Single-molecule characterization of SV40 replisome and novel factors: human FPC and Mcm10

Author:

Ouyang Yujing1,Al-Amodi Amani1,Tehseen Muhammad1,Alhudhali Lubna1,Shirbini Afnan1,Takahashi Masateru1,Raducanu Vlad-Stefan1,Yi Gang1,Danazumi Ammar Usman1,De Biasio Alfredo1,Hamdan Samir M1ORCID

Affiliation:

1. Bioscience Program, Division of Biological and Environmental Sciences and Engineering, King Abdullah University of Science and Technology , Thuwal 23955, Saudi Arabia

Abstract

Abstract The simian virus 40 (SV40) replisome only encodes for its helicase; large T-antigen (L-Tag), while relying on the host for the remaining proteins, making it an intriguing model system. Despite being one of the earliest reconstituted eukaryotic systems, the interactions coordinating its activities and the identification of new factors remain largely unexplored. Herein, we in vitro reconstituted the SV40 replisome activities at the single-molecule level, including DNA unwinding by L-Tag and the single-stranded DNA-binding protein Replication Protein A (RPA), primer extension by DNA polymerase δ, and their concerted leading-strand synthesis. We show that RPA stimulates the processivity of L-Tag without altering its rate and that DNA polymerase δ forms a stable complex with L-Tag during leading-strand synthesis. Furthermore, similar to human and budding yeast Cdc45–MCM–GINS helicase, L-Tag uses the fork protection complex (FPC) and the mini-chromosome maintenance protein 10 (Mcm10) during synthesis. Hereby, we demonstrate that FPC increases this rate, and both FPC and Mcm10 increase the processivity by stabilizing stalled replisomes and increasing their chances of restarting synthesis. The detailed kinetics and novel factors of the SV40 replisome establish it as a closer mimic of the host replisome and expand its application as a model replication system.

Funder

King Abdullah University of Science and Technology

Competitive Research Award

Publisher

Oxford University Press (OUP)

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