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Effect of Increasing the Copy Number of Bacteriophage Origins of Replication, in trans, on Incoming-Phage Proliferation
Authors:Daniel J O'Sullivan  Colin Hill  and Todd R Klaenhammer
Abstract:Bacteriophage resistance mechanisms which are derived from a bacteriophage genome are termed Per (phage-encoded resistance). When present in trans in Lactococcus lactis NCK203, Per50, the cloned origin of replication from phage var phi]50, interferes with var phi]50 replication. The per50 fragment was found to afford negligible protection to NCK203 against var phi]50 infection when present in a low-copy-number plasmid, pTRK325. A high-copy-number Per50 construct (pTRK323) dramatically affected var phi]50 infection, reducing the efficiency of plaquing (EOP) to 2.5 × 10-4 and the plaque size to pinhead proportions. This clone also afforded significant protection against other related small isometric phages. Per31 was cloned from phage var phi]31 and demonstrated to function as an origin of replication by enabling replication of per31-containing plasmids, in NCK203, on var phi]31 infection. A low-copy-number Per31 plasmid (pTRK360) reduced the EOP of var phi]31 on NCK203 to 0.3 and the plaque diameter from 1.5 to 0.5 mm. When this plasmid was cloned in high copy number, the EOP was further reduced to 7.2 × 10-7 but the plaques were large and contained Per31-resistant phages. Characterization of these “new” phages revealed at least two different types that were similar to var phi]31, except that DNA alterations were noted in the region containing the origin. This novel and powerful abortive phage resistance mechanism should prove useful when directed at specific, problematic phages.
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