The Relationship Between the Chemical Structure and Neurotoxicity of Alkyl Organophosphorus Compounds

Davies, D. R.; Holland, P.; Rumens, M. J.

doi:10.1111/j.1476-5381.1960.tb01243.x

Cited by 41 publications

(27 citation statements)

References 10 publications

(7 reference statements)

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“…We have not studied the type of linkage and the site of attachment of the polysaccharide portion [25] to the lipid A component in Ch. violaceurn lipopolysaccharide.…”

Section: Discussionmentioning

confidence: 99%

The Chemical Structure of the Lipid A Component of Lipopolysaccharides from Chromobacterium violaceum NCTC 9694

Hase

Rietschel

1977

Eur J Biochem

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The chemical structure of the lipid A component of lipopolysaccharides from Chromobacterium violaceum NCTC9694 was studied. Sequential treatment of lipopolysaccharide with alkali, acid, sodium borohydride and hydrazine allowed the isolation of a reduced glucosamine disaccharide. According to methylation studies and enzymic analysis with β‐N‐acetylglucosaminidase the D‐glucosamine residues are β(1 → 6) linked. The disaccharide carries two phosphate groups, one being linked glycosidically, the other being linked as an ester to the non‐reducing glucosamine. Application of a different degradation pathway shows that the ester‐bound phosphate group is substituted by a 4‐aminoarabinosyl residue and that the glycosidically linked phosphate group is substituted by a glucosaminyl residue. Neither the amino nor the hydroxyl groups of both these substituents are acylated. This backbone structure is shown in the following formula: The amino groups of the central glucosamine disaccharide are substituted by D‐3‐hydroxy‐dodecanoic acid, the hydroxyl groups by dodecanoic, L‐2‐hydroxydodecanoic and D‐3‐hydroxy‐decanoic acid.

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“…We have not studied the type of linkage and the site of attachment of the polysaccharide portion [25] to the lipid A component in Ch. violaceurn lipopolysaccharide.…”

Section: Discussionmentioning

confidence: 99%

The Chemical Structure of the Lipid A Component of Lipopolysaccharides from Chromobacterium violaceum NCTC 9694

Hase

Rietschel

1977

Eur J Biochem

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“…Up to the present time all the dialkyl phosphorofluoridates (Davies et al, 1960) and all the triaryl phosphates (Hine, Dunlap, Rice, Coursey, Gross & Anderson, 1956) that produce the neurotoxic syndrome are anticholinesterases in vivo, although the converse does not hold.…”

Section: Resultsmentioning

confidence: 89%

“…Adult hens (1 to 2 years of age), pure strain white leghorns, were used in all experiments. All agents were injected into the breast muscle 10 min after an intramuscular injection of 100 mg/kg of pralidoxime (2-hydroxyiminomethyl-N-methylpyridinium) methanesulphonate and 1 mg/kg atropine sulphate (Davies, Holland & Rumens, 1960).…”

Section: Methodsmentioning

confidence: 99%

COMPARISON OF THE FUNCTIONAL EFFECTS OF DYFLOS, TRI‐O‐CRESYL PHOSPHATE AND TRI‐p‐ETHYLPHENYL PHOSPHATE IN CHICKENS

Cavanagh

Davies

Holland

et al. 1961

British Journal of Pharmacology and Chemotherapy

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Tri-p-ethylphenyl phosphate is unique amongst the organophosphorus compounds which produce neurotoxic effects in not being an inhibitor of cholinesterase. The dysfunction it produces is also marked by some unusual features. Thus it produces a characteristic high-stepping gait which develops at varying periods after intramuscular injection but more regularly following oral administration. A careful comparison of the character, onset and development of the effects of diisopropyl phosphorofluoridate (dyflos), tri-o-cresyl phosphate and tri-p-ethylphenyl phosphate has illustrated the differences between the two former substances and tri-p-ethylphenyl phosphate. It has also confirmed a previous suggestion that this substance acts in a different manner from the other two, a suggestion supported by the histological evidence.

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“…The nature of the biochemical lesion effected by certain organophosphate esters to produce ataxia in chickens is not known. Many organofluoro phosphorus compounds that are potent esterase inhibitors will produce this effect at intramuscular doses as low as 0.25 mg/kg (Davies et al, 1960). The tri-o-cresyl phosphate metabolite is a potent esterase inhibitor and will cause ataxia with intraperitoneal doses of 4 to 8 mg/kg, while certain anti-esterase analogues of this cyclic phosphate are effective below 1 mg/kg (Baron, Casida & Eto, unpublished observations).…”

Section: Discussionmentioning

confidence: 99%

“…The critical reaction producing ataxia probably occurs within the nerve to yield a phosphorylated esteratic site on some protein with the release of fluoride or a substituted-phenolate ion. Davies et al (1960) have proposed that the ion released produces the lesion. It appears more probable that the damage to nerve fibre results from changes in metabolism initiated by phosphorylation at a critical esteratic site of an as yet undefined protein.…”

Section: Discussionmentioning

confidence: 99%

NEUROTOXIC SYNDROME PRODUCED IN CHICKENS BY A CYCLIC PHOSPHATE METABOLITE OF TRI‐o‐CRESYL PHOSPHATE—A CLINICAL AND PATHOLOGICAL STUDY

Baron

Bennett

Casida

1962

British Journal of Pharmacology and Chemotherapy

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A clinical and neuropathological comparison was made between chickens poisoned with tri-o-cresyl phosphate and those treated with the major cyclic phosphate metabolite of tri-o-cresyl phosphate. Ataxia was evident with both materials, and the degree of peripheral neuropathy increased with higher doses of these agents. Morphological changes were evident with the onset of symptoms and increased in number as the neurological signs progressed. Demyelination of the spinal cord following administration of the metabolite occurred at doses considerably below those necessary to effect peripheral nerve degeneration. Axon and myelin damage was prominent with both agents. The relationship between these effects and those produced by certain other organophosphates such as dyflos (diisopropyl fluorophosphonate) is discussed.

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The Relationship Between the Chemical Structure and Neurotoxicity of Alkyl Organophosphorus Compounds

Cited by 41 publications

References 10 publications

The Chemical Structure of the Lipid A Component of Lipopolysaccharides from Chromobacterium violaceum NCTC 9694

The Chemical Structure of the Lipid A Component of Lipopolysaccharides from Chromobacterium violaceum NCTC 9694

COMPARISON OF THE FUNCTIONAL EFFECTS OF DYFLOS, TRI‐O‐CRESYL PHOSPHATE AND TRI‐p‐ETHYLPHENYL PHOSPHATE IN CHICKENS

NEUROTOXIC SYNDROME PRODUCED IN CHICKENS BY A CYCLIC PHOSPHATE METABOLITE OF TRI‐o‐CRESYL PHOSPHATE—A CLINICAL AND PATHOLOGICAL STUDY

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