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A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker

The streptomycin counter-selection system is a useful tool for constructing unmarked in-frame gene deletions, which is a fundamental approach to study bacteria and their pathogenicity at the molecular level. A prerequisite for this system is acquiring a streptomycin-resistant strain due to rpsL muta...

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Autores principales: Tsai, Yu-Kuo, Liou, Ci-Hong, Lin, Jung-Chung, Ma, Ling, Fung, Chang-Phone, Chang, Feng-Yee, Siu, L. Kristopher
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4182516/
https://www.ncbi.nlm.nih.gov/pubmed/25268958
http://dx.doi.org/10.1371/journal.pone.0109258
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author Tsai, Yu-Kuo
Liou, Ci-Hong
Lin, Jung-Chung
Ma, Ling
Fung, Chang-Phone
Chang, Feng-Yee
Siu, L. Kristopher
author_facet Tsai, Yu-Kuo
Liou, Ci-Hong
Lin, Jung-Chung
Ma, Ling
Fung, Chang-Phone
Chang, Feng-Yee
Siu, L. Kristopher
author_sort Tsai, Yu-Kuo
collection PubMed
description The streptomycin counter-selection system is a useful tool for constructing unmarked in-frame gene deletions, which is a fundamental approach to study bacteria and their pathogenicity at the molecular level. A prerequisite for this system is acquiring a streptomycin-resistant strain due to rpsL mutations, which encodes the ribosomal protein S12. However, in this study no streptomycin resistance was found to be caused by rpsL mutations in all 127 clinical strains of Klebsiella pneumoniae isolated from liver abscess patients. By screening 107 spontaneous mutants of streptomycin resistance from a clinical strain of K. pneumoniae, nucleotide substitution or insertion located within the rpsL was detected in each of these strains. Thirteen different mutants with varied S12 proteins were obtained, including nine streptomycin-dependent mutants. The virulence of all four streptomycin-resistant mutants was further evaluated. Compared with the parental strain, the K42N, K42T and K87R mutants showed a reduction in growth rate, and the K42N and K42T mutants became susceptible to normal human serum. In the mice LD(50) (the bacterial dose that caused 50% death) assay, the K42N and K42T mutants were ∼1,000-fold less lethal (∼2×10(5) CFU) and the K87R mutant was ∼50-fold less lethal (∼1×10(4) CFU) than the parental strain (∼2×10(2) CFU). A K42R mutant showed non-observable effects on the above assays, while this mutant exhibited a small cost (P<0.01) in an in vitro growth competition experiment. In summary, most of the K. pneumoniae strains with streptomycin resistance caused by rpsL mutations are less virulent than their parental strain in the absence of streptomycin. The K42R mutant showed similar pathogenicity to its parental strain and should be one of the best choices when using rpsL as a counter-selection marker.
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spelling pubmed-41825162014-10-07 A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker Tsai, Yu-Kuo Liou, Ci-Hong Lin, Jung-Chung Ma, Ling Fung, Chang-Phone Chang, Feng-Yee Siu, L. Kristopher PLoS One Research Article The streptomycin counter-selection system is a useful tool for constructing unmarked in-frame gene deletions, which is a fundamental approach to study bacteria and their pathogenicity at the molecular level. A prerequisite for this system is acquiring a streptomycin-resistant strain due to rpsL mutations, which encodes the ribosomal protein S12. However, in this study no streptomycin resistance was found to be caused by rpsL mutations in all 127 clinical strains of Klebsiella pneumoniae isolated from liver abscess patients. By screening 107 spontaneous mutants of streptomycin resistance from a clinical strain of K. pneumoniae, nucleotide substitution or insertion located within the rpsL was detected in each of these strains. Thirteen different mutants with varied S12 proteins were obtained, including nine streptomycin-dependent mutants. The virulence of all four streptomycin-resistant mutants was further evaluated. Compared with the parental strain, the K42N, K42T and K87R mutants showed a reduction in growth rate, and the K42N and K42T mutants became susceptible to normal human serum. In the mice LD(50) (the bacterial dose that caused 50% death) assay, the K42N and K42T mutants were ∼1,000-fold less lethal (∼2×10(5) CFU) and the K87R mutant was ∼50-fold less lethal (∼1×10(4) CFU) than the parental strain (∼2×10(2) CFU). A K42R mutant showed non-observable effects on the above assays, while this mutant exhibited a small cost (P<0.01) in an in vitro growth competition experiment. In summary, most of the K. pneumoniae strains with streptomycin resistance caused by rpsL mutations are less virulent than their parental strain in the absence of streptomycin. The K42R mutant showed similar pathogenicity to its parental strain and should be one of the best choices when using rpsL as a counter-selection marker. Public Library of Science 2014-09-30 /pmc/articles/PMC4182516/ /pubmed/25268958 http://dx.doi.org/10.1371/journal.pone.0109258 Text en © 2014 Tsai et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Tsai, Yu-Kuo
Liou, Ci-Hong
Lin, Jung-Chung
Ma, Ling
Fung, Chang-Phone
Chang, Feng-Yee
Siu, L. Kristopher
A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title_full A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title_fullStr A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title_full_unstemmed A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title_short A Suitable Streptomycin-Resistant Mutant for Constructing Unmarked In-Frame Gene Deletions Using rpsL as a Counter-Selection Marker
title_sort suitable streptomycin-resistant mutant for constructing unmarked in-frame gene deletions using rpsl as a counter-selection marker
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4182516/
https://www.ncbi.nlm.nih.gov/pubmed/25268958
http://dx.doi.org/10.1371/journal.pone.0109258
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