Factors in Standardizing Automated Cholinesterase Assays

Wilson, Barry W.; Padilla, Stephanie; Henderson, John D.; Brimijoin, S.; Dass, P. D.; Elliot, Glenn; Jaeger, Bruce; Lanz, David; Pearson, Renee; Spies, R

doi:10.1080/009841096161429

Cited by 44 publications

(33 citation statements)

References 15 publications

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“…Therefore, studies performed on isolated or dispersed populations require longer sample storage times under limited storage conditions prior to delivery to the laboratory for analysis. Methods have been developed for ChE measurement in the field but are not as sensitive and accurate as laboratory-based methods (Wilson et al, 1996;Oliveira et al, 2002). The measurement of stored biomarkers can be affected by several conditions including protein denaturation, oxidation, proteolysis, and microbial contamination, which may be dependent on storage conditions such as temperature, freeze/thaw cycles, and storage time.…”

Section: Discussionmentioning

confidence: 99%

“…However, surrogate neurochemical biomarkers in blood have been shown to reflect changes in the brain in response to neurotoxicants and offer an ethical way to evaluate neurotoxicity in human populations (Manzo et al, 1996). For example, cholinesterase (ChE) activity in blood is currently used as a surrogate biomarker to monitor the toxic effects and degree of organophosphate and carbamate exposure in agricultural workers who frequently use pesticides (Wilson et al, 1996(Wilson et al, ,1997. Other studies have linked manganese and styrene exposure in industrial workers with decreased monoamine oxidase (MAO) activity in peripheral blood platelets (Checkoway et al, 1992;Smargiassi et al, 1995;Bergamaschi et al, 1997;Cohen et al, 2002).…”

mentioning

confidence: 99%

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Biochemical Markers of Neurotoxicity in Wildlife and Human Populations: Considerations for Method Development

Stamler

Basu

Chan

2005

Journal of Toxicology and Environmental Health, Part A

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Disruption of neurochemical parameters in blood and brain tissues can be used as early biomarkers of neurotoxicity in human and wildlife epidemiological studies. To investigate the feasibility of biomarker measurements in field samples obtained from remote locations, tissue storage limits were determined with human blood and mink cortex tissue using efficient and cost-effective microplate assays. Results show that isolated blood platelets and plasma can be stored at 4 degrees C for 4 wk before measurement of monoamine oxidase (MAO) and cholinesterase (ChE) activities, while human lymphocytes can be stored at 4 degrees C for up to 2 d before muscarinic acetylcholine (mACh) receptor binding analysis. Blood cells stored frozen resulted in decreased MAO activity and mACh receptor function. These data suggest that mink brain tissue obtained from field samples can be stored at various temperatures without affecting dopamine (D2) and mACh receptor densities; however, MAO and ChE activities were most stable in samples stored in a -20 degrees C domestic freezer or at 4 degrees C. Multiple freeze/thaw cycles alter mACh and D2 receptors and MAO activity in mink cortex samples and should therefore be minimized. In conclusion, these neurochemical biomarkers can efficiently be measured in large human and wildlife neurotoxicity studies, provided proper storage conditions are maintained.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Biochemical Markers of Neurotoxicity in Wildlife and Human Populations: Considerations for Method Development

Stamler

Basu

Chan

2005

Journal of Toxicology and Environmental Health, Part A

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“…These measures have greatly improved the quality of RBC-ChE results, and other laboratories may benefit from adopting similar quality assurance measures. Recent reports indicate that interlaboratory reproducibility for ChE testing is still problematic within the civilian community (27,28 ), although the situation appears to be improving (3 ).…”

Section: Discussionmentioning

confidence: 99%

Intraindividual Stability of Human Erythrocyte Cholinesterase Activity

et al. 2007

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Background: Erythrocyte cholinesterase (RBC-ChE) activities serve as useful and sensitive biomarkers to monitor exposure to cholinesterase-inhibiting substances, such as chemical warfare nerve agents and pesticides. Although the interindividual variation of RBC-ChE is well characterized, the magnitude of intraindividual variation for RBC-ChE remains controversial. An accurate measure of intraindividual variation is critical for establishing the appropriate frequency of RBC-ChE testing. Methods: We retrospectively tracked the intraindividual variation of RBC-ChE activities among 46 male nerve agent workers from a single US Army depot that participated in a medical surveillance program requiring periodic RBC-ChE monitoring. All RBC-ChE analysis was performed by the same medical laboratory technician by the delta pH method. Results: A mean of 38 and a median of 37 RBC-ChE measurements were available for each worker. The mean duration of employment for these workers was 20 years (median, 21 years). The mean CV for RBC-ChE in this set of 46 workers was 3.9%. Linear regression analysis of the data for each worker resulted in a mean slope of 0.0010 delta pH units/h per year. Conclusions: RBC-ChE activities increased in each person by a mean of 0.01 delta pH units/h every 10 years, which is a negligible rate. These findings highlight the

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“…Specific methodology for the cholinesterase assay is as described previously, although modifications to the method have been recommended by the U.S. EPA taking account of concerns about AChE assays raised by Wilson et al (1996). In well-conducted studies, it is possible to detect statistically significant differences on the order of 5-10% in brain, 10% in red blood cells, and 20% in plasma.…”

Section: Acute Cholinesterase Comparative Sensitivity Studiesmentioning

confidence: 99%

Regulatory Aspects of Acute Neurotoxicity Assessment

Allen

2010

Hayes' Handbook of Pesticide Toxicology

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Factors in Standardizing Automated Cholinesterase Assays

Cited by 44 publications

References 15 publications

Biochemical Markers of Neurotoxicity in Wildlife and Human Populations: Considerations for Method Development

Biochemical Markers of Neurotoxicity in Wildlife and Human Populations: Considerations for Method Development

Intraindividual Stability of Human Erythrocyte Cholinesterase Activity

Regulatory Aspects of Acute Neurotoxicity Assessment

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