Holly Kathleen Emerson

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Featured researches published by Holly Kathleen Emerson.

Bioorganic & Medicinal Chemistry Letters | 2009

Kyle Allen Emmitte; C. Webb Andrews; Jennifer Gabriel Badiang; Ronda G. Davis-Ward; Hamilton D. Dickson; David H. Drewry; Holly Kathleen Emerson; Andrea H. Epperly; Daniel F. Hassler; Victoria B. Knick; Kevin Wayne Kuntz; Timothy J. Lansing; James A. Linn; Robert A. Mook; Kristen E. Nailor; James Michael Salovich; Glenn M. Spehar; Mui Cheung

The discovery and development of a series of thiophenes as potent and selective inhibitors of PLK is described. Identification and characterization of 2, a useful in vitro PLK inhibitor tool compound, is also presented.

Bioorganic & Medicinal Chemistry Letters | 2009

Kyle Allen Emmitte; Brian John Wilson; Erich W. Baum; Holly Kathleen Emerson; Kevin Wayne Kuntz; Kristen E. Nailor; James Michael Salovich; Stephon C. Smith; Mui Cheung; Roseanne M. Gerding; Kirk L. Stevens; David E. Uehling; Robert A. Mook; Ganesh S. Moorthy; Scott Howard Dickerson; Anne M. Hassell; M. Anthony Leesnitzer; Lisa M. Shewchuk; Arthur Groy; Jason L. Rowand; Kelly Anderson; Charity Atkins; Jingsong Yang; Peter Sabbatini; Rakesh Kumar

The optimization of imidazo[1,2-a]pyridine inhibitors as potent and selective inhibitors of IGF-1R is presented. Further optimization of oral exposure in mice is also discussed. Detailed selectivity, in vitro activity, and in vivo PK profiles of an optimized compound is also highlighted.

Bioorganic & Medicinal Chemistry Letters | 2008

Robert D. Hubbard; Scott Howard Dickerson; Holly Kathleen Emerson; Robert J. Griffin; Michael J. Reno; Keith R. Hornberger; David W. Rusnak; Edgar R. Wood; David E. Uehling; Alex G. Waterson

A novel class of substituted pyrrolidinyl-acetylenic thieno[3,2-d]pyrimidines has been identified that are potent and selective inhibitors of both EGFR/ErbB-2 receptor tyrosine kinases. The inhibitors are found to display a range of enzyme and cellular potency and also to display a varying level of covalent modification of the kinase targets. Selected molecules, including compound 15h, were found to be potent in enzymatic and cellular assays while also demonstrating exposure in the mouse from an oral dose.

Bioorganic & Medicinal Chemistry Letters | 2009

Kirk L. Stevens; Krystal J. Alligood; Jennifer G. Badiang Alberti; Thomas R. Caferro; Stanley D. Chamberlain; Scott Howard Dickerson; Hamilton D. Dickson; Holly Kathleen Emerson; Robert J. Griffin; Robert D. Hubbard; Barry R. Keith; Robert J. Mullin; Kimberly G. Petrov; Roseanne M. Gerding; Michael J. Reno; Tara Renae Rheault; David W. Rusnak; Douglas Mccord Sammond; Stephon C. Smith; David E. Uehling; Alex G. Waterson; Edgar R. Wood

A novel class of pyrrolidinyl-acetyleneic thieno[3,2-d]pyrimidines has been identified which potently inhibit the EGFR and ErbB-2 receptor tyrosine kinases. Synthetic modifications of the pyrrolidine carbamate moiety result in a range of effects on enzyme and cellular potency. In addition, the impact of the absolute stereochemical configuration on cellular potency and oral mouse pharmacokinetics is described.

Archive | 2003

Stanley D. Chamberlain; Mui Cheung; Holly Kathleen Emerson; Neil W. Johnson; Kristen E. Nailor; Douglas Mccord Sammond; Marcus Semones

Archive | 2006

Holly Kathleen Emerson; David L. Musso; Stanley D. Chamberlain; Gregory Peckham

Cancer Research | 2007

Kevin Wayne Kuntz; James Michael Salovich; Robert A. Mook; Kyle Allen Emmitte; Stanley D. Chamberlain; Tara Renae Rheault; Keith R. Hornberger; Holly Kathleen Emerson; Stephon C. Smith; Brian John Wilson; Ronda G. Davis-Ward; Kelly Horne Donaldson; George M. Adjabeng; Kristen E. Nailor; Daniel F. Hassler; Gary K. Smith; Timothy J. Lansing; Derek Duckett; Victoria B. Knick; Randy T. McConnell; Jeffrey Jackson; Mui Cheung

Archive | 2009