Paul A. Bartlett scite author profile

Six phosphorus-containing peptide analogues of the form Cbz-NHCH2PO2--L-Leu-Y (Y = D-Ala, NH2, Gly, L-Phe, L-Ala, L-Leu) have been prepared and evaluated as inhibitors of thermolysin. The Ki values for these compounds range from 1.7 microM to 9.1 nM and correlate well with the Km/kcat values for the corresponding peptide substrates [Morihara, K., & Tsuzuki, H. (1970) Eur. J. Biochem. 15, 374-380] but not with the Km values alone. The correlation noted between inhibitor Ki and substrate Km/kcat is the most extensive one of this type, providing strong evidence that the phosphonamidates are transition-state analogues and not simply multisubstrate ground-state analogues. Cbz-NH2CH2PO2--L-Leu-L-Leu (Ki = 9.1 nM) is the most potent inhibitor yet reported for thermolysin.

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CAVEAT: A program to facilitate the design of organic molecules

Lauri

Bartlett

1994

J Computer-Aided Mol Des

254

181

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A frequently encountered problem in the design of enzyme inhibitors and other biologically active molecules is the identification of molecular frameworks to serve as templates or linking units that can position functional groups in specific relative orientations. The program CAVEAT was designed to address this problem by searching 3D databases for such molecular fragments. Key innovations introduced in CAVEAT are a focus on relationships between bonds and the provision of automated methods to identify and classify structural frameworks. Performance has been a particular concern in formulating CAVEAT, since it is intended to be used in an interactive manner. The focus in this report is the design and implementation of the principal algorithms and the performance achieved.

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Synthesis of water-soluble undecagold cluster compounds of potential importance in electron microscopic and other studies of biological systems

Bartlett¹,

Bauer²,

Singer³

1978

J. Am. Chem. Soc.

167

122

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Paul A. Bartlett

Binding Energy and Catalysis: The Implications for Transition-State Analogs and Catalytic Antibodies

Phosphonamidates as transition-state analog inhibitors of thermolysin

CAVEAT: A program to facilitate the design of organic molecules

Synthesis of water-soluble undecagold cluster compounds of potential importance in electron microscopic and other studies of biological systems

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