CLONING, EXPRESSION, AND SEQUENCE DETERMINATION OF A BACTERIOPHAGE FRAGMENT ENCODING BACTERIOPHAGE RESISTANCE IN LACTOCOCCUS-LACTIS

被引:75
作者
HILL, C
MILLER, LA
KLAENHAMMER, TR
机构
[1] N CAROLINA STATE UNIV,SE CTR DAIRY FOODS RES,DEPT FOOD SCI,RALEIGH,NC 27695
[2] N CAROLINA STATE UNIV,SE CTR DAIRY FOODS RES,DEPT MICROBIOL,RALEIGH,NC 27695
关键词
D O I
10.1128/jb.172.11.6419-6426.1990
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
A number of host-encoded phage resistance mechanisms have been described in lactococci. However, the phage genome has not been exploited as a source of additional resistance determinants. A 4.5-kb BamHI-HindIII fragment of phage nck202.50 (Φ50) was subcloned in streptococcus-Escherichia coli shuttle plasmid pSA3 and introduced into Lactococcus lactis (NCK203 and MG1363 by protoplast transformation. This cloned phage fragment directed a bacteriophage resistance phenotype designated Per (phage-encoded resistance). Both Φ50 and a distantly related phage, nck202.48 (Φ48), formed small plaques on strain NCK213 at a slightly reduced efficiency of plaquing on the Per+ host. The per locus was further reduced to a 1.4-kb fragment through in vitro deletion analysis. The 1.4-kb fragment was sequenced, and the Per phenotype was found to be associated with a ca. 500-bp region rich in direct and inverted repeats. We present evidence that the Per region contains a phage origin of replication which, in trans, may interfere with phage replication by titration of DNA polymerase or other essential replication factors. It was demonstrated that the Per+ phenotype is not a result of reduced adsorption or action of a restriction and modification system. Per+ activity was not detected against six independent phages which were previously shown to be sensitive to the Hsp+ mechanism. The mutually exclusive resistance mechanisms could be combined to confer resistance to both types of phages (Hsp resistant and Per resistant) in a single host. This is the first description in lactococci of a phage resistance phenotype, other than superinfection immunity, originating from a lactococcal phage genome.
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页码:6419 / 6426
页数:8
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