Your search keyword '"Bemis, Guy"' showing total 4 results

1. Extensive phosphorylation with overlapping specificity by Mycobacterium tuberculosis serine/threonine protein kinases.

Author

Prisic, Sladjana, Dankwa, Selasi, Schwartz, Daniel, Chou, Michael F., Locasale, Jason W., Choong-Min Kang, Bemis, Guy, Church, George M., Steen, Hanno, and Husson, Robert N.

Subjects

PHOSPHORYLATION, MYCOBACTERIUM tuberculosis, SERINE proteinases, PROTEIN kinases, EUKARYOTIC cells, PHOSPHOPROTEINS

Abstract

The Mycobacterium tuberculosis genome encodes 11 serine/threonine protein kinases (STPKs) that are structurally related to eukaryotic kinases. To gain insight into the role of Ser/Thr phosphorylation in this major global pathogen, we used a phosphoproteomic approach to carry out an extensive analysis of protein phosphorylation in M. tuberculosis. We identified more than 500 phosphorylation events in 301 proteins that are involved in a broad range of functions. Bioinformatic analysis of quantitative in vitro kinase assays on peptides containing a subset of these phosphorylation sites revealed a dominant motif shared by six of the M. tuberculosis STPKs. Kinase assays on a second set of peptides incorporating targeted substitutions surrounding the phosphoacceptor validated this motif and identified additional residues preferred, by individual kinases. Our data provide insight into processes regulated by STPKs in M. tuberculosis and create a resource for understanding how specific phosphorylation events modulate protein activity. The results further provide the potential to predict likely cognate STPKs for newly identified phosphoproteins. [ABSTRACT FROM AUTHOR]

Published

2010

2. A minimalist approach to fragment-based ligand design using common rings and linkers: Application to kinase inhibitors.

Author

Aronov, Alex M. and Bemis, Guy W.

Abstract

We present a novel method for stepwise scaffold assembly that integrates fragment-by-fragment ligand design approaches with high-throughput virtual library screening (COREGEN). As an extension of our earlier studies of common features present in drug molecules, we investigate the hypothesis that most pharmaceutically interesting ligands can be expressed in terms of the ring-linker frameworks that comprise them. Analysis of 119 published kinase inhibitors from at least 18 different targets illustrates that a basis set of 4 rings and 8 linkers is sufficient to describe approximately 90% of ring and linker occurrences, respectively. A similar result was derived from a larger set of approximately 40,000 kinase inhibitors from curated patents. A method for ring-linker-based assembly of scaffold libraries that uses experimental information to guide the placement of anchor fragments is validated using a set of reported kinase inhibitors of Bcr-Abl, Cdk2, and Src. In every case, the predominant structural motif of reported ligand cores is reproduced and variations are suggested. To underscore generality of this approach, a novel scaffold for a cyclooxygenase-2 (COX-2) selective ligand is proposed. Proteins 2004. © 2004 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2004

3. Kinase inhibitors and the case for CH...O hydrogen bonds in protein-ligand binding.

Author

Pierce, Albert C., Sandretto, Kathryn L., and Bemis, Guy W.

Published

2002

4. ChemInform Abstract: Inhibitors of p38 MAP Kinase: Therapeutic Intervention in Cytokine-Mediated Diseases.

Author

Salituro, Francesco G., Germann, Ursula A., Wilson, Keith P., Bemis, Guy W., Fox, Ted, and Su, Michael S.-S.

Published

1999