Sarah Vincent scite author profile

Sarah Vincent

2Publications

27Citation Statements Received

40Citation Statements Given

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Cornell University

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Mapping of chorismate mutase and prephenate dehydrogenase domains in the Escherichia coli T‐protein

Chen

Vincent

Wilson³

et al. 2003

European Journal of Biochemistry

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The Escherichia coli bifunctional T-protein transforms chorismic acid to p-hydroxyphenylpyruvic acid in the L-tyrosine biosynthetic pathway. The 373 amino acid T-protein is a homodimer that exhibits chorismate mutase (CM) and prephenate dehydrogenase (PDH) activities, both of which are feedback-inhibited by tyrosine. Fifteen genes coding for the T-protein and various fragments thereof were constructed and successfully expressed in order to characterize the CM, PDH and regulatory domains. Residues 1-88 constituted a functional CM domain, which was also dimeric. Both the PDH and the feedback-inhibition activities were localized in residues 94-373, but could not be separated into discrete domains. The activities of cloned CM and PDH domains were comparatively low, suggesting some cooperative interactions in the native state. Activity data further indicate that the PDH domain, in which NAD, prephenate and tyrosine binding sites were present, was more unstable than the CM domain.

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Probing the overlap of chorismate mutase and prephenate dehydrogenase sites in the escherichia coli T-protein: a dehydrogenase-selective inhibitor

Vincent

Chen

Wilson

et al. 2002

Bioorganic & Medicinal Chemistry Letters

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Sarah Vincent

Mapping of chorismate mutase and prephenate dehydrogenase domains in the Escherichia coli T‐protein

Probing the overlap of chorismate mutase and prephenate dehydrogenase sites in the escherichia coli T-protein: a dehydrogenase-selective inhibitor

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