A new link between pesticides and Parkinson's disease

PD is characterized clinically by rigidity, tremor and bradykinesia, which result from the progressive death of dopaminergic neurons in the substantia nigra. The defining feature of idiopathic PD is the accumulation of Lewy bodies in the substantia nigra and other brainstem nuclei². Classical Lewy bodies are small (5−25 m) spherical inclusions, consisting of a dense granular core surrounded by a halo of radiating filaments, and it is suspected that these deposits are involved in triggering the death of dopaminergic neurons.

The etiology of PD is diverse and complex. Some cases can be attributed to genetic factors, and several mutations have recently been described that lead to familial PD³. Two of these mutations, in the genes encoding parkin and ubiquitin carboxy-terminal hydrolase-L1 (UCH-L1), lead to diseases that are somewhat distinct, both clinically and pathologically, from idiopathic cases, and how they relate to classical PD remains unclear. The third class of mutations, in contrast, has been more informative. These affect the gene for -synuclein, a synaptic protein of unknown function that subsequently proved to be a major component of the filaments associated with Lewy bodies. In addition, -synuclein is the major constituent of several other disease-specific lesions, including cortical Lewy bodies, swollen neurites (known as Lewy neurites) and glial cell inclusions⁴. The term 'synucleinopathy' has been coined to designate this broad class of neurodegenerative disorders, and the genetic link between -synuclein and familial PD suggests that Lewy body formation may be an important trigger in the disease process. Further evidence for this idea comes from experiments in which -synuclein is overexpressed in flies or mice. Mutant flies carrying the human gene undergo adult-onset loss of dopaminergic neurons, accompanied by formation of filamentous -synuclein inclusions as well as locomotor dysfunction⁵. In mice, overexpression of human -synuclein results in impaired motor function, neuronal degeneration and perikaryal, neuritic and (unexpectedly) nuclear -synuclein aggregates. These deposits, however, are not filamentous^{6, 7}, suggesting that the mechanisms leading to polymerization of -synuclein fibrils are more complex than mere protein accumulation.

The authors show that chronic i.v. administration of rotenone in rats produces effects that closely resemble human PD. The treated rats showed several cardinal behavioral features of the disease, including bradykinesia, postural instability, unsteady gait and some evidence of tremor. Histological examination indicated that rotenone treatment leads to progressive degeneration of the nigrostriatal dopaminergic system. Importantly, the surviving nigral neurons developed intracytoplasmic -synuclein-rich inclusions that appeared similar to Lewy bodies by light and electron microscopy. Although some of these inclusions resembled 'pale bodies', presumptive precursors of Lewy bodies, others showed the characteristic features of authentic human Lewy bodies, including a distinct core surrounded by a fibrillar halo.

Unlike MPP+, which targets dopaminergic neurons because of its affinity for the dopamine transporter, rotenone can cross cell membranes and is therefore likely to affect all cells. Consistent with this, the authors confirmed that their treatment protocol led to complex I inhibition throughout the brain. However, they observed PD-like symptoms even at low concentrations, for which the degree of complex I inhibition is insufficient to significantly impair oxidative phosphorylation in the brain. This argues against ATP depletion as a mechanism for the loss of dopaminergic neurons. An alternative possibility, consistent with earlier suggestions¹³, is that free radicals, such as superoxide anions, which are known to result from mitochondrial inhibition, may be responsible for the damage. Oxidative damage has long been implicated in neurodegenerative diseases, and it may be of particular importance in synucleinopathies, given the extensive and widespread oxidative modification of -synuclein in the deposits characteristic of these diseases¹⁴. Moreover, oxidative damage is at least partly responsible for the toxic effects of MPTP.

Figure 1 summarizes some of the complex mechanisms that may be involved in PD and related diseases. The importance of -synuclein Lewy body pathology is not fully understood, but it is likely that the accumulation of -synuclein filaments, possibly as a consequence of oxidative damage, contributes to impairment of cellular function, eventually resulting in cell death. Unraveling the interplay of genetic and environmental factors will be crucial in dictating the future direction of research and in guiding the development of novel therapies for synucleinopathies. The results of Betarbet et al.¹ should provide a valuable new model for assaying the efficacy of such treatments.

Figure 1. Possible mechanisms of selective cell death in Parkinson's and related diseases. Mutations in -synuclein may enhance its propensity to polymerize, resulting in the formation of inclusions that may comprise neuronal viability. Unidentified genetic mutations or polymorphisms may contribute directly to cell death or modulate the propensity of -synuclein to form inclusions, and they may also affect vulnerability to oxidative damage. Known mutations in genes such as UCH-L1 and parkin lead to the death of dopaminergic neurons, but it is unclear whether -synuclein pathology is involved. Environmental factors may also induce cell death, either directly or by initiating pathological cascades involving oxidative damage and -synuclein aggregation. Full Figure and legend (16K)

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