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大肠杆菌噬菌体P1的遗传学研究。III. 扩展的遗传图谱。

Genetic studies of coliphage P1. III. Extended genetic map.

作者信息

Walker D H, Walker J T

出版信息

J Virol. 1976 Oct;20(1):177-87. doi: 10.1128/JVI.20.1.177-187.1976.

Abstract

An extensive genetic map of coliphage P1 has been constructed for 113 amber mutants, using primarily a modification of the conventional complementation spot test. These spot tests failed to classify the mutants into cistrons, but when they were quantitated they permitted assignment of the mutants into 10 linkage clusters. Furthermore, a linear order could be deduced for most of the mutants within each cluster. This strongly suggested that recombination was the predominant event generating plaques and that, for the practical purpose of rapid genetic mapping, such spot tests could be considered as a series of two-factor crosses. Six of the 10 linkage clusters correlated with the P1 genetic map established by Scott (1968). The locations of the remaining four clusters were determined by three-factor crosses and by prophage deletion mapping. The nonrandom occurrence of termini for 14 deletion prophages, which we established previously (Walker and Walker, 1975), and the coincidence of these termini with five out of ten regions demarcating the linkage clusters are discussed. Complementation tests in liquid frequently gave ambiguous results. Therefore, cistron designations were not assigned.

摘要

利用对传统互补斑点试验的一种改进方法,已为113个琥珀突变体构建了大肠杆菌噬菌体P1的广泛遗传图谱。这些斑点试验未能将突变体分类到顺反子中,但当对其进行定量时,可将突变体分配到10个连锁群中。此外,每个连锁群内的大多数突变体都可推导出线性顺序。这有力地表明重组是产生噬菌斑的主要事件,并且就快速遗传图谱绘制的实际目的而言,此类斑点试验可被视为一系列双因子杂交。10个连锁群中的6个与Scott(1968年)建立的P1遗传图谱相关。其余4个连锁群的位置通过三因子杂交和原噬菌体缺失图谱分析确定。讨论了我们之前确定的14个缺失原噬菌体末端的非随机出现情况,以及这些末端与划分连锁群的10个区域中的5个区域的重合情况。液体中的互补试验经常给出不明确的结果。因此,未指定顺反子名称。

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