Replication of the origin region of simian virus 40 DNA in permeabilized monkey cells.

Eur J Biochem

Department of Metabolic Regulation, Boston Biomedical Research Institute, Massachusetts 02114.

Published: October 1987

AI Article Synopsis

  • The study investigated the replication of Simian virus 40 (SV40) DNA in monkey CV-1 cells, finding that around 30% of the synthesized DNA was in the form of covalently closed circular DNA (form I) after 60 minutes.
  • It required all four deoxynucleotide triphosphates (dNTPs) for successful replication, and this process was inhibited by aphidicolin, indicating the involvement of DNA polymerase alpha.
  • The analysis showed that SV40 DNA replication occurred consistently across the entire chromosome, with the rate of labeling being proportional to the length of the DNA fragments, demonstrating continuous replication initiation and termination throughout the experiment.

Article Abstract

Simian virus 40 (SV40) DNA replication was studied in monolayers of infected monkey CV-1 cells, permeabilized with lysolecithin, by incubation with [alpha-32P]dTTP, the other dNTPs and rNTPs and an ATP-regenerating system. Analysis of the labeled SV40 DNA by sedimentation in alkaline sucrose gradients showed that about 30% of the material synthesized by the permeable cells in the course of 60 min consisted of covalently closed circular SV40 DNA (form I), with the remainder sedimenting as relaxed circles (form II) and replicative intermediates between 18 S and 4 S. The synthesis of SV40 DNA in the permeabilized cell system required the presence of all four dNTPs and was completely inhibited by aphidicolin, consistent with the involvement of DNA polymerase alpha. A detailed analysis of the distribution of radioactivity in the DNA synthesized involved cleavage with BstNI restriction endonuclease, followed by polyacrylamide gel electrophoresis and radioautography. The extent of labeling of all restriction fragments was nearly proportional to their length, suggesting that the entire SV40 chromosome was being replicated. This was confirmed by the careful comparison of the rate of labeling of a DNA fragment which includes the replication origin, and a fragment which includes the replication terminus. Their labeling was proportional to their size, regardless of the time for which the labeling was carried out. This demonstrated that the replication of the entire SV40 chromosome occurred in a steady state and that the start and termination of replication continuously occurred throughout the labeling period. The availability of an in vitro system in which replication of SV40 DNA undergoes multiple replication cycles should be of considerable value in the analysis of the mechanism of replication of this viral genome.

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Source
http://dx.doi.org/10.1111/j.1432-1033.1987.tb13415.xDOI Listing

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