Sally Pyle scite author profile

Two commonly employed solvents, n-hexane and carbon disulfide (CS2), although chemically dissimilar, result in identical neurofilament-filled swellings of the distal axon in both the central and peripheral nervous systems. Whereas CS2 is itself a neurotoxicant, hexane requires metabolism to the gamma-diketone, 2,5-hexanedione (HD). Both HD and CS2 react with protein amino functions to yield initial adducts (pyrrolyl or dithiocarbamate derivatives, respectively), which then undergo oxidation or decomposition to an electrophile (oxidized pyrrole ring or isothiocyanate), that then reacts with protein nucleophiles to result in protein cross-linking. It is postulated that progressive cross-linking of the stable neurofilament during its anterograde transport in the longest axons ultimately results in the accumulation of neurofilaments within axonal swellings. Reaction with additional targets appears to be responsible for the degeneration of the axon distal to the swellings.

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Adrenergic receptor modulation of hippocampal CA3 network activity

Jurgens¹,

Boese²,

King³

et al. 2005

Epilepsy Research

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The Role of Pyrrole Formation in the Alteration of Neurofilament Transport Induced during Exposure to 2,5-Hexanedione

Pyle

Amarnath

Graham

et al. 1992

Journal of Neuropathology and Experimental Neurology

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Cytoskeletal Elements in Neurotoxicity*

Pyle

Reuhl

2010

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Sally Pyle

Pathogenetic Studies of Hexane and Carbon Disulfide Neurotoxicity

Adrenergic receptor modulation of hippocampal CA3 network activity

The Role of Pyrrole Formation in the Alteration of Neurofilament Transport Induced during Exposure to 2,5-Hexanedione

Cytoskeletal Elements in Neurotoxicity*

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