , Tanner , N A , Lee , J-B , Qimron , U , Tabor , S , Oijen , A M V & Richardson , C C 2007 , ' Dynamic DNA Helicase-DNA Polymerase Interactions Assure Processive Replication Fork Movement ' Molecular Cell , vol 27 , no. 4 , pp. 539-549 . DOI: 10.1016/j.molcel.2007.06.020
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn932440843
Document Type :
Electronic Resource