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Dive into the research topics where Melody Mcwherter is active.

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Featured researches published by Melody Mcwherter.


ACS Medicinal Chemistry Letters | 2013

[(11)C]MK-4232: The First Positron Emission Tomography Tracer for the Calcitonin Gene-Related Peptide Receptor.

Ian M. Bell; Steven N. Gallicchio; Craig A. Stump; Joseph G. Bruno; Hong Fan; Liza Gantert; Eric Hostetler; Amanda L. Kemmerer; Melody Mcwherter; Eric L. Moore; Scott D. Mosser; Mona Purcell; Kerry Riffel; Christopher A. Salvatore; Sandra M. Sanabria-Bohórquez; Donnette D. Staas; Rebecca B. White; Mangay Williams; C. Blair Zartman; Jacquelynn J. Cook; Richard Hargreaves; Stefanie A. Kane; Samuel L. Graham; Harold G. Selnick

Rational modification of the potent calcitonin gene-related peptide (CGRP) receptor antagonist MK-3207 led to a series of analogues with enhanced CNS penetrance and a convenient chemical handle for introduction of a radiolabel. A number of (11)C-tracers were synthesized and evaluated in vivo, leading to the identification of [(11)C]8 ([(11)C]MK-4232), the first positron emission tomography tracer for the CGRP receptor.


Bioorganic & Medicinal Chemistry Letters | 2015

Methyl-substitution of an iminohydantoin spiropiperidine β-secretase (BACE-1) inhibitor has a profound effect on its potency

Melissa S. Egbertson; Georgia B. McGaughey; Steven M. Pitzenberger; Shaun R. Stauffer; Craig A. Coburn; Shawn J. Stachel; Wenjin Yang; James C. Barrow; Lou Anne Neilson; Melody Mcwherter; Debra S. Perlow; Bruce Fahr; Sanjeev Munshi; Timothy J. Allison; Katharine M Holloway; Harold G. Selnick; Zhi-Qiang Yang; John Swestock; Adam J. Simon; Sethu Sankaranarayanan; Dennis Colussi; Katherine Tugusheva; Ming Tain Lai; Beth Pietrak; Shari Haugabook; Lixia Jin; I. W. Chen; Marie Holahan; Maria Stranieri-Michener; Jacquelynn J. Cook

The IC50 of a beta-secretase (BACE-1) lead compound was improved ∼200-fold from 11 μM to 55 nM through the addition of a single methyl group. Computational chemistry, small molecule NMR, and protein crystallography capabilities were used to compare the solution conformation of the ligand under varying pH conditions to its conformation when bound in the active site. Chemical modification then explored available binding pockets adjacent to the ligand. A strategically placed methyl group not only maintained the required pKa of the piperidine nitrogen and filled a small hydrophobic pocket, but more importantly, stabilized the conformation best suited for optimized binding to the receptor.


Bioorganic & Medicinal Chemistry Letters | 2015

Novel oxazolidinone calcitonin gene-related peptide (CGRP) receptor antagonists for the acute treatment of migraine

Brendan M. Crowley; Craig A. Stump; Diem N. Nguyen; Craig M. Potteiger; Melody Mcwherter; Daniel V. Paone; Amy G. Quigley; Joseph G. Bruno; Dan Cui; J. Christopher Culberson; Andrew Danziger; Christine Fandozzi; Danny Gauvreau; Amanda L. Kemmerer; Karsten Menzel; Eric L. Moore; Scott D. Mosser; Vijay Bhasker G. Reddy; Rebecca B. White; Christopher A. Salvatore; Stefanie A. Kane; Ian M. Bell; Harold G. Selnick; Mark E. Fraley; Christopher S. Burgey

In our efforts to develop CGRP receptor antagonists as backups to MK-3207, 2, we employed a scaffold hopping approach to identify a series of novel oxazolidinone-based compounds. The development of a structurally diverse, potent (20, cAMP+HS IC50=0.67 nM), and selective compound (hERG IC50=19 μM) with favorable rodent pharmacokinetics (F=100%, t1/2=7h) is described. Key to this development was identification of a 3-substituted spirotetrahydropyran ring that afforded a substantial gain in potency (10 to 35-fold).


Bioorganic & Medicinal Chemistry Letters | 2014

(E)-Alkenes as replacements of amide bonds: development of novel and potent acyclic CGRP receptor antagonists.

June J. Kim; Michael R. Wood; Shawn J. Stachel; Pablo De Leon; Ashley Nomland; Craig A. Stump; Melody Mcwherter; Kathy M. Schirripa; Eric L. Moore; Christopher A. Salvatore; Harold G. Selnick

A new class of CGRP receptor antagonists was identified by replacing the central amide of a previously identified anilide lead structure with ethylene, ethane, or ethyne linkers. (E)-Alkenes as well as alkynes were found to preserve the proper bioactive conformation of the amides, necessary for efficient receptor binding. Further exploration resulted in several potent compounds against CGRP-R with low susceptibility to P-gp mediated efflux.


Archive | 2005

Spiropiperidine compounds useful as beta-secretase inhibitors for the treatment of alzhermer’s disease

James C. Barrow; Craig A. Coburn; Melissa S. Egbertson; Georgia B. McGaughey; Melody Mcwherter; Lou Anne Neilson; Harold G. Selnick; Shaun R. Stauffer; Zhi-Qiang Yang; Wenjin Yang; Wanli Lu; Bruce Fahr; Kenneth E. Rittle


Archive | 2008

Cgrp receptor antagonists with tertiary amide, sulfonamide, carbamate and urea end groups

Michael R. Wood; June Kim; Melody Mcwherter; Harold G. Selnick; Kathy M. Schirripa


Archive | 2009

MONOCYCLIC CGRP RECEPTOR ANTAGONISTS

Ian M. Bell; Melody Mcwherter; Harold G. Selnick; Donnette D. Staas; Shawn J. Stachel; Thomas G. Steele; Craig A. Stump; Michael R. Wood; C. Blair Zartman


Archive | 2009

IMIDAZOLINONE DERIVATIVES AS CGRP RECEPTOR ANTAGONISTS

Harold G. Selnick; Michael R. Wood; Melody Mcwherter; Ivory D. Hills; Craig A. Stump


Archive | 2015

BENZAMIDE CGRP RECEPTOR ANTAGONISTS

Brendan M. Crowley; Mark E. Fraley; Craig M. Potteiger; Robert Gilfillan; Ken Arrington; Helen J. Mitchell; Kathy M. Schirripa; Melody Mcwherter; Tesfaye Biftu; Anilkumar G. Nair; Cheng Wang; De-Yi Yang; Cheng Zhu; Nam Fung Kar; Xianhai Huang; Lei Chen; Wei Zhou; Qingsheng Liu; Jiaqiang Cai


Archive | 2009

Antagonistes des récepteurs cgrp monocycliques

Ian M. Bell; Melody Mcwherter; Harold G. Selnick; Donnette D. Staas; Shawn J. Stachel; Thomas H. Steele; Craig A. Stump; Michael R. Wood; C. Blair Zartman

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Shawn J. Stachel

United States Military Academy

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Bruce Fahr

Sunesis Pharmaceuticals

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C. Blair Zartman

United States Military Academy

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Craig A. Coburn

United States Military Academy

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Donnette D. Staas

United States Military Academy

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