Synthesis of Functionalized Derivatives of the Gamma-Secretase Modulator BMS-932481 and Identification of its Major Metabolite

Yunhui Zhang,Kenneth M. Boy,Yong-Jin Wu,Antonio Ramirez,Jeremy H. Toyn,Michael K. Ahlijanian,Charles F. Albright,Xiaoliang Zhuo,Benjamin M. Johnson,Rex Denton,Richard E. Olson,Lorin A. Thompson,John E. Macor

Synthesis of Functionalized Derivatives of the Gamma-Secretase Modulator BMS-932481 and Identification of its Major Metabolite

2020

Yunhui Zhang
Kenneth M. Boy
Yong-Jin Wu
Antonio Ramirez
Jeremy H. Toyn
Michael K. Ahlijanian
Charles F. Albright
Xiaoliang Zhuo
Benjamin M. Johnson
Rex Denton
Richard E. Olson
Lorin A. Thompson
John E. Macor

In an effort to improve physical properties by introducing polar functionality into the bicyclic pyrimidine gamma-secretase modulator (GSM) clinical candidate BMS-932481, we prepared several oxidative products of BMS-932481. Among the analogs that were prepared, the C-5 alcohol 3 was identified as the predominant metabolite of BMS-932481 found in rat and human liver microsomes. Alcohol 3 was determined to be chemically unstable, leading to the hypothesis that 3 may lead to the production of reactive species both in vitro and in vivo.

Keywords:

Biochemistry
In vivo
Alcohol
Chemistry
Microsome
In vitro
Metabolite
Pyrimidine
Bicyclic molecule
Gamma secretase

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