Morgan Welzel scite author profile

A series of inhibitors of Pim-2 kinase identified by high-throughput screening is described. Details of the hit validation and lead generation process and structure-activity relationship (SAR) studies are presented. Disclosure of an unconventional binding mode for 1, as revealed by X-ray crystallography using the highly homologous Pim-1 protein, is also presented, and observed binding features are shown to correlate with the Pim-2 SAR. While highly selective within the kinase family, the series shows similar potency for both Pim-1 and Pim-2, which was expected on the basis of homology, but unusual in light of reports in the literature documenting a bias for Pim-1. A rationale for these observations based on Pim-1 and Pim-2 K(M(ATP)) values is suggested. Some interesting cross reactivity with casein kinase-2 was also identified, and structural features which may contribute to the association are discussed.

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Regioselective Intramolecular Dipolar Cycloaddition of Azides and Unsymmetrical Alkynes

Brawn

Welzel

Lowe

et al. 2009

Org. Lett.

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Enantioenriched allenylsilanes are used in three component propargylation reactions with aldehydes and silyl ethers to form syn-homopropargylic ethers that contain an imbedded azide. These materials then undergo thermally induced intramolecular 1,3-dipolar cycloaddition reactions, resulting in unique fused ring systems containing 1,2,3-triazoles. The ability to modify all three components of the reaction allows for expedient access to compounds containing significant structural and stereochemical variation.

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Structural confirmation of the dihydrosphinganine and fatty acid constituents of the dental pathogen Porphyromonas gingivalis

et al. 2007

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Porphyromonas gingivalis, a recognized periodontal pathogen, is a source of sphinganine bases, fatty acids, free ceramides as well as complex lipids that potentiate interleukin-1b-mediated secretory responses in gingival fibroblasts. The purpose of this study is the structural verification of the sphinganine bases and fatty acids that had been proposed as major components of the complex lipids found in P. gingivalis. The putative C17, C18, and C19 sphinganine bases were prepared from Garner's aldehyde (1) or from a protected serine Weinreb's amide (2). We confirmed that isobranched sphinganine bases are the major structural feature of the ceramides observed from P. gingivalis. We also prepared a C17 unsaturated fatty acid, along with an isobranched C17 3-hydroxy fatty acid, and determined that the major component of the active lipids was the latter.

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Tandem Alkylation/Ester Hydrolysis Using Polymer-Supported Hydroxide for Catch and Release Isolation of a Series of Benzoimidazolonecarboxylic Acids

Welzel

Morwick

2008

J. Comb. Chem.

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ChemInform Abstract: Tandem Alkylation/Ester Hydrolysis Using Polymer‐Supported Hydroxide for Catch and Release Isolation of a Series of Benzoimidazolonecarboxylic Acids.

Welzel

Morwick

2008

ChemInform

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Morgan Welzel

Hit to Lead Account of the Discovery of a New Class of Inhibitors of Pim Kinases and Crystallographic Studies Revealing an Unusual Kinase Binding Mode

Regioselective Intramolecular Dipolar Cycloaddition of Azides and Unsymmetrical Alkynes

Structural confirmation of the dihydrosphinganine and fatty acid constituents of the dental pathogen Porphyromonas gingivalis

Tandem Alkylation/Ester Hydrolysis Using Polymer-Supported Hydroxide for Catch and Release Isolation of a Series of Benzoimidazolonecarboxylic Acids

ChemInform Abstract: Tandem Alkylation/Ester Hydrolysis Using Polymer‐Supported Hydroxide for Catch and Release Isolation of a Series of Benzoimidazolonecarboxylic Acids.

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