Your search keyword '"Oakeshott, JG"' showing total 26 results

1. Isomer-specific comparisons of the hydrolysis of synthetic pyrethroids and their fluorogenic analogues by esterases from the cotton bollworm Helicoverpa armigera.

Author

Yuan G, Li Y, Farnsworth CA, Coppin CW, Devonshire AL, Scott C, Russell RJ, Wu Y, and Oakeshott JG

Subjects

Animals, Cell Line, Esterases genetics, Hydrolysis, Insecticides chemistry, Isomerism, Larva drug effects, Larva enzymology, Moths enzymology, Pyrethrins chemistry, Esterases metabolism, Insecticides pharmacology, Moths drug effects, Pyrethrins pharmacology

Abstract

The low aqueous solubility and chiral complexity of synthetic pyrethroids, together with large differences between isomers in their insecticidal potency, have hindered the development of meaningful assays of their metabolism and metabolic resistance to them. To overcome these problems, Shan and Hammock (2001) [7] therefore developed fluorogenic and more water-soluble analogues of all the individual isomers of the commonly used Type 2 pyrethroids, cypermethrin and fenvalerate. The analogues have now been used in several studies of esterase-based metabolism and metabolic resistance. Here we test the validity of these analogues by quantitatively comparing their hydrolysis by a battery of 22 heterologously expressed insect esterases with the hydrolysis of the corresponding pyrethroid isomers by these esterases in an HPLC assay recently developed by Teese et al. (2013) [14]. We find a strong, albeit not complete, correlation (r = 0.7) between rates for the two sets of substrates. The three most potent isomers tested were all relatively slowly degraded in both sets of data but three esterases previously associated with pyrethroid resistance in Helicoverpa armigera did not show higher activities for these isomers than did allelic enzymes derived from susceptible H. armigera. Given their amenability to continuous assays at low substrate concentrations in microplate format, and ready detection of product, we endorse the ongoing utility of the analogues in many metabolic studies of pyrethroids., (Copyright © 2014 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015

2. Organophosphate and pyrethroid hydrolase activities of mutant Esterases from the cotton bollworm Helicoverpa armigera.

Author

Li Y, Farnsworth CA, Coppin CW, Teese MG, Liu JW, Scott C, Zhang X, Russell RJ, and Oakeshott JG

Subjects

Animals, Aspartic Acid genetics, Aspartic Acid metabolism, Hydrolysis, Insecticides, Lepidoptera genetics, Lepidoptera metabolism, Leucine genetics, Leucine metabolism, Moths genetics, Moths metabolism, Esterases genetics, Esterases metabolism, Lepidoptera enzymology, Moths enzymology, Mutation genetics, Organophosphates metabolism, Pyrethrins metabolism

Abstract

Two mutations have been found in five closely related insect esterases (from four higher Diptera and a hymenopteran) which each confer organophosphate (OP) hydrolase activity on the enzyme and OP resistance on the insect. One mutation converts a Glycine to an Aspartate, and the other converts a Tryptophan to a Leucine in the enzymes' active site. One of the dipteran enzymes with the Leucine mutation also shows enhanced activity against pyrethroids. Introduction of the two mutations in vitro into eight esterases from six other widely separated insect groups has also been reported to increase substantially the OP hydrolase activity of most of them. These data suggest that the two mutations could contribute to OP, and possibly pyrethroid, resistance in a variety of insects. We therefore introduced them in vitro into eight Helicoverpa armigera esterases from a clade that has already been implicated in OP and pyrethroid resistance. We found that they do not generally enhance either OP or pyrethroid hydrolysis in these esterases but the Aspartate mutation did increase OP hydrolysis in one enzyme by about 14 fold and the Leucine mutation caused a 4-6 fold increase in activity (more in one case) of another three against some of the most insecticidal isomers of fenvalerate and cypermethrin. The Aspartate enzyme and one of the Leucine enzymes occur in regions of the H. armigera esterase isozyme profile that have been previously implicated in OP and pyrethroid resistance, respectively.

Published

2013

3. Heterologous expression and biochemical characterisation of fourteen esterases from Helicoverpa armigera.

Author

Teese MG, Farnsworth CA, Li Y, Coppin CW, Devonshire AL, Scott C, East P, Russell RJ, and Oakeshott JG

Subjects

Animals, Aryldialkylphosphatase metabolism, DNA, Complementary, Esterases metabolism, Expressed Sequence Tags, Glycosylphosphatidylinositols metabolism, Isoenzymes genetics, Isoenzymes metabolism, Native Polyacrylamide Gel Electrophoresis, Esterases genetics, Moths enzymology

Abstract

Esterases have recurrently been implicated in insecticide resistance in Helicoverpa armigera but little is known about the underlying molecular mechanisms. We used a baculovirus system to express 14 of 30 full-length esterase genes so far identified from midgut cDNA libraries of this species. All 14 produced esterase isozymes after native PAGE and the isozymes for seven of them migrated to two regions of the gel previously associated with both organophosphate and pyrethroid resistance in various strains. Thirteen of the enzymes obtained in sufficient yield for further analysis all showed tight binding to organophosphates and low but measurable organophosphate hydrolase activity. However there was no clear difference in activity between the isozymes from regions associated with resistance and those from elsewhere in the zymogram, or between eight of the isozymes from a phylogenetic clade previously associated with resistance in proteomic and quantitative rtPCR experiments and five others not so associated. By contrast, the enzymes differed markedly in their activities against nine pyrethroid isomers and the enzymes with highest activity for the most insecticidal isomers were from regions of the gel and, in some cases, the phylogeny that had previously been associated with pyrethroid resistance. Phospholipase treatment confirmed predictions from sequence analysis that three of the isozymes were GPI anchored. This unusual feature among carboxylesterases has previously been suggested to underpin an association that some authors have noted between esterases and resistance to the Cry1Ac toxin from Bacillus thuringiensis. However these three isozymes did not migrate to the zymogram region previously associated with Cry1Ac resistance.

Published

2013

4. Overexpressed esterases in a fenvalerate resistant strain of the cotton bollworm, Helicoverpa armigera.

Author

Wu S, Yang Y, Yuan G, Campbell PM, Teese MG, Russell RJ, Oakeshott JG, and Wu Y

Subjects

Amino Acid Sequence, Animals, China, Esterases metabolism, Gene Dosage, Gene Expression drug effects, Hydrolysis drug effects, Insecticide Resistance drug effects, Insecticide Resistance genetics, Insecticides pharmacology, Larva enzymology, Mass Spectrometry, Molecular Sequence Data, Moths enzymology, Naphthaleneacetic Acids chemistry, Nitriles pharmacology, Phylogeny, Pyrethrins pharmacology, Esterases genetics, Genes, Insect, Moths genetics

Abstract

Enhanced detoxification is the major mechanism responsible for pyrethroid resistance in Chinese populations of Helicoverpa armigera. Previous work has shown that enhanced oxidation contributes to resistance in the fenvalerate-selected Chinese strain, YGF. The current study provides evidence that enhanced hydrolysis by esterase isozymes also contributes to the resistance in this strain. The average esterase activity of third instar YGF larvae was 1.9-fold compared with that of a susceptible SCD strain. Much of this difference was attributed to isozymes at two zones which hydrolysed the model carboxylester substrate 1-naphthyl acetate and also a 1-naphthyl analogue of fenvalerate. A preparation enriched for enzymes migrating to one of these zones from YGF was shown to hydrolyse fenvalerate with a specific activity of about 2.9 nmol/min/mg. This material was also matched by mass spectrometry with four putative carboxylesterase genes, all of which clustered within a phylogenetic clade of secreted midgut esterases. Quantitative PCR on these four genes showed several-fold greater expression in tissues of YGF compared to SCD but no differences was found in the number of copies of the genes between the strains., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

5. Cloning and biochemical characterization of a novel carbendazim (methyl-1H-benzimidazol-2-ylcarbamate)-hydrolyzing esterase from the newly isolated Nocardioides sp. strain SG-4G and its potential for use in enzymatic bioremediation.

Author

Pandey G, Dorrian SJ, Russell RJ, Brearley C, Kotsonis S, and Oakeshott JG

Subjects

Base Sequence, Biodegradation, Environmental, Cloning, Molecular, Esterases chemistry, Esterases genetics, Gram-Positive Bacteria isolation & purification, Hydrolysis, Molecular Sequence Data, Benzimidazoles metabolism, Carbamates metabolism, Esterases metabolism, Gram-Positive Bacteria enzymology

Abstract

A highly efficient carbendazim (methyl-1H-benzimidazol-2-ylcarbamate, or MBC)-mineralizing bacterium was isolated from enrichment cultures originating from MBC-contaminated soil samples. This bacterium, Nocardioides sp. strain SG-4G, hydrolyzed MBC to 2-aminobenzimidazole, which in turn was converted to the previously unknown metabolite 2-hydroxybenzimidazole. The initial steps of this novel metabolic pathway were confirmed by growth and enzyme assays and liquid chromatography-mass spectrometry (LC-MS) studies. The enzyme responsible for carrying out the first step was purified and subjected to N-terminal and internal peptide sequencing. The cognate gene, named mheI (for MBC-hydrolyzing enzyme), was cloned using a reverse genetics approach. The MheI enzyme was found to be a serine hydrolase of 242 amino acid residues. Its nearest known relative is an uncharacterized hypothetical protein with only 40% amino acid identity to it. Codon optimized mheI was heterologously expressed in Escherichia coli, and the His-tagged enzyme was purified and biochemically characterized. The enzyme has a K(m) and k(cat) of 6.1 muM and 170 min(-1), respectively, for MBC. Radiation-killed, freeze-dried SG-4G cells showed strong and stable MBC detoxification activity suitable for use in enzymatic bioremediation applications.

Published

2010

6. Developmental expression and gene/enzyme identifications in the alpha esterase gene cluster of Drosophila melanogaster.

Author

Campbell PM, de Q Robin GC, Court LN, Dorrian SJ, Russell RJ, and Oakeshott JG

Subjects

Animals, Blotting, Northern, Drosophila melanogaster embryology, Electrophoresis, Gel, Two-Dimensional, Mass Spectrometry, Peptide Mapping, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Esterases genetics, Evolution, Molecular, Gene Expression Profiling

Abstract

Here we show how the 10 genes of the alpha esterase cluster of Drosophila melanogaster have diverged substantially in their expression profiles. Together with previously described sequence divergence this suggests substantial functional diversification. By peptide mass fingerprinting and in vitro gene expression we have also shown that two of the genes encode the isozymes EST9 (formerly ESTC) and EST23. EST9 is the major 'alpha staining' esterase in zymograms of gut tissues in feeding stages while orthologues of EST23 confer resistance to organophosphorus insecticides in other higher Diptera. The results for EST9 and EST23 concur with previous suggestions that the products of the alpha esterase cluster function in digestion and detoxification of xenobiotic esters. However, many of the other genes in the cluster show developmental or tissue-specific expression that seems inconsistent with such roles. Furthermore, there is generally poor correspondence between the mRNA expression patterns of the remaining eight genes and isozymes previously characterized by standard techniques of electrophoresis and staining, suggesting that the alpha cluster might only account for a small minority of the esterase isozyme profile.

Published

2003

7. The phosphotriesterase gene opdA in Agrobacterium radiobacter P230 is transposable.

Author

Horne I, Qiu X, Russell RJ, and Oakeshott JG

Subjects

Amino Acid Sequence, Aryldialkylphosphatase, Chromosomes, Bacterial, Escherichia coli, Esterases metabolism, Molecular Sequence Data, Organophosphorus Compounds metabolism, Phylogeny, RNA, Ribosomal, 16S genetics, Rhizobium enzymology, DNA Transposable Elements, Esterases genetics, Rhizobium genetics

Abstract

We report a transposase gene (tnpA) upstream of the opdA phosphotriesterase gene of Agrobacterium radiobacter P230, as well as inverted repeats indicative of insertion sequences, flanking the two genes. Both the tnpA gene and the inverted repeats resemble the Tn610 transposon from Mycobacterium fortuitum. Two additional putative open reading frames separate opdA and tnpA with inferred translation products with similarity to two proteins encoded on the Geobacillus stearothermophilus IS5376 transposon. To test the proposition that these genes were contained on a transposon, an artificial composite transposon was constructed. This artificial transposon was then delivered into Escherichia coli DH10beta cells. Transposition was demonstrated by the presence of opdA on the E. coli chromosome and confirmation of insertion by inverse polymerase chain reaction. The data presented suggest a possible role of transposition in the distribution of the opd/opdA genes across a wide range of soil bacteria.

Published

2003

8. Cloning and expression of the phosphotriesterase gene hocA from Pseudomonas monteilii C11.

Author

Horne I, Sutherland TD, Oakeshott JG, and Russell RJ

Subjects

Aryldialkylphosphatase, Cloning, Molecular, Coumaphos chemistry, Coumaphos metabolism, Esterases biosynthesis, Esterases isolation & purification, Gene Expression Regulation, Bacterial, Gene Expression Regulation, Enzymologic, Genomic Library, Molecular Sequence Data, Open Reading Frames, Phosphates metabolism, Plasmids, Pseudomonas enzymology, Pseudomonas growth & development, Regulon physiology, Substrate Specificity, Coumaphos analogs & derivatives, Esterases genetics, Pseudomonas genetics

Abstract

The cloning of a gene encoding the novel phosphotriesterase from Pseudomonas monteilii C11, which enabled it to use the organophosphate (OP) coroxon as its sole phosphorus source, is described. The gene, called hocA (hydrolysis of coroxon) consists of 501 bp and encodes a protein of 19 kDa. This protein had no sequence similarity to any proteins in the SWISS-PROT/GenBank databases. When a spectinomycin-resistance cassette was placed in this gene, phosphotriesterase activity was abolished and P. monteilii C11 could no longer grow with coroxon as the sole phosphorus source. Overexpression and purification of HocA as a maltose-binding protein fusion produced a protein having a broad substrate specificity across oxon and thion OPs. Michaelis-Menten kinetics were observed with the oxon OPs, but not with the thion OPs. End-product inhibition was observed for coroxon-hydrolytic activity. Increased expression of hocA was observed from an integrative hocA-lacZ fusion when cultures were grown in the absence of phosphate, suggesting that it might be part of the Pho regulon, but the phosphate-regulated promoter was not cloned in this study. This is believed to be the first study in which a gene required for an organism to grow with OP pesticides as a phosphorus source has been isolated.

Published

2002

9. Identification of an opd (organophosphate degradation) gene in an Agrobacterium isolate.

Author

Horne I, Sutherland TD, Harcourt RL, Russell RJ, and Oakeshott JG

Subjects

Amino Acid Sequence, Aryldialkylphosphatase, Cloning, Molecular, Coumaphos chemistry, Coumaphos metabolism, Esterases metabolism, Molecular Sequence Data, Phosphoric Monoester Hydrolases genetics, Phosphoric Monoester Hydrolases metabolism, Sequence Homology, Amino Acid, Structure-Activity Relationship, Substrate Specificity, Coumaphos analogs & derivatives, Esterases genetics, Rhizobium genetics

Abstract

We isolated a bacterial strain, Agrobacterium radiobacter P230, which can hydrolyze a wide range of organophosphate (OP) insecticides. A gene encoding a protein involved in OP hydrolysis was cloned from A. radiobacter P230 and sequenced. This gene (called opdA) had sequence similarity to opd, a gene previously shown to encode an OP-hydrolyzing enzyme in Flavobacterium sp. strain ATCC 27551 and Brevundimonas diminuta MG. Insertional mutation of the opdA gene produced a strain lacking the ability to hydrolyze OPs, suggesting that this is the only gene encoding an OP-hydrolyzing enzyme in A. radiobacter P230. The OPH and OpdA proteins, encoded by opd and opdA, respectively, were overexpressed and purified as maltose-binding proteins, and the maltose-binding protein moiety was cleaved and removed. Neither protein was able to hydrolyze the aliphatic OP malathion. The kinetics of the two proteins for diethyl OPs were comparable. For dimethyl OPs, OpdA had a higher k(cat) than OPH. It was also capable of hydrolyzing the dimethyl OPs phosmet and fenthion, which were not hydrolyzed at detectable levels by OPH.

Published

2002

10. Isolation of a Pseudomonas monteilli strain with a novel phosphotriesterase.

Author

Horne I, Harcourt RL, Sutherland TD, Russell RJ, and Oakeshott JG

Subjects

Aryldialkylphosphatase, Biodegradation, Environmental, Coumaphos metabolism, Culture Media, Esterases antagonists & inhibitors, Esterases genetics, Gene Expression Regulation, Bacterial, Insecticides metabolism, Phosphates metabolism, Pseudomonas classification, Pseudomonas enzymology, Pseudomonas genetics, Pseudomonas growth & development, Soil Pollutants metabolism, Coumaphos analogs & derivatives, Esterases metabolism, Pseudomonas isolation & purification, Soil Microbiology

Abstract

A Pseudomonas monteilli strain (designated C11) that uses the phosphotriester coroxon as its sole phosphorus source has been isolated. Native PAGE and activity staining identified a single isozyme with significant phosphotriesterase activity in the soluble fraction of the cell. This phosphotriesterase could hydrolyse both coumaphos and coroxon. The hydrolysis product of coroxon, diethylphosphate, and the thion analogue, coumaphos, could not serve as phosphorus sources when added to the growth medium. The majority of the phosphotriesterase and phosphatase activity was contained in the soluble fraction of the cell. Phosphatase activity was inhibited by vanadate as well as by dialysis against the metal chelator, EDTA. Phosphotriesterase activity was not affected by either vanadate or dialysis with EDTA or 1,10-phenanthroline. Phosphotriesterase activity was regulated by the amounts of both phosphate and coroxon in the medium, whereas total phosphatase activity was regulated by phosphate but not coroxon. A lack of hybridisation using a probe against the opd (organophosphate degradation) gene encoding a phosphotriesterase from Flavobacterium sp. ATCC27551 against bulk DNA from P. monteilli C11 suggested that this strain does not contain opd. The work presented here indicates the presence of a novel phosphotriesterase in P. monteilli C11.

Published

2002

11. Reconstructing the diversification of alpha-esterases: comparing the gene clusters of Drosophila buzzatii and D. melanogaster.

Author

de Q Robin GC, Claudianos C, Russell RJ, and Oakeshott JG

Subjects

Animals, Chromosome Mapping, Cloning, Molecular, Drosophila melanogaster genetics, Esterases metabolism, Molecular Sequence Data, Sequence Analysis, DNA, Structure-Activity Relationship, Drosophila genetics, Esterases genetics, Evolution, Molecular, Multigene Family, Phylogeny

Abstract

A cluster composed of 10 active alpha-esterase genes and a pseudogene is distributed over 60 kb in the Drosophila melanogaster genome. This paper describes the corresponding cluster in Drosophila buzzatii, whose lineage diverged from that of D. melanogaster when the subgenera Drosophila and Sophophora diverged about 50 Mya. With three exceptions we find that the composition of the cluster is conserved in the two lineages. The location of alpha E1 in D. melanogaster differs from that of its nearest relative in D. buzzatii, and alpha E4 has duplicated independently in the two lineages. The nature of these differences indicates that a mechanism exists whereby copies of genes can be placed in opposite orientation and nonadjacent positions within a gene cluster, although this does not seem to be a feature of earlier events in the cluster's evolution. The rates of amino acid change are not significantly different between orthologs, but the rates differ sevenfold among paralogs, indicating that very different selective forces are acting on the genes of the cluster. Mapping of sequence differences onto a model of the tertiary structure of the enzymes indicates that motifs contributing to substrate binding and catalysis have changed radically in the alphaE4s and suggest that this subgroup of alpha-esterases may be evolving into a substantially different functional niche.

Published

2000

12. The evolution of an alpha-esterase pseudogene inactivated in the Drosophila melanogaster lineage.

Author

Robin GC, Russell RJ, Cutler DJ, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, DNA Mutational Analysis, Genetic Variation, Molecular Sequence Data, Polymerase Chain Reaction, Polymorphism, Genetic, Sequence Homology, Amino Acid, Drosophila melanogaster genetics, Esterases genetics, Evolution, Molecular, Pseudogenes genetics

Abstract

Previous analyses of the alpha-esterase cluster of Drosophila melanogaster revealed 10 active genes and the DmalphaE4a-Psi pseudogene. Here, we reconstruct the evolution of the pseudogene from the sequences of 12 alleles from widely scattered D. melanogaster populations and single alleles from Drosophila simulans and Drosophila yakuba. All of the DmalphaE4a-Psi alleles contain numerous inactivating mutations, suggesting that pseudogene alleles are fixed in natural populations. Several lines of evidence also suggest that DmalphaE4a is now evolving without selective constraint in the D. melanogaster lineage. There are three polymorphic indels which result in frameshifts; a key nucleotide of the intron splice acceptor is polymorphic; the neutral mutation parameter is the same for replacement and silent sites; one of the nonsilent polymorphisms results in a stop codon; only 1 of the 13 replacement polymorphisms is biochemically conservative; residues that are conserved among active esterases have different states in DmalphaE4a-Psi; and there are about half as many transitional polymorphisms as transversional ones. In contrast, the D. simulans and D. yakuba orthologs DsalphaE4a and DyalphaE4a do not have the inactivating mutations of DmalphaE4a-Psi and appear to be evolving under the purifying selection typical of protein- encoding genes. For instance, there have been more substitutions in the introns than in the exons, and more in silent sites than in replacement sites. Furthermore, most of the amino acid substitutions that have occurred between DyalphaE4a and DsalphaE4a are located in sites that typically vary among active alpha-esterases rather than those that are usually conserved. We argue that the original alphaE4a gene had a function which it has lost since the divergence of the D. melanogaster and D. simulans lineages.

Published

2000

13. The same amino acid substitution in orthologous esterases confers organophosphate resistance on the house fly and a blowfly.

Author

Claudianos C, Russell RJ, and Oakeshott JG

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Base Sequence, DNA, Complementary, Esterases classification, Esterases metabolism, Hydrolysis, Insecticide Resistance, Molecular Sequence Data, Sequence Homology, Amino Acid, Diptera enzymology, Esterases genetics, Houseflies enzymology, Insecticides, Organophosphorus Compounds

Abstract

Organophosphate (OP) insecticide resistance in certain strains of Musca domestica is associated with reduction in the carboxylesterase activity of a particular esterase isozyme. This has been attributed to a 'mutant ali-esterase hypothesis', which invokes a structural mutation to an ali-esterase resulting in the loss of its carboxylesterase activity but acquisition of OP hydrolase activity. It has been shown that the mutation in Lucilia cuprina is a Gly137-->Asp substitution in the active site of an esterase encoded by the Lc alpha E7 gene (Newcomb, R.D., Campbell, P.M., Ollis, D.L., Cheah, E., Russell, R.J., Oakeshott, J.G., 1997. A single amino acid substitution converts a carboxylesterase to an organophosphate hydrolase and confers insecticide resistance on a blowfly. Proc. Natl. Acad. Sci. USA 94, 7464-7468). We now report the cloning and characterisation of the orthologous M. domestica Md alpha E7 gene, including the sequencing of cDNAs from the OP resistant Rutgers and OP susceptible sbo and WHO strains. The Md alpha E7 gene has the same intron structure as Lc alpha E7 and encodes a protein with 76% amino acid identity to Lc alpha E7. Comparisons between susceptible and resistance alleles show resistance in M. domestica is associated with the same Gly137-->Asp mutation as in L. cuprina. Bacterial expression of the Rutgers allele shows its product has OP hydrolase activity. The data indicate identical catalytic mechanisms have evolved in orthologous Md alpha E7 and Lc alpha E7 molecules to endow diazinon-type resistance on the two species of higher Diptera.

Published

1999

14. A single amino acid substitution converts a carboxylesterase to an organophosphorus hydrolase and confers insecticide resistance on a blowfly.

Author

Newcomb RD, Campbell PM, Ollis DL, Cheah E, Russell RJ, and Oakeshott JG

Subjects

Alleles, Amino Acids genetics, Animals, Aryldialkylphosphatase, Carboxylesterase, Diptera drug effects, Point Mutation, Carboxylic Ester Hydrolases genetics, Diptera genetics, Esterases genetics, Insecticide Resistance genetics

Abstract

Resistance to organophosphorus (OP) insecticides is associated with decreased carboxylesterase activity in several insect species. It has been proposed that the resistance may be the result of a mutation in a carboxylesterase that simultaneously reduces its carboxylesterase activity and confers an OP hydrolase activity (the "mutant ali-esterase hypothesis"). In the sheep blowfly, Lucilia cuprina, the association is due to a change in a specific esterase isozyme, E3, which, in resistant flies, has a null phenotype on gels stained using standard carboxylesterase substrates. Here we show that an OP-resistant allele of the gene that encodes E3 differs at five amino acid replacement sites from a previously described OP-susceptible allele. Knowledge of the structure of a related enzyme (acetylcholinesterase) suggests that one of these substitutions (Gly137 --> Asp) lies within the active site of the enzyme. The occurrence of this substitution is completely correlated with resistance across 15 isogenic strains. In vitro expression of two natural and two synthetic chimeric alleles shows that the Asp137 substitution alone is responsible for both the loss of E3's carboxylesterase activity and the acquisition of a novel OP hydrolase activity. Modeling of Asp137 in the homologous position in acetylcholinesterase suggests that Asp137 may act as a base to orientate a water molecule in the appropriate position for hydrolysis of the phosphorylated enzyme intermediate.

Published

1997

15. Biochemistry of esterases associated with organophosphate resistance in Lucilia cuprina with comparisons to putative orthologues in other Diptera.

Author

Campbell PM, Trott JF, Claudianos C, Smyth KA, Russell RJ, and Oakeshott JG

Subjects

Animals, Carboxylesterase, Carboxylic Ester Hydrolases drug effects, Carboxylic Ester Hydrolases genetics, Dialysis, Diptera genetics, Drosophila melanogaster drug effects, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Electrophoresis, Polyacrylamide Gel, Enzyme Inhibitors pharmacology, Esterases drug effects, Esterases genetics, Female, Genetic Variation, Hydrogen-Ion Concentration, Isoflurophate pharmacology, Kinetics, Larva, Muscidae drug effects, Muscidae enzymology, Muscidae genetics, Mutation, Phosphoric Monoester Hydrolases drug effects, Phosphoric Monoester Hydrolases genetics, Phosphoric Monoester Hydrolases metabolism, Species Specificity, Diptera drug effects, Diptera enzymology, Esterases physiology, Insecticide Resistance, Insecticides toxicity

Abstract

Esterase activities associated with organophosphate insecticide resistance in the Australian sheep blowfly, Lucilia cuprina, are compared with similar activities in other Diptera. The enzymes making the major contribution to methyl butyrate hydrolysis ("ali-esterase") in L. cuprina, M. domestica, and D. melanogaster comigrate during electrophoresis. The enzymes in L. cuprina and D. melanogaster correspond to the naphthyl acetate hydrolyzing E3 and EST23 isozymes of those species. These and previously published data suggest that the ali-esterases of all three species are orthologous. Strains of L. cuprina fall into four groups on the basis of quantitative determinations of their ali-estesterase, OP hydrolase, and malathion carboxylesterase activities and these groups correspond to their status with respect to two types of OP resistance. Strains susceptible to OP's have high ali-esterase, low OP hydrolase, and intermediate MCE activities; those resistant to malathion but not diazinon have low ali-esterase, intermediate OP hydrolase, and high MCE activities; those resistant to diazinon but not malathion have low ali-esterase, high OP hydrolase, and low MCE activities; those resistant to both OPs have low ali-esterase, high OP hydrolase, and high MCE activities. The correlated changes among the three biochemical and two resistance phenotypes suggest that they are all properties of one gene/enzyme system; three major allelic variants of that system explain OP susceptibility and the two types of OP resistance. Models are proposed to explain the joint contribution of OP hydrolase and MCE activities to malathion resistance and the invariant association of low ali-esterase and elevated OP hydrolase activities in either type of resistance.

Published

1997

16. Duplication and divergence of the genes of the alpha-esterase cluster of Drosophila melanogaster.

Author

Robin C, Russell RJ, Medveczky KM, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, Base Sequence, Consensus Sequence, Esterases biosynthesis, Esterases chemistry, Frameshift Mutation, Introns, Ligases chemistry, Ligases genetics, Molecular Sequence Data, Open Reading Frames, Pseudogenes, Sequence Homology, Amino Acid, TATA Box, Tropomyosin chemistry, Tropomyosin genetics, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Esterases genetics, Genes, Insect, Genetic Variation, Multigene Family, Phylogeny

Abstract

The alpha-esterase cluster of D. melanogaster contains 11 esterase genes dispersed over 60 kb. Embedded in the cluster are two unrelated open reading frames that have sequence similarity with genes encoding ubiquitin-conjugating enzyme and tropomyosin. The esterase amino acid sequences show 37-66% identity with one another and all but one have all the motifs characteristic of functional members of the carboxyl/cholinesterase multigene family. The exception has several frameshift mutations and appears to be a pseudogene. Patterns of amino acid differences among cluster members in relation to generic models of carboxyl/cholinesterase protein structure are broadly similar to those among other carboxyl/cholinesterases sequenced to date. However the alpha-esterases differ from most other members of the family in: their lack of a signal peptide; the lack of conservation in cysteines involved in disulfide bridges; and in four indels, two of which occur in or adjacent to regions that align with proposed substrate-binding sites of other carboxyl/cholinesterases. Phylogenetic analyses clearly identify three simple gene duplication events within the cluster. The most recent event involved the pseudogene which is located in an intron of another esterase gene. However, relative rate tests suggest that the pseudogene remained functional after the duplication event and has become inactive relatively recently. The distribution of indels also suggests a deeper node in the gene phylogeny that separates six genes at the two ends of the cluster from a block of five in the middle.

Published

1996

17. Isolation of alpha cluster esterase genes associated with organophosphate resistance in Lucilia cuprina.

Author

Newcomb RD, East PD, Russell RJ, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, Base Sequence, DNA, Complementary, Molecular Sequence Data, Phylogeny, Polymerase Chain Reaction, Sequence Homology, Amino Acid, Diptera enzymology, Esterases genetics, Insecticide Resistance genetics, Insecticides, Organophosphorus Compounds

Abstract

PCR primers designed from the alpha-esterase gene cluster of Drosophila melanogaster have been used to isolate fragments from eight esterase genes in the Australian sheep blowfly, Lucilia cuprina. Phylogenetic analysis suggests that three are homologues of the alpha E7, alpha E8 and alpha E9 genes of the alpha-esterase cluster of D. melanogaster. A further three are also probably alpha-esterases, whereas the remaining two more closely resemble beta-esterases. Transcripts for five of the alpha-esterase genes were detected by PCR in adult midgut, consistent with a role for these enzymes in digestion and/or detoxification. Based on the tissue distribution of these transcripts, Lc alpha E7 may possibly encode the esterase, E3, which is involved in organophosphate resistance.

Published

1996

18. Mutational analysis of N-linked glycosylation of esterase 6 in Drosophila melanogaster.

Author

Myers MA, Healy MJ, and Oakeshott JG

Subjects

Animals, Drosophila melanogaster genetics, Esterases genetics, Female, Glycosylation, Male, Mutagenesis, Drosophila melanogaster enzymology, Esterases metabolism

Abstract

The primary sequence of the esterase 6 (EST6) enzyme of Drosophila melanogaster contains four potential N-linked glycosylation sites, at residues 21, 399, 435, and 485. Here we determine the extent to which EST6 is glycosylated and how the glycosylation affects the biochemistry and physiology of the enzyme. We have abolished each of the four potential glycosylation sites by replacing the required Asn residues with Gln by in vitro mutagenesis. Five mutant genes were made, four containing mutations of each site individually and the fifth site containing all four mutations. Germline transformation was used to introduce the mutant genes into a strain of D. melanogaster null for EST6. Electrophoretic and Western blot comparisons of the mutant strains and wild-type controls showed that each of the four potential N-linked glycosylation sites in the wild-type protein is glycosylated. However, the fourth site is not utilized on all EST6 molecules, resulting in two molecular forms of the enzyme. Digestion with specific endoglycosidases showed that the glycan attached at the second site is of the high-mannose type, while the other three sites carry more complex oligosaccharides. The thermostability of the enzyme is not affected by abolition of the first, third, or fourth glycosylation sites but is reduced by abolition of the second site. Anomalously, abolition of all four sites together does not reduce thermostability. Quantitative comparisons of EST6 activities showed that abolition of glycosylation does not affect the secretion of the enzyme into the male sperm ejaculatory duct, its transfer to the female vagina during mating, or its subsequent translocation into her hemolymph. However, the activity of the mutant enzymes does not persist in the female's hemolymph for as long as wild-type esterase 6. The latter effect may compromise the role of the transferred enzyme in stimulating egg-laying and delaying receptivity to remating.

Published

1996

19. Molecular cloning of an alpha-esterase gene cluster on chromosome 3r of Drosophila melanogaster.

Author

Russell RJ, Robin GC, Kostakos P, Newcomb RD, Boyce TM, Medveczky KM, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, Base Sequence, Chromosome Walking, Chromosomes, Chromosomes, Artificial, Yeast, Cloning, Molecular, Molecular Sequence Data, Multigene Family, Sequence Homology, Amino Acid, Chromosome Mapping, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Esterases genetics, Genes, Insect genetics

Abstract

All or part of the alpha-esterase gene cluster in Drosophila melanogaster has been isolated by screening a YAC clone that spans cytological region 84D3-10 with consensus carboxyl/cholinesterase oligonucleotides. The cluster encompasses 11 putative esterase genes within 65 kb of genomic DNA and is one of the largest clusters of related protein-coding genes yet reported in Drosophila. The cluster must include the gene encoding the major alpha-esterase isozyme, EST9, which has previously been mapped to 84D3-5. It probably also includes the genes encoding the EST23, MCE and ALI esterases that have previously been mapped to 84D3-E2. The latter three are homologs of genes involved in organophosphate insecticide resistance in the sheep blowfly, Lucilia cuprina and the housefly, Musca domestica. Sequencing of one of the putative esterase genes in the Drosophila cluster, alpha E1, shows that it would encode features characteristic of an active carboxyl/cholinesterase, including the so-called catalytic triad, the nucleophilic elbow and oxyanion hole. It also shows that the closest relative of alpha E1 amongst previously published esterase sequences is ESTB1, which confers organophosphate resistance in Culex mosquitoes. We argue that we have cloned the D. melanogaster version of a major cluster of esterase genes which have variously mutated to confer organophosphate resistance in diverse Diptera.

Published

1996

20. A cluster of at least three esterase genes in Lucilia cuprina includes malathion carboxylesterase and two other esterases implicated in resistance to organophosphates.

Author

Smyth KA, Russell RJ, and Oakeshott JG

Subjects

Animals, Chromosome Mapping, Crosses, Genetic, Diptera enzymology, Female, Genetic Linkage, Homozygote, Insecticide Resistance genetics, Male, Sheep, Carboxylic Ester Hydrolases genetics, Diptera genetics, Esterases genetics, Malathion toxicity, Multigene Family

Abstract

Three distinct malathion carboxylesterase (MCE) phenotypes have been identified among strains of Lucilia cuprina. The high-activity phenotype shows 1.6- and 33-fold more MCE specific activity than the intermediate- and low-activity phenotypes, respectively. Flies with high MCE activity are 1000-fold more resistant to malathion than flies with either low or intermediate MCE phenotypes, which are equally susceptible. High and low MCE specific activity are allelic and encoded by the Rmal gene on chromosome 4. Rmal is clustered within one map unit of two other esterase genes, Rop1 and E9, which are implicated in resistance to other organophosphate insecticides. Intermediate MCE specific activity is also inherited within the cluster, although its allelism to Rmal, Rop1, or E9 is unclear. The cluster does not contain the gene for the hemolymph esterase E4, which maps 6.1 map units from Rop1, on the other side of the bubbled wing marker. The cluster appears to be homologous to part of a tandem array of 11 esterase genes on chromosome 3R of Drosophila melanogaster.

Published

1994

21. A cluster of esterase genes on chromosome 3R of Drosophila melanogaster includes homologues of esterase genes conferring insecticide resistance in Lucilia cuprina.

Author

Spackman ME, Oakeshott JG, Smyth KA, Medveczky KM, and Russell RJ

Subjects

Animals, Carboxylesterase, Carboxylic Ester Hydrolases genetics, Chromosome Mapping, Crosses, Genetic, Diptera enzymology, Drosophila melanogaster enzymology, Female, Fenitrothion analogs & derivatives, Fenitrothion pharmacology, Hydrogen-Ion Concentration, Insecticide Resistance genetics, Isoelectric Point, Isoenzymes genetics, Male, Organ Specificity, Paraoxon pharmacology, Substrate Specificity, Drosophila melanogaster genetics, Esterases antagonists & inhibitors, Esterases chemistry, Esterases genetics, Esterases isolation & purification, Esterases metabolism, Genes, Insect genetics, Multigene Family genetics

Abstract

We identify an esterase isozyme in Drosophila melanogaster, EST 23, which shares biochemical, physiological, and genetic properties with esterase E3, which is involved in resistance to organophosphate insecticides in Lucilia cuprina. Like E3, the D. melanogaster EST 23 is a membrane-bound alpha-esterase which migrates slowly toward the anode at pH 6.8. Both enzymes have similar preferences for substrates with shorter acid side chain lengths. Furthermore, on the basis of their high sensitivity to inhibition by paraoxon and their insensitivity to inhibition by eserine sulfate, both enzymes were classified as subclass I carboxylesterases. The activity of each enzyme peaks early in development and, again, in the adult stage. Both enzymes are found in the male reproductive system and larval and adult digestive tissues, the latter being consistent with a role for these enzymes in organophosphate resistance. Fine structure deficiency mapping localized Est 23 to cytological region 84D3 to E1-2 on the right arm of chromosome 3. Moreover, we show that the genes encoding three other esterase phenotypes also map to the same region; these phenotypes involve allozymic differences in EST 9 (formerly EST C), ali-esterase activity, defined by the hydrolysis of methyl butyrate, and malathion carboxylesterase activity, defined by hydrolysis of the organophosphate malathion. This cluster corresponds closely to that encompassing E3 and malathion carboxylesterase on chromosome 4 in L. cuprina, the homologue of chromosome 3R in D. melanogaster.

Published

1994

22. Evolutionary genetics of Drosophila esterases.

Author

Oakeshott JG, van Papenrecht EA, Boyce TM, Healy MJ, and Russell RJ

Subjects

Amino Acid Sequence, Animals, Drosophila melanogaster genetics, Genes, Insect, Humans, Molecular Sequence Data, Multigene Family, Species Specificity, Biological Evolution, Drosophila melanogaster enzymology, Esterases genetics

Abstract

Over 30 carboxylester hydrolases have been identified in D. melanogaster. Most are classified as acetyl, carboxyl or cholinesterases. Sequence similarities among most of the carboxyl and all the cholinesterases so far characterised from D. melanogaster and other eukaryotes justify recognition of a carboxyl/cholinesterase multigene family. This family shows minimal sequence similarities with other esterases but crystallographic data for a few non-drosophilid enzymes show that the family shares a distinctive overall structure with some other carboxyl and aryl esterases, so they are all put in one superfamily of/beta hydrolases. Fifteen esterase genes have been mapped in D. melanogaster and twelve are clustered at two chromosomal sites. The constitution of each cluster varies across Drosophila species but two carboxyl esterases in one cluster are sufficiently conserved that their homologues can be identified among enzymes conferring insecticide resistance in other Diptera. Sequence differences between two other esterases, the EST6 carboxyl esterase and acetylcholinesterase, have been interpreted against the consensus super-secondary structure for the carboxyl/cholinesterase multigene family; their sequence differences are widely dispersed across the structure and include substantial divergence in substrate binding sites and the active site gorge. This also applies when EST6 is compared across species where differences in its expression indicate a difference in function. However, comparisons within and among species where EST6 expression is conserved show that many aspects of the predicted super-secondary structure are tightly conserved. Two notable exceptions are a pair of polymorphisms in the substrate binding site of the enzyme in D. melanogaster. These polymorphisms are associated with differences in substrate interactions in vitro and demographic data indicate that the alternative forms are not selectively equivalent in vivo.

Published

1993

23. Biochemical and physiological studies of soluble esterases from Drosophila melanogaster.

Author

Healy MJ, Dumancic MM, and Oakeshott JG

Subjects

Animals, Drosophila melanogaster enzymology, Drosophila melanogaster growth & development, Embryo, Nonmammalian enzymology, Esterases antagonists & inhibitors, Esterases physiology, Female, Larva enzymology, Male, Pupa enzymology, Solubility, Substrate Specificity, Tissue Distribution, Drosophila melanogaster genetics, Esterases genetics

Abstract

Twenty-two soluble esterases have been identified in D. melanogaster by combining the techniques of native polyacrylamide gel electrophoresis and isoelectric focusing. The sensitivity of each isozyme to three types of inhibitors (organophosphates, eserine sulfate, and sulfydryl reagents) identified 10 as carboxylesterases, 6 as cholinesterases, and 3 as acetylesterases. Three isozymes could not be classified and no arylesterases were identified. The carboxyl- and cholinesterases could each be further divided into two subclasses on the basis of inhibition by organophosphates and sulfhydryl reagents, respectively. Choline- and acetylesterases have characteristic substrate preferences but both subclasses of carboxylesterases are heterogeneous in substrate utilization. Subclass 2 carboxylesterases exhibit diverse temporal expression patterns, with subclass 1 carboxylesterases generally found in larvae and subclass 1 cholinesterases and acetylesterases more characteristic of pupae and adults. Tissues showing the greatest number of isozymes are larval body wall (eight) and digestive tract (six in larvae, six in adults). Carboxylesterases are distributed across a wide range of tissues, but subclass 1 cholinesterases are generally associated with neural or neurosecretory tissues and subclass 2 cholinesterases with digestive tissues.

Published

1991

24. Cloning of the esterase-5 locus from Drosophila pseudoobscura and comparison with its homologue in D. melanogaster.

Author

Brady JP, Richmond RC, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Northern, Blotting, Southern, Carboxylesterase, Carboxylic Ester Hydrolases genetics, Cloning, Molecular, DNA Transposable Elements, Drosophila enzymology, Drosophila melanogaster enzymology, Electrophoresis, Polyacrylamide Gel, Genes, Molecular Sequence Data, Restriction Mapping, Sequence Homology, Nucleic Acid, Transformation, Genetic, Drosophila genetics, Drosophila Proteins, Drosophila melanogaster genetics, Esterases genetics

Abstract

A clone of the esterase-5 (Est-5) gene from Drosophila pseudoobscura has been isolated by hybridization to the cloned Est-6 gene of D. melanogaster. Southern analysis and sequencing of the cloned DNA revealed three regions of similarity to Est-6 that have been tentatively identified as genes, Est-5A, Est-5B, and Est-5C. Introduction of each of the three genes separately into D. melanogaster by P-element transformation has demonstrated that Est-5B encodes an enzyme with the same physical properties as EST 5 in D. pseudoobscura. Sequence analysis indicates that Est-5B encodes a 545-amino-acid protein and is composed of two exons separated by a 55-bp intron in the same position as the 51-bp intron in Est-6. Comparison of the Est-5B coding region with that of Est-6 reveals an overall similarity (73% at both the nucleotide and amino acid levels) that is substantially lower than that for other genes sequenced in both of these species. Total nucleotide and nonsynonymous site differences between Est-6 and Est-5B are more abundant in the second exon than in the first, suggesting differential effects of selection or mutation on these two exons. Comparisons of the 5'-flanking DNA of Est-5B and Est-6 reveal four short conserved sequence elements, but the remaining upstream sequences show no significant similarity. Conservation in the 3'-flanking DNA is limited to the presence of two polyadenylation sites that may correlate with the existence of two transcripts from both Est-5B and Est-6. The patterns of nucleotide substitutions and amino acid replacements between Est-5B and Est-6 are consistent with the hypothesis that mutation and genetic drift are responsible for the differences between these two genes.

Published

1990

25. Molecular analysis of duplicated esterase genes in Drosophila melanogaster.

Author

Collet C, Nielsen KM, Russell RJ, Karl M, Oakeshott JG, and Richmond RC

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Northern, Blotting, Southern, DNA genetics, Exons, Female, Male, Molecular Sequence Data, Regulatory Sequences, Nucleic Acid, Restriction Mapping, Sequence Homology, Nucleic Acid, Transcription, Genetic, Drosophila melanogaster genetics, Esterases genetics, Multigene Family

Abstract

Genomic clones containing sequences homologous to an esterase 6 (Est-6) cDNA clone were isolated from a library of Drosophila melanogaster DNA. Comparison of the genomic and cDNA sequences revealed that the Est-6 gene comprises two exons, one of 1,387 bp and one of 248 bp, separated by a short intron of 51 bp. Further sequencing revealed the presence of a tandem duplication of the Est-6 gene (denoted Est-P) which also has an exon of 1,387 bp and an exon of 248 bp, separated by a short intron of 56 bp. The two genes show similarities of 64% and 60% at the DNA and protein levels, respectively. The coding regions of the genes are 197 bases apart, and presumptive 5' regulatory sequences of Est-P overlap at least the 3' noncoding region of Est-6. Transcripts homologous to Est-P were detected in late larvae and adults of each sex, whereas Est-6 transcripts are present in all life stages but are predominant in adult males. This suggests different physiological functions for the products of the two genes. Southern and Northern blot hybridization analyses of the 20-kb region surrounding the Est-6/Est-P duplication failed to detect any other duplicated esterase genes, although this region is actively transcribed.

Published

1990

26. On the origins of esterases.

Author

Myers M, Richmond RC, and Oakeshott JG

Subjects

Amino Acid Sequence, Animals, Binding Sites, Biological Evolution, Cholinesterases genetics, Humans, Molecular Sequence Data, Protein Conformation, Sequence Homology, Nucleic Acid, Serine Endopeptidases genetics, Esterases genetics, Multigene Family

Abstract

Comparisons among the primary sequences of five cloned eukaryotic esterases reveal two distinct lineages, neither bearing any significant overall sequence similarity to the functionally related serine protease multigene family. We have not eliminated the possibility that the esterases may have residual conformational similarities to the serine proteases. However, our profile analysis and analyses of the predicted conformations of the esterases reveal little similarity to the serine proteases. Four of the esterase proteins share 27%-53% overall sequence similarity and evidence of a catalytic mechanism involving the same Arg-Asp-Ser or His-Asp-Ser charge relay. We propose that these four esterases, three of them cholinesterases, form part of a multigene family essentially separate from the serine proteases.

Published

1988