Privileged structure based ligands for melanocortin receptors—Substituted benzylic piperazine derivatives

Matthew Joseph Fisher,Ryan T. Backer,Ivan Collado,Óscar de Frutos,Saba Husain,Hansen M. Hsiung,Steve L. Kuklish,Ana I. Mateo,Jeffrey T. Mullaney,Paul L. Ornstein,Cristina Garcia-Paredes,Thomas P. O’Brian,Timothy Ivo Richardson,Jikesh Shah,John M. Zgombick,Karin Briner

Privileged structure based ligands for melanocortin receptors—Substituted benzylic piperazine derivatives

2005

Matthew Joseph Fisher
Ryan T. Backer
Ivan Collado
Óscar de Frutos
Saba Husain
Hansen M. Hsiung
Steve L. Kuklish
Ana I. Mateo
Jeffrey T. Mullaney
Paul L. Ornstein
Cristina Garcia-Paredes
Thomas P. O’Brian
Timothy Ivo Richardson
Jikesh Shah
John M. Zgombick
Karin Briner

Replacement of the aryl piperazine moiety in compound 1 with a variety of substituted benzylic piperazines (6) yields compounds that afford melanocortin receptor 4 (MCR4) activity. Analogs with ortho substitution on the aromatic ring afforded the highest affinity. Resolution of the stereocenter of the benzylic piperazine based privileged structure revealed that the R-enantiomer was more active.

Keywords:

Stereocenter
Melanocortin
Chemical synthesis
Organic chemistry
Aryl
Melanocortin receptor
Moiety
Piperazine
Biochemistry
Structure–activity relationship
Stereochemistry
Chemistry
tertiary amine

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