Brad R. Henke
GlaxoSmithKline
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Publication
Featured researches published by Brad R. Henke.
Journal of Medicinal Chemistry | 2015
Curt Dale Haffner; J. David Becherer; Eric E. Boros; Rodolfo Cadilla; Tiffany Carpenter; David John Cowan; David N. Deaton; Yu Guo; W. Wallace Harrington; Brad R. Henke; Michael Jeune; Istvan Kaldor; Naphtali Milliken; Kim G. Petrov; Frank Preugschat; Christie Schulte; Barry George Shearer; Todd W. Shearer; Terrence L. Jr. Smalley; Eugene L. Stewart; J. Darren Stuart; John C. Ulrich
A series of thiazoloquin(az)olinones were synthesized and found to have potent inhibitory activity against CD38. Several of these compounds were also shown to have good pharmacokinetic properties and demonstrated the ability to elevate NAD levels in plasma, liver, and muscle tissue. In particular, compound 78c was given to diet induced obese (DIO) C57Bl6 mice, elevating NAD > 5-fold in liver and >1.2-fold in muscle versus control animals at a 2 h time point. The compounds described herein possess the most potent CD38 inhibitory activity of any small molecules described in the literature to date. The inhibitors should allow for a more detailed assessment of how NAD elevation via CD38 inhibition affects physiology in NAD deficient states.
Journal of Biological Chemistry | 2017
Jon Paczkowski; Sampriti Mukherjee; Amelia R. McCready; Jian-Ping Cong; Christopher Joseph Aquino; Hahn Kim; Brad R. Henke; Chari Smith; Bonnie L. Bassler
Quorum sensing is a process of cell-cell communication that bacteria use to regulate collective behaviors. Quorum sensing depends on the production, detection, and group-wide response to extracellular signal molecules called autoinducers. In many bacterial species, quorum sensing controls virulence factor production. Thus, disrupting quorum sensing is considered a promising strategy to combat bacterial pathogenicity. Several members of a family of naturally produced plant metabolites called flavonoids inhibit Pseudomonas aeruginosa biofilm formation by an unknown mechanism. Here, we explore this family of molecules further, and we demonstrate that flavonoids specifically inhibit quorum sensing via antagonism of the autoinducer-binding receptors, LasR and RhlR. Structure-activity relationship analyses demonstrate that the presence of two hydroxyl moieties in the flavone A-ring backbone are essential for potent inhibition of LasR/RhlR. Biochemical analyses reveal that the flavonoids function non-competitively to prevent LasR/RhlR DNA binding. Administration of the flavonoids to P. aeruginosa alters transcription of quorum sensing-controlled target promoters and suppresses virulence factor production, confirming their potential as anti-infectives that do not function by traditional bacteriocidal or bacteriostatic mechanisms.
ACS Chemical Biology | 2016
Andrew N. Billin; Marcus Bantscheff; Gerard Drewes; Sonja Ghidelli-Disse; Jason A. Holt; Henning F. Kramer; Alan J. McDougal; Terry L. Smalley; Carrow I. Wells; William J. Zuercher; Brad R. Henke
Skeletal muscle progenitor stem cells (referred to as satellite cells) represent the primary pool of stem cells in adult skeletal muscle responsible for the generation of new skeletal muscle in response to injury. Satellite cells derived from aged muscle display a significant reduction in regenerative capacity to form functional muscle. This decrease in functional recovery has been attributed to a decrease in proliferative capacity of satellite cells. Hence, agents that enhance the proliferative abilities of satellite cells may hold promise as therapies for a variety of pathological settings, including repair of injured muscle and age- or disease-associated muscle wasting. Through phenotypic screening of isolated murine satellite cells, we identified a series of 2,4-diaminopyrimidines (e.g., 2) that increased satellite cell proliferation. Importantly, compound 2 was effective in accelerating repair of damaged skeletal muscle in an in vivo mouse model of skeletal muscle injury. While these compounds were originally prepared as c-Jun N-terminal kinase 1 (JNK-1) inhibitors, structure-activity analyses indicated JNK-1 inhibition does not correlate with satellite cell activity. Screening against a broad panel of kinases did not result in identification of an obvious molecular target, so we conducted cell-based proteomics experiments in an attempt to identify the molecular target(s) responsible for the potentiation of the satellite cell proliferation. These data provide the foundation for future efforts to design improved small molecules as potential therapeutics for muscle repair and regeneration.
bioRxiv | 2018
Bonnie L. Bassler; Amelia R. McCready; Jon Paczkowski; Brad R. Henke
Quorum sensing is a cell-cell communication process that bacteria use to orchestrate group behaviors. Quorum sensing is mediated by extracellular signal molecules called autoinducers. Autoinducers are often structurally similar, raising questions concerning how bacteria distinguish among them. Here, we use the Pseudomonas aeruginosa LasR quorum-sensing receptor to explore receptor sensitivity and selectivity. Alteration of LasR amino acid S129 increases ligand selectivity and decreases ligand sensitivity. Conversely, the L130F mutation enhances LasR sensitivity while reducing selectivity. We solve crystal structures of LasR ligand binding domains complexed with non-cognate autoinducers. Comparison to existing structures reveals that ligand selectivity/sensitivity is mediated by a flexible loop adjacent to the ligand binding site. We show that P. aeruginosa harboring LasR variants with modified selectivity or sensitivity exhibit altered quorum-sensing responses. We suggest that an evolutionary trade-off between ligand selectivity and sensitivity enables LasR to optimally regulate quorum-sensing traits.
Journal of Medicinal Chemistry | 2000
Timothy M. Willson; Peter J. Brown; Daniel D. Sternbach; Brad R. Henke
Journal of Medicinal Chemistry | 1998
Brad R. Henke; Steven G. Blanchard; Marcus Brackeen; Kathleen K. Brown; Jeff E. Cobb; Jon L. Collins; W. Wallace Harrington; Mir Hashim; Emily A. Hull-Ryde; Istvan Kaldor; Steven A. Kliewer; Debra H. Lake; Lisa M. Leesnitzer; Jürgen M. Lehmann; James M. Lenhard; Lisa A. Orband-Miller; John Miller; Robert A. Mook; Stewart A. Noble; William R. Oliver; Derek J. Parks; Kelli D. Plunket; Jerzy Ryszard Szewczyk; Timothy M. Willson
Diabetes | 1999
Kathleen K. Brown; Brad R. Henke; Steven G. Blanchard; Jeffery E. Cobb; Robert A. Mook; Istvan Kaldor; Steven A. Kliewer; Jürgen M. Lehmann; James M. Lenhard; W. Wallace Harrington; P J Novak; W Faison; J G Binz; Mir Hashim; W O Oliver; H R Brown; Derek J. Parks; Kelli D. Plunket; Wei-Qin Tong⊥; J A Menius; K Adkison; Stewart A. Noble; Timothy M. Willson
Journal of Medicinal Chemistry | 1998
Jeff E. Cobb; Steven G. Blanchard; Evan G. Boswell; Kathleen K. Brown; Paul S. Charifson; Joel P. Cooper; Jon L. Collins; Milana Dezube; Brad R. Henke; Emily A. Hull-Ryde; Debra H. Lake; James M. Lenhard; William R. Oliver; Jeffery Oplinger; Mila Pentti; Derek J. Parks; Kelli D. Plunket; Wei-Qin Tong⊥
Journal of Medicinal Chemistry | 1994
Timothy M. Willson; Brad R. Henke; Tanya Momtahen; Paul S. Charifson; Kenneth W. Batchelor; Dennis B. Lubahn; Linda B. Moore; Beverly B. Oliver; Howard R. Sauls; James A. Triantafillou; Steven G. Wolfe; Philip G. Baer
Journal of Medicinal Chemistry | 1998
Jon L. Collins; Steven G. Blanchard; G. Evan Boswell; Paul S. Charifson; Jeff E. Cobb; Brad R. Henke; Emily A. Hull-Ryde; Wieslaw M. Kazmierski; Debra H. Lake; Lisa M. Leesnitzer; Jürgen M. Lehmann; James M. Lenhard; Lisa A. Orband-Miller; † Yolanda Gray-Nunez; Derek J. Parks; and Kelli D. Plunkett; Wei-Qin Tong⊥
