par Pearlman, Starr;Levivier, Marc 
;Collier, Timothy;Sladek Jr., John;Gash, Don Marshall
Référence Experimental Brain Research, 84, 2, page (303-310)
Publication Publié, 1991-04
;Collier, Timothy;Sladek Jr., John;Gash, Don MarshallRéférence Experimental Brain Research, 84, 2, page (303-310)
Publication Publié, 1991-04
Article révisé par les pairs
| Résumé : | Quinolinic acid (QA) and related excitotoxins produce a pattern of neuronal loss and neurochemical changes in the rat striatum similar to that of patients suffering from Huntington's disease, suggesting neurotoxicity is important in the etiology of that disease. Thus, strategies for limiting excitotoxin-induced striatal damage, like that caused by QA, may be of great benefit to these individuals. Accordingly, we tested the ability of both neural and non-neural tissue implants to protect the rat striatum against a subsequent QA challenge. Our results demonstrated that recipients of fetal striatal grafts were significantly less affected by striatal injections of QA than non-grafted animals. In contrast to the latter, fetal striatal tissue recipients did not exhibit apomorphine-induced rotation behavior and showed a sparing of cholinergic and enkephalinergic systems normally lost following QA injections. Animals grafted with adult rat sciatic nerve, adrenal medulla or adipose tissue all showed a less dramatic behavioral protection and sparing of cholinergic and enkephalinergic systems. These results suggest that fetal striatal tissue exerts an optimal, and perhaps specific protective influence on the host brain. © 1991 Springer-Verlag. |
