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Dive into the research topics where Tai-An Lin is active.

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Featured researches published by Tai-An Lin.


Molecular Cancer Therapeutics | 2008

Identification of a nonkinase target mediating cytotoxicity of novel kinase inhibitors.

Petra Ross-MacDonald; Heshani de Silva; Qi Guo; Hong Xiao; Chen-Yi Hung; Becky Penhallow; Jay A. Markwalder; Liqi He; Ricardo M. Attar; Tai-An Lin; Steven P. Seitz; Charles Tilford; Judith Wardwell-Swanson; Donald G. Jackson

In developing inhibitors of the LIM kinases, the initial lead molecules combined potent target inhibition with potent cytotoxic activity. However, as subsequent compounds were evaluated, the cytotoxic activity separated from inhibition of LIM kinases. A rapid determination of the cytotoxic mechanism and its molecular target was enabled by integrating data from two robust core technologies. High-content assays and gene expression profiling both indicated an effect on microtubule stability. Although the cytotoxic compounds are still kinase inhibitors, and their structures did not predict tubulin as an obvious target, these results provided the impetus to test their effects on microtubule polymerization directly. Unexpectedly, we confirmed tubulin itself as a molecular target of the cytotoxic kinase inhibitor compounds. This general approach to mechanism of action questions could be extended to larger data sets of quantified phenotypic and gene expression data. [Mol Cancer Ther 2008;7(11):3490–8]


Bioorganic & Medicinal Chemistry Letters | 2002

Discovery and initial SAR of imidazoquinoxalines as inhibitors of the Src-family kinase p56Lck

Ping Chen; Derek J. Norris; Edwin J. Iwanowicz; Steven H. Spergel; James Lin; Henry H. Gu; Zhongqi Shen; John Wityak; Tai-An Lin; Suhong Pang; Henry de Fex; Sidney Pitt; Ding Ren Shen; Arthur M. Doweyko; Donna A. Bassolino; Jacques Y. Roberge; Michael A. Poss; Bang-Chi Chen; Gary L. Schieven; Joel C. Barrish

We have identified a novel series of 1,5-imidazoquinoxalines as inhibitors of Lck with excellent potency (IC50s<5 nM) as well as good cellular activity against T-cell proliferation (IC50s<1 microM). Structure-activity studies demonstrate the requirement for the core heterocycle in addition to an optimal 2,6-disubstituted aniline group.


Bioorganic & Medicinal Chemistry Letters | 2012

Modulation of cofilin phosphorylation by inhibition of the Lim family kinases.

Liqi He; Steven P. Seitz; George L. Trainor; David R. Tortolani; Wayne Vaccaro; Michael A. Poss; Christine M. Tarby; John S. Tokarski; Becky Penhallow; Chen-Yi Hung; Ricardo M. Attar; Tai-An Lin

A series of aminothiazoles that are potent inhibitors of LIM kinases 1 and 2 is described. Appropriate choice of substituents led to molecules with good selectivity for either enzyme. An advanced member of the series was shown to effectively interfere with the phosphorylation of the LIM kinases substrate cofilin. Consistent with the important role of the LIM kinases in regulating cytoskeletal structure, treated cells displayed dramatically reduced F-actin content.


Journal of Medicinal Chemistry | 2005

Discovery of a (1H-benzoimidazol-2-yl)-1H-pyridin-2-one (BMS-536924) inhibitor of insulin-like growth factor I receptor kinase with in vivo antitumor activity.

Mark D. Wittman; Joan M. Carboni; Ricardo M. Attar; Balu Balasubramanian; Praveen Balimane; Patrick Brassil; Francis Beaulieu; Chiehying Chang; Wendy Clarke; Janet Dell; Jeffrey Eummer; David B. Frennesson; Marco M. Gottardis; Ann Greer; Steven Hansel; Warren Hurlburt; Bruce L. Jacobson; Subramaniam Krishnananthan; Francis Y. Lee; Aixin Li; Tai-An Lin; Peiying Liu; Carl Ouellet; Xiaopeng Sang; Mark G. Saulnier; Karen Stoffan; Yax Sun; Upender Velaparthi; Henry Wong; Zheng Yang


Biochemistry | 2004

Selective Itk Inhibitors Block T-Cell Activation and Murine Lung Inflammation

Tai-An Lin; Kim W. McIntyre; Jagabandhu Das; Chunjian Liu; Kathleen O'Day; Becky Penhallow; Chen-Yi Hung; Gena S. Whitney; David J. Shuster; Xiaoxia Yang; Robert Townsend; Jennifer Postelnek; Steven H. Spergel; James Lin; Robert V. Moquin; Joseph A. Furch; Amrita Kamath; Hongjian Zhang; Punit Marathe; Juan J. Perez-villar; Arthur M. Doweyko; Loran Killar; John H. Dodd; Joel C. Barrish; and John Wityak; Steven B. Kanner


Bioorganic & Medicinal Chemistry Letters | 2006

Discovery and SAR of 2-amino-5-[(thiomethyl)aryl]thiazoles as potent and selective Itk inhibitors

Jagabandhu Das; Joseph A. Furch; Chunjian Liu; Robert V. Moquin; James Lin; Steven H. Spergel; Kim W. McIntyre; David J. Shuster; Kathleen D. O’Day; Becky Penhallow; Chen-Yi Hung; Arthur M. Doweyko; Amrita Kamath; Hongjian Zhang; Punit Marathe; Steven B. Kanner; Tai-An Lin; John H. Dodd; Joel C. Barrish; John Wityak


Biochemistry | 2002

Phosphorylation of the linker for activation of T-cells by Itk promotes recruitment of Vav.

Juan J. Perez-Villar; Gena S. Whitney; Mitchell T. Sitnick; Robert J. Dunn; Srividhya Venkatesan; Kathleen O'Day; Gary L. Schieven; Tai-An Lin; Steven B. Kanner


Archive | 2006

Phenyl-substituted pyrimidine compounds useful as kinase inhibitors

Stephen T. Wrobleski; Shuqun Lin; Katerina Leftheris; Liqi He; Steven P. Seitz; Tai-An Lin; Wayne Vaccaro


Bioorganic & Medicinal Chemistry Letters | 2006

Corrigendum to “Discovery and SAR of 2-amino-5-[(thiomethyl)aryl]thiazoles as potent and selective Itk inhibitors” [Bioorg. Med. Chem. Lett. 16 (2006) 2411–2415]

Jagabandhu Das; Chunjian Liu; Robert V. Moquin; James Lin; Joseph A. Furch; Steven H. Spergel; Arthur M. Doweyko; Kim W. McIntyre; David J. Shuster; Kathleen D. O’Day; Becky Penhallow; Chen-Yi Hung; Steven B. Kanner; Tai-An Lin; John H. Dodd; Joel C. Barrish; John Wityak


Archive | 2006

Phenylsubstituierte pyrimidinverbindungen zur verwendung als kinasehemmer Phenyl-substituted pyrimidine compounds for use as kinase inhibitors

Stephen T Wrobelski; Shuqun Lin; Katerina Leftheris; Liqi He; Steven P. Seitz; Tai-An Lin; Wayne Vaccaro

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Liqi He

Bristol-Myers Squibb

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