Your search keyword '"Adrian D. Hall"' showing total 5 results

1. 62Cu-PTSM and PET used for the assessment of angiotensin II-induced blood flow changes in patients with colorectal liver metastases

Author

John Mundy, T G Allen-Mersh, Jamal Zweit, R. J. Ott, M M Davies, M J Dworkin, Maggie A Flower, D Burke, V. Ralph McCready, P. Carnochan, Adrian D. Hall, and H. Young

Subjects

Thiosemicarbazones, Zinc Radioisotopes, Hemodynamics, Image Processing, Computer-Assisted, Organometallic Compounds, Humans, Vasoconstrictor Agents, Medicine, Distribution (pharmacology), Radiology, Nuclear Medicine and imaging, Reproducibility, medicine.diagnostic_test, business.industry, Angiotensin II, Liver Neoplasms, Reproducibility of Results, General Medicine, Blood flow, Copper Radioisotopes, Liver, Positron emission tomography, Calibration, Cardiovascular agent, Radiopharmaceuticals, Colorectal Neoplasms, business, Nuclear medicine, Algorithms, Emission computed tomography, Liver Circulation, Tomography, Emission-Computed

Abstract

The aim of this study was to establish a quantitative positron emission tomography (PET) method for investigating angiotensin II (AII)-induced changes in blood flow distribution in the liver. This was in order to evaluate the role of vascular manipulation applied to locoregional chemotherapy treatment in patients with colorectal liver metastases. The tracer selected was copper-62 (II) pyruvaldehyde bis-(N4-methyl)thiosemicarbazone (62Cu-PTSM), which exhibits high first-pass extraction and tissue retention following intra-arterial administration. The short half-life of the tracer and its availability from a 62Zn/62Cu generator enabled short-interval repeat PET scans on patients in a single imaging session. Distribution of tracer within the liver was imaged in a single view using a PET camera with rotating large-area detectors. By optimisation of the acquisition protocol, it was possible to acquire sufficient data to produce good-quality images and to quantify tracer uptake with an accuracy of

Published

2000

2. The interaction of hydroxypyridinones with human serum transferrin and ovotransferrin

Author

Stefano Cavallo, Victoria Saez, Simonetta Stefanini, Emilia Chiancone, Robert C. Hider, and Adrian D. Hall

Subjects

Denticity, Pyridones, Iron, Kinetics, Biochemistry, Inorganic Chemistry, Metal, Structure-Activity Relationship, Humans, Chelation, Chelating Agents, chemistry.chemical_classification, Iron Radioisotopes, Chromatography, biology, Transferrin saturation, Transferrin, Ovotransferrin, Ligand (biochemistry), chemistry, visual_art, visual_art.visual_art_medium, biology.protein, Apoproteins, Conalbumin, Nuclear chemistry

Abstract

The interaction of hydroxypyridinones with human serum transferrin and ovotransferrin has been studied by analyzing the distribution of iron between the chelator and the proteins as a function of both ligand concentration and transferrin saturation. The kinetics of iron removal by 3-hydroxypyridin-4-ones from both transferrins is slow; in ovotransferrin it appears to be monophasic, in contrast to that observed for serum transferrin. After 24 hours incubation at a 40:1 chelator:protein molar ratio, the percentage of iron removed from Fe(III)-ovotransferrin is 50%–60%, and is somewhat higher in the case of serum transferrin, in line with the respective affinity constants for the metal. The 3-hydroxypyridin-2-ones and the 3-hydroxypyran-4-ones, both of which have lower affinities for Fe(III), remove smaller proportions of the metal. The percentage of desaturation obtained with bidentate and hexadentate pyridinones appears to be similar for both transferrin classes at chelator:protein molar ratios from 40:1. The degree of transferrin saturation influences the extent of chelator mediated iron mobilization in the case of serum transferrin, but not of ovotransferrin. 59 Fe competition studies demonstrate that bidentate pyridin-4-ones are capable of donating iron to serum apotransferrin; the relative concentrations of ligand and protein influence the distribution of iron because their effective binding constants (at pH 7.4) for Fe(III) are similar.

Published

1991

3. Charge description of base-catalyzed alcoholysis of aryl phosphodiesters: a ribonuclease model

Author

Adrian D. Hall, Andrew Williams, and Andrew M. Davis

Subjects

chemistry.chemical_classification, biology, Base (chemistry), Stereochemistry, Chemistry, Aryl, Charge (physics), General Chemistry, Biochemistry, Combinatorial chemistry, Catalysis, chemistry.chemical_compound, Colloid and Surface Chemistry, Reaction rate constant, Enzyme model, biology.protein, Ribonuclease

Published

1988

4. Leaving group dependence in the phosphorylation of Escherichia coli alkaline phosphatase by monophosphate esters

Author

Adrian D. Hall and Andrew Williams

Subjects

Steric effects, chemistry.chemical_classification, Chemistry, Stereochemistry, Metaphosphate, Aryl, Leaving group, Substrate (chemistry), Alkaline Phosphatase, Biochemistry, Substrate Specificity, chemistry.chemical_compound, Kinetics, Non-competitive inhibition, Organophosphorus Compounds, Escherichia coli, Enzyme kinetics, Phosphorylation, Alkyl, Protein Binding

Abstract

Values of kcat and Km have been measured for the Escherichia coli alkaline phosphatase catalyzed hydrolysis of 18 aryl and 12 alkyl monophosphate esters at pH 8.00 and 25 degrees C. A Bronsted plot of log (kcat/Km) (M-1 s-1) vs. the pK of the leaving hydroxyl group exhibits two regression lines: log (kcat/Km) = -0.19 (+/- 0.02) pKArOH + 8.14 (+/- 0.15) log (kcat/Km) = -0.19 (+/- 0.01) pKROH + 5.89 (+/- 0.17) Alkyl phosphates with aryl or large lipophilic side chains are not correlated by the above equations and occupy positions intermediate between the two lines. The observed change in effective charge on the leaving oxygen of the ester (-0.2) is very small, consistent with substantial electrophilic participation of the enzyme with this atom. Cyclohexylammonium ion is a noncompetitive inhibitor against 4-nitrophenyl phosphate substrate at pH 8.00, and neutral phenol is a competitive inhibitor (Ki = 82.6 mM); these data and the 100-fold larger reactivity of aryl over alkyl esters are consistent with the existence of a lipophilic binding site for the leaving group of the substrate. The absence of a major steric effect in kcat/Km for substituted aryl esters confirms that the leaving group in the enzyme--substrate complex points away from the surface of the enzyme. Arguments are advanced to exclude a dissociative mechanism (involving a metaphosphate ion) for the enzyme-catalyzed substitution at phosphorus.

Published

1986

5. Effective charge in the controlling transition-state in the phosphorylation of Escherichia coli alkaline phosphatase

Author

Andrew Williams and Adrian D. Hall

Subjects

Transition (genetics), Hydroxy group, Inorganic chemistry, medicine.disease_cause, Medicinal chemistry, Effective nuclear charge, chemistry.chemical_compound, Oxygen atom, chemistry, medicine, Molecular Medicine, Alkaline phosphatase, Phosphorylation, Escherichia coli

Abstract

The Bronsted relationship for the leaving hydroxy group in the phosphorylatin of alkaline phosphatase has a β value of –0.19; by comparison with βeq. for the overall equilibrium (–1.35) there is little change in the charge on the leaving oxygen atom between the ground- and transition-states.

Published

1985