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The role of recombination in the formation of circular oligomers of the lambda plasmid
Authors:G Hobom  D S Hogness
Affiliation:Department of Biochemistry Stanford University School of Medicine Stanford, Calif. 94305 U.S.A.
Abstract:The λdv1 plasmid forms an extensive oligomeric series of circular DNA molecules in recombination-proficient (recsu+) Escherichia coli. These rec+ [λdv1]+ strains can be typed into the following four classes according to which member of the oligomeric series is most frequent: monomer, dimer, trimer, and tetramer strains. Each of these strains forms a set of circular λdv1 DNA molecules in which most members belong to the series l, 2l, 3l, 4l, where l is the length of the most frequent circular DNA that characterizes the strain—i.e. l equals the length of the most frequent oligomer in the respective strain. In a given strain, the frequency of a molecular species decreases as its length becomes a larger multiple of l. For example, the dimer strains produce dimers, tetramers, hexamers, octomers, etc., in decreasing frequencies, which reach the limits of detection at about the hexadecamer.When recA? mutations that are absolutely defective for host recombination are introduced into each of these four strains, l retains the same values as in the parent rec+ strain, but oligomers larger than 2l are not formed, and the frequency of the 2l oligomer is much reduced. The introduction of recB? or recC? mutations, which are only partially defective for host recombination, produces a much smaller perturbation of the rec+ distributions, and rec+recA? merodiploids exhibit the rec+ phenotype with respect to both oligomerization and host recombination.The effects of rec? mutations on the distribution of λdv1 oligomers and the nature of the oligomeric series produced in rec+ cells all indicate that an intermolecular reciprocal recombination between two circular λdv1 DNAs is the principal reaction responsible for oligomerization. It is suggested that the small residual oligomerization that yields 2l oligomers in recA?cells results from aberrant segregation of the DNA strands at the termination of the replication of l-sized molecules.The inactivation of recA, but not of recB or C, also results in a marked reduction in the frequency of spontaneous curing which in recA+dv1+]hosts leads to the segregation of [λdv?]cells. However, spontaneous curing does not appear to be dependent upon the recombination reactions that yield the [λdv 1+]oligomers, since the frequency of oligomerization in recA+ hosts decreases with increasing l, whereas the frequency of curing increases with increasing l.
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