Synthesis of Pyrazolofuropyrazine via One-Pot S N Ar Reaction and Intramolecular Direct C-H Arylation

Shinichiro Fuse; Megumi Inaba; Shinichi Sato; Manjusha Joshi; Hiroyuki Nakamura

doi:10.1055/s-0036-1591885

Synthesis of Pyrazolofuropyrazine via One-Pot S _N Ar Reaction and Intramolecular Direct C-H Arylation

Shinichiro Fuse, Megumi Inaba, Shinichi Sato, Manjusha Joshi, Hiroyuki Nakamura

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

5 Citations (Scopus)

Abstract

Fused-ring systems containing heterocycles are attractive templates for drug discovery. Biologically active 6-5-5+6 fused-ring systems that possess heterocycles are available, but these require a relatively large number of synthetic steps for preparation. Therefore, pyrazolofuropyrazine was designed as a 6-5-5+6 ring system template that incorporates ready accessibility for drug discovery. Pyrazolofuropyrazines were successfully constructed in only a few steps via one-pot S _N Ar reaction/intramolecular C-H direct arylation. As a drug candidate, pyrazolofuropyrazine has earned a favorable LogP, although significant biological activity has yet to be established; the ready accessibility of pyrazolofuropyrazine template, however, offers an opportunity for the rapid development of promising new drug candidates.

Original language	English
Article number	ss-2017-f0762-op
Pages (from-to)	1493-1498
Number of pages	6
Journal	Synthesis (Germany)
Volume	50
Issue number	7
DOIs	https://doi.org/10.1055/s-0036-1591885
Publication status	Published - 2018 Apr 3
Externally published	Yes

Keywords

C-H activation
antitumor agents
cyclization
fused-ring systems
heterocycles

ASJC Scopus subject areas

Catalysis
Organic Chemistry

Access to Document

10.1055/s-0036-1591885

Cite this

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title = "Synthesis of Pyrazolofuropyrazine via One-Pot S N Ar Reaction and Intramolecular Direct C-H Arylation",

abstract = "Fused-ring systems containing heterocycles are attractive templates for drug discovery. Biologically active 6-5-5+6 fused-ring systems that possess heterocycles are available, but these require a relatively large number of synthetic steps for preparation. Therefore, pyrazolofuropyrazine was designed as a 6-5-5+6 ring system template that incorporates ready accessibility for drug discovery. Pyrazolofuropyrazines were successfully constructed in only a few steps via one-pot S N Ar reaction/intramolecular C-H direct arylation. As a drug candidate, pyrazolofuropyrazine has earned a favorable LogP, although significant biological activity has yet to be established; the ready accessibility of pyrazolofuropyrazine template, however, offers an opportunity for the rapid development of promising new drug candidates.",

keywords = "C-H activation, antitumor agents, cyclization, fused-ring systems, heterocycles",

author = "Shinichiro Fuse and Megumi Inaba and Shinichi Sato and Manjusha Joshi and Hiroyuki Nakamura",

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AU - Fuse, Shinichiro

AU - Inaba, Megumi

AU - Sato, Shinichi

AU - Joshi, Manjusha

AU - Nakamura, Hiroyuki

N1 - Publisher Copyright: © Georg Thieme Verlag Stuttgart New York.

PY - 2018/4/3

Y1 - 2018/4/3

N2 - Fused-ring systems containing heterocycles are attractive templates for drug discovery. Biologically active 6-5-5+6 fused-ring systems that possess heterocycles are available, but these require a relatively large number of synthetic steps for preparation. Therefore, pyrazolofuropyrazine was designed as a 6-5-5+6 ring system template that incorporates ready accessibility for drug discovery. Pyrazolofuropyrazines were successfully constructed in only a few steps via one-pot S N Ar reaction/intramolecular C-H direct arylation. As a drug candidate, pyrazolofuropyrazine has earned a favorable LogP, although significant biological activity has yet to be established; the ready accessibility of pyrazolofuropyrazine template, however, offers an opportunity for the rapid development of promising new drug candidates.

AB - Fused-ring systems containing heterocycles are attractive templates for drug discovery. Biologically active 6-5-5+6 fused-ring systems that possess heterocycles are available, but these require a relatively large number of synthetic steps for preparation. Therefore, pyrazolofuropyrazine was designed as a 6-5-5+6 ring system template that incorporates ready accessibility for drug discovery. Pyrazolofuropyrazines were successfully constructed in only a few steps via one-pot S N Ar reaction/intramolecular C-H direct arylation. As a drug candidate, pyrazolofuropyrazine has earned a favorable LogP, although significant biological activity has yet to be established; the ready accessibility of pyrazolofuropyrazine template, however, offers an opportunity for the rapid development of promising new drug candidates.

KW - C-H activation

KW - antitumor agents

KW - cyclization

KW - fused-ring systems

KW - heterocycles

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