Early Developmental Destruction of Terminals in the Striatal Target Induces Apoptosis in Dopamine Neurons of the Substantia Nigra

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Volume 17, Number 6, Issue of March 15, 1997 pp. 2030-2039
Copyright ©1997 Society for Neuroscience

Early Developmental Destruction of Terminals in the Striatal Target Induces Apoptosis in Dopamine Neurons of the Substantia Nigra

Received Dec. 19, 1996; accepted Dec. 31, 1996.
Maria J. Marti, Christopher J. James, Tinmarlar F. Oo, William J. Kelly, and Robert E. Burke
Department of Neurology, College of Physicians and Surgeons, Columbia University, New York, New York 10032
Many developing neural systems with peripheral projections depend on their target for trophic support during a critical periodof natural cell death. Much less is known about central systems.That dopaminergic neurons of the substantia nigra may depend ontheir target, the striatum, during development is suggested bythe presence of a natural apoptotic cell death event in theseneurons that can be augmented by an early developmental axon-sparingstriatal injury. To further assess the target dependence of theseneurons, we have used the selective neurotoxin 6-hydroxydopamineto lesion their terminals within the striatum during development,while sparing intrinsic striatal target neurons. This lesion resultsin an induction of apoptotic cell death in phenotypically defineddopaminergic neurons that appears on the third postlesion dayand persists until the tenth. This inducibility of cell deathis dependent on developmental age: it is most marked before postnatalday (PND) 14. As late as PND42, inducibility is still detectablebut much less so. In addition, at day 42 the morphology of celldeath changes and becomes nonapoptotic in some cells. We concludethat terminal injury during a critical period of postnatal development,like axon-sparing target injury, induces augmented apoptotic deathin mesencephalic dopaminergic neurons. These results suggest thatthese neurons have a period of target dependence. Regulation ofthis dependence is likely to influence the mature adult numberof dopaminergic neurons.

Key words: apoptosis; programmed cell death; 6-hydroxydopamine; substantia nigra; dopamine; Parkinson's disease

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