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Ortiz, G. G., M. E. Crespo-Lopez, et al. (2001). "Protective
role of melatonin against MPTP-induced mouse brain cell DNA fragmentation and
apoptosis in vivo." Neuroendocrinol Lett 22(2): 101-8.
OBJECTIVES: 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) is a neurotoxin
that induces a Parkinsonian-type syndrome in animals which is similar to
Parkinson's disease in humans. MPTP toxicity partially depends on the production
of free radicals which in turn play a key role in the apoptotic death of
neurons. In the present study melatonin, a potent free radical scavenger with
antiapoptotic properties, was given to determine whether it would reduce
oxidative stress in mice treated with MPTP. MATERIALS AND METHODS: Male mice
were given MPTP with or without melatonin and the brain was studied either 6h,
24h, 7 days or 15 days after the last MPTP injection. RESULTS: The results show
that melatonin counteracted in vivo MPTP-induced apoptosis in midbrain neurons
at 6 and 24 h after MPTP treatment, and partially prevented apoptosis at 7 and
15 days after MPTP administration. MPTP treatment also produced time-dependent
cell damage, whereas melatonin reduced the percentage of damaged cells at all
time points, the effect being most evident at 15 days after treatment. Moreover,
melatonin counteracted MPTP-dependent DNA fragmentation in the midbrain and
striatum at 7 and 15 days after drug administration. CONCLUSION: These results
support a role for melatonin in protecting neurons against MPTP toxicity in
vivo, and suggest that its antiapoptotic action is one of the mechanisms by
which melatonin protects neuronal cells from neurotoxic insults.
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