2,7-Pyrrolo[2,1-f][1,2,4]triazines as JAK2 inhibitors: Modification of target structure to minimize reactive metabolite formation

Linda Weinberg,Mark S. Albom,Thelma S. Angeles,Henry J. Breslin,Diane E. Gingrich,Zeqi Huang,Joseph G. Lisko,Jennifer L. Mason,Karen L. Milkiewicz,Tho V. Thieu,Ted L. Underiner,Gregory J. Wells,Kevin J. Wells-Knecht,Bruce D. Dorsey

2,7-Pyrrolo[2,1-f][1,2,4]triazines as JAK2 inhibitors: Modification of target structure to minimize reactive metabolite formation

2011

Linda Weinberg
Mark S. Albom
Thelma S. Angeles
Henry J. Breslin
Diane E. Gingrich
Zeqi Huang
Joseph G. Lisko
Jennifer L. Mason
Karen L. Milkiewicz
Tho V. Thieu
Ted L. Underiner
Gregory J. Wells
Kevin J. Wells-Knecht
Bruce D. Dorsey

Abstract The JAK2/STAT pathway has important roles in hematopoiesis. With the discovery of the JAK2 V617F mutation and its presence in many patients with myeloproliferative neoplasms, research in the JAK2 inhibitor arena has dramatically increased. We report a novel series of potent JAK2 inhibitors containing a 2,7-pyrrolotriazine core. To minimize potential drug-induced toxicity, targets were analyzed for the ability to form a glutathione adduct. Glutathione adduct formation was decreased by modification of the aniline substituent at C2.

Keywords:

JAK-STAT signaling pathway
Glutathione
Metabolite
Adduct
Aniline
Mutation
Organic chemistry
Biochemistry
Substituent
Toxicity
Chemistry
Stereochemistry
Janus kinase 2
Myeloproliferative Disorders
Structure–activity relationship

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