An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization

M. Giustiniano; VALENTINA MERCALLI; E. Novellino; Gian Cesare TRON

doi:10.1039/C6RA01442A

An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization

M. Giustiniano
, VALENTINA MERCALLI
, E. Novellino
, Gian Cesare TRON

Department of Pharmaceutical Sciences

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

Abstract

A convergent and efficient two-step synthesis of pharmaceutically relevant 1-arylindazole-3-carboxamides is reported. These molecules have been obtained in good to excellent yields (up to 98%) starting from a strategic reaction between isocyanides, 2-iodo-N-arylbenzohydrazonoyl chlorides and 2-hydroxymethylbenzoic acid followed by a chemoselective Buchwald–Hartwig intramolecular cyclization. This novel strategy provides an additional indazole synthesis to those already reported in literature both in the type of substrate as well as the substitution pattern obtainable in the products. Furthermore benzylisocyanide is herein reported for the first time as a convertible isocyanide providing an expeditious access to N-arylindazole-3-carbonitriles

Original language	English
Pages (from-to)	34913-34920
Number of pages	8
Journal	RSC Advances
Volume	6
DOIs	https://doi.org/10.1039/C6RA01442A
Publication status	Published - 2016

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10.1039/C6RA01442A

http://hdl.handle.net/11579/77793

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@article{2b9e4088ab394147aca9f44763dd2c2a,

title = "An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization",

abstract = "A convergent and efficient two-step synthesis of pharmaceutically relevant 1-arylindazole-3-carboxamides is reported. These molecules have been obtained in good to excellent yields (up to 98\%) starting from a strategic reaction between isocyanides, 2-iodo-N-arylbenzohydrazonoyl chlorides and 2-hydroxymethylbenzoic acid followed by a chemoselective Buchwald–Hartwig intramolecular cyclization. This novel strategy provides an additional indazole synthesis to those already reported in literature both in the type of substrate as well as the substitution pattern obtainable in the products. Furthermore benzylisocyanide is herein reported for the first time as a convertible isocyanide providing an expeditious access to N-arylindazole-3-carbonitriles",

author = "M. Giustiniano and VALENTINA MERCALLI and E. Novellino and TRON, \{Gian Cesare\}",

note = "Publisher Copyright: {\textcopyright} The Royal Society of Chemistry 2016.",

year = "2016",

doi = "10.1039/C6RA01442A",

language = "English",

volume = "6",

pages = "34913--34920",

journal = "RSC Advances",

issn = "2046-2069",

publisher = "Royal Society of Chemistry",

}

An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization. / Giustiniano, M.; MERCALLI, VALENTINA; Novellino, E. et al.
In: RSC Advances, Vol. 6, 2016, p. 34913-34920.

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

TY - JOUR

T1 - An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization

AU - Giustiniano, M.

AU - MERCALLI, VALENTINA

AU - Novellino, E.

AU - TRON, Gian Cesare

PY - 2016

Y1 - 2016

N2 - A convergent and efficient two-step synthesis of pharmaceutically relevant 1-arylindazole-3-carboxamides is reported. These molecules have been obtained in good to excellent yields (up to 98%) starting from a strategic reaction between isocyanides, 2-iodo-N-arylbenzohydrazonoyl chlorides and 2-hydroxymethylbenzoic acid followed by a chemoselective Buchwald–Hartwig intramolecular cyclization. This novel strategy provides an additional indazole synthesis to those already reported in literature both in the type of substrate as well as the substitution pattern obtainable in the products. Furthermore benzylisocyanide is herein reported for the first time as a convertible isocyanide providing an expeditious access to N-arylindazole-3-carbonitriles

AB - A convergent and efficient two-step synthesis of pharmaceutically relevant 1-arylindazole-3-carboxamides is reported. These molecules have been obtained in good to excellent yields (up to 98%) starting from a strategic reaction between isocyanides, 2-iodo-N-arylbenzohydrazonoyl chlorides and 2-hydroxymethylbenzoic acid followed by a chemoselective Buchwald–Hartwig intramolecular cyclization. This novel strategy provides an additional indazole synthesis to those already reported in literature both in the type of substrate as well as the substitution pattern obtainable in the products. Furthermore benzylisocyanide is herein reported for the first time as a convertible isocyanide providing an expeditious access to N-arylindazole-3-carbonitriles

UR - https://iris.uniupo.it/handle/11579/77793

U2 - 10.1039/C6RA01442A

DO - 10.1039/C6RA01442A

M3 - Article

SN - 2046-2069

VL - 6

SP - 34913

EP - 34920

JO - RSC Advances

JF - RSC Advances

ER -

An efficient synthesis of 1-arylindazole-3-carboxamides using nitrile imines, isocyanides and 2-hydroxymethylbenzoic acid, followed by a chemoselective Buchwald–Hartwig intramolecular cyclization

Abstract

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