par Malaisse, Willy 
;Doherty, Margaret;Malaisse Lagae, Francine ;Ladrière, Laurence
Référence International Journal of Molecular Medicine, 7, 3, page (311-315)
Publication Publié, 2001-03
;Doherty, Margaret;Malaisse Lagae, Francine ;Ladrière, Laurence Référence International Journal of Molecular Medicine, 7, 3, page (311-315)
Publication Publié, 2001-03
Article révisé par les pairs
| Résumé : | The uptake of [2-(14)C]alloxan by the pancreatic gland was investigated in control and streptozotocin-induced diabetic (STZ) rats, using both in vitro and in vivo techniques. Whether after 10 to 60 min incubation of pieces of pancreas in the presence of [2-(14)C]alloxan or 60 min to 24 h after intravenous injection of [2-(14)C]alloxan to control and insulin-treated STZ rats, the radioactive content of the pancreas (dpm/mg wet weight) only represented, in the STZ rats, about two thirds of the reference value found in control animals. These findings indicate that insulin-producing islet B-cells participate to a sizeable extent to the overall uptake of [2-(14)C]- alloxan by the whole pancreatic gland, despite the fact that they account for no more than about one percent of the total pancreas mass. Hence, it should be possible to preferentially label the endocrine moiety of the pancreas, in the perspective of its imaging and quantification by a non-invasive procedure, by use of a suitable radiolabelled molecule selectively taken up by islet, as distinct from acinar, pancreatic cells. |
