C-H activation for the synthesis of C1-(hetero)aryl glycosides

Morgane de Robichon; Juba Ghouilem; Angélique Ferry; Samir Messaoudi

doi:10.1002/9781119774167.ch16

C-H activation for the synthesis of C1-(hetero)aryl glycosides

Morgane de Robichon
, Juba Ghouilem
, Angélique Ferry
, Samir Messaoudi

Résultats de recherche: Le chapitre dans un livre, un rapport, une anthologie ou une collection › Chapitre › Revue par des pairs

Résumé

Because of the persistent need of drug discovery programs for simple methods to access bioactive C-aryl glycosides, the C-H activation approach has emerged as an efficient and sustainable alternative for classical reactions that limits the number of steps in a synthetic route as much as possible. In the present chapter, we highlight the different established strategies for C(sp2)-H and C(sp3)-H functionalization to access C-aryl glycosides. Two main strategies will be discussed: (a) C-H functionalization of aglycon partners bearing a directing group with different sugars as coupling partners (1-halosugras or glycals); and (b) C(sp2)-H or C(sp3)-H arylation of sugars bearing the directing group.

langue originale	Anglais
titre	Transition-Metal-Catalyzed C-H Functionalization of Heterocycles
Editeur	wiley
Pages	657-681
Nombre de pages	25
Volume	2
ISBN (Electronique)	9781119774150
ISBN (imprimé)	9781119774136
Les DOIs	https://doi.org/10.1002/9781119774167.ch16
état	Publié - 7 mars 2023
Modification externe	Oui

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10.1002/9781119774167.ch16

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title = "C-H activation for the synthesis of C1-(hetero)aryl glycosides",

abstract = "Because of the persistent need of drug discovery programs for simple methods to access bioactive C-aryl glycosides, the C-H activation approach has emerged as an efficient and sustainable alternative for classical reactions that limits the number of steps in a synthetic route as much as possible. In the present chapter, we highlight the different established strategies for C(sp2)-H and C(sp3)-H functionalization to access C-aryl glycosides. Two main strategies will be discussed: (a) C-H functionalization of aglycon partners bearing a directing group with different sugars as coupling partners (1-halosugras or glycals); and (b) C(sp2)-H or C(sp3)-H arylation of sugars bearing the directing group.",

keywords = "C(sp2)-H activation, C(sp3)-H activation, C-aryl glycosides, Directing group strategy, Glycals, Glycosyl chlorides, Glycosylation, Palladium catalysis",

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AU - de Robichon, Morgane

AU - Ghouilem, Juba

AU - Ferry, Angélique

AU - Messaoudi, Samir

PY - 2023/3/7

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N2 - Because of the persistent need of drug discovery programs for simple methods to access bioactive C-aryl glycosides, the C-H activation approach has emerged as an efficient and sustainable alternative for classical reactions that limits the number of steps in a synthetic route as much as possible. In the present chapter, we highlight the different established strategies for C(sp2)-H and C(sp3)-H functionalization to access C-aryl glycosides. Two main strategies will be discussed: (a) C-H functionalization of aglycon partners bearing a directing group with different sugars as coupling partners (1-halosugras or glycals); and (b) C(sp2)-H or C(sp3)-H arylation of sugars bearing the directing group.

AB - Because of the persistent need of drug discovery programs for simple methods to access bioactive C-aryl glycosides, the C-H activation approach has emerged as an efficient and sustainable alternative for classical reactions that limits the number of steps in a synthetic route as much as possible. In the present chapter, we highlight the different established strategies for C(sp2)-H and C(sp3)-H functionalization to access C-aryl glycosides. Two main strategies will be discussed: (a) C-H functionalization of aglycon partners bearing a directing group with different sugars as coupling partners (1-halosugras or glycals); and (b) C(sp2)-H or C(sp3)-H arylation of sugars bearing the directing group.

KW - C(sp2)-H activation

KW - C(sp3)-H activation

KW - C-aryl glycosides

KW - Directing group strategy

KW - Glycals

KW - Glycosyl chlorides

KW - Glycosylation

KW - Palladium catalysis

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BT - Transition-Metal-Catalyzed C-H Functionalization of Heterocycles

PB - wiley

ER -

C-H activation for the synthesis of C1-(hetero)aryl glycosides

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