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Dive into the research topics where Terry Vincent Hughes is active.

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Featured researches published by Terry Vincent Hughes.


Molecular Pharmacology | 2007

Cellular and in Vivo Activity of JNJ-28871063, A Nonquinazoline Pan-ErbB Kinase Inhibitor That Crosses the Blood-Brain Barrier and Displays Efficacy against Intracranial Tumors

Stuart Emanuel; Terry Vincent Hughes; Mary Adams; Catherine A. Rugg; Angel R. Fuentes-Pesquera; Peter J. Connolly; Niranjan B. Pandey; Sandra Moreno-Mazza; Jeannene Butler; Virna Borowski; Steven Middleton; Robert H. Gruninger; Jennifer R. Story; Cheryl Napier; Beth Hollister; Lee M. Greenberger

JNJ-28871063 is a potent and highly selective pan-ErbB kinase inhibitor from a novel aminopyrimidine oxime structural class that blocks the proliferation of epidermal growth factor receptor (EGFR; ErbB1)- and ErbB2-overexpressing cells but does not affect the growth of non-ErbB-overexpressing cells. Treatment of human cancer cells with JNJ-28871063 inhibited phosphorylation of functionally important tyrosine residues in both EGFR and ErbB2 and blocked downstream signal transduction pathways responsible for proliferation and survival. A single dose of compound reduced phosphorylation of ErbB2 receptors in tumor-bearing mice, demonstrating target suppression in vivo. Tissue distribution studies show that JNJ-28871063 crosses the blood-brain barrier and penetrates into tumors, where it is able to accumulate to higher levels than those found in the plasma. JNJ-28871063 showed oral antitumor activity in human tumor xenograft models that overexpress EGFR and ErbB2. In an intracranial ErbB2-overexpressing tumor model, JNJ-28871063 extended survival relative to untreated animals. The brain is a primary site of metastasis for EGFR-overexpressing lung cancers and ErbB2-overexpressing breast cancers. Therefore, the ability to penetrate into the brain could be an advantage over existing therapies such as trastuzumab (Herceptin) and cetuximab (Erbitux), which are antibodies and do not cross the blood-brain barrier. These results show that JNJ-28871063 is orally bioavailable, has activity against EGFR and ErbB2-dependent tumor xenografts, and can penetrate into the brain and inhibit ErbB2-overexpressing tumor growth.


ACS Medicinal Chemistry Letters | 2018

Identification of Quinoline-Based RIP2 Kinase Inhibitors with an Improved Therapeutic Index to the hERG Ion Channel

Pamela A. Haile; Linda N. Casillas; Michael Jonathan Bury; John F. Mehlmann; Robert R. Singhaus; Adam Kenneth Charnley; Terry Vincent Hughes; Michael P. DeMartino; Gren Z. Wang; Joseph J. Romano; Xiaoyang Dong; Nikolay V. Plotnikov; Ami S. Lakdawala; Bartholomew J. Votta; David B. Lipshutz; Biva Desai; Barbara Swift; Carol Capriotti; Scott B. Berger; Mukesh K. Mahajan; Michael Reilly; Elizabeth J. Rivera; Helen H. Sun; Rakesh Nagilla; Carol LePage; Michael T. Ouellette; Rachel Totoritis; Brian T. Donovan; Barry S. Brown; Khuram W. Chaudhary

RIP2 kinase was recently identified as a therapeutic target for a variety of autoimmune diseases. We have reported previously a selective 4-aminoquinoline-based RIP2 inhibitor GSK583 and demonstrated its effectiveness in blocking downstream NOD2 signaling in cellular models, rodent in vivo models, and human ex vivo disease models. While this tool compound was valuable in validating the biological pathway, it suffered from activity at the hERG ion channel and a poor PK/PD profile thereby limiting progression of this analog. Herein, we detail our efforts to improve both this off-target liability as well as the PK/PD profile of this series of inhibitors through modulation of lipophilicity and strengthening hinge binding ability. These efforts have led to inhibitor 7, which possesses high binding affinity for the ATP pocket of RIP2 (IC50 = 1 nM) and inhibition of downstream cytokine production in human whole blood (IC50 = 10 nM) with reduced hERG activity (14 μM).


Archive | 2011

PYRAZOLYL-PYRIMIDINES AS KINASE INHIBITORS

Linda N. Casillas; Subhas J. Chakravorty; Patrick M. Eidam; Pamela A. Haile; Terry Vincent Hughes; Ami Lakdawala Shah; Lara Kathryn Leister; Nathan A. Miller; Attiq Rahman; Clark A. Sehon; Gren Z. Wang; Daohua Zhang


Archive | 2012

QUINOLYL AMINES AS KINASE INHIBITORS

Linda N. Casillas; Adam Kenneth Charnley; Pamela A. Haile; Terry Vincent Hughes; Robert W. Marquis; John F. Mehlmann; Michael Reilly; Joseph J. Romano; Robert R. Singhaus


Archive | 2011

INDAZOLYL-PYRIMIDINES AS KINASE INHIBITORS

Linda N. Casillas; Subhas J. Chakravorty; Adam Kenneth Charnley; Pamela A. Haile; Terry Vincent Hughes; Jae U. Jeong; Jianxing Kang; Ami Lakdawala Shah; Lara Kathryn Leister; Robert W. Marquis; Nathan A. Miller; Daniel J. Price; Clark A. Sehon; Gren Z. Wang; Daohua Zhang; Patrick M. Eidam


Archive | 2010

Oxazoles as modulators of chemokine receptors

Xuan Hong; Terry Vincent Hughes; Nathan A. Miller; Tamara Ann Miskowski; Clark A. Sehon


Archive | 2008

Spirodihydrobenzofurans as modulators of chemokine receptors

Brian W. Budzik; Pamela A. Haile; Terry Vincent Hughes; Clark A. Sehon; Gren Z. Wang


Archive | 2017

COMPUESTO DE PIRAZOL-4-CARBOXAMIDA, COMPOSICIÓN FARMACÉUTICA QUE LO COMPRENDE Y SU USO PARA LA FABRICACIÓN DE UN MEDICAMENTO

Albane Marie Kessler; Terry Vincent Hughes; Mark Elban; Ignacio Cotillo Torrejon; Adam Kenneth Charnley; Julio Alonso Padilla; Beth Anne Knapp-Reed; Yiqian Lian; Jose Julio Martin; Imanol Pea Urquiza; Ana Rodriguez


Archive | 2017

AMIDAS HETEROCÍCLICAS ÚTILES COMO MODULADORES DE PROTEÍNAS

Lian Yiqian; Gren Z. Wang; Ye Guosen; Jason W. Dodson; Lara Kathryn Leister; Michael G Darcy; Terry Vincent Hughes; Dong Xiaoyang; Li Yue; Nevins Neysa; Adam Kenneth Charnley; John F. Mehlmann; Joseph J. Romano; Zhang Daohua; Kang Jianxing; Joshi M. Ramanjulu


Archive | 2017

HETEROCYCLIC AMIDES USEFUL AS PROTEIN MODULATORS

Adam Kenneth Charnley; Michael G Darcy; Jason W. Dodson; Xiaoyang Dong; Terry Vincent Hughes; Jianxing Kang; Lara Kathryn Leister; Yiqian Lian; Yue Li; John F. Mehlmann; Neysa Nevins; Joshi M. Ramanjulu; Joseph J. Romano; Gren Z. Wang; Guosen Ye; Daohua Zhang

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