Zobrazeno 1 - 10
of 19
pro vyhledávání: '"Kornfeld Edmund C"'
Autor:
Ray W. Fuller, Norman R. Mason, Robert Daniel Titus, Hynes, Hahn Ra, Kornfeld Edmund C, E. B. Smalstig, Foreman Mark Mortensen, David T.W. Wong, Noel D. Jones, James A. Clemens
Publikováno v:
Journal of Medicinal Chemistry. 26:1112-1116
The title compound (+/-)-5 (R = Pro) (LY141865) has been resolved into a (-) isomer and a (+) isomer as the D- and L-tartrate salts, respectively. Biological studies have shown that dopamine agonist activity is a property of only the (-) isomer. Crys
Publikováno v:
Life Sciences. 38:317-322
LY163502, a partial ergoline and a trans-levorotatory enantiomer, does not stimulate adenylate cyclase in striatal membranes but inhibits 50% binding of 3H-apomorphine, 3H-pergolide and 3H-spiperone at 10, 13 and 151 nM (IC50), respectively. The race
Autor:
Bach Nicholas J, Kornfeld Edmund C
Publikováno v:
Tetrahedron Letters. 15:3225-3228
Publikováno v:
Journal of Medicinal Chemistry. 17:312-314
Autor:
Kornfeld Edmund C, Robert C. A. Frederickson, E. Barry Smalstig, Bach Nicholas J, James A. Clemens
Publikováno v:
Journal of Medicinal Chemistry. 23:492-494
Autor:
Bach Nicholas J, E. Barry Smalstig, James A. Clemens, Kornfeld Edmund C, Ray W. Fuller, Harold D. Snoddy
Publikováno v:
Life sciences. 24(4)
(8β)-8-[(Methylthio)methyl]-6-propylergoline induced contralateral turning in rats with nigrostriatal lesions, lowered serum prolactin in reserpinized rats, and caused stereotyped hyperactivity. In addition to these functional effects typical of dop
Publikováno v:
Journal of medicinal chemistry. 20(8)
9,10-Didehydro-6-methyl-8beta-arylergolines 2, in which the carboxyl group of lysergic acid and isolysergic acid is replaced by various aryl groups, were prepared in two steps by alkylation of aromatic substrates with the tetracyclic allylic alcohol
Publikováno v:
Chemischer Informationsdienst. 8
9,10-Didehydro-6-methyl-8beta-arylergolines 2, in which the carboxyl group of lysergic acid and isolysergic acid is replaced by various aryl groups, were prepared in two steps by alkylation of aromatic substrates with the tetracyclic allylic alcohol
Autor:
Martin D. Hynes, E. B. Smalstig, Norman R. Mason, R. A. Hahn, R. W. Fuller, David T. Wong, James A. Clemens, Noel D. Jones, Foreman Mark Mortensen, Robert Daniel Titus, Kornfeld Edmund C
Publikováno v:
Chemischer Informationsdienst. 14
Publikováno v:
Endocrinology. 94(4)
Peptide-containing ergot alkaloids and synthetic ergoline derivatives were administered to reserpine-treated male rats in order to evaluate their prolactin-inhibiting properties. Each compound was administered ip at a standard 50 ¼g/kg dose. The 9,1