J. E. Brown scite author profile

The asthma CPG improved some processes and all outcomes. The diabetes CPG improved two of the eight measured processes but had no effect on outcomes. Education and screening, but not counseling, improved with the tobacco CPG. CPGs appear to improve diagnostic and educational processes more than provider-dependent treatment processes. Outcomes were improved after implementation of the asthma CPG but not after the diabetes CPG.

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Interaction of a Novel GDP Exchange Inhibitor with the Ras Protein

Ganguly

Wang²,

Pramanik³

et al. 1998

Biochemistry

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Mutated, tumorigenic Ras is present in a variety of human tumors. Compounds that inhibit tumorigenic Ras function may be useful in the treatment of Ras-related tumors. The interaction of a novel GDP exchange inhibitor (SCH-54292) with the Ras-GDP protein was studied by NMR spectroscopy. The binding of the inhibitor to the Ras protein was enhanced at low Mg2+ concentrations, which enabled the preparation of a stable complex for NMR study. To understand the enhanced inhibitor binding and the increased GDP dissociation rates of the Ras protein, the conformational changes of the Ras protein at low Mg2+ concentrations was investigated using two-dimensional 1H-15N HSQC experiments. The Ras protein existed in two conformations in slow exchange on the NMR time scale under such conditions. The conformational changes mainly occurred in the GDP binding pocket, in the switch I and the switch II regions, and were reversible. The Ras protein resumed its regular conformation after an excess amount of Mg2+ was added. A model of the inhibitor in complex with the Ras-GDP protein was derived from intra- and intermolecular NOE distance constraints, and revealed that the inhibitor bound to the critical switch II region of the Ras protein.

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Two related neurokinin-1 receptor antagonists have overlapping but different binding sites

Greenfeder¹,

Cheewatrakoolpong²,

Anthes³

et al. 1998

Bioorganic & Medicinal Chemistry

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Detection and structural characterization of ras oncoprotein-inhibitors complexes by electrospray mass spectrometry

Ganguly¹,

Pramanik²,

Huang³

et al. 1997

Bioorganic & Medicinal Chemistry

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J. E. Brown

Ras oncoprotein inhibitors: The discovery of potent, ras nucleotide exchange inhibitors and the structural determination of a drug-protein complex

Do Clinical Practice Guidelines Improve Processes or Outcomes in Primary Care?

Interaction of a Novel GDP Exchange Inhibitor with the Ras Protein

Two related neurokinin-1 receptor antagonists have overlapping but different binding sites

Detection and structural characterization of ras oncoprotein-inhibitors complexes by electrospray mass spectrometry

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