Silent cholinesterase gene: variations in the properties of serum enzyme in apparent homozygotes

Rubinstein, Herbert M.; Dietz, Albert A.; Hodges, LaVerne K.; Lubrano, Tina; Czebotar, Virginia

doi:10.1172/jci106257

Cited by 52 publications

(17 citation statements)

References 23 publications

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“…It can be assumed that the structural modifi cation or disorientation of the cholinester ase molecules in these individuals restricts the binding of all 4 monoclonals to their antigenic sites. These findings of weaker than normal affinity of the antibodies sup port the observations of Rubinstein et al [1970] and suggest that this group may be type II, which is controlled by the Ej gene, and probably represent the homozygotes EjEV Our third group of patients (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22) show definite but low levels of immunoreactive protein -in fact, intermediate between our first and second groups of patients. The enzymic activity, by either substrate, in this third group is less than that found in our secound group.…”

Section: Discussionsupporting

confidence: 82%

“…it has been recognised for many years that the so-called 'silent gene' represents a heterogeneous complex [Goedde and Altland, 1968;Rubinstein et al, 1970], At present, 3 separate genes, Ej, E\ and Ei, have been described [Scott, 1973;Scott and Wright, 1976], The relative affinities for different substrates [Altland and Goedde, 1970], electrophoresis [Rubin stein et al, 1970] as well as immunodiffu sion [Goedde and Atland, 1968;Rubin stein et al, 1975] have been used to differ entiate the different variants. Our current results using an ELISA technique with 4 different monoclonal and the sheep conju gated polyclonal antibodies are in close agreement with those obtained by rocket electrophoresis (table 1) using the 3 un conjugated polyclonals.…”

Section: Discussionmentioning

confidence: 99%

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Heterogeneity of the Silent Gene for Plasma Cholinesterase

Whíttaker¹,

Jones

Braven³

1990

Hum Hered

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Rocket immuno-electrophoresis and enzyme-linked immunosorbent assays were used to estimate the amount of cholinesterase present in 29 apparent silent homozygotes. 26 of these samples were segregated into four groups representing zero, very low, low and high levels of immunoreactive protein. These groups may represent the genotypes E^s₁, E^s₁, E^s₁, E^t₁, Ε^t₁, E^t₁ and a new genotype E^x₁, E^x₁, respectively. The possible genotypes of the remaining 3 individuals are discussed.

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Section: Discussionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 99%

Heterogeneity of the Silent Gene for Plasma Cholinesterase

Whíttaker¹,

Jones

Braven³

1990

Hum Hered

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“…Rubinstein et al [95] proposed the idea that there are several silent genes to explain their findings of accurate enzymatic evaluations on 25 supposed silent homozygotes. Continuing their work on Alaskan Eskimos, Scott & Wright have identified these allelic genes and labelled them S (silent), T (trace) and R (residual) [96,97].…”

Section: Inherited Variationsmentioning

confidence: 99%

Cholinesterase Its significance in anaesthetic practice

1997

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SummaryPlasma cholinesterase is an enzyme which has importance to the anaesthetist primarily for its rôle in the metabolism of suxamethonium, although other anaesthetic related drugs that this enzyme metabolises are also increasingly important. In this article we review current thoughts on the function, profile and chemistry of plasma cholinesterase. Causes of variations in the activity of the enzyme are described and the basis of genetic variations is explained.

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“…At this point, one has to remember that ( I ) this may not always be true: e.g.. 4 in dividuals of Ch1 / Ch1 , have relatively low enzyme activity, and (2) individuals possessing Ch* could reveal biochemically different types of phenotypic expression depending upon the techniques employed (since various workers demonstrated the complex nature of the 'silent' cholinesterase variants [3,4,14]. This can only be better understood when investigations are carried Copies of the complete pedigrees may be obtained from the author.…”

Section: Significance O F Family Sstudiesmentioning

confidence: 99%

Suxamethonium Sensitivity and Segregation of Human Serum Cholinesterase Variants at Locus(Ch<sub>1</sub>) Among Twelve British Families

Pk¹

1975

Hum Hered

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Sera from 39 individuals with suxamethonium apnoea have been examined. The likelihood of the Ch₁^U Ch₁^D heterozygotes developing suxamethonium apnoea has been calculated. The results indicate that 1 in 4,000 of normal homozygotes and 1 in 400 of Ch₁^U Ch₁^D heterozygotes develop suxamethonium apnoea. The period of suxamethonium apnoea in these individuals has been found shorter than that usually seen in Ch₁^D Ch₁^D homozygotes. An approximate estimate of the frequency of the Ch₁^F and Ch₁^S genes has also been calculated. Twelve British families of these suxamethonium apnoea propositi have been examined. The inheritance pattern in all these families was found to be of the Mendelian type. Three of these families have been found to be segregating for the rarer Ch₁^F gene and two for Ch₁^S gene, respectively. This present study provides an additional piece of support to the hypothesis that the Ch₁^U and Ch₁^D are alleies determining the synthesis of usual and atypical cholinesterase together with the likelihood of Chy Chy heterozygotes having occasional suxamethonium apnoea. In addition, the present report indicates that there may be cholinesterase variants besides dibucaine and fluoride-resistant, ‘silent’ and C₅.

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Silent cholinesterase gene: variations in the properties of serum enzyme in apparent homozygotes

Abstract: A B S T R A C

Cited by 52 publications

References 23 publications

Heterogeneity of the Silent Gene for Plasma Cholinesterase

Heterogeneity of the Silent Gene for Plasma Cholinesterase

Cholinesterase Its significance in anaesthetic practice

Suxamethonium Sensitivity and Segregation of Human Serum Cholinesterase Variants at Locus(Ch<sub>1</sub>) Among Twelve British Families

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