Distribution of N-methyl-14C-labeled selegiline in the rat

•Whole body autoradiography of 14C-methyl-selegiline was studied in rats.•Blood, CSF and tissue distribution of selegiline was measured by HPLC.•Data verified both BBB and blood–testis barrier's penetration of the compound.•Binding of selegiline to the MAO enzyme both in brain and testis is sug...

Full description

Saved in:
Bibliographic Details
Published in:Journal of pharmaceutical and biomedical analysis 2015-07, Vol.111, p.147-152
Main Authors: Tekes, Kornélia, Pöstényi, Zita, Faigl, Erzsébet B., Magyar, Kálmán, Polyák, András, Trencsényi, György, Balogh, Lajos, Kalász, Huba
Format: Article
Language:English
Subjects:
HPLC
Radiolabeled ligand
Rat
Selegiline
Whole body autoradiography
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:•Whole body autoradiography of 14C-methyl-selegiline was studied in rats.•Blood, CSF and tissue distribution of selegiline was measured by HPLC.•Data verified both BBB and blood–testis barrier's penetration of the compound.•Binding of selegiline to the MAO enzyme both in brain and testis is suggested. Tissue distribution of selegiline including N-methyl-14C-selegiline was studied with three different techniques. Whole body autoradiography of labeled selegiline in rats completed the former results obtained in mice. Counting radioactivity by liquid scintillation method in various body compartments gave an in-depth numerical estimation of distribution, while RP-HPLC determination of selegiline determined the fate of intact, non-metabolized parent compound. Whole body autoradiography following 15 and 60min of intraperitoneal application of N-methyl-14C-selegiline verified definite and time-dependent blood–brain penetration of selegiline. Quantitative determination of tissue concentrations by liquid scintillation and RP-HPLC methods following 5, 15, 60 and 180min of intraperitoneal administration of selegiline unanimously verified both blood–brain and blood–testis penetration of the compound through the barrier.
ISSN:0731-7085
1873-264X
DOI:10.1016/j.jpba.2015.03.022