Protecting-group-free synthesis of the bisindolylmaleimide GF109203X

Yong Chen Gao; Yu Hui Jia; Ting Ting Li; Ze Huan Hei; Feng Ling Yang; Mu Hua Huang; Yun Jun Luo

doi:10.3998/ark.5550190.p008.950

Protecting-group-free synthesis of the bisindolylmaleimide GF109203X

Yong Chen Gao, Yu Hui Jia, Ting Ting Li, Ze Huan Hei, Feng Ling Yang, Mu Hua Huang, Yun Jun Luo

School of Material Science and Engineering

Research output: Contribution to journal › Article › peer-review

3 Citations (Scopus)

Abstract

The bisindolylmaleimide GF109203X is a highly selective inhibitor to Protein Kinase C (PKC) and has attracted much attention. However, its reported synthesis required protecting groups. In order to achieve a short and N-protecting-group-free synthesis of GF109203X, an investigation on N-alkylation of arcyriarubin A was carried out using different bases, solvents and equivalents of bromododecane. It is found that mono-N-alkylation and mono-N′-alkylation could be achieved respectively. Thus, a protecting-group-free synthesis of GF109203X was accomplished in 40% overall yield starting from indole. This work will lead to a short synthesis of mono-N′-alkylated arcyriarubins to accelerate drug discovery.

Original language	English
Pages (from-to)	153-163
Number of pages	11
Journal	Arkivoc
Volume	2015
Issue number	5
DOIs	https://doi.org/10.3998/ark.5550190.p008.950
Publication status	Published - 26 Mar 2015

Keywords

Arcyriarubin A
Bisindolylmaleimide
GF109203X
PKC inhibitors
Protecting group-free synthesis

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10.3998/ark.5550190.p008.950

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title = "Protecting-group-free synthesis of the bisindolylmaleimide GF109203X",

abstract = "The bisindolylmaleimide GF109203X is a highly selective inhibitor to Protein Kinase C (PKC) and has attracted much attention. However, its reported synthesis required protecting groups. In order to achieve a short and N-protecting-group-free synthesis of GF109203X, an investigation on N-alkylation of arcyriarubin A was carried out using different bases, solvents and equivalents of bromododecane. It is found that mono-N-alkylation and mono-N′-alkylation could be achieved respectively. Thus, a protecting-group-free synthesis of GF109203X was accomplished in 40% overall yield starting from indole. This work will lead to a short synthesis of mono-N′-alkylated arcyriarubins to accelerate drug discovery.",

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AU - Gao, Yong Chen

AU - Jia, Yu Hui

AU - Li, Ting Ting

AU - Hei, Ze Huan

AU - Yang, Feng Ling

AU - Huang, Mu Hua

AU - Luo, Yun Jun

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PY - 2015/3/26

Y1 - 2015/3/26

N2 - The bisindolylmaleimide GF109203X is a highly selective inhibitor to Protein Kinase C (PKC) and has attracted much attention. However, its reported synthesis required protecting groups. In order to achieve a short and N-protecting-group-free synthesis of GF109203X, an investigation on N-alkylation of arcyriarubin A was carried out using different bases, solvents and equivalents of bromododecane. It is found that mono-N-alkylation and mono-N′-alkylation could be achieved respectively. Thus, a protecting-group-free synthesis of GF109203X was accomplished in 40% overall yield starting from indole. This work will lead to a short synthesis of mono-N′-alkylated arcyriarubins to accelerate drug discovery.

AB - The bisindolylmaleimide GF109203X is a highly selective inhibitor to Protein Kinase C (PKC) and has attracted much attention. However, its reported synthesis required protecting groups. In order to achieve a short and N-protecting-group-free synthesis of GF109203X, an investigation on N-alkylation of arcyriarubin A was carried out using different bases, solvents and equivalents of bromododecane. It is found that mono-N-alkylation and mono-N′-alkylation could be achieved respectively. Thus, a protecting-group-free synthesis of GF109203X was accomplished in 40% overall yield starting from indole. This work will lead to a short synthesis of mono-N′-alkylated arcyriarubins to accelerate drug discovery.

KW - Arcyriarubin A

KW - Bisindolylmaleimide

KW - GF109203X

KW - PKC inhibitors

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VL - 2015

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JO - Arkivoc

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ER -

Protecting-group-free synthesis of the bisindolylmaleimide GF109203X

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Keywords

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