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Dive into the research topics where Stefan Bengtsson is active.

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Featured researches published by Stefan Bengtsson.


European Journal of Pharmacology | 1991

Synthesis and binding properties of the fluorinated substituted benzamide [3H]NCQ 115, a new selective dopamine D2 receptor ligand

Håkan Hall; Thomas Högberg; Christer Halldin; Stefan Bengtsson; Ilse Wedel

[3H]NCQ 115 [R)-5-bromo-2,3-dimethoxy-N-[1-([2,5-3H]-4- fluorobenzyl)-2-pyrrolidinyl)methyl)benzamide) was prepared by acylation of (R)-(2-aminomethyl)-1- ([2,5-3H]-4-fluorobenzyl)pyrrolidine, which was obtained in a stereo-conservative synthesis from (R)-prolinamide. Purification by reversed phase high performance liquid chromatography (HPLC) gave [3H]NCQ 115 with a radiochemical purity of greater than 99% and a specific activity of 0.97 GBq/mumol (36 Ci/mmol). Saturation analyses, association and dissociation kinetics as well as binding competition with several compounds of various classes were performed with [3H]NCQ 115 in rat striatal homogenates. Saturation analyses in vitro showed that [3H]NCQ 115 bound to a single binding site with a Kd = 214 pM and Bmax = 35.4 fmol/mg. The binding of [3H]NCQ 115 was dependent upon sodium ions, since the number of binding sites was altered when sodium ions were excluded from the incubation medium. NCQ 115 inhibited the binding of [3H]raclopride to dopamine D2 receptors with high affinity (Ki = 147 pM), having much lower affinity for other receptors. The affinity of this substituted 1-benzyl-2-pyrrolidinylmethyl benzamide was confined to the (R)-enantiomer, which contrasts with that of the corresponding N-ethyl derivatives such as FLB 457, raclopride, eticlopride, sulpiride and NCQ 298, where the pharmacological activity is found in the (S)-enantiomer. It can be concluded that [3H]NCQ 115 binds to dopamine D2 receptors in the rat striatum with high affinity and high selectivity. [3H]NCQ 115 can also be used for in vivo binding studies of the brain. [18F]NCQ 115 may be a suitable ligand for positron emission tomography (PET) studies of the human brain in vivo.


Journal of Medicinal Chemistry | 1978

Inhibitors of neuronal monoamine uptake. 2. Selective inhibition of 5-hydroxytryptamine uptake by alpha-amino acid esters of phenethyl alcohols.

Ulf Henrik Anders Lindberg; Seth Olof Thorberg; Stefan Bengtsson; Anna L. Renyi; Svante B. Ross; Sven Ove Ögren


Journal of Medicinal Chemistry | 1990

Potential antipsychotic agents 5. Synthesis and antidopaminergic properties of substituted 5,6-dimethoxysalicylamides and related compounds.

Thomas Hoegberg; Stefan Bengtsson; Tomas de Paulis; Lars Johansson; Peter Stroem; H. Hall; Sven Ove Oegren


Archive | 1993

NOVEL AMIDOALKYL- AND IMIDOALKYL-PIPERAZINES.

Stefan Bengtsson; Lennart Florvall; Gerd Hallnemo; David M. Jackson; Svante B. Ross; Bo-Ragnar Tolf; Bengt Ulff; Lian Zhang; Christina Elizabeth Akesson


Journal of Organic Chemistry | 1993

Pivaloyl-directed regioselective syntheses of 2,3,6-trioxygenated benzamides: phenolic metabolites of remoxipride

Stefan Bengtsson; Thomas Hoegberg


Journal of Labelled Compounds and Radiopharmaceuticals | 1985

Synthesis and 3H NMR of 3H‐alaproclate of high specific activity

Stefan Bengtsson; Lars Gawell; Thomas Högberg; Christer Sahlberg


European Journal of Medicinal Chemistry | 1986

Synthesis and neuroleptic activity of substituted benzamides related to metoclopramide

Yatendra Kumar; T. De Paulis; Stefan Bengtsson; H. Hall; M. Sallemark; K. Angeby; S.O. Ögren


Archive | 1995

Novel phenylethyl and phenylpropylamines

Stefan Bengtsson; Sven Hellberg; Nina Mohell; Lian Zhang; Gerd Hallnemo; David M. Jackson; Bengt Ulff


Archive | 1994

Phenylethyl and phenylpropylamines

Stefan Bengtsson; Sven Hellberg; Nina Mohell; Lian Zhang; Gerd Hallnemo; David M. Jackson; Bengt Ulff


Archive | 1999

Fenüületüül- ja fenüülpropüülamiinid, nende valmistamise protsessid ja neid sisaldavad ravimpreparaadid

Stefan Bengtsson; Sven Hellberg; Nina Mohell; Lian Zhang; Gerd Hallnemo; D. M. Jackson; Bengt Ulff

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