Your search keyword '"David J. Timson"' showing total 370 results

1. Galactose epimerase deficiency: lessons from the GalNet registry

Author

Britt Derks, Didem Demirbas, Rodrigo R. Arantes, Samantha Banford, Alberto B. Burlina, Analía Cabrera, Ana Chiesa, M. Luz Couce, Carlo Dionisi-Vici, Matthias Gautschi, Stephanie Grünewald, Eva Morava, Dorothea Möslinger, Sabine Scholl-Bürgi, Anastasia Skouma, Karolina M. Stepien, David J. Timson, Gerard T. Berry, and M. Estela Rubio-Gozalbo

Subjects

Galactose epimerase deficiency, Galactosemia type III, Galactosemias Network, Galactose-restricted diet, Medicine

Abstract

Abstract Background Galactose epimerase (GALE) deficiency is a rare hereditary disorder of galactose metabolism with only a few cases described in the literature. This study aims to present the data of patients with GALE deficiency from different countries included through the Galactosemia Network to further expand the existing knowledge and review the current diagnostic strategy, treatment and follow-up of this not well characterized entity. Methods Observational study collecting medical data from December 2014 to April 2022 of 22 not previously reported patients from 14 centers in 9 countries. Patients were classified as generalized or non-generalized based on their genotype, enzyme activities in different tissues and/or clinical picture and professional judgment of the treating physician. Results In total 6 patients were classified as generalized and 16 as non-generalized. In the generalized group, acute neonatal illness was reported in 3, cognitive and developmental delays were present in 5 and hearing problems were reported in 3. Four generalized patients were homozygous for the genetic variant NM_001008216.2:c.280G > A (p.Val94Met). In the non-generalized group, no clearly related symptoms were found. Ten novel genetic variants were reported in this study population. Conclusion The phenotypic spectrum of GALE deficiency ranges from asymptomatic to severe. The generalized patients have a phenotype that is in line with the 9 described cases in the literature and prescribing dietary interventions is the cornerstone for treatment. In the non-generalized group, treatment advice is more difficult. To be able to offer proper counseling, in addition to red blood cell enzyme activity, genetic studies, transferrin glycoform analysis and enzymatic measurements in fibroblasts are recommended. Due to lack of facilities, additional enzymatic testing is not common practice in many centers nor a tailored long-term follow-up is performed.

Published

2022

2. [13C]‐galactose breath test in a patient with galactokinase deficiency and spastic diparesis

Author

Can Ficicioglu, Didem Demirbas, Britt Derks, G. Shashidhar Pai, David J. Timson, Maria Estela Rubio‐Gozalbo, and Gerard T. Berry

Subjects

galactosemia, GALK1 deficiency, in vivo galactose oxidation, stable‐isotope labeled galactose, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Galactokinase deficiency is an inborn error of carbohydrate metabolism due to a block in the formation of galactose‐1‐phosphate from galactose. Although the association of galactokinase deficiency with formation of cataracts is well established, the extent of the clinical phenotype is still under investigation. We describe a 6‐year‐old female who was diagnosed with galactokinase deficiency due to cataract formation when she was 10 months of age and initially started on galactose‐restricted diet at that time for 5 months. She developed gait abnormality at 4 years of age. Breath tests via measurement of 13C isotope in exhaled carbon dioxide following 13C‐labeled galactose administration at carbon‐1 and carbon‐2 positions revealed oxidation rates within the normal range. The results in this patient strikingly contrast with the results of another patient with GALK1 deficiency that underwent breath testing with [1‐14C]‐galactose and [2‐14C]‐galactose. Extension of in vivo breath tests to other galactokinase patients is needed to better understand the pathophysiology of this disease.

Published

2021

3. RNA interference dynamics in juvenile Fasciola hepatica are altered during in vitro growth and development

Author

Paul McCusker, Wasim Hussain, Paul McVeigh, Erin McCammick, Nathan G. Clarke, Emily Robb, Fiona M. McKay, Peter M. Brophy, David J. Timson, Angela Mousley, Nikki J. Marks, and Aaron G. Maule

Subjects

Fasciola, Liver fluke, RNAi, Argonaute, Calmodulin, σGST, Infectious and parasitic diseases, RC109-216

Abstract

For over a decade RNA interference (RNAi) has been an important molecular tool for functional genomics studies in parasitic flatworms. Despite this, our understanding of RNAi dynamics in many flatworm parasites, such as the temperate liver fluke (Fasciola hepatica), remains rudimentary. The ability to maintain developing juvenile fluke in vitro provides the opportunity to perform functional studies during development of the key pathogenic life stage. Here, we investigate the RNAi competence of developing juvenile liver fluke. Firstly, all life stages examined possess, and express, core candidate RNAi effectors encouraging the hypothesis that all life stages of F. hepatica are RNAi competent. RNAi effector analyses supported growing evidence that parasitic flatworms have evolved a separate clade of RNAi effectors with unknown function. Secondly, we assessed the impact of growth/development during in vitro culture on RNAi in F. hepatica juveniles and found that during the first week post-excystment liver fluke juveniles exhibit quantitatively lower RNAi mediated transcript knockdown when maintained in growth inducing media. This did not appear to occur in older in vitro juveniles, suggesting that rapidly shifting transcript dynamics over the first week following excystment alters RNAi efficacy after a single 24 h exposure to double stranded (ds)RNA. Finally, RNAi efficiency was found to be improved through use of a repeated dsRNA exposure methodology that has facilitated silencing of genes in a range of tissues, thereby increasing the utility of RNAi as a functional genomics tool in F. hepatica.

Published

2020

4. Yeast Cellular Stress: Impacts on Bioethanol Production

Author

Joshua Eardley and David J. Timson

Subjects

bioethanol, chaotropicity, fermentation, biofuel yield, compatible solute, cell stress, Fermentation industries. Beverages. Alcohol, TP500-660

Abstract

Bioethanol is the largest biotechnology product and the most dominant biofuel globally. Saccharomyces cerevisiae is the most favored microorganism employed for its industrial production. However, obtaining maximum yields from an ethanol fermentation remains a technical challenge, since cellular stresses detrimentally impact on the efficiency of yeast cell growth and metabolism. Ethanol fermentation stresses potentially include osmotic, chaotropic, oxidative, and heat stress, as well as shifts in pH. Well-developed stress responses and tolerance mechanisms make S. cerevisiae industrious, with bioprocessing techniques also being deployed at industrial scale for the optimization of fermentation parameters and the effective management of inhibition issues. Overlap exists between yeast responses to different forms of stress. This review outlines yeast fermentation stresses and known mechanisms conferring stress tolerance, with their further elucidation and improvement possessing the potential to improve fermentation efficiency.

Published

2020

5. The Catalytic Cycle of the Antioxidant and Cancer-Associated Human NQO1 Enzyme: Hydride Transfer, Conformational Dynamics and Functional Cooperativity

Author

Ernesto Anoz-Carbonell, David J. Timson, Angel L. Pey, and Milagros Medina

Subjects

antioxidant enzyme, antioxidant response, cancer, oxidoreductase, enzyme kinetic analysis, functional cooperativity, Therapeutics. Pharmacology, RM1-950

Abstract

Human NQO1 [NAD(H):quinone oxidoreductase 1] is a multi-functional and stress-inducible dimeric protein involved in the antioxidant defense, the activation of cancer prodrugs and the stabilization of oncosuppressors. Despite its roles in human diseases, such as cancer and neurological disorders, a detailed characterization of its enzymatic cycle is still lacking. In this work, we provide a comprehensive analysis of the NQO1 catalytic cycle using rapid mixing techniques, including multiwavelength and spectral deconvolution studies, kinetic modeling and temperature-dependent kinetic isotope effects (KIEs). Our results systematically support the existence of two pathways for hydride transfer throughout the NQO1 catalytic cycle, likely reflecting that the two active sites in the dimer catalyze two-electron reduction with different rates, consistent with the cooperative binding of inhibitors such as dicoumarol. This negative cooperativity in NQO1 redox activity represents a sort of half-of-sites activity. Analysis of KIEs and their temperature dependence also show significantly different contributions from quantum tunneling, structural dynamics and reorganizations to catalysis at the two active sites. Our work will improve our understanding of the effects of cancer-associated single amino acid variants and post-translational modifications in this protein of high relevance in cancer progression and treatment.

Published

2020

6. Four Challenges for Better Biocatalysts

Author

David J. Timson

Subjects

protein folding, enzyme engineering, hydrophobic effect, chaotropicity, enzyme mechanism, water activity, green chemistry, enzyme specificity, biotechnology, protein structure, Fermentation industries. Beverages. Alcohol, TP500-660

Abstract

Biocatalysis (the use of biological molecules or materials to catalyse chemical reactions) has considerable potential. The use of biological molecules as catalysts enables new and more specific syntheses. It also meets many of the core principles of “green chemistry”. While there have been some considerable successes in biocatalysis, the full potential has yet to be realised. This results, partly, from some key challenges in understanding the fundamental biochemistry of enzymes. This review summarises four of these challenges: the need to understand protein folding, the need for a qualitative understanding of the hydrophobic effect, the need to understand and quantify the effects of organic solvents on biomolecules and the need for a deep understanding of enzymatic catalysis. If these challenges were addressed, then the number of successful biocatalysis projects is likely to increase. It would enable accurate prediction of protein structures, and the effects of changes in sequence or solution conditions on these structures. We would be better able to predict how substrates bind and are transformed into products, again leading to better enzyme engineering. Most significantly, it may enable the de novo design of enzymes to catalyse specific reactions.

Published

2019

7. Expression, purification and crystallization of a novel metagenome-derived salicylaldehyde dehydrogenase from Alpine soil

Author

Shamsudeen Umar Dandare, Maria Håkansson, L. Anders Svensson, David J. Timson, and Christopher C. R. Allen

Subjects

purification, Biophysics, alphaproteobacteria, Ligands, Crystallography, X-Ray, Condensed Matter Physics, Aldehyde Oxidoreductases, Biochemistry, salicylaldehyde dehydrogenase, Soil, Alpine soil, Structural Biology, Escherichia coli, Genetics, Metagenome, Crystallization, crystallography, Escherichia coli - genetics

Abstract

Salicylaldehyde dehydrogenase (SALD) catalyses the last reaction in the upper pathway of naphthalene degradation: the oxidation of salicylaldehyde to salicylate. This enzyme has been isolated and studied from a few organisms that belong to the betaproteobacteria and gammaproteobacteria, predominantly Pseudomonas putida. Furthermore, there is only one crystal structure of this enzyme, which was obtained from P. putida G7. Here, crystallographic studies and analysis of the crystal structure of an Alpine soil metagenome-derived SALD (SALDAP) from an alphaproteobacterium are presented. The SALDAP gene was discovered using gene-targeted sequence assembly and it was cloned into a pLATE51 vector. The recombinant protein was overexpressed in Escherichia coli BL21 (DE3) cells and the soluble protein was purified to homogeneity. The protein crystallized at 20°C and diffraction data from the crystals were collected at a resolution of 1.9 Å. The crystal belonged to the orthorhombic space group C2221, with unit-cell parameters a = 116.8, b = 121.7, c = 318.0 Å. Analysis of the crystal structure revealed its conformation to be similar to the organization of the aldehyde dehydrogenase superfamily with three domains: the catalytic, NAD+-binding and bridging domains. The crystal structure of NahF from P. putida G7 was found to be the best structural homologue of SALDAP, even though the enzymes share only 48% amino-acid identity. Interestingly, a carboxylic acid (protocatechuic acid) was found to be a putative ligand of the enzyme and differential scanning fluorimetry was employed to confirm ligand binding. These findings open up the possibility of studying the mechanism(s) of product inhibition and biocatalysis of carboxylic acids using this enzyme and other related aldehyde dehydrogenases.

Published

2022

8. [13C]‐galactose breath test in a patient with galactokinase deficiency and spastic diparesis

Author

Britt Derks, Didem Demirbas, David J. Timson, M. E. Rubio-Gozalbo, Gerard T. Berry, Can Ficicioglu, G Shashidhar Pai, Kindergeneeskunde, RS: GROW - R4 - Reproductive and Perinatal Medicine, and MUMC+: MA Medische Staf Kindergeneeskunde (9)

Subjects

medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, stable‐isotope labeled galactose, Carbohydrate metabolism, QH426-470, Biochemistry, Genetics and Molecular Biology (miscellaneous), Gastroenterology, Diseases of the endocrine glands. Clinical endocrinology, Cataracts, Internal medicine, Internal Medicine, medicine, in vivo galactose oxidation, Genetics, galactosemia, Breath test, medicine.diagnostic_test, business.industry, Galactosemia, medicine.disease, RC648-665, Galactokinase, Galactokinase deficiency, Pathophysiology, GALK1 deficiency, Gait abnormality, medicine.symptom, business

Abstract

Galactokinase deficiency is an inborn error of carbohydrate metabolism due to a block in the formation of galactose‐1‐phosphate from galactose. Although the association of galactokinase deficiency with formation of cataracts is well established, the extent of the clinical phenotype is still under investigation. We describe a 6‐year‐old female who was diagnosed with galactokinase deficiency due to cataract formation when she was 10 months of age and initially started on galactose‐restricted diet at that time for 5 months. She developed gait abnormality at 4 years of age. Breath tests via measurement of 13C isotope in exhaled carbon dioxide following 13C‐labeled galactose administration at carbon‐1 and carbon‐2 positions revealed oxidation rates within the normal range. The results in this patient strikingly contrast with the results of another patient with GALK1 deficiency that underwent breath testing with [1‐14C]‐galactose and [2‐14C]‐galactose. Extension of in vivo breath tests to other galactokinase patients is needed to better understand the pathophysiology of this disease.

Published

2021

9. Galactokinase deficiency

Author

M. Estela Rubio-Gozalbo, Patrick Verloo, Sabine Scholl-Bürgi, U. Meyer, Ina Knerr, David Cassiman, Aurélie Empain, Dorothea Möslinger, Mariela M. De Los Santos De Pelegrin, Britt Derks, Can Ficicioglu, Matthias Gautschi, Natalia Juliá Palacios, Didem Demirbas, David J. Timson, Eileen P. Treacy, Annet M. Bosch, M. Luz Couce, Philippe Labrune, Gerard T. Berry, Isabel Rivera, Anastasia Skouma, Anibh M. Das, Saskia B. Wortmann, Kindergeneeskunde, MUMC+: MA Medische Staf Kindergeneeskunde (9), RS: GROW - R4 - Reproductive and Perinatal Medicine, Paediatric Metabolic Diseases, and AGEM - Amsterdam Gastroenterology Endocrinology Metabolism

Subjects

cataract, galactosemias registry, Galactosemias, Pediatrics, medicine.medical_specialty, galactokinase 1 deficiency, Population, Encephalopathy, GALK1 gene variants, VARIANT, 610 Medicine & health, Article, Galactokinase, ERYTHROCYTES, Medicine and Health Sciences, Medicine, Humans, Genetics(clinical), Registries, education, MUTATION, Genetics (clinical), education.field_of_study, Newborn screening, business.industry, Neonatal hypoglycemia, Homozygote, Infant, Newborn, neonatal complications, Childhood cataract, medicine.disease, Galactokinase deficiency, Bleeding diathesis, GALK1gene variants, Elevated transaminases, business, GALACTOSEMIA

Abstract

PURPOSE: Galactokinase (GALK1) deficiency is a rare hereditary galactose metabolism disorder. Beyond cataract, the phenotypic spectrum is questionable. Data from affected patients included in the Galactosemias Network registry were collected to better characterize the phenotype. METHODS: Observational study collecting medical data of 53 not previously reported GALK1 deficient patients from 17 centers in 11 countries from December 2014 to April 2020. RESULTS: Neonatal or childhood cataract was reported in 15 and 4 patients respectively. The occurrence of neonatal hypoglycemia and infection were comparable with the general population, whereas bleeding diathesis (8.1% versus 2.17-5.9%) and encephalopathy (3.9% versus 0.3%) were reported more often. Elevated transaminases were seen in 25.5%. Cognitive delay was reported in 5 patients. Urinary galactitol was elevated in all patients at diagnosis; five showed unexpected Gal-1-P increase. Most patients showed enzyme activities ≤1%. Eleven different genotypes were described, including six unpublished variants. The majority was homozygous for NM_000154.1:c.82C>A (p.Pro28Thr). Thirty-five patients were diagnosed following newborn screening, which was clearly beneficial. CONCLUSION: The phenotype of GALK1 deficiency may include neonatal elevation of transaminases, bleeding diathesis, and encephalopathy in addition to cataract. Potential complications beyond the neonatal period are not systematically surveyed and a better delineation is needed. ispartof: GENETICS IN MEDICINE vol:23 issue:1 pages:202-210 ispartof: location:United States status: published

Published

2021

10. Targeting HIF-1α Function in Cancer through the Chaperone Action of NQO1: Implications of Genetic Diversity of NQO1

Author

Eduardo Salido, David J. Timson, Isabel Betancor-Fernández, Rogelio Palomino-Morales, Ernesto Anoz-Carbonell, Juan Luis Pacheco-García, Milagros Medina, and Angel L. Pey

Subjects

Proteasomal degradation, protein interactions [Protein], HIF-1alpha, Medicine (miscellaneous), NQO1, Genetic variability, Angiogenesis, Hypoxia, Ligand binding, Cancer

Abstract

This research was funded by the ERDF/Spanish Ministry of Science, Innovation and Universities-State Research Agency (Grant RTI2018-096246-B-I00, to A.L.P., PID2019-110900GBI00 to M.M. and SAF2015-69796 to E.S.), Consejeriia de Economiia, Conocimiento, Empresas y Universidad, Junta de Andalucia (Grant P18-RT-2413, to A.L.P.), and the Government of AragonFEDER (Grant E35-20R to M.M.)., HIF-1 alpha is a master regulator of oxygen homeostasis involved in different stages of cancer development. Thus, HIF-1 alpha inhibition represents an interesting target for anti-cancer therapy. It was recently shown that the HIF-1 alpha interaction with NQO1 inhibits proteasomal degradation of the former, thus suggesting that targeting the stability and/or function of NQO1 could lead to the destabilization of HIF-1 alpha as a therapeutic approach. Since the molecular interactions of NQO1 with HIF-1 alpha are beginning to be unraveled, in this review we discuss: (1) Structure-function relationships of HIF-1 alpha; (2) our current knowledge on the intracellular functions and stability of NQO1; (3) the pharmacological modulation of NQO1 by small ligands regarding function and stability; (4) the potential effects of genetic variability of NQO1 in HIF-1 alpha levels and function; (5) the molecular determinants of NQO1 as a chaperone of many different proteins including cancer-associated factors such as HIF-1 alpha, p53 and p73 alpha. This knowledge is then further discussed in the context of potentially targeting the intracellular stability of HIF-1 alpha by acting on its chaperone, NQO1. This could result in novel anti-cancer therapies, always considering that the substantial genetic variability in NQO1 would likely result in different phenotypic responses among individuals., ERDF/Spanish Ministry of Science, Innovation and Universities-State Research Agency RTI2018-096246-B-I00 PID2019-110900GBI00 SAF2015-69796, Junta de Andalucia P18-RT-2413, Government of AragonFEDER E35-20R

Published

2022

11. A ligand predication tool based on modeling and reasoning with imprecise probabilistic knowledge.

Author

Weiru Liu, Anbu Yue, and David J. Timson

Published

2010

12. Destressing Yeast for Higher Biofuel Yields: Can Excess Chaotropicity Be Mitigated?

Author

David J. Timson and Joshua Eardley

Subjects

0106 biological sciences, Kosmotropic, 010405 organic chemistry, Bioengineering, General Medicine, Pulp and paper industry, 01 natural sciences, Applied Microbiology and Biotechnology, Biochemistry, Yeast, 0104 chemical sciences, chemistry.chemical_compound, Chaotropic agent, chemistry, Bioenergy, Biofuel, 010608 biotechnology, Yield (chemistry), Carbon dioxide, Fermentation, Molecular Biology, Biotechnology

Abstract

Biofuels have the capacity to contribute to carbon dioxide emission reduction and to energy security as oil reserves diminish and/or become concentrated in politically unstable regions. However, challenges exist in obtaining the maximum yield from industrial fermentations. One challenge arises from the nature of alcohols. These compounds are chaotropic (i.e. causes disorder in the system) which causes stress in the microbes producing the biofuel. Brewer’s yeast (Saccharomyces cerevisiae) typically cannot grow at ethanol concentration much above 17% (v/v). Mitigation of these properties has the potential to increase yield. Previously, we have explored the effects of chaotropes on model enzyme systems and attempted (largely unsuccessfully) to offset these effects by kosmotropes (compounds which increase the order of the system, i.e. the “opposite” of chaotropes). Here we present some theoretical results which suggest that high molecular mass polyethylene glycols may be the most effective kosmotropic additives in terms of both efficacy and cost. The assumptions and limitations of these calculations are also presented. A deeper understanding of the effects of chaotropes on biofuel-producing microbes is likely to inform improvements in bioethanol yields and enable more rational approaches to the “neutralisation” of chaotropicity.

Published

2020

13. In SilicoAnalysis of the Effects of Point Mutations on α-Globin: Implications for α-Thalassemia

Author

Agathe Horri-Naceur and David J. Timson

Subjects

Genetics, Heme binding, Thalassemia, Point mutation, In silico, Biochemistry (medical), Clinical Biochemistry, Single-nucleotide polymorphism, Hematology, Biology, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, SNP, Hemoglobin, Gene, Genetics (clinical), 030215 immunology

Abstract

Hemoglobinopathies are inherited diseases that impair the structure and function of the oxygen-carrying pigment hemoglobin (Hb). Adult Hb consists of two α and two β subunits. α-Thalassemia (α-thal) affects the genes that code for the α-globin chains, HBA1 and HBA2. Mutations can result in asymptomatic, mild or severe outcomes depending on several factors, such as mutation type, number of mutations and the location at which they occur. PredictSNP was used to estimate whether every possible single nucleotide polymorphism (SNP) would have a neutral or deleterious effect on the protein. These results were then used to create a plot of predicted tolerance to change for each residue in the protein. Tolerance to change was negatively correlated with the residue's sequence conservation score. The PredictSNP data were compared to clinical reports of 110 selected variants in the literature. There were 29 disagreements between the two data types. Some of these could be resolved by considering the role of the affected residue in binding other molecules. The three-dimensional structures of some of these variant proteins were modeled. These models helped explain variants which affect heme binding. We predict that where a point mutation alters a residue that is intolerant to change, is well conserved and or involved in interactions, it is likely to be associated with disease. Overall, the data from this study could be used alongside biochemical and clinical data to assess novel α-globin variants.

Published

2020

14. Therapies for galactosemia: a patent landscape

Author

David J. Timson

Subjects

Galactosemias, Patents as Topic, Salubrinal, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cataracts, Aldehyde Reductase, Animals, Humans, Medicine, Transferase, RNA, Messenger, Enzyme Inhibitors, 030304 developmental biology, Genetics, 0303 health sciences, business.industry, Galactosemia, Thiourea, Galactose, Uridylyltransferase activity, General Medicine, medicine.disease, Leloir pathway, chemistry, Cinnamates, Inherited metabolic disease, business, 030217 neurology & neurosurgery

Abstract

Galactosemia is the inherited inability to metabolise galactose. The most common results from a lack of galactose 1-phosphate uridylyltransferase activity. The current treatment, removal of galactose from the diet, is inadequate and often fails to prevent long-term complications. Since 2015, three patents have been filed describing novel therapies. These are: the use of aldose reductase inhibitors to reduce cataracts and, possibly, other symptoms; salubrinal to stimulate cellular stress responses; mRNA therapy to increase cellular galactose 1-phosphate uridylyltransferase activity. The viability of all three is supported by academic studies. The potential and drawbacks of all three are discussed and evaluated.

Published

2020

15. Repurposing drugs for the treatment of galactosemia

Author

David J. Timson

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Health Policy, Galactosemia, nutritional and metabolic diseases, medicine.disease, Bioinformatics, eye diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, 030220 oncology & carcinogenesis, Galactose, Dietary antioxidant, Medicine, Idebenone, Pharmacology (medical), Inherited metabolic disease, business, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), 030217 neurology & neurosurgery, Repurposing, medicine.drug

Abstract

Introduction: Galactosemia results from mutations in genes which code for enzymes involved in the metabolism of galactose. It has a wide range of symptoms ranging from the relatively mild (early on...

Published

2019

16. Evidence for chaotropicity/kosmotropicity offset in a yeast growth model

Author

John E. Hallsworth, David J. Timson, Marcus K. Dymond, Joshua Eardley, and Cinzia Dedi

Subjects

Glycerol, 0106 biological sciences, 0301 basic medicine, Kosmotropic, Entropy, Bioengineering, Saccharomyces cerevisiae, Models, Biological, 01 natural sciences, Applied Microbiology and Biotechnology, 03 medical and health sciences, chemistry.chemical_compound, Betaine, 010608 biotechnology, Urea, Ammonium, Ethanol, General Medicine, Culture Media, Chaotropic agent, 030104 developmental biology, chemistry, Ammonium Sulfate, Biofuels, Fermentation, Biophysics, Osmoprotectant, Biotechnology

Abstract

Chaotropes are compounds which cause the disordering, unfolding and denaturation of biological macromolecules. It is the chaotropicity of fermentation products that often acts as the primary limiting factor in ethanol and butanol fermentations. Since ethanol is mildly chaotropic at low concentrations, it prevents the growth of the producing microbes via its impacts on a variety of macromolecular systems and their functions. Kosmotropes have the opposite effect to chaotropes and we hypothesised that it might be possible to use these to mitigate chaotrope-induced inhibition of Saccharomyces cerevisiae growth. We also postulated that kosmotrope-mediated mitigation of chaotropicity is not quantitatively predictable. The chaotropes ethanol and urea, and compatible solutes glycerol and betaine (kosmotrope), and the highly kosmotropic salt ammonium sulphate all inhibited the growth rate of Saccharomyces cerevisiae in the concentration range 5-15%. They resulted in increased lag times, decreased maximum specific growth rates, and decreased final optical densities. Surprisingly, neither the stress protectants nor ammonium sulphate reduced the inhibition of growth caused by ethanol. Whereas, in some cases, compatible solutes and kosmotropes mitigated against the inhibitory effects of urea. However, this effect was not mathematically additive from the quantification of chao-/kosmotropicity of each individual compound. The potential effects of glycerol, betaine and/or ammonium sulphate may have been reduced or masked by the metabolic production of compatible solutes. It may nevertheless be that the addition of kosmotropes to fermentations which produce chaotropic products can enhance metabolic activity, growth rate, and/or product formation.

Published

2019

17. Catalytic mechanism of mevalonate kinase revisited, a QM/MM study

Author

David J. Timson, Jian Zhang, James McClory, Meilan Huang, and Jun-Tang Lin

Subjects

Protein Conformation, alpha-Helical, 0301 basic medicine, Conformational change, Protein Conformation, Stereochemistry, Mevalonic Acid, 01 natural sciences, Biochemistry, QM/MM, 03 medical and health sciences, chemistry.chemical_compound, Adenosine Triphosphate, Protein structure, Biosynthesis, 0103 physical sciences, Animals, Magnesium, Phosphorylation, Physical and Theoretical Chemistry, 010304 chemical physics, biology, Kinase, Chemistry, Organic Chemistry, Mevalonate kinase, Rats, Molecular Docking Simulation, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, biology.protein, Quantum Theory, Mevalonate pathway, Protein Binding

Abstract

Mevalonate Kinase (MVK) catalyses the ATP-Mg2+ mediated phosphate transfer of mevalonate to produce mevalonate 5-phosphate and is a key kinase in the mevalonate pathway in the biosynthesis of isopentenyl diphosphate, the precursor of isoprenoid-based biofuels. However, the crystal structure in complex with the native substrate mevalonate, ATP and Mg2+ has not been resolved, which has limited the understanding of its reaction mechanism and therefore its application in the production of isoprenoid-based biofuels. Here using molecular docking, molecular dynamic (MD) simulations and a hybrid QM/MM study, we revisited the location of Mg2+ resolved in the crystal structure of MVK and determined a catalytically competent MVK structure in complex with the native substrate mevalonate and ATP. We demonstrated that significant conformational change on a flexilble loop connecting the α6 and α7 helix is induced by the substrate binding. Further, we found that Asp204 is coordinated to the Mg2+ ion. Arg241 plays a crucial role in organizing the triphosphoryl tail of ATP for in-line phosphate transfer and stabilizing the negative charge that accumulates at the β,γ-bridging oxygen of ATP upon bond cleavage. Remarkably, we revealed that the phosphorylation of mevalonate catalyzed by MVK occurs via a direct phosphorylation mechanism, instead of the conventionally postulated catalytic base mechanism. The catalytically competent complex structure of MVK as well as the mechanism of reaction will pave the way for the rational engineering of MVK to exploit its applications in the production of biofuels.

Published

2019

18. Galactosemia: Towards Pharmacological Chaperones

Author

Angel L. Pey, David J. Timson, Thomas J. McCorvie, and Samantha Banford

Subjects

0301 basic medicine, Galactose metabolism, UDP-galactose 4′-epimerase, ligand binding, Medicine (miscellaneous), lcsh:Medicine, galactose 1-phosphate uridylyltransferase, Disease, Review, Protein degradation, Bioinformatics, galactokinase, Galactose mutarotase, 03 medical and health sciences, Galactokinase, 0302 clinical medicine, medicine, drug screening, protein misfolding, education, Pathological, Ligand binding, education.field_of_study, UDP-galactose 40-epimerase, Galactose 1-phosphate uridylyltransferase, business.industry, Galactosemia, lcsh:R, medicine.disease, Phenotype, Enzymes, enzyme, 030104 developmental biology, Drug screening, protein degradation, business, galactose mutarotase, galactose metabolism, 030217 neurology & neurosurgery, Function (biology), Protein misfolding

Abstract

Galactosemia is a rare inherited metabolic disease resulting from mutations in the four genes which encode enzymes involved in the metabolism of galactose. The current therapy, the removal of galactose from the diet, is inadequate. Consequently, many patients suffer lifelong physical and cognitive disability. The phenotype varies from almost asymptomatic to life-threatening disability. The fundamental biochemical cause of the disease is a decrease in enzymatic activity due to failure of the affected protein to fold and/or function correctly. Many novel therapies have been proposed for the treatment of galactosemia. Often, these are designed to treat the symptoms and not the fundamental cause. Pharmacological chaperones (PC) (small molecules which correct the folding of misfolded proteins) represent an exciting potential therapy for galactosemia. In theory, they would restore enzyme function, thus preventing downstream pathological consequences. In practice, no PCs have been identified for potential application in galactosemia. Here, we review the biochemical basis of the disease, identify opportunities for the application of PCs and describe how these might be discovered. We will conclude by considering some of the clinical issues which will affect the future use of PCs in the treatment of galactosemia., ERDF/Spanish Ministry of Science, Innovation and Universities-State Research Agency RTI2018-096246-B-I00, FEDER/Junta de Andalucía - Consejería de Transformación Económica, Industria, Conocimiento y Universidades P18-RT-2413

Published

2021

19. The structural and molecular biology of type IV galactosemia

Author

Samantha Banford and David J. Timson

Subjects

0301 basic medicine, Galactosemias, Anomer, Biochemistry, 03 medical and health sciences, medicine, Monosaccharide, Humans, education, Gene, chemistry.chemical_classification, education.field_of_study, 030102 biochemistry & molecular biology, Chemistry, Galactosemia, Galactose, General Medicine, medicine.disease, Galactokinase deficiency, 030104 developmental biology, Enzyme, Pyranose, Mutation, Protein Conformation, beta-Strand, Galactose mutarotase, Carbohydrate Epimerases

Abstract

Type IV galactosemia is a recently discovered inherited metabolic disease. It is caused by mutations in the GALM gene which result in reduced activity of the enzyme galactose mutarotase. This enzyme catalyses the interconversion of the α- and β-anomers of d-galactose and some other monosaccharides. Human galactose mutarotase is monomeric and its structure is largely composed of β-sheets. The catalytic mechanism requires a histidine residue acting as an acid, and a glutamate acting as a base. Together, these residues open the pyranose ring of d-galactose enabling free rotation of the bond between the first two carbon atoms in the monosaccharide. This can cause reversal of the configuration of the hydroxyl group attached to carbon 1. Type IV galactosemia manifests with similar symptoms to type II galactosemia (galactokinase deficiency), i.e. early onset cataracts. However, as a recently discovered disease, the longer-term consequences are unknown. The physiological role, if any, of galactose mutarotase's reactions with other monosaccharides are not yet known. The possible associations with other proteins also require further investigation.

Published

2020

20. The Catalytic Cycle of the Antioxidant and Cancer-Associated Human NQO1 Enzyme: Hydride Transfer, Conformational Dynamics and Functional Cooperativity

Author

David J. Timson, Milagros Medina, Ernesto Anoz-Carbonell, Angel L. Pey, Ministerio de Ciencia, Innovación y Universidades (España), Junta de Andalucía, and Gobierno de Aragón

Subjects

0301 basic medicine, antioxidant enzyme, Enzyme kinetic analysis, antioxidant response, Antioxidant responses, Physiology, Dimer, conformational dynamics, Clinical Biochemistry, Cooperativity, Hydride transfer, Quinone oxidoreductase, Biochemistry, Article, Functional cooperativity, Conformational dynamics, 03 medical and health sciences, chemistry.chemical_compound, Oxidoreductase, hydride transfer, cancer, Quantum tunneling, Molecular Biology, oxidoreductase, Cancer, chemistry.chemical_classification, functional cooperativity, 030102 biochemistry & molecular biology, lcsh:RM1-950, Antioxidant response, Kinetic isotope effects, Cooperative binding, Cell Biology, enzyme kinetic analysis, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Enzyme, chemistry, Catalytic cycle, kinetic isotope effects, Biophysics, Antioxidant enzymes, NAD+ kinase, Oxidoreductases, quantum tunneling

Abstract

Human NQO1 [NAD(H):quinone oxidoreductase 1] is a multi-functional and stress-inducible dimeric protein involved in the antioxidant defense, the activation of cancer prodrugs and the stabilization of oncosuppressors. Despite its roles in human diseases, such as cancer and neurological disorders, a detailed characterization of its enzymatic cycle is still lacking. In this work, we provide a comprehensive analysis of the NQO1 catalytic cycle using rapid mixing techniques, including multiwavelength and spectral deconvolution studies, kinetic modeling and temperature-dependent kinetic isotope e ects (KIEs). Our results systematically support the existence of two pathways for hydride transfer throughout the NQO1 catalytic cycle, likely reflecting that the two active sites in the dimer catalyze two-electron reduction with di erent rates, consistent with the cooperative binding of inhibitors such as dicoumarol. This negative cooperativity in NQO1 redox activity represents a sort of half-of-sites activity. Analysis of KIEs and their temperature dependence also show significantly di erent contributions from quantum tunneling, structural dynamics and reorganizations to catalysis at the two active sites. Our work will improve our understanding of the e ects of cancer-associated single amino acid variants and post-translational modifications in this protein of high relevance in cancer progression and treatment., ERDF/Spanish Ministry of Science, Innovation and Universities-State Research Agency RTI2018-096246-B-I00, Spanish Ministry of Science and Innovation-State Research Agency PID2019-103901GB-I00, Junta de Andalucía P11-CTS-07187 P18-RT-2413, Gobierno de Aragón-FEDER E35_20R

Published

2020

21. Pilot Evaluation of Two Fasciola hepatica Biomarkers for Supporting Triclabendazole (TCBZ) Efficacy Diagnostics

Author

Clare F. Collett, David J. Timson, Peter M. Brophy, Russell M. Morphew, and Helen Phillips

Subjects

Drug, media_common.quotation_subject, 030231 tropical medicine, Pharmaceutical Science, Analytical Chemistry, calreticulin, lcsh:QD241-441, 03 medical and health sciences, 0302 clinical medicine, lcsh:Organic chemistry, Hepatica, Drug Discovery, parasitic diseases, medicine, diagnostics, Parasite hosting, Fasciola hepatica, Anthelmintic, Fasciolosis, Physical and Theoretical Chemistry, 030304 developmental biology, media_common, 0303 health sciences, biology, Organic Chemistry, triose phosphate isomerase, triclabendazole, biology.organism_classification, medicine.disease, Triclabendazole, Chemistry (miscellaneous), Immunology, Molecular Medicine, Biomarker (medicine), biomarker, fasciolosis, medicine.drug

Abstract

Fasciola hepatica, the causative agent of fasciolosis, is a global threat to public health, animal welfare, agricultural productivity, and food security. In the ongoing absence of a commercial vaccine, independent emergences of anthelmintic-resistant parasite populations worldwide are threatening the sustainability of the few flukicides presently available, and particularly triclabendazole (TCBZ) as the drug of choice. Consequently, prognoses for future fasciolosis control and sustained TCBZ application necessitate improvements in diagnostic tools to identify anthelmintic efficacy. Previously, we have shown that proteomic fingerprinting of F. hepatica excretory/secretory (ES) products offered new biomarkers associated with in vitro TCBZ-sulfoxide (SO) recovery or death. In the current paper, two of these biomarkers (calreticulin (CRT) and triose phosphate isomerase (TPI)) were recombinantly expressed and evaluated to measure TCBZ efficacy via a novel approach to decipher fluke molecular phenotypes independently of molecular parasite resistance mechanism(s), which are still not fully characterised or understood. Our findings confirmed the immunoreactivity and diagnostic potential of the present target antigens by sera from TCBZ-susceptible (TCBZ-S) and TCBZ-resistant (TCBZ-R) F. hepatica experimentally infected sheep.

Published

2020

22. RNA interference dynamics in juvenile Fasciola hepatica are altered during in vitro growth and development

Author

David J. Timson, Fiona M. McKay, Emily Robb, Angela Mousley, Paul McCusker, Paul McVeigh, Wasim Hussain, Nikki J. Marks, Erin McCammick, Nathan G. Clarke, Aaron G. Maule, and Peter M. Brophy

Subjects

Gene knockdown, RNA silencing, RNA interference, parasitic diseases, Gene silencing, RNA, Fasciola hepatica, Liver fluke, Biology, biology.organism_classification, Functional genomics, Cell biology

Abstract

For over a decade RNA interference (RNAi) has been an important molecular tool for functional genomics studies in parasitic flatworms. Despite this, our understanding of RNAi dynamics in many flatworm parasites, such as the temperate liver fluke (Fasciola hepatica), remains rudimentary. The ability to maintain developing juvenile fluke in vitro provides the opportunity to perform functional studies during development of the key pathogenic life stage. Here, we investigate the RNAi competence of developing juvenile liver fluke. Firstly, all life stages examined possess, and express, core candidate RNAi effectors encouraging the hypothesis that all life stages of F. hepatica are RNAi competent. RNAi effector analyses supported growing evidence that parasitic flatworms have evolved a separate clade of RNAi effectors with unknown function. Secondly, we assessed the impact of growth / development during in vitro culture on RNAi in F. hepatica juveniles and found that during the first week post-excystment liver fluke juveniles exhibit quantitatively lower RNAi mediated transcript knockdown when maintained in growth inducing media. This did not appear to occur in older in vitro juveniles, suggesting that rapidly shifting transcript dynamics over the first week following excystment alters RNAi efficacy after a single 24 hour exposure to double stranded (ds)RNA. Finally, RNAi efficiency was found to be improved through use of a repeated dsRNA exposure methodology that has facilitated silencing of genes in a range of tissues, thereby increasing the utility of RNAi as a functional genomics tool in F. hepatica.

Published

2020

23. The roles and applications of chaotropes and kosmotropes in industrial fermentation processes

Author

David J. Timson

Subjects

Glycerol, 0106 biological sciences, Kosmotropic, Physiology, Butanols, Genes, Fungal, Industrial fermentation, Saccharomyces cerevisiae, Sulfides, 01 natural sciences, Applied Microbiology and Biotechnology, Protein Structure, Secondary, Methylamines, 03 medical and health sciences, Bioreactors, Yeasts, 010608 biotechnology, Urea, Zymomonas, 0303 health sciences, Ethanol, 030306 microbiology, Chemistry, Amino Acids, Diamino, Water, General Medicine, Chaotropic agent, Genes, Bacterial, Alcohols, Biofuels, Fermentation, Biochemical engineering, Bacillus subtilis, Biotechnology

Abstract

Chaotropicity has long been recognised as a property of some compounds. Chaotropes tend to disrupt non-covalent interactions in biological macromolecules (e.g. proteins and nucleic acids) and supramolecular assemblies (e.g. phospholipid membranes). This results in the destabilisation and unfolding of these macromolecules and assemblies. Unsurprisingly, these compounds are typically harmful to living cells since they act against multiple targets, comprising cellular integrity and function. Kosmotropes are the opposite of chaotropes and these compounds promote the ordering and rigidification of biological macromolecules and assemblies. Since many biological macromolecules have optimum levels of flexibility, kosmotropes can also inhibit their activity and can be harmful to cells. Some products of industrial fermentations, most notably alcohols, are chaotropic. This property can be a limiting factor on rates of production and yields. It has been hypothesised that the addition of kosmotropes may mitigate the chaotropicity of some fermentation products. Some microbes naturally adapt to chaotropic environments by producing kosmotropic compatible solutes. Exploitation of this in industrial fermentations has been hampered by scientific and economic issues. The cost of the kosmotropes and their removal during purification needs to be considered. We lack a complete understanding of the chemistry of chaotropicity and a robust, quantitative framework for estimating overall chaotropicities of mixtures. This makes it difficult to predict the amount of kosmotrope required to neutralise the chaotropicity. This review considers examples of industrial fermentations where chaotropicity is an issue and suggests possible mitigations.

Published

2020

24. Praziquantel: An Enigmatic, Yet Effective, Drug

Author

David J, Timson

Subjects

Animals, Humans, Schistosomiasis, Models, Biological, Praziquantel

Abstract

Praziquantel is a remarkably effective drug for the treatment of schistosomiasis. It has few side effects, some of which have been attributed to its inactive enantiomer. Few, if any, verified cases of drug resistance have been reported in a clinical setting. The preponderance of scientific evidence suggests that the drug works by dysregulating calcium homeostasis in the worm. Voltage-gated calcium channels have been proposed as the main pharmacological target of praziquantel, although no direct evidence of interaction with this protein is available. Here, the biochemical pharmacology of praziquantel is briefly reviewed and a hypothesis for its mechanism proposed. This hypothesis suggests that the drug works, in part, by disrupting an interaction between a voltage-gated calcium channel (SmCav1B) and an accessory protein, SmTAL1.

Published

2020

25. In silico analysis of the effects of disease-associated mutations of β-hexosaminidase A in Tay‒Sachs disease

Author

David J. Timson, Mohammad Ihsan Fazal, and Rafal Kacprzyk

Subjects

0106 biological sciences, 0301 basic medicine, Genetics, endocrine system, Mutation, In silico, Tay-Sachs disease, Metabolic disorder, Neurodegeneration, Disease, Biology, medicine.disease, medicine.disease_cause, 01 natural sciences, 03 medical and health sciences, 030104 developmental biology, medicine, Sphingolipidosis, Age of onset, 010606 plant biology & botany

Abstract

Tay‒Sachs disease (TSD), a deficiency of β-hexosaminidase A (Hex A), is a rare but debilitating hereditary metabolic disorder. Symptoms include extensive neurodegeneration and often result in death in infancy. We report an in silico study of 42 Hex A variants associated with the disease. Variants were separated into three groups according to the age of onset: infantile (n=28), juvenile (n=9) and adult (n=5). Protein stability, aggregation potential and the degree of conservation of residues were predicted using a range of in silico tools. We explored the relationship between these properties and the age of onset of TSD. There was no significant relationship between protein stability and disease severity or between protein aggregation and disease severity. Infantile TSD had a significantly higher mean conservation score than nondisease associated variants. This was not seen in either juvenile or adult TSD. This study has established that the degree of residue conservation may be predictive of infantile TSD. It is possible that these more highly conserved residues are involved in trafficking of the protein to the lysosome. In addition, we developed and validated software tools to automate the process of in silico analysis of proteins involved in inherited metabolic diseases. Further work is required to identify the function of well-conserved residues to establish an in silico predictive model of TSD severity.

Published

2020

26. Targeting HIF-1α Function in Cancer through the Chaperone Action of NQO1

Author

Rogelio Palomino-Morales, David J. Timson, Eduardo Salido, Isabel Betancor-Fernández, and Angel L. Pey

Subjects

biology, Chemistry, Angiogenesis, Chaperone (protein), biology.protein, oncology_oncogenics, Cell biology, Protein–protein interaction

Abstract

HIF-1α is a master regulator of oxygen homeostasis involved in different stages of cancer development. Thus, HIF-1α inhibition represents an interesting target for anti-cancer therapy. It was recently shown that HIF-1α interaction with NQO1 inhibits its proteasomal degradation, thus suggesting that targeting the stability of NQO1 could led to destabilization of HIF-1α as a therapeutic approach. Since the molecular interactions of NQO1 with HIF-1α are beginning to be unraveled, we review here our current knowledge on the intracellular functions and stability of NQO1, its pharmacological modulation by small ligands, and the molecular determinants of its roles as a chaperone of many different proteins including cancer-associated factors such as p53 and p73α. This knowledge is then discussed in the context of potentially targeting the intracellular stability of HIF-1α by acting on its chaperone, NQO1. This could result in novel anti-cancer therapies.

Published

2020

27. The Schistosoma mansoni tegumental allergen protein, SmTAL1: binding to an IQ-motif from a voltage-gated ion channel and effects of praziquantel

Author

David J. Timson and Charlotte M. Thomas

Subjects

0301 basic medicine, Voltage-gated calcium channel, Physiology, Amino Acid Motifs, Protozoan Proteins, EF-hand, Ion Channels, Praziquantel, 03 medical and health sciences, 0302 clinical medicine, Calmodulin, Protein Domains, Calcium-binding protein, parasitic diseases, Animals, Schistosomiasis, Amino Acid Sequence, Calcium ion binding, EF Hand Motifs, Molecular Biology, Ions, Voltage-dependent calcium channel, Voltage-gated ion channel, biology, Chemistry, EF hand, Calcium channel, Cooperative binding, Schistosoma mansoni, Cell Biology, Allergens, biology.organism_classification, IQ-motif, 030104 developmental biology, Proteolysis, Biophysics, Calcium, Protein Multimerization, Peptides, Calcium binding proteins, 030217 neurology & neurosurgery, Protein Binding

Abstract

SmTAL1 is a calcium binding protein from the parasitic worm, Schistosoma mansoni. Structurally it is comprised of two domains - an N-terminal EF-hand domain and a C-terminal dynein light chain (DLC)-like domain. The protein has previously been shown to interact with the anti-schistosomal drug, praziquantel (PZQ). Here, we demonstrated that both EF-hands in the N-terminal domain are functional calcium ion binding sites. The second EF-hand appears to be more important in dictating affinity and mediating the conformational changes which occur on calcium ion binding. There is positive cooperativity between the four calcium ion binding sites in the dimeric form of SmTAL1. Both the EF-hand domain and the DLC-domain dimerise independently suggesting that both play a role in forming the SmTAL1 dimer. SmTAL1 binds non-cooperatively to PZQ and cooperatively to an IQ-motif from SmCav1B, a voltage-gated calcium channel. PZQ tends to strengthen this interaction, although the relationship is complex. These data suggest the hypothesis that SmTAL1 regulates at least one voltage-gated calcium channel and PZQ interferes with this process. This may be important in the molecular mechanism of this drug. It also suggests that compounds which bind SmTAL1, such as six from the Medicines for Malaria Box identified in this work, may represent possible leads for the discovery of novel antagonists.

Published

2020

28. Novel and selective inactivators of Triosephosphate isomerase with anti-trematode activity

Author

Guzmán Álvarez, Xavier Robert, Teresa Freire, Florencia Ferraro, Ileana Corvo, Andrea Ilarraz, Conor R. Caffrey, Lucia Bergalli, J. Gil, Mauricio Cabrera, Christophe Guillon, Brian M. Susuki, and David J. Timson

Subjects

0301 basic medicine, Male, Models, Molecular, Parasitic infection, Fascioliasis, 030106 microbiology, lcsh:Medicine, Trematode Infections, Biology, Crystallography, X-Ray, Article, Triosephosphate isomerase, Microbiology, 03 medical and health sciences, Mice, In vivo, Drug Discovery, medicine, Fasciola hepatica, Animals, Drug discovery and development, Enzyme Inhibitors, lcsh:Science, IC50, Anthelmintics, Mice, Inbred BALB C, Multidisciplinary, Mesocricetus, Drug discovery, lcsh:R, Schistosoma mansoni, biology.organism_classification, Schistosomiasis mansoni, 3. Good health, 030104 developmental biology, Triclabendazole, Mechanism of action, lcsh:Q, Female, Trematoda, medicine.symptom, medicine.drug, Triose-Phosphate Isomerase

Abstract

Trematode infections such as schistosomiasis and fascioliasis cause significant morbidity in an estimated 250 million people worldwide and the associated agricultural losses are estimated at more than US$ 6 billion per year. Current chemotherapy is limited. Triosephosphate isomerase (TIM), an enzyme of the glycolytic pathway, has emerged as a useful drug target in many parasites, including Fasciola hepatica TIM (FhTIM). We identified 21 novel compounds that selectively inhibit this enzyme. Using microscale thermophoresis we explored the interaction between target and compounds and identified a potent interaction between the sulfonyl-1,2,4-thiadiazole (compound 187) and FhTIM, which showed an IC50 of 5 µM and a Kd of 66 nM. In only 4 hours, this compound killed the juvenile form of F. hepatica with an IC50 of 3 µM, better than the reference drug triclabendazole (TCZ). Interestingly, we discovered in vitro inhibition of FhTIM by TCZ, with an IC50 of 7 µM suggesting a previously uncharacterized role of FhTIM in the mechanism of action of this drug. Compound 187 was also active against various developmental stages of Schistosoma mansoni. The low toxicity in vitro in different cell types and lack of acute toxicity in mice was demonstrated for this compound, as was demonstrated the efficacy of 187in vivo in F. hepatica infected mice. Finally, we obtained the first crystal structure of FhTIM at 1.9 Å resolution which allows us using docking to suggest a mechanism of interaction between compound 187 and TIM. In conclusion, we describe a promising drug candidate to control neglected trematode infections in human and animal health.

Published

2020

29. Contributors

Author

Olga Abian, Ilaria Bellezza, Ganeko Bernardo-Seisdedos, Isabel Betancor-Fernandez, Jean-Marc Blouin, Kerensa Broersen, Giulia Calloni, Barbara Cellini, Caspar E. Christensen, Francisco Conejero-Lara, Joana S. Cristóvão, Marte I. Flydal, Nicole Fontana, Douglas M. Fowler, David Gil, Cláudio M. Gomes, Sarah Good, Andreas M. Grabrucker, Fedora Grande, Silvia Grottelli, Aylin C. Hanyaloglu, Rasmus Hartmann-Petersen, Emil Hausvik, Jo Ann Janovick, Michael Maglegaard Jepsen, Kresten Lindorff-Larsen, Aurora Martinez, Thomas J. McCorvie, Oscar Millet, Guilherme G. Moreira, Bertrand Morel, Athi N. Naganathan, Jose L. Neira, Sofie V. Nielsen, Angel L. Pey, Emmanuel Richard, Bruno Rizzuti, Eduardo Salido, Signe M. Schenstrøm, Svein I. Støve, Amelie Stein, David J. Timson, Alfredo Ulloa-Aguirre, Jarl Underhaug, R. Martin Vabulas, Patricija van Oosten-Hawle, Sonia Vega, Adrian Velazquez-Campoy, Wyatt W. Yue, and Teresa Zariñán

Published

2020

30. Galactosemia: opportunities for novel therapies

Author

David J. Timson and Thomas J. McCorvie

Subjects

education.field_of_study, business.industry, Galactosemia, Enzyme replacement therapy, Pharmacology, medicine.disease, Galactokinase, Leloir pathway, Pharmacological chaperone, Uridine diphosphate, chemistry.chemical_compound, chemistry, Galactose, medicine, Galactose mutarotase, education, business, medicine.drug

Abstract

Galactosemia is an inherited metabolic disease affecting enzymes of the Leloir pathway of galactose metabolism. There are four types: type I (galactose 1-phosphate uridylyltransferase; GALT), type II (galactokinase; GALK1), type III (uridine diphosphate [UDP]-galactose 4’-epimerase; GALE), and type IV (galactose mutarotase; GALM). The range of symptoms is wide, ranging from almost asymptomatic to life-threatening damage to the liver, kidneys, and brain. Severely affected patients suffer cognitive disabilities. Current treatment relies on the restriction of galactose (and its precursors such as lactose) from the diet. This is imperfect and often slows, rather than prevents, the development of symptoms. Potential new treatment approaches include enzyme replacement therapy (ERT), inhibition of galactokinase, antioxidants, phosphate supplementation, and pharmacological chaperones. ERT has been successfully applied in other diseases, but it is likely that the proteins would need to be delivered to the brain to be fully effective. This would present problems with currently available technologies. Antioxidant therapy and phosphate supplementation would treat downstream effects of the disease and not the fundamental causes. They may be useful in conjunction with galactose restriction but are unlikely to provide a complete solution for the most severely affected patients. Galactokinase inhibition has the most underpinning research with several promising compounds identified. It has yet to be tested in clinical trials. Pharmacological chaperone therapy offers the opportunity to correct protein folding and restore activity. Challenges include development of suitable assays, potential for long-term toxicity of drugs that may be taken for a lifetime, and identifying compounds that work with different disease-associated variants.

Published

2020

31. Praziquantel: An Enigmatic, Yet Effective, Drug

Author

David J. Timson

Subjects

0301 basic medicine, Drug, Voltage-dependent calcium channel, business.industry, Calcium channel, media_common.quotation_subject, 030231 tropical medicine, Schistosomiasis, Drug resistance, Pharmacology, medicine.disease, Praziquantel, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, parasitic diseases, Medicine, business, Biochemical Pharmacology, Calcium signaling, medicine.drug, media_common

Abstract

Praziquantel is a remarkably effective drug for the treatment of schistosomiasis. It has few side effects, some of which have been attributed to its inactive enantiomer. Few, if any, verified cases of drug resistance have been reported in a clinical setting. The preponderance of scientific evidence suggests that the drug works by dysregulating calcium homeostasis in the worm. Voltage-gated calcium channels have been proposed as the main pharmacological target of praziquantel, although no direct evidence of interaction with this protein is available. Here, the biochemical pharmacology of praziquantel is briefly reviewed and a hypothesis for its mechanism proposed. This hypothesis suggests that the drug works, in part, by disrupting an interaction between a voltage-gated calcium channel (SmCav1B) and an accessory protein, SmTAL1.

Published

2020

32. Antioxidant properties and global metabolite screening of the probiotic yeastSaccharomyces cerevisiaevar.boulardii

Author

Uday S. Annapure, David J. Timson, and Suprama Datta

Subjects

0301 basic medicine, chemistry.chemical_classification, Nutrition and Dietetics, Antioxidant, biology, medicine.medical_treatment, Metabolite, 030106 microbiology, Saccharomyces cerevisiae, Flavonoid, biology.organism_classification, Yeast, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Biochemistry, chemistry, Polyphenol, medicine, Vanillic acid, Metabolome, Agronomy and Crop Science, Food Science, Biotechnology

Abstract

Background: Saccharomyces cerevisiae var. boulardii is the only yeast species with probiotic properties. It is considered to have therapeutic significance in gastrointestinal disorders. In the present study, a comparative physiological study between this yeast and Saccharomyces cerevisiae (BY4742) was performed by evaluating two prominent traits of probiotic species, responses to different stress conditions and antioxidant capacity. A global metabolite profile was also developed aiming to identify which therapeutically important secondary metabolites are produced.; Results: Saccharomyces cerevisiae var. boulardii showed no significant difference in growth patterns but greater stress tolerance compared to S. cerevisiae. It also demonstrated a six- to 10-fold greater antioxidant potential (judged by the 1,1-diphenyl-2-picrylhydrazyl assay), with a 70-fold higher total phenolic content and a 20-fold higher total flavonoid content in the extracellular fraction. These features were clearly differentiated by principal component analysis and further indicated by metabolite profiling. The extracellular fraction of the S. cerevisiae var. boulardii cultures was found to be rich in polyphenolic metabolites: vanillic acid, cinnamic acid, phenyl ethyl alcohol (rose oil), erythromycin, amphetamine and vitamin B6 , which results in the antioxidant capacity of this strain.; Conclusion: The present study presents a new perspective for differentiating the two genetically related strains of yeast, S. cerevisiae and S. cerevisiae var. boulardii by assessing their metabolome fingerprints. In addition to the correlation of the phenotypic properties with the secretory metabolites of these two yeasts, the present study also emphasizes the potential to exploit S. cerevisiae var. boulardii in the industrial production of these metabolites. © 2016 Society of Chemical Industry.; © 2016 Society of Chemical Industry.

Published

2017

33. Negative Cooperativity in NAD(P)H Quinone Oxidoreductase 1 (NQO1)

Author

Karen A. Nolan, Hoda Abdel-Aal Bettley, M. Clare Caraher, Thomas A. Jowitt, Ian J. Stratford, Katherine A. Scott, David J. Timson, Clare F. Megarity, Aldo Gutierrez, Roger C. Whitehead, and Richard A. Bryce

Subjects

Dicumarol, Stereochemistry, cancer-associated proteins, Cooperativity, Ligands, 010402 general chemistry, Quinone oxidoreductase, 01 natural sciences, Biochemistry, Cofactor, Allosteric Regulation, Catalytic Domain, Cell Line, Tumor, NAD(P)H Dehydrogenase (Quinone), medicine, Humans, Enzyme Inhibitors, Binding site, Molecular Biology, biology, 010405 organic chemistry, Chemistry, protein flexibility, Organic Chemistry, Cooperative binding, Dicoumarol, enzyme cooperativity, 0104 chemical sciences, Quinone, Amino Acid Substitution, quinone oxidoreductases, biology.protein, elastic network models, Molecular Medicine, NAD+ kinase, Tumor Suppressor Protein p53, Protein Binding, medicine.drug

Abstract

NAD(P)H quinone oxidoreductase-1 (NQO1) is a homodimeric protein that acts as a detoxifying enzyme or as a chaperone protein. Dicourmarol interacts with NQO1 at the NAD(P)H binding site and can both inhibit enzyme activity and modulate the interaction of NQO1 with other proteins. We show that the binding of dicoumarol and related compounds to NQO1 generates negative cooperativity between the monomers. This does not occur in the presence of the reducing cofactor, NAD(P)H, alone. Alteration of Gly150 (but not Gly149 or Gly174) abolished the dicoumarol-induced negative cooperativity. Analysis of the dynamics of NQO1 with the Gaussian network model indicates a high degree of collective motion by monomers and domains within NQO1. Ligand binding is predicted to alter NQO1 dynamics both proximal to the ligand binding site and remotely, close to the second binding site. Thus, drug-induced modulation of protein motion might contribute to the biological effects of putative inhibitors of NQO1.

Published

2019

34. Cancer-associated variants of human NQO1: impacts on inhibitor binding and cooperativity

Author

David J. Timson and Clare F. Megarity

Subjects

Niacinamide, 0301 basic medicine, Dicumarol, Biophysics, Cooperativity, resveratrol, Resveratrol, Biochemistry, DT-diaphorase, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Oxidoreductase, Neoplasms, Enzyme Stability, NAD(P)H quinone oxidoreductase, NAD(P)H Dehydrogenase (Quinone), medicine, Humans, dicoumarol, Quinone Reductases, Molecular Biology, Research Articles, chemistry.chemical_classification, Polymorphism, Genetic, Nicotinamide, Cooperative binding, Cell Biology, Dicoumarol, cancer-associated polymorphism, Kinetics, 030104 developmental biology, Enzyme, chemistry, 030220 oncology & carcinogenesis, NAD+ kinase, negative cooperativity, Research Article, Protein Binding, medicine.drug

Abstract

Human NAD(P)H quinone oxidoreductase (DT-diaphorase, NQO1) exhibits negative cooperativity towards its potent inhibitor, dicoumarol. Here, we addressed the hypothesis that the effects of the two cancer-associated polymorphisms (p.R139W and p.P187S) may be partly mediated by their effects on inhibitor binding and negative cooperativity. Dicoumarol stabilized both variants and bound with much higher affinity for p.R139W than p.P187S. Both variants exhibited negative cooperativity towards dicoumarol; in both cases, the Hill coefficient (h) was approximately 0.5 and similar to that observed with the wild-type protein. NQO1 was also inhibited by resveratrol and by nicotinamide. Inhibition of NQO1 by resveratrol was approximately 10,000-fold less strong than that observed with the structurally similar enzyme, NRH quinine oxidoreductase 2 (NQO2). The enzyme exhibited non-cooperative behaviour towards nicotinamide, whereas resveratrol induced modest negative cooperativity (h = 0.85). Nicotinamide stabilized wild-type NQO1 and p.R139W towards thermal denaturation but had no detectable effect on p.P187S. Resveratrol destabilized the wild-type enzyme and both cancer-associated variants. Our data suggest that neither polymorphism exerts its effect by changing the enzyme’s ability to exhibit negative cooperativity towards inhibitors. However, it does demonstrate that resveratrol can inhibit NQO1 in addition to this compound’s well-documented effects on NQO2. The implications of these findings for molecular pathology are discussed.

Published

2019

35. Dynamic origins of substrate promiscuity in bacterial galactokinases

Author

Meilan Huang, Margaret McAuley, and David J. Timson

Subjects

Molecular Dynamics Simulation, 010402 general chemistry, medicine.disease_cause, 01 natural sciences, Biochemistry, Protein Structure, Secondary, Analytical Chemistry, Substrate Specificity, chemistry.chemical_compound, Galactokinase, Catalytic Domain, medicine, Escherichia coli, Humans, chemistry.chemical_classification, biology, 010405 organic chemistry, Organic Chemistry, Lactococcus lactis, Active site, Substrate (chemistry), General Medicine, biology.organism_classification, 0104 chemical sciences, Enzyme, chemistry, Galactose, biology.protein, Biocatalysis, Phosphorylation

Abstract

Galactokinase catalyses the ATP-dependent phosphorylation of galactose and structurally related sugars. The enzyme has attracted interest as a potential biocatalyst for the production of sugar 1-phosphates and several attempts have been made to broaden its specificity. In general, bacterial galactokinases have wider substrate ranges than mammalian ones. The enzymes from Escherichia coli and Lactococcus lactis have received particular attention and a number of variants with increased promiscuity have been identified. Here, we present a molecular dynamics study designed to investigate the molecular causes of the wider substrate ranges of these enzymes and their variants with particular reference to protein mobility. Some regions close to the active site of the enzyme have different structures in the bacterial enzymes compared to the human one. Alterations known to increase the substrate range (e.g. Y371H in the E. coli enzyme), tend to alter the conformation of a key α-helical region (residues 216–232 in the E. coli enzyme). The equivalent helix in the human enzyme has previously been predicted to be altered in variants which affect catalytic activity or protein stability. This helix appears to be a key region in galactokinases from a range of species and may represent an interesting target for future attempts to broaden the specificity of galactokinases.

Published

2019

36. Escherichia coliModulator of Drug Activity B (MdaB) Has Different Enzymological Properties to Eukaryote Quinone Oxidoreductases

Author

Clare F. Megarity and David J. Timson

Subjects

biology, Chemistry, Organic Chemistry, Cooperativity, Protein engineering, Dicoumarol, Quinone oxidoreductase, medicine.disease_cause, biology.organism_classification, Biochemistry, Catalysis, Enzyme catalysis, Quinone, Inorganic Chemistry, Drug Discovery, medicine, Eukaryote, Physical and Theoretical Chemistry, Escherichia coli, medicine.drug

Published

2019

37. NQO1: A target for the treatment of cancer and neurological diseases, and a model to understand loss of function disease mechanisms

Author

Noel Mesa-Torres, David J. Timson, Sarah K. Beaver, and Angel L. Pey

Subjects

0301 basic medicine, Protein Folding, Multiple Sclerosis, Allosteric regulation, Biophysics, Biochemistry, Cofactor, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Alzheimer Disease, Neoplasms, medicine, NAD(P)H Dehydrogenase (Quinone), Animals, Humans, Binding site, Molecular Biology, Loss function, Polymorphism, Genetic, biology, Chemistry, Cell biology, Pharmacological chaperone, 030104 developmental biology, Cancer cell, biology.protein, Flavin-Adenine Dinucleotide, Protein folding, NAD+ kinase, Tumor Suppressor Protein p53, 030217 neurology & neurosurgery, medicine.drug, Genome-Wide Association Study, Molecular Chaperones

Abstract

NAD(P)H quinone oxidoreductase 1 (NQO1) is a multi-functional protein that catalyses the reduction of quinones (and other molecules), thus playing roles in xenobiotic detoxification and redox balance, and also has roles in stabilising apoptosis regulators such as p53. The structure and enzymology of NQO1 is well-characterised, showing a substituted enzyme mechanism in which NAD(P)H binds first and reduces an FAD cofactor in the active site, assisted by a charge relay system involving Tyr-155 and His-161. Protein dynamics play important role in physio-pathological aspects of this protein. NQO1 is a good target to treat cancer due to its overexpression in cancer cells. A polymorphic form of NQO1 (p.P187S) is associated with increased cancer risk and certain neurological disorders (such as multiple sclerosis and Alzheimer´s disease), possibly due to its roles in the antioxidant defence. p.P187S has greatly reduced FAD affinity and stability, due to destabilization of the flavin binding site and the C-terminal domain, which leading to reduced activity and enhanced degradation. Suppressor mutations partially restore the activity of p.P187S by local stabilization of these regions, and showing long-range allosteric communication within the protein. Consequently, the correction of NQO1 misfolding by pharmacological chaperones is a viable strategy, which may be useful to treat cancer and some neurological conditions, targeting structural spots linked to specific disease-mechanisms. Thus, NQO1 emerges as a good model to investigate loss of function mechanisms in genetic diseases as well as to improve strategies to discriminate between neutral and pathogenic variants in genome-wide sequencing studies.

Published

2019

38. Phosphorylation Mechanism of N-acetyl-L-Glutamate Kinase, a QM/MM Study

Author

Meilan Huang, David J. Timson, James McClory, Gui-Xiang Hu, and Jian-Wei Zou

Subjects

Models, Molecular, Conformational change, 010304 chemical physics, Protein Conformation, Chemistry, Stereochemistry, Kinase, Substrate (chemistry), Phosphotransferases (Carboxyl Group Acceptor), 010402 general chemistry, 01 natural sciences, Molecular mechanics, 0104 chemical sciences, Surfaces, Coatings and Films, QM/MM, Protein structure, 0103 physical sciences, Glycine, Materials Chemistry, Quantum Theory, Phosphorylation, Physical and Theoretical Chemistry

Abstract

In microorganisms and plants, N-acetyl-l-glutamate kinase (NAGK) catalyzes the second step in l-arginine synthesis, the phosphorylation of N-Acetyl-l-glutamate (NAG) to give N-acetyl-l-glutamate-5-phosphate. NAGK is only present in microorganisms and plants but absent in mammals, which makes it an attractive target for antimicrobial or biocidal development. Understanding the substrate binding mode and reaction mechanism of NAGK is crucial for targeting the kinase to develop potential therapies. Here, the substrate binding mode was studied by comparing the conformational change of NAGK in the presence and in the absence of the NAG substrate based on molecular dynamics simulations. We revealed that with substrate binding, the catalytic site of the kinase involving three loops in NAGK exhibits a closed conformation, which is predominantly controlled by an interaction between Arg98 and the α-COO- of NAG. Lys41 is found to guide phosphate transfer through the interactions with the β-,γ-, and γ-phosphate oxygen atoms of adenosine 5'-triphosphate surrounded by two highly conserved glycine residues (Gly44 and Gly76), while Arg98 helps to position the NAG substrate in the catalytic site, which facilitates the phosphate transfer. Furthermore, we elucidated phosphate-transfer reaction mechanism using hybrid density functional theory-based quantum mechanics/molecular mechanics calculations (B97D/AMBER99) and found that the catalysis follows a dissociative mechanism.

Published

2019

39. Myosin Va and spermine synthase: partners in exosome transport

Author

David J. Timson

Subjects

0301 basic medicine, Gene knockdown, Messenger RNA, biology, Biophysics, Spermine, Cell Biology, medicine.disease, Biochemistry, Cell biology, Spermidine, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, MYO5A Gene, chemistry, Spermine synthase, 030220 oncology & carcinogenesis, Myosin, biology.protein, medicine, Molecular Biology, Griscelli syndrome

Abstract

A recent paper in Bioscience Reports (BSR20182189) describes the discovery of an interaction between the motor protein myosin Va and the metabolic enzyme spermine synthase. Myosin Va is a molecular motor which plays a key role in vesicle transport. Mutations in the gene which encodes this protein are associated with Griscelli syndrome type 1 and the ‘dilute’ phenotype in animals. Spermine synthase catalyzes the conversion of spermidine to spermine. This largely cytoplasmic enzyme can also be localized to the soluble fraction in exosomes. Mutations in the spermine synthase gene are associated with Snyder Robinson mental retardation syndrome. The interaction between the two proteins was detected using the yeast two hybrid method and verified by microscale thermophoresis of recombinant proteins. Knockdown of the MYO5A gene reduced the expression of mRNA coding for spermine synthase. The amount of this transcript was also reduced in cells derived from a patient with Griscelli syndrome type 1. This suggests that, in addition to a direct physical interaction between the two proteins, myosin Va also modulates the transcription of the spermine synthase gene. The mechanism for this modulation is currently unknown. These findings have implications for Griscelli syndrome type 1 and Snyder Robinson mental retardation syndrome. They also suggest that interactions between myosin Va and soluble exosome proteins such as spermine synthase may be important in the mechanism of exosome transport.

Published

2019

40. Fructose 1,6-bisphosphatase: getting the message across

Author

David J. Timson

Subjects

0301 basic medicine, Swine, Allosteric regulation, renal cancer, Biophysics, Fructose 1,6-bisphosphatase, allosteric enzyme, AMP binding, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Commentaries, Catalytic Domain, Animals, Humans, Glycolysis, fructose 1,6-bisphosphatase deficiency, Molecular Biology, chemistry.chemical_classification, type II diabetes, Binding Sites, biology, Active site, Fructose, Cell Biology, Adenosine Monophosphate, Recombinant Proteins, Fructose-Bisphosphatase, Enzyme Activation, 030104 developmental biology, Enzyme, gluconeogenesis, chemistry, Allosteric enzyme, 030220 oncology & carcinogenesis, Mutation, biology.protein, Commentary, Mutagenesis, Site-Directed, FBPase, Sequence Alignment

Abstract

Fructose 1,6-bisphosphatase (FBPase) is a key enzyme in gluconeogenesis. It is a potential drug target in the treatment of type II diabetes. The protein is also associated with a rare inherited metabolic disease and some cancer cells lack FBPase activity which promotes glycolysis facilitating the Warburg effect. Thus, there is interest in both inhibiting the enzyme (for diabetes treatment) and restoring its activity (in relevant cancers). The mammalian enzyme is tetrameric, competitively inhibited by Fructose 2,6-bisphosphate and negatively allosterically regulated by AMP. This allosteric regulation requires information transmission between the AMP binding site and the active site of the enzyme. A recent paper by Topaz et al. (Bioscience Reports (2019) 39, pii:BSR20180960) has added additional detail to our understanding of this information transmission process. Two residues in the AMP binding site (Lys112 and Tyr113) were shown to be involved in initiating the message between the two sites. This tyrosine residue has recently be shown to be important with protein’s interaction with the antidiabetic drug metformin. A variant designed to increase metal ion affinity (M248D) resulted in a five-fold increase in enzymatic activity. Interestingly alterations of two residues at the subunit interfaces (Tyr164 and Met177) resulted in increased responsiveness to AMP. Overall, these findings may have implications in the design of novel FBPase inhibitors or activators.

Published

2019

41. Characterization of Calcium-Binding Proteins from Parasitic Worms

Author

Charlotte M, Thomas and David J, Timson

Subjects

Models, Molecular, Pharmaceutical Preparations, Calcium-Binding Proteins, Animals, Calcium Signaling, Helminth Proteins, Fasciola hepatica, Protein Multimerization, Protein Binding

Abstract

Parasitic diseases caused by helminths (worms) represent a major burden on humanity with hundreds of millions of people infected worldwide. However, there are relatively few drugs to treat these diseases, and resistance is emerging to some of these. Therefore, there is a pressing need to characterize proteins from helminths as potential drug targets. Calcium signalling proteins represent attractive targets due to the vital nature of properly regulated calcium-mediated signalling and the presence of unusual calcium-binding proteins in helminths. Here we present methods to characterize these proteins in terms of their ion-binding properties, drug-binding properties, and oligomeric state, including a method to correct for the effects of non-spherical proteins in analytical gel filtration. In addition we present an overview of their recombinant expression and purification and methods to predict their structures.

Published

2019

42. Characterization of Calcium-Binding Proteins from Parasitic Worms

Author

David J. Timson and Charlotte M. Thomas

Subjects

0301 basic medicine, Recombinant expression, Native gel electrophoresis, EF hand, 030231 tropical medicine, Protein modelling, Computational biology, Biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Calcium-binding protein, parasitic diseases, Helminths, Calcium signaling

Abstract

Parasitic diseases caused by helminths (worms) represent a major burden on humanity with hundreds of millions of people infected worldwide. However, there are relatively few drugs to treat these diseases, and resistance is emerging to some of these. Therefore, there is a pressing need to characterize proteins from helminths as potential drug targets. Calcium signalling proteins represent attractive targets due to the vital nature of properly regulated calcium-mediated signalling and the presence of unusual calcium-binding proteins in helminths. Here we present methods to characterize these proteins in terms of their ion-binding properties, drug-binding properties, and oligomeric state, including a method to correct for the effects of non-spherical proteins in analytical gel filtration. In addition we present an overview of their recombinant expression and purification and methods to predict their structures.

Published

2019

43. NAD(P)H quinone oxidoreductase (NQO1): an enzyme which needs just enough mobility, in just the right places

Author

David J. Timson, Clare F. Megarity, and Angel L. Pey

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, alpha-Helical, Dicumarol, Biophysics, Gene Expression, Quinone oxidoreductase, Biochemistry, Cofactor, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Catalytic Domain, Neoplasms, Enzyme Stability, medicine, NAD(P)H Dehydrogenase (Quinone), Humans, Protein Interaction Domains and Motifs, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Cooperative binding, Cell Biology, Dicoumarol, 030104 developmental biology, Enzyme, chemistry, 030220 oncology & carcinogenesis, Cancer cell, Mutation, biology.protein, Flavin-Adenine Dinucleotide, Protein Conformation, beta-Strand, NAD+ kinase, Protein Multimerization, Xenobiotic, medicine.drug, Protein Binding

Abstract

NAD(P)H quinone oxidoreductase 1 (NQO1) catalyses the two electron reduction of quinones and a wide range of other organic compounds. Its physiological role is believed to be partly the reduction of free radical load in cells and the detoxification of xenobiotics. It also has non-enzymatic functions stabilising a number of cellular regulators including p53. Functionally, NQO1 is a homodimer with two active sites formed from residues from both polypeptide chains. Catalysis proceeds via a substituted enzyme mechanism involving a tightly bound FAD cofactor. Dicoumarol and some structurally related compounds act as competitive inhibitors of NQO1. There is some evidence for negative cooperativity in quinine oxidoreductases which is most likely to be mediated at least in part by alterations to the mobility of the protein. Human NQO1 is implicated in cancer. It is often over-expressed in cancer cells and as such is considered as a possible drug target. Interestingly, a common polymorphic form of human NQO1, p.P187S, is associated with an increased risk of several forms of cancer. This variant has much lower activity than the wild-type, primarily due to its substantially reduced affinity for FAD which results from lower stability. This lower stability results from inappropriate mobility of key parts of the protein. Thus, NQO1 relies on correct mobility for normal function, but inappropriate mobility results in dysfunction and may cause disease., This work was supported by the Junta de Andalucía [grant number P11-CTS-07187 (to A.L.P.)].

Published

2019

44. UDP-N-acetyl-D-galactosamine:polypeptide N-acetylgalactosaminyltransferase- 6 (pp-GalNAc-T6): Role in Cancer and Prospects as a Drug Target

Author

David J. Timson and Samantha Banford

Subjects

0301 basic medicine, Cancer Research, Glycosylation, Polypeptide N-acetylgalactosaminyltransferase, Biology, Metastasis, Malignant transformation, Cell membrane, 03 medical and health sciences, chemistry.chemical_compound, Neoplasms, Drug Discovery, medicine, Humans, Molecular Targeted Therapy, Enzyme Inhibitors, Pharmacology, Mucin, Cancer, medicine.disease, carbohydrates (lipids), 030104 developmental biology, medicine.anatomical_structure, Oncology, Biochemistry, chemistry, Cancer cell, N-Acetylgalactosaminyltransferases, lipids (amino acids, peptides, and proteins)

Abstract

UDP-N-acetyl-D-galactosamine: polypeptide N-acetylgalactosaminyl transferase-6 (pp-GalNAc-T6) is a member of the N-acetyl-D-galactosamine transferase family. It catalyzes the addition of N-acetyl-D-galactosamine to proteins, often the first step in O-glycosylation of proteins. Glycosylated proteins play important roles in vivo in the cell membrane. These are often involved in cell-cell adhesion, cytoskeleton regulation and immune recognition. pp-GalNAc-T6 has been shown to be upregulated in a number of types of cancer. Abnormally glycosylated forms of mucin 1 (a substrate of the enzyme), are used clinically as a biomarker for breast cancer. There is potential for other products of the pp-GalNAc- T6 catalyzed reaction to be used. It is also possible that pp-GalNAc-T6 itself could be used as a biomarker, since levels of this protein tend to be low in non-malignant tissues. pp- GalNAc-T6 has been implicated in malignant transformation and metastasis of cancer cells. As such, it has considerable potential as a target for chemotherapy. To date, no selective inhibitors of the enzyme have been identified. However, general inhibitors of the enzyme family result in reduced cell surface O-linked glycosylation and induce apoptosis in cultured cells. Thus, a selective inhibitor of pp-GalNAc-T6 is likely to target cancer cells and could be developed into a novel anticancer therapy.

Published

2016

45. IQGAP1 Interaction with RHO Family Proteins Revisited

Author

Lutz Schmitt, Dieter Willbold, Kazem Nouri, Lothar Gremer, Radovan Dvorsky, Ehsan Amin, David J. Timson, Eyad K. Fansa, and Mohammad Reza Ahmadian

Subjects

0301 basic medicine, Scaffold protein, GTPase-activating protein, C-terminus, RAC1, Cell Biology, CDC42, Biology, Biochemistry, Protein–protein interaction, Cell biology, 03 medical and health sciences, 030104 developmental biology, IQGAP1, Binding site, Molecular Biology

Abstract

IQ motif-containing GTPase activating protein 1 (IQGAP1) plays a central role in the physical assembly of relevant signaling networks that are responsible for various cellular processes, including cell adhesion, polarity, and transmigration. The RHO family proteins CDC42 and RAC1 have been shown to mainly interact with the GAP-related domain (GRD) of IQGAP1. However, the role of its RASGAP C-terminal (RGCT) and C-terminal domains in the interactions with RHO proteins has remained obscure. Here, we demonstrate that IQGAP1 interactions with RHO proteins underlie a multiple-step binding mechanism: (i) a high affinity, GTP-dependent binding of RGCT to the switch regions of CDC42 or RAC1 and (ii) a very low affinity binding of GRD and a C terminus adjacent to the switch regions. These data were confirmed by phosphomimetic mutation of serine 1443 to glutamate within RGCT, which led to a significant reduction of IQGAP1 affinity for CDC42 and RAC1, clearly disclosing the critical role of RGCT for these interactions. Unlike CDC42, an extremely low affinity was determined for the RAC1-GRD interaction, suggesting that the molecular nature of IQGAP1 interaction with CDC42 partially differs from that of RAC1. Our study provides new insights into the interaction characteristics of IQGAP1 with RHO family proteins and highlights the complementary importance of kinetic and equilibrium analyses. We propose that the ability of IQGAP1 to interact with RHO proteins is based on a multiple-step binding process, which is a prerequisite for the dynamic functions of IQGAP1 as a scaffolding protein and a critical mechanism in temporal regulation and integration of IQGAP1-mediated cellular responses.

Published

2016

46. Natural Small Molecules as Stabilizers and Activators of Cancer-Associated NQO1 Polymorphisms

Author

David J. Timson, Angel L. Pey, Encarnación Medina-Carmona, and Clare F. Megarity

Subjects

0301 basic medicine, Stereochemistry, Clinical Biochemistry, Antineoplastic Agents, Biology, Detoxification enzymes, Quinone oxidoreductase, Antioxidants, law.invention, 03 medical and health sciences, law, Neoplasms, Drug Discovery, NAD(P)H Dehydrogenase (Quinone), Animals, Humans, Genetic Predisposition to Disease, Molecular Targeted Therapy, Pharmacology, Polymorphism, Genetic, Small molecule, 030104 developmental biology, Drug Design, Cancer research, Molecular Medicine, Suppressor, NAD+ kinase, Cancer development, Intracellular

Abstract

NAD(P)H: quinone oxidoreductase 1 (NQO1) is an antioxidant and detoxifying enzyme involved in the two-electron reduction of a wide variety of quinones. As a non-enzymatic function, it is involved in the stabilization of several tumour suppressors such as p53, p33 and p73α. NQO1 is overexpressed in several types of tumours, and two common polymorphisms are associated with increased cancer risk, making NQO1 a potential target for new cancer treatments. Here we review the structural and enzymological properties of NQO1, as well as its roles in cancer development and treatment. Particularly, we focus on recent developments on the understanding of the molecular basis leading to loss-of-function in cancer-associated polymorphisms, and propose new approaches to target these molecular defects to develop new pharmacological agents to rescue them. We will focus on pharmacological therapies aimed at correcting the abnormal properties of polymorphic proteins (such as protein stability and dynamics) and modulating intracellular factors leading to loss-of-function (such as accelerated proteasomal degradation).

Published

2016

47. Modulating Mobility: a Paradigm for Protein Engineering?

Author

Margaret McAuley and David J. Timson

Subjects

Models, Molecular, 0301 basic medicine, Protein Conformation, Allosteric regulation, Bioengineering, Cooperativity, Molecular Dynamics Simulation, Ligands, Protein Engineering, Applied Microbiology and Biotechnology, Biochemistry, 03 medical and health sciences, Molecular dynamics, Catalytic Domain, Molecular Biology, chemistry.chemical_classification, Protein function, Binding Sites, biology, Proteins, Active site, General Medicine, Protein engineering, 030104 developmental biology, Enzyme, chemistry, Biocatalysis, biology.protein, Biophysics, Function (biology), Protein Binding, Biotechnology

Abstract

Proteins are highly mobile structures. In addition to gross conformational changes occurring on, for example, ligand binding, they are also subject to constant thermal motion. The mobility of a protein varies through its structure and can be modulated by ligand binding and other events. It is becoming increasingly clear that this mobility plays an important role in key functions of proteins including catalysis, allostery, cooperativity, and regulation. Thus, in addition to an optimum structure, proteins most likely also require an optimal dynamic state. Alteration of this dynamic state through protein engineering will affect protein function. A dramatic example of this is seen in some inherited metabolic diseases where alternation of residues distant from the active site affects the mobility of the protein and impairs function. We postulate that using molecular dynamics simulations, experimental data or a combination of the two, it should be possible to engineer the mobility of active sites. This may be useful in, for example, increasing the promiscuity of enzymes. Thus, a paradigm for protein engineering is suggested in which the mobility of the active site is rationally modified. This might be combined with more "traditional" approaches such as altering functional groups in the active site.

Published

2016

48. Characterization of Cd36_03230p, a putative vanillin dehydrogenase from Candida dubliniensis

Author

Uday S. Annapure, Suprama Datta, and David J. Timson

Subjects

0301 basic medicine, chemistry.chemical_classification, biology, Chemistry, General Chemical Engineering, Vanillin, Aldehyde dehydrogenase, Active site, General Chemistry, biology.organism_classification, Cofactor, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Enzyme, Biochemistry, Vanillin dehydrogenase, biology.protein, Isoleucine, Candida dubliniensis

Abstract

A coding sequence (CD36-03230) from the yeast Candida dubliniensis had been previously annotated as a vanillin dehydrogenase (VDH). The corresponding protein (CD36-03230p) was recombinantly expressed in Escherichia coli and analysed. The protein is most likely a tetramer in solution as judged by crosslinking and gel filtration experiments. CD36-03230p is an active aldehyde dehydrogenase favouring cyclic and aromatic substrates. Positive cooperativity and substrate inhibition were observed with some substrates. The redox cofactor NADP+ and substrates affected the thermal stability of the protein. Interestingly, the enzyme had no detectable activity with vanillin suggesting that the annotation is incorrect. It has been previously hypothesized that a methionine residue at a key position in the active site of yeast aldehyde dehydrogenases sterically hinders cyclic substrates and restricts specificity to aliphatic aldehydes. Molecular modeling of CD36-03230p demonstrates that it has an isoleucine residue (Ile-156) at this position, further strengthening this hypothesis.

Published

2016

49. Type IV galactosemia

Author

David J. Timson

Subjects

0301 basic medicine, Galactosemias, medicine.medical_specialty, education.field_of_study, Chemistry, Galactosemia, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, Internal medicine, medicine, Humans, Galactose mutarotase, education, 030217 neurology & neurosurgery, Genetics (clinical)

Published

2018

50. Water-mediated network in the resistance mechanism of fosfomycin

Author

Jun Tang Lin, James McClory, Meilan Huang, Jian Zhang, and David J. Timson

Subjects

0301 basic medicine, Reaction mechanism, Protein Conformation, General Physics and Astronomy, Fosfomycin, Physics and Astronomy(all), Molecular Dynamics Simulation, 01 natural sciences, Molecular mechanics, 03 medical and health sciences, Protein structure, Bacterial Proteins, Catalytic Domain, 0103 physical sciences, medicine, Nucleotide, Physical and Theoretical Chemistry, Phosphorylation, chemistry.chemical_classification, 010304 chemical physics, Kinase, Chemistry, Water, Drug Resistance, Microbial, Hydrogen Bonding, Associative substitution, biochemical phenomena, metabolism, and nutrition, Streptomyces, 030104 developmental biology, Models, Chemical, Mutation, Biophysics, Quantum Theory, Protein Kinases, medicine.drug

Abstract

Fosfomycin Resistance Kinase A (FomA) catalyzes the phosphorylation of fosfomycin, which is an effective antibiotic for treating urinary tract infections. Understanding the chemical reaction mechanism is essential for developing strategies to counter the resistance of fosfomycin in clinical settings. Here the catalytic mechanism of FomA was investigated using molecular dynamic simulations in conjunction with quantum mechanics/molecular mechanics calculations (B97d/AMBER99). Our QM/MM study disclosed that the phosphorylation reaction catalyzed by FomA follows a dissociative mechanism, in contrast to the previously proposed associative mechanism. In addition, we found that His58, a characteristic residue in the AAK family, plays a key role in positioning the phosphate group of fosfomycin in the transition state. Molecular dynamic simulations revealed the important roles of Lys9 and Lys18 in arranging the nucleotide for phosphate transfer. Furthermore, we identified a four-membered water network mediated by Asp171 and Ser13 that is critical in ordering ATP for phosphate transfer. The active structure and reaction mechanism of FomA will provide valuable insights for developing new strategies to tackle the resistance to Fosfomycin-based antibiotic therapies.

Published

2018