ARTIFICIAL MUTANTS GENERATED BY THE INSERTION OF RANDOM OLIGONUCLEOTIDES INTO THE PUTATIVE NUCLEOSIDE BINDING-SITE OF THE HSV-1 THYMIDINE KINASE GENE

作者:DUBE DK; PARKER JD; FRENCH DC; CAHILL DS; DUBE S; HORWITZ MSZ; MUNIR KM; LOEB LA
来源:Biochemistry, 1991, 30(51): 11760-11767.
DOI:10.1021/bi00115a004

摘要

We have obtained 42 active artificial mutants of HSV-1 thymidine kinase (ATP:thymidine 5'-phosphotransferase, EC 2.7.1.21) by replacing codons 166 and 167 with random nucleotide sequences. Codons 166 and 167 are within the putative nucleoside binding site in the HSV-1 tk gene. The spectrum of active mutations indicates that neither Ile166 nor Ala167 is absolutely required for thymidine kinase activity. Each of these amino acids can be replaced by some but not all of the 19 other amino acids. The active mutants can be classified as high activity or low activity on two bases: (1) growth of Escherichia coli KY895 (a strain lacking thymidine kinase activity) in the presence of thymidine and (2) uptake of thymidine by this strain, when harboring plasmids with the random insertions. E. coli KY895 harboring high-activity plasmids or wild-type plasmids can grow in the presence of low amounts of thymidine (< 1-mu-g/mL), but are unable to grow in the presence of high amounts of thymidine. On the other hand, E. coli KY895 harboring low-activity plasmids can grow at a high concentration of thymidine (> 50-mu-g/mL) in the media. The high-activity plasmids also have an enhanced [H-3]dT uptake. The amounts of thymidine kinase activity in vitro in unfractionated extracts do not correlate with either growth at low thymidine concentration or the rate of thymidine uptake. Heat inactivation studies indicate that the mutant enzymes are without exception more temperature-sensitive than the wild-type enzyme. This thermolability could account for the less than expected thymidine kinase activity in the extracts and suggests that amino acid substitutions at Ile166 and Ala167 have produced major changes in protein stability.

  • 出版日期1991-12-24

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