AI Article Synopsis

  • Glutamate dehydrogenase becomes quickly inactivated when exposed to Rose Bengal or ethoxyformic anhydride, with four histidine residues being affected by photo-oxidation during the Rose Bengal treatment.
  • The oxidation of three histidine residues has minimal impact on enzyme activity, but the oxidation of the fourth residue nearly completely deactivates the enzyme, while acylation at different pH levels modifies histidine residues and reduces activity by varying degrees.
  • Glutamate slightly reduces inactivation and alkylation at pH7.5, while NAD(+) influences acylation but not inactivation; ADP activity remains unchanged whereas GTP response changes under both pH conditions.

Article Abstract

1. Glutamate dehydrogenase was subject to rapid inactivation when irradiated in the presence of Rose Bengal or incubated in the presence of ethoxyformic anhydride. 2. Inactivation in the presence of Rose Bengal led to the photo-oxidation of four histidine residues. Oxidation of three histidine residues had little effect on enzyme activity, but oxidation of the fourth residue led to the almost total loss of activity. 3. Acylation of glutamate dehydrogenase with ethoxyformic anhydride at pH6.1 led to the modification of three histidine residues with a corresponding loss of half the original activity. Acylation at pH7.5 led to the modification of two histidine residues and a total loss of enzyme activity. 4. One of the histidine residues undergoing reaction at pH6.1 also undergoes reaction at pH7.5. 5. The presence of either glutamate or NAD(+) in the reaction mixtures at pH6.1 had no appreciable effect. At pH7.5 glutamate caused a marked decrease in both the degree of alkylation and degree of inactivation. NAD(+) had no effect on the degree of inactivation at pH7.5 but did modify the extent of acylation. 6. The normal response of the enzyme towards ADP was unaffected by acylation at pH6.1 or 7.5. 7. The normal response of the enzyme towards GTP was altered by treatment at both pH6.1 and 7.5.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1174091PMC
http://dx.doi.org/10.1042/bj1290419DOI Listing

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