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Merck
  • R164H and V240H replacements by site-directed mutagenesis of TEM-149 extended-spectrum β-lactamase: kinetic analysis of TEM-149H240 and TEM-149H164-H240 laboratory mutants.

R164H and V240H replacements by site-directed mutagenesis of TEM-149 extended-spectrum β-lactamase: kinetic analysis of TEM-149H240 and TEM-149H164-H240 laboratory mutants.

Antimicrobial agents and chemotherapy (2012-11-28)
Mariagrazia Perilli, Giuseppe Celenza, Paola Sandra Mercuri, Moreno Galleni, Cristina Pellegrini, Bernardetta Segatore, Gianfranco Amicosante
要旨

Two laboratory mutant forms, TEM-149(H240) and TEM-149(H164-H240), of the TEM-149 extended-spectrum β-lactamase enzyme were constructed by site-directed mutagenesis. TEM-149(H240) and TEM-149(H164-H240) were similar in kinetic behavior, except with respect to benzylpenicillin and ceftazidime. Molecular modeling of the two mutant enzymes demonstrated the role of histidine at position 240 in the reduction of the affinity of the enzyme for ceftazidime.

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製品内容

Sigma-Aldrich
ペニシリンG ナトリウム塩, powder, BioReagent, suitable for cell culture
Sigma-Aldrich
ペニシリンG カリウム塩, powder, BioReagent, suitable for cell culture
Sigma-Aldrich
ペニシリンG ナトリウム塩, 96.0-102.0%
Sigma-Aldrich
ペニシリンG ナトリウム塩, ~1650 U/mg
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ペニシリンG カリウム塩, 95.0 - 102.0%
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ペニシリンG カリウム塩