A group of toxic chemicals results in the intra-axonal accumulation of neurofilaments. Studies of the pathogenesis of these neurofilbrillary aggregates have shown that the accumulations result from an impaired transport of the neurofilaments down the axon in the slow component (SCa) of axonal transport. A major issue is whether the impairment of transport represents an alteration of the transport mechanism, or whether there is an inherent alteration of the neurofilament. Evidence from a series of Gamma-diketones suggests that the neurofilament accumulations are the result of an alteration of the neurofilament, specifically covalent crosslinking of the neurofilament. It is hypothesized that in the Gamma-diketone series the neurofibrillary pathology results from cyclization of the Gamma-diketone with lysyl residues to form pyrroles, autoxidation of the unstable pyrrolyl residues to form reactive intermediates, and subsequent attack of the reactive pyrrole species by an adjacent residue to form a covalent bridge. This covalent crosslinking of neurofilament proteins is proposed to be a cumulative process that ultimately results in neurofilamentous tangles which preclude their normal transport down the axon and lead to their accumulation. These findings are pertinent to several human disorders in which neurofibrillary changes are secondary to an apparent alteration of the neurofilament. The paired helical filaments of Alzheimer's disease contain some neurofilament determinants as well as some specific determinants. Neurofilamentous aggregates also occur in ALS, giant axonal neuropathy, Lewy bodies, and Pick bodies. The relevance of the Gamma-disktone model to the human disorders is accentuated by the facts that paired helical filaments of Alzheimer's disease appear to be high molecular weight neurofilament polymers, and that there is a high molecular weight component of purified neurofilament preparations in normal adult animals. The basis of this proposal is to examine the mechanism of neurofilamentous aggregation under the premise that the neurofilament bundles in these disorders are the result of an inherent alteration of the neurofilament itself. The following approach is proposed: (1) to identify and quantify pyrrole formation following exposure to Gamma-diketones, (2) to identify the chemical structure of the pyrrole-mediated crossbridges, (3) to document the crosslinking of neurofilament proteins and other long-lived proteins in vivo and correlate this process with the intra-axonal neurofilament accumulation, (4) to isolate and characterize the high molecular weight species in normal neurofilament preparations, (5) to identify at the ultrastructural level which subunits of the neurofilament are involved in the toxic neurofilament tangles by immunogold methodology, and (6) to apply these immunogold techniques in the study of human disease in which neurofibrillary pathology is a major component.

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Clinical Investigator Award (CIA) (K08)
Project #
1K08NS001208-01
Application #
3084004
Study Section
Neurological Disorders Program Project Review A Committee (NSPA)
Project Start
1987-07-01
Project End
1992-06-30
Budget Start
1987-07-01
Budget End
1988-06-30
Support Year
1
Fiscal Year
1987
Total Cost
Indirect Cost
Name
Duke University
Department
Type
Schools of Medicine
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705
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Pyle, S J; Amarnath, V; Graham, D G et al. (1993) Decreased levels of the high molecular weight subunit of neurofilaments and accelerated neurofilament transport during the recovery phase of 2,5-hexanedione exposure. Cell Motil Cytoskeleton 26:133-43
Denlinger, R H; Anthony, D C; Amarnath, V et al. (1992) Comparison of location, severity, and dose response of proximal axonal lesions induced by 3,3'-iminodipropionitrile and deuterium substituted analogs. J Neuropathol Exp Neurol 51:569-76
Valentine, W M; Amarnath, V; Graham, D G et al. (1992) Covalent cross-linking of proteins by carbon disulfide. Chem Res Toxicol 5:254-62
Pyle, S J; Amarnath, V; Graham, D G et al. (1992) The role of pyrrole formation in the alteration of neurofilament transport induced during exposure to 2,5-hexanedione. J Neuropathol Exp Neurol 51:451-8
Amarnath, V; Anthony, D C; Valentine, W M et al. (1991) The molecular mechanism of the carbon disulfide mediated cross-linking of proteins. Chem Res Toxicol 4:148-50
Genter St Clair, M B; Amarnath, V; Moody, M A et al. (1988) Pyrrole oxidation and protein cross-linking as necessary steps in the development of gamma-diketone neuropathy. Chem Res Toxicol 1:179-85