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DNA polymerases delta and zeta switching by sharing the accessory subunits of DNA polymerase delta.

J Biol Chem.. 2012-05; 
Andrey G. Baranovskiy, Artem G. Lada, Hollie Siebler, Yinbo Zhang, Youri I. Pavlov and Tahir H. Tahirov. Eppley Institute for Research in Cancer and Allied Diseases, University of Nebraska Medical Center, Omaha, Nebraska 68198, USA.
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摘要

Translesion DNA synthesis is an important branch of the DNA damage tolerance pathway that assures genomic integrity of living organisms. The mechanisms of DNA polymerase (Pol) switches during lesion bypass are not known. Here, we show that the C-terminal domain of the Pol catalytic subunit interacts with accessory subunits of replicative DNA Pol δ. We also show that, unlike other members of the human B-family of DNA polymerases, the highly conserved and similar C-terminal domains of Pol δ and Pol contain a [4Fe-4S] cluster coordinated by four cysteines. Amino acid changes in Pol that prevent the assembly of the [4Fe-4S] cluster abrogate Pol function in UV mutagenesis. On the basis of these data,... More

关键词

DNA Damage Response; DNA Polymerase; DNA Replication; Iron-Sulfur Protein; Protein-Protein Interactions; DNA Polymerase δ; DNA Polymerase ; Translesion DNA Synthesis