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Dive into the research topics where Maud Urbanski is active.

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Featured researches published by Maud Urbanski.


Bioorganic & Medicinal Chemistry Letters | 2017

Identification and structure activity relationships of quinoline tertiary alcohol modulators of RORγt

David A. Kummer; Maxwell D. Cummings; Marta Cristina Abad; Joseph Kent Barbay; Glenda Castro; Ronald L. Wolin; Kevin D. Kreutter; Umar Maharoof; Cynthia M. Milligan; Rachel Nishimura; Joan Pierce; Celine Schalk-Hihi; John Spurlino; Maud Urbanski; Hariharan Venkatesan; Aihua Wang; Craig R. Woods; Xiaohua Xue; James P. Edwards; Anne Fourie; Kristi A. Leonard

A high-throughput screen of the ligand binding domain of the nuclear receptor retinoic acid-related orphan receptor gamma t (RORγt) employing a thermal shift assay yielded a quinoline tertiary alcohol hit. Optimization of the 2-, 3- and 4-positions of the quinoline core using structure-activity relationships and structure-based drug design methods led to the discovery of a series of modulators with improved RORγt inhibitory potency and inverse agonism properties.


Bioorganic & Medicinal Chemistry Letters | 2017

6-Substituted quinolines as RORγt inverse agonists

J. Kent Barbay; Maxwell D. Cummings; Marta Cristina Abad; Glenda Castro; Kevin D. Kreutter; David A. Kummer; Umar Maharoof; Cynthia M. Milligan; Rachel Nishimura; Joan Pierce; Celine Schalk-Hihi; John Spurlino; Virginia M. Tanis; Maud Urbanski; Hariharan Venkatesan; Aihua Wang; Craig R. Woods; Ronald L. Wolin; Xiaohua Xue; James P. Edwards; Anne Fourie; Kristi A. Leonard

We identified 6-substituted quinolines as modulators of the retinoic acid receptor-related orphan receptor gamma t (RORγt). The synthesis of this class of RORγt modulators is reported, and optimization of the substituents at the quinoline 6-position that produced compounds with high affinity for the receptor is detailed. This effort identified molecules that act as potent, full inverse agonists in a RORγt-driven cell-based reporter assay. The X-ray crystal structures of two full inverse agonists from this chemical series bound to the RORγt ligand binding domain are disclosed, and we highlight the interaction of a hydrogen-bond acceptor on the 6-position substituent of the inverse agonist with Glu379:NH as a conserved binding contact.


Archive | 2004

Substituted fused heterocyclic c-glycosides

Philip Rybczynski; Maud Urbanski; Xiaoyan Zhang


Archive | 2004

Substituted indazole-o-glucosides

Mona Patel; Philip Rybczynski; Maud Urbanski; Xiaoyan Zhang


Archive | 2004

Substituted benzimidazole-, benztriazole-, and benzimidazolone-O-glucosides

Maud Urbanski


Archive | 2006

Substituted Cycloalkylpyrrolones As Allosteric Modulators Of Glucokinase

Maud Urbanski; Amy Xiang; Roxanne Zeck


Archive | 2006

Substituted pyrrolones as allosteric modulators of glucokinase

Maud Urbanski; Amy Xiang; Roxanne Zeck


Archive | 2013

SECONDARY ALCOHOL QUINOLINYL MODULATORS OF RORyt

Kristi A. Leonard; Kent Barbay; James P. Edwards; Kevin D. Kreutter; David A. Kummer; Umar Maharoof; Rachel Nishimura; Maud Urbanski; Hariharan Venkatesan; Aihua Wang; Ronald L. Wolin; Craig R. Woods; Anne Fourie; Xiaohua Xue; Maxwell D. Cummings


Archive | 2006

Substituted dihydroisoindolones as allosteric modulators of glucokinase

Joseph Dudash; Philip Rybczynski; Maud Urbanski; Amy Xiang; Roxanne Zeck; Xiaoyan Zhang; Yongzheng Zhang


Archive | 2013

Methylene linked quinolinyl modulators of RORγt

Kristi A. Leonard; Kent Barbay; James P. Edwards; Kevin D. Kreutter; David A. Kummer; Umar Maharoof; Rachel Nishimura; Maud Urbanski; Hariharan Venkatesan; Aihua Wang; Ronald L. Wolin; Craig R. Woods; Anne Fourie; Xiaohua Xue; Maxwell D. Cummings; William M. Jones; Steven Goldberg

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Aihua Wang

University of Science and Technology

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