Summary
The cause for the rather selective degeneration of the nigrostriatal dopaminergic (DA) neurons in Parkinson’s disease (PD) is still enigmatic. The major current hypothesis suggests that nigral neuronal death in PD is due to excessive oxidant stress generated by auto- and enzymatic oxidation of DA, formation of neuromelanin and presence of high concentrations of iron. Such cell death is generally regarded as a passive, necrotic process, mainly resulting from membrane lipid peroxidation, leading to its dysfunction and rupture and then to neuronal disintegration.
We suggest a novel approach, that views neuronal degeneration in PD as an active process that occurs mainly the nuclear level. Our concept is based on the following observations: (1) Nigral histopathology in PD is characterized by a slow, protracted degeneration of individual neurons. We propose that it may be due to apoptosis [programmed cell-death (PCD), an active, genetically-controlled, intrinsic program of cell “suicide”] rather than to necrotic cell death. (2) DA exerts antitumor effect on melanoma and neuroblastoma cells. (3) Many anticancer drugs, trigger PCD by causing DNA damage. (4) DA has been shown to be genotoxic. (5) We recently first showed that DA, the endogenous neurotransmitter in the nigra, can trigger apoptosis in cultured, postmitotic sympathetic neurons. (6) We have also shown that PC-12 cells, transfected with the bcl-2 gene (a proto-oncogene that inhibits PCD) are relatively resistant to DA-apoptotic effect.
Degeneration of nigrostriatal neurons in PD may therefore be linked to dysregulation of the control mechanisms that normally restrain the PCD-triggering-potential of their own neurotransmitter.
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References
Barinaga M (1993) Death gives birth to the nervous system. But how? Science 259:762–763
Boobis AR, Fawthrop DJ, Davies DS (1989) Mechanisms of cell death. Trends Pharmacol Sci 10: 275–280
Bursch W, Oberhammer F, Sculte-Hermann R (1992) Cell death by apoptosis and its protective role against disease. Trends Pharmacol Sci 13: 245–251
Cohen JJ (1993) Apoptosis. Immunol Today 14: 126–130
Eastman A (1990) Activation of programmed cell death by anticancer agents: cisplatin as a model system. Cancer Cells 2: 275–280
Fahn S, Cohen G (1992) The oxidant stress hypothesis in Parkinson’s disease: evidence supporting it. Ann Neurol 32: 804–812
Garcia I, Martinou I, Tsushimoto Y, Martinou JC (1992) Prevention of programmed cell death of sympathetic neurons by the bcl-2 proto-oncogene. Science 258: 302–304
Graham DJ, Tiffany SM, Bell WR, Gutknecht WF (1978) Autoxidation versus covalent binding of quinones as the mechanism of toxicity of dopamine, 6-hydroxydopamine, and related compounds toward cl300 neuroblastoma cells in vitro. Mol Pharmacol 14:644–653
Hirsch EC (1992) Why are nigral catecholaminergic neurons more vulnerable than other cells in Parkinson’s disease? Ann Neurol 32: S88–S93
Jenner P, Dexter DT, Sian J (1992) Oxidative stress as a cause of nigral cell death in Parkinson’s disease and incidental Lewy body disease. Ann Neurol 32: S82–S87
Lin LFH, Doherty DH, Lile JD (1993) GDNF: a glial cell line-derived neurotrophic factor for midbrain dopaminergic neurons. Science 260: 1131–1132
Martin DP, Schmidt RE, Distefano PS, Johnson EN (1988) Inhibitors of protein synthesis and RNA synthesis prevent neuronal death caused by NGF deprivation. J Cell Biol 106: 829–843
Michel PP, Hefti F (1990) Toxicity of 6-hydroxydopamine and dopamine for dopaminergic neurons in culture. J Neurosci Res 26: 428–435
Moldeus P, Nordenskjold M, Bolcsfoldi G (1983) Genetic toxicity of dopamine. Mut Res 124: 9–23.
Olanow CW (1993) A radical hypothesis for neurodegeneration. Trends Neurosci 16:439–444
Orrenius S, Burkitt M, Kass GEN (1992) Calcium ions and oxidative cell injury. Ann Neurol 32: S33–S42
Robbins Jh, Otsuka F, Nee LE (1985) Parkinson’s disease and Alzheimer’s disease: hypersensitivity to x-rays in cultured cell lines. J Neurol Neurosurg Psychiatry 48: 916–923
Schraufstatter IU, Hyslop PA, Hinshaw DB (1986) Hydrogen peroxide-induced injury of cells and its prevention by inhibitors of poly (ADP-ribose) polymerase. Proc Natl Acad Sci 83: 4908–4912
Scudiero DA, Tarone RE, Robbins JH (1982) Parkinson’s disease and Alzheimer’s disease fibroblasts are hypersensitive to killing by MNNG. Clin Res 30: 857(A)
Tooyama I, Kawamata T, Walker D, Mcgeer PL (1993) Loss of basic fibroblast growth factor in substantia nigra neurons in Parkinson’s disease. Neurology 43: 372–376
Ueda N, Shah SV (1992) Endonuclease-induced DNA damage and cell death in oxidant injury to renal tubular epithelial cells. J Clin Invest 90: 2593–2597
Wick MM (1978) Dopamine: a novel antitumor agent active against B-16 melanoma in vivo. J Invest Dermatol 71: 163–164
Wick MM (1980) Levodopa and dopamine analogs as DNA polymerase inhibitors and antitumor agents in humsn melanoma. Cancer Res 40: 1414–1418
Wick MM (1989) Levodopa/dopamine analogs as inhibitors of DNA synthesis in human melanoma cells. J Invest Dermatol 92: 329S–331S
Wyllie AH (1980) Glucocorticocoid-induced thymocyte apoptosis is associated with endogenous endonuclease activation. Nature 284: 555–557
Ziv I, Melamed E, Nardi N, Luria D, Achiron A, Offen D, Barzilai A (1994) Dopamine induces apoptosis-like cell death in cultured sympathetic neurons — a possible novel pathogenetic mechanism in Parkinson’s disease. Neurosci Lett 170: 136–140
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Ziv, I., Barzilai, A., Offen, D., Nardi, N., Melamed, E. (1997). Nigrostriatal neuronal death in Parkinson’s disease — a passive or an active genetically-controlled process?. In: Mizuno, Y., Youdim, M.B.H., Calne, D.B., Horowski, R., Poewe, W., Riederer, P. (eds) Advances in Research on Neurodegeneration. Springer, Vienna. https://doi.org/10.1007/978-3-7091-6844-8_7
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DOI: https://doi.org/10.1007/978-3-7091-6844-8_7
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