Development of M13 as a Single-stranded Cloning Vector: Insertion of the Tn3 Transposon into the Genome of M13
Abstract
To establish that the transducing activity is associated with the M13 phage produced by resistant cells, we have investigated the ability of antibodies against the M13 coat protein to inactivate both the plaque-forming ability and the transducing activity of the M13 Tn3-15 phage. Table 1 shows that both plaque formation and transduction to drug resistance are inactivated by purified antibodies to the viral coat protein. Gamma globulins from rabbits that had not been injected with coat protein had no effect on either plaque formation or transduction.
Electron microscopic observation of the M13 Tn3-15 phages shows them to have a mean length approximately 1.7 times that of the M13 unit length. Figure 1 shows M13 and M13 Tn3-15 in a mixture of the two phages. Replicative forms (RF) of the M13 Tn3-15 DNA have been isolated...
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PDFDOI: http://dx.doi.org/10.1101/0.455-459