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2. Prototheca zopfiimastitis in a herd of dairy cows

Author

Hodges Rt, Wallace Nm, Holland Jt, and Neilson Fj

Subjects
Veterinary medicine, Prototheca zopfii, General Veterinary, biology, food and beverages, General Medicine, Prototheca, Culling, biology.organism_classification, medicine.disease, Milking, Mastitis, medicine.anatomical_structure, Animal science, Environmental water, medicine, Herd, Udder
Abstract

Mastitis caused by the colourless alga Prototheca zopfii was diagnosed in 17 of 120 cows in a dairy herd. Infection occurred in animals varying from 3-14 years old and was present in one to four quarters of each cow. Nine cases were associated with clinical mastitis characterised by the presence in milk of flakes or small clots. Somatic cell counts consistent with subclinical mastitis (>500 x 10(3) cells/ml) were recorded in five of the eight remaining cows. Histological examination of udder tissue showed the presence of granulomatous lesions associated with the presence of Prototheca. The problem was identified and controlled by repeated microbiological examination of milk samples from all lactating cows and immediate culling of infected animals. P. zopfii was also recovered from environmental water samples on this farm. It is suggested that infection may have occurred as a result of teat sores caused by trauma from a milking machine, and the tendency for cows to lay down on a race, the surface of which was sometimes flooded by drain water in which Prototheca were present.

Published
1985
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4. Arsenic Speciation in Bituminous Coal Fly Ash and Transformations in Response to Redox Conditions.

Author

Deonarine A, Kolker A, Foster AL, Doughten MW, Holland JT, and Bailoo JD

Subjects
Adsorption, Coal, Oxidation-Reduction, Arsenic chemistry, Coal Ash chemistry
Abstract

The risk of the mobilization of coal ash into the environment has highlighted the need for the assessment of the environmental behavior of coal ash, particularly with respect to toxic trace elements such as arsenic (As). Here, we examined As speciation in coal fly ash samples and transformations in response to aquatic redox conditions. X-ray absorption spectroscopy indicated that 92-97% of total As occurred as As(V), with the remainder present as As(III). Major As-bearing hosts in unamended ashes were glass, iron (oxyhydr)oxides, and calcium arsenate. Oxic leaching resulted in immediate As mobilization to the aqueous phase, reprecipitation of As-iron ferrihydrite, and As adsorption to mineral surfaces. Under anoxic conditions, the (reductive) dissolution of As-bearing phases such as iron ferrihydrite resulted in increased dissolved As compared to oxic conditions and reprecipitation of iron arsenate. Overall, As in coal ash is not environmentally stable and can participate in local biogeochemical cycles.

Published
2016
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6. Visualization of glutamine transporter activities in living cells using genetically encoded glutamine sensors.

Author

Gruenwald K, Holland JT, Stromberg V, Ahmad A, Watcharakichkorn D, and Okumoto S

Subjects
Animals, Carrier Proteins chemistry, Cell Line, Enzyme Activation, Fluorescence Resonance Energy Transfer methods, Glutamine chemistry, Hydrogen-Ion Concentration, Luminescent Proteins metabolism, Protein Binding, Protein Conformation, Substrate Specificity, Biosensing Techniques, Carrier Proteins metabolism, Glutamine metabolism, Molecular Imaging
Abstract

Glutamine plays a central role in the metabolism of critical biological molecules such as amino acids, proteins, neurotransmitters, and glutathione. Since glutamine metabolism is regulated through multiple enzymes and transporters, the cellular glutamine concentration is expected to be temporally dynamic. Moreover, differentiation in glutamine metabolism between cell types in the same tissue (e.g. neuronal and glial cells) is often crucial for the proper function of the tissue as a whole, yet assessing cell-type specific activities of transporters and enzymes in such heterogenic tissue by physical fractionation is extremely challenging. Therefore, a method of reporting glutamine dynamics at the cellular level is highly desirable. Genetically encoded sensors can be targeted to a specific cell type, hence addressing this knowledge gap. Here we report the development of Föster Resonance Energy Transfer (FRET) glutamine sensors based on improved cyan and yellow fluorescent proteins, monomeric Teal Fluorescent Protein (mTFP)1 and venus. These sensors were found to be specific to glutamine, and stable to pH-changes within a physiological range. Using cos7 cells expressing the human glutamine transporter ASCT2 as a model, we demonstrate that the properties of the glutamine transporter can easily be analyzed with these sensors. The range of glutamine concentration change in a given cell can also be estimated using sensors with different affinities. Moreover, the mTFP1-venus FRET pair can be duplexed with another FRET pair, mAmetrine and tdTomato, opening up the possibility for real-time imaging of another molecule. These novel glutamine sensors will be useful tools to analyze specificities of glutamine metabolism at the single-cell level.

Published
2012
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7. Rational redesign of glucose oxidase for improved catalytic function and stability.

Author

Holland JT, Harper JC, Dolan PL, Manginell MM, Arango DC, Rawlings JA, Apblett CA, and Brozik SM

Subjects
Aspergillus niger enzymology, Biocatalysis, Enzyme Stability, Glucose Oxidase chemistry, Glucose Oxidase genetics, Models, Molecular, Mutagenesis, Site-Directed, Penicillium enzymology, Substrate Specificity, Glucose Oxidase metabolism
Abstract

Glucose oxidase (GOx) is an enzymatic workhorse used in the food and wine industries to combat microbial contamination, to produce wines with lowered alcohol content, as the recognition element in amperometric glucose sensors, and as an anodic catalyst in biofuel cells. It is naturally produced by several species of fungi, and genetic variants are known to differ considerably in both stability and activity. Two of the more widely studied glucose oxidases come from the species Aspergillus niger (A. niger) and Penicillium amagasakiense (P. amag.), which have both had their respective genes isolated and sequenced. GOx from A. niger is known to be more stable than GOx from P. amag., while GOx from P. amag. has a six-fold superior substrate affinity (K(M)) and nearly four-fold greater catalytic rate (k(cat)). Here we sought to combine genetic elements from these two varieties to produce an enzyme displaying both superior catalytic capacity and stability. A comparison of the genes from the two organisms revealed 17 residues that differ between their active sites and cofactor binding regions. Fifteen of these residues in a parental A. niger GOx were altered to either mirror the corresponding residues in P. amag. GOx, or mutated into all possible amino acids via saturation mutagenesis. Ultimately, four mutants were identified with significantly improved catalytic activity. A single point mutation from threonine to serine at amino acid 132 (mutant T132S, numbering includes leader peptide) led to a three-fold improvement in k(cat) at the expense of a 3% loss of substrate affinity (increase in apparent K(M) for glucose) resulting in a specify constant (k(cat)/K(M)) of 23.8 (mM(-1) · s(-1)) compared to 8.39 for the parental (A. niger) GOx and 170 for the P. amag. GOx. Three other mutant enzymes were also identified that had improvements in overall catalysis: V42Y, and the double mutants T132S/T56V and T132S/V42Y, with specificity constants of 31.5, 32.2, and 31.8 mM(-1) · s(-1), respectively. The thermal stability of these mutants was also measured and showed moderate improvement over the parental strain.

Published
2012
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8. Engineering of glucose oxidase for direct electron transfer via site-specific gold nanoparticle conjugation.

Author

Holland JT, Lau C, Brozik S, Atanassov P, and Banta S

Subjects
Catalytic Domain, Enzymes, Immobilized chemistry, Enzymes, Immobilized metabolism, Glucose analysis, Glucose metabolism, Glucose Oxidase chemistry, Glucose Oxidase metabolism, Models, Molecular, Protein Engineering, Sulfhydryl Compounds chemistry, Aspergillus niger enzymology, Biosensing Techniques methods, Enzymes, Immobilized genetics, Glucose Oxidase genetics, Gold chemistry, Nanoparticles chemistry
Abstract

Optimizing the electrical communication between enzymes and electrodes is critical in the development of biosensors, enzymatic biofuel cells, and other bioelectrocatalytic applications. One approach to address this limitation is the attachment of redox mediators or relays to the enzymes. Here we report a simple genetic modification of a glucose oxidase enzyme to display a free thiol group near its active site. This facilitates the site-specific attachment of a maleimide-modified gold nanoparticle to the enzyme, which enables direct electrical communication between the conjugated enzyme and an electrode. Glucose oxidase is of particular interest in biofuel cell and biosensor applications, and the approach of "prewiring" enzyme conjugates in a site-specific manner will be valuable in the continued development of these systems., (© 2011 American Chemical Society)

Published
2011
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9. Unilateral facial myokymia in a dog with an intracranial meningioma.

Author

Holland CT, Holland JT, and Rozmanec M

Subjects
Animals, Dogs, Electromyography veterinary, Facial Nerve Diseases complications, Facial Nerve Diseases pathology, Facial Paralysis complications, Facial Paralysis pathology, Fatal Outcome, Histocytochemistry veterinary, Male, Meningeal Neoplasms complications, Meningeal Neoplasms pathology, Meningioma complications, Meningioma pathology, Dog Diseases pathology, Facial Nerve Diseases veterinary, Facial Paralysis veterinary, Meningeal Neoplasms veterinary, Meningioma veterinary
Abstract

A 23-month-old castrated male Cavalier King Charles spaniel was evaluated because of a 6-month history of unusual rippling/undulating movements of the right facial muscles that were continuous and persisted during sleep. Neurological examination revealed narrowing of the right palpebral fissure and unilateral right-sided facial myokymia that was characterised by myokymic, and to a lesser degree, neuromyotonic discharges on concentric needle electromyographic examination. After persisting unchanged for almost 2.5 years from its onset, the facial myokymia gradually disappeared over a 6-month period concomitant with the emergence of a persistent ipsilateral facial paralysis and head tilt. At 5 years and 9 months after the first examination, signs of ipsilateral lacrimal, pharyngeal and laryngeal dysfunction became evident and the dog was euthanased. Postmortem examination identified a malignant (WHO grade III) meningioma in the right cerebellopontomedullary angle that compressed the ventrolateral cranial medulla, effaced the jugular foramen and internal acoustic meatus and extended into the facial canal of the petrous temporal bone. Novel findings were the unique observation of isolated unilateral facial myokymia preceding diagnosis of a meningioma affecting facial nerve function within the caudal cranial fossa and the remarkably long duration of neurological signs (75 months) attributable to the neoplasm.

Published
2010
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10. The Q-cycle reviewed: How well does a monomeric mechanism of the bc(1) complex account for the function of a dimeric complex?

Author

Crofts AR, Holland JT, Victoria D, Kolling DR, Dikanov SA, Gilbreth R, Lhee S, Kuras R, and Kuras MG

Subjects
Binding Sites, Dimerization, Homeostasis, Kinetics, Models, Molecular, Oxidation-Reduction, Protein Conformation, Electron Transport Complex III chemistry, Electron Transport Complex III metabolism
Abstract

Recent progress in understanding the Q-cycle mechanism of the bc(1) complex is reviewed. The data strongly support a mechanism in which the Q(o)-site operates through a reaction in which the first electron transfer from ubiquinol to the oxidized iron-sulfur protein is the rate-determining step for the overall process. The reaction involves a proton-coupled electron transfer down a hydrogen bond between the ubiquinol and a histidine ligand of the [2Fe-2S] cluster, in which the unfavorable protonic configuration contributes a substantial part of the activation barrier. The reaction is endergonic, and the products are an unstable ubisemiquinone at the Q(o)-site, and the reduced iron-sulfur protein, the extrinsic mobile domain of which is now free to dissociate and move away from the site to deliver an electron to cyt c(1) and liberate the H(+). When oxidation of the semiquinone is prevented, it participates in bypass reactions, including superoxide generation if O(2) is available. When the b-heme chain is available as an acceptor, the semiquinone is oxidized in a process in which the proton is passed to the glutamate of the conserved -PEWY- sequence, and the semiquinone anion passes its electron to heme b(L) to form the product ubiquinone. The rate is rapid compared to the limiting reaction, and would require movement of the semiquinone closer to heme b(L) to enhance the rate constant. The acceptor reactions at the Q(i)-site are still controversial, but likely involve a "two-electron gate" in which a stable semiquinone stores an electron. Possible mechanisms to explain the cyt b(150) phenomenon are discussed, and the information from pulsed-EPR studies about the structure of the intermediate state is reviewed. The mechanism discussed is applicable to a monomeric bc(1) complex. We discuss evidence in the literature that has been interpreted as shown that the dimeric structure participates in a more complicated mechanism involving electron transfer across the dimer interface. We show from myxothiazol titrations and mutational analysis of Tyr-199, which is at the interface between monomers, that no such inter-monomer electron transfer is detected at the level of the b(L) hemes. We show from analysis of strains with mutations at Asn-221 that there are coulombic interactions between the b-hemes in a monomer. The data can also be interpreted as showing similar coulombic interaction across the dimer interface, and we discuss mechanistic implications.

Published
2008
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11. Hydrogen bonds between nitrogen donors and the semiquinone in the Qi-site of the bc1 complex.

Author

Dikanov SA, Holland JT, Endeward B, Kolling DR, Samoilova RI, Prisner TF, and Crofts AR

Subjects
Amino Acid Substitution, Bacterial Proteins genetics, Binding Sites, Electron Transport Complex III genetics, Hydrogen Bonding, Mutation, Missense, Protein Structure, Quaternary, Rhodobacter sphaeroides genetics, Structure-Activity Relationship, X-Ray Diffraction, Bacterial Proteins chemistry, Benzoquinones chemistry, Electron Transport Complex III chemistry, Models, Molecular, Rhodobacter sphaeroides enzymology
Abstract

The ubisemiquinone stabilized at the Qi-site of the bc1 complex of Rhodobacter sphaeroides forms a hydrogen bond with a nitrogen from the local protein environment, tentatively identified as ring N from His-217. The interactions of 14N and 15N have been studied by X-band (approximately 9.7 GHz) and S-band (3.4 GHz) pulsed EPR spectroscopy. The application of S-band spectroscopy has allowed us to determine the complete nuclear quadrupole tensor of the 14N involved in H-bond formation and to assign it unambiguously to the Nepsilon of His-217. This tensor has distinct characteristics in comparison with H-bonds between semiquinones and Ndelta in other quinone-processing sites. The experiments with 15N showed that the Nepsilon of His-217 was the only nitrogen carrying any considerable unpaired spin density in the ubiquinone environment, and allowed calculation of the isotropic and anisotropic couplings with the Nepsilon of His-217. From these data, we could estimate the unpaired spin density transferred onto 2s and 2p orbitals of nitrogen and the distance from the nitrogen to the carbonyl oxygen of 2.38+/-0.13A. The hyperfine coupling of other protein nitrogens with semiquinone is <0.1 MHz. This did not exclude the nitrogen of the Asn-221 as a possible hydrogen bond donor to the methoxy oxygen of the semiquinone. A mechanistic role for this residue is supported by kinetic experiments with mutant strains N221T, N221H, N221I, N221S, N221P, and N221D, all of which showed some inhibition but retained partial turnover.

Published
2007
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12. Hydrogen bonds involved in binding the Qi-site semiquinone in the bc1 complex, identified through deuterium exchange using pulsed EPR.

Author

Dikanov SA, Samoilova RI, Kolling DR, Holland JT, and Crofts AR

Subjects
Benzoquinones metabolism, Deuterium metabolism, Electron Spin Resonance Spectroscopy, Electron Transport Complex III analysis, Hydrogen Bonding, Protons, Electron Transport Complex III metabolism, Rhodobacter sphaeroides metabolism
Abstract

Exchangeable protons in the immediate neighborhood of the semiquinone (SQ) at the Qi-site of the bc1 complex (ubihydroquinone:cytochrome c oxidoreductase (EC 1.10.2.2)) from Rhodobacter sphaeroides have been characterized using electron spin echo envelope modulation (ESEEM) and hyperfine sublevel correlation spectroscopy (HYSCORE) and visualized by substitution of H2O by 2H2O. Three exchangeable protons interact with the electron spin of the SQ. They possess different isotropic and anisotropic hyperfine couplings that allow a clear distinction between them. The strength of interactions indicates that the protons are involved in hydrogen bonds with SQ. The hyperfine couplings differ from values typical for in-plane hydrogen bonds previously observed in model experiments. It is suggested that the two stronger couplings involve formation of hydrogen bonds with carbonyl oxygens, which have a significant out-of-plane character due to the combined influence of bulky substituents and the protein environment. These two hydrogen bonds are most probably to side chains suggested from crystallographic structures (His-217 and Asp-252 in R. sphaeroides). Assignment of the third hydrogen bond is more ambiguous but may involve either a bond between Asn-221 and a methoxy O-atom or a bond to water. The structural and catalytic roles of the exchangeable protons are discussed in the context of three high resolution crystallographic structures for mitochondrial bc1 complexes. Potential H-bonds, including those to water molecules, form a network connecting the quinone (ubiquinone) occupant and its ligands to the propionates of heme bH and the external aqueous phase. They provide pathways for exchange of protons within the site and with the exteriors, needed to accommodate the different hydrogen bonding requirements of different quinone species during catalysis.

Published
2004
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13. Exploration of ligands to the Qi site semiquinone in the bc1 complex using high-resolution EPR.

Author

Kolling DR, Samoilova RI, Holland JT, Berry EA, Dikanov SA, and Crofts AR

Subjects
Binding Sites, Electron Spin Resonance Spectroscopy, Hydrogen Bonding, Ligands, Models, Molecular, Oxidation-Reduction, Quinones chemistry, Rhodobacter sphaeroides enzymology, Electron Transport Complex III chemistry, Electron Transport Complex III metabolism
Abstract

Pulsed EPR spectroscopy was used to explore the structural neighborhood of the semiquinone (SQ) stabilized at the Qi site of the bc1 complex of Rhodobacter sphaeroides (EC 1.10.2.2) and to demonstrate that the nitrogen atom of a histidine imidazole group donates an H-bond to the SQ. Crystallographic structures show two different configurations for the binding of ubiquinone at the Qi site of mitochondrial bc1 complexes in which histidine (His-201 in bovine sequence) is either a direct H-bond donor or separated by a bridging water. The paramagnetic properties of the SQ formed at the site provide an independent method for studying the liganding of this intermediate species. The antimycin-sensitive SQ formed at the Qi site by either equilibrium redox titration, reduction of the oxidized complex by ascorbate, or addition of decylubihydroquinone to the oxidized complex in the presence of myxothiazol all showed similar properties. The electron spin echo envelope modulation spectra in the 14N region were dominated by lines with frequencies at 1.7 and 3.1 MHz. Hyperfine sublevel correlation spectroscopy spectra showed that these were contributed by a single nitrogen. Further analysis showed that the 14N nucleus was characterized by an isotropic hyperfine coupling of approximately 0.8 MHz and a quadrupole coupling constant of approximately 0.35 MHz. The nitrogen was identified as the N-epsilon or N-delta imidazole nitrogen of a histidine (it is likely to be His-217, or His-201 in bovine sequence). A distance of 2.5-3.1 A for the O-N distance between the carbonyl of SQ and the nitrogen was estimated. The mechanistic significance is discussed in the context of a dynamic role for the movement of His-217 in proton transfer to the site.

Published
2003
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14. Interaction of an uuter membrane protein of enterotoxigenic Escherichia coli with cell surface heparan sulfate proteoglycans.

Author

Fleckenstein JM, Holland JT, and Hasty DL

Subjects
Animals, Antimicrobial Cationic Peptides, Bacterial Adhesion, Blood Proteins metabolism, Carrier Proteins metabolism, Cell Line, Cricetinae, Epithelial Cells microbiology, Protein Binding, Bacterial Outer Membrane Proteins metabolism, Escherichia coli pathogenicity, Escherichia coli Proteins metabolism, Heparan Sulfate Proteoglycans metabolism, Membrane Proteins metabolism
Abstract

We have previously shown that enterotoxigenic invasion protein A (Tia), a 25-kDa outer membrane protein encoded on an apparent pathogenicity island of enterotoxigenic Escherichia coli (ETEC) strain H10407, mediates attachment to and invasion into cultured human gastrointestinal epithelial cells. The epithelial cell receptor(s) for Tia has not been identified. Here we show that Tia interacts with cell surface heparan sulfate proteoglycans. Recombinant E. coli expressing Tia mediated invasion into wild-type epithelial cell lines but not invasion into proteoglycan-deficient cells. Furthermore, wild-type eukaryotic cells, but not proteoglycan-deficient eukaryotic cells, attached to immobilized polyhistidine-tagged recombinant Tia (rTia). Binding of epithelial cells to immobilized rTia was inhibited by exogenous heparan sulfate glycosaminoglycans but not by hyaluronic acid, dermatan sulfate, or chondroitin sulfate. Similarly, pretreatment of eukaryotic cells with heparinase I, but not pretreatment of eukaryotic cells with chrondroitinase ABC, inhibited attachment to rTia. In addition, we also observed heparin binding to both immobilized rTia and recombinant E. coli expressing Tia. Heparin binding was inhibited by a synthetic peptide representing a surface loop of Tia, as well as by antibodies directed against this peptide. Additional studies indicated that Tia, as a prokaryotic heparin binding protein, may also interact via sulfated proteoglycan molecular bridges with a number of mammalian heparan sulfate binding proteins. These findings suggest that the binding of Tia to host epithelial cells is mediated at least in part through heparan sulfate proteoglycans and that ETEC belongs on the growing list of pathogens that utilize these ubiquitous cell surface molecules as receptors.

Published
2002
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15. Night-to-night variability of disturbed breathing during sleep in an elderly community sample.

Author

Lord S, Sawyer B, O'Connell D, King M, Pond D, Eyland A, Mant A, Holland JT, Hensley MJ, and Saunders NA

Subjects
Aged, Female, Humans, Male, Microcomputers, Monitoring, Physiologic instrumentation, Reference Values, Signal Processing, Computer-Assisted instrumentation, Sleep Apnea Syndromes physiopathology, Circadian Rhythm physiology, Respiration physiology, Sleep Apnea Syndromes diagnosis, Sleep Stages physiology
Abstract

Night-to-night variability of breathing and oxygenation during sleep was examined with portable monitoring equipment in 30 residents of a retirement village. Subjects had a variety of health problems as might be expected in the elderly, but all were living independently in self-contained units. None had clinical features to suggest obstructive sleep apnea. Two pairs of consecutive nights were studied, separated by 4-6 months. Satisfactory recordings on all four nights were obtained in 15 subjects, and in these subjects variability of measurements was examined across nights 1-4 using the kappa (K) statistic. There was low but significant agreement in estimated total sleep time (K = 0.23, p less than 0.01) and estimated wakefulness after sleep onset (K = 0.18, p less than 0.05) as assessed with a wrist actigraph. Good agreement was found among measures of disturbed breathing during sleep whether expressed in terms of numbers of events [respiratory disturbance index (RDI), K = 0.62, p less than 0.0001], their duration (event minutes, K = 0.53, p less than 0.0001), or associated disturbance of oxygenation (% cumulative time less than 90% SaO2, K = 0.50, p less than 0.001, n = 9). Twenty-eight subjects had at least two nights' satisfactory recordings. Although some of these individuals showed considerable variation in RDI, this had little overall effect on classification of them into normal (RDI less than or equal to 15) and abnormal groups. The accuracy of the first night's recording in predicting classification derived from recording on three or four nights was 83%.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1991

16. The epidemiology of multiple sclerosis in three Australian cities: Perth, Newcastle and Hobart.

Author

Hammond SR, McLeod JG, Millingen KS, Stewart-Wynne EG, English D, Holland JT, and McCall MG

Subjects
Age Factors, Australia, Humans, Ireland ethnology, Multiple Sclerosis classification, Multiple Sclerosis mortality, United Kingdom ethnology, Multiple Sclerosis epidemiology
Abstract

An epidemiological survey of multiple sclerosis (MS) in three Australian cities, Perth, Newcastle and Hobart, was undertaken with its prevalence day being the national census day on June 30, 1981, exactly twenty years after a previous survey of the same cities. The relationship between increasing prevalence and increasing south latitude found in the 1961 survey was confirmed in this present study. Prevalence rates had increased significantly over the twenty years between the studies. Over the same time period incidence rates had also increased in Newcastle and Hobart but had remained essentially stable in Perth although these changes were not significant. The rise in prevalence was due to a combination of factors of differing importance in each city. These factors included better case ascertainment, increased recognition of the less severely disabled patient, increased survival time and differential immigration of a population at a higher risk of developing MS than the indigenous population. Finally, analysis of MS prevalence rates amongst migrant populations in Perth and Hobart suggested that either the risk of acquisition of MS may extend over a wider age range than is generally accepted or that environmental factors prevalent in the former city have modified disease expression there.

Published
1988
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17. Leptospirosis: II. Investigation of clinical disease in dairy cattle in the Waikato district of New Zealand.

Author

Carter ME, Cordes DO, Holland JT, Lewis SF, and Lake DE

Abstract

Investigations were carried out in 1975, 1976 and 1977 in 16 dairy herds where leptospiral abortions were suspected and in five other herds where clinical disease was not present. Both Leptospira interrogans serovars pomona and hardjo were isolated from cattle in herds with leptospirosis, but only pomona was recovered from those that had aborted. There was no evidence that hardjo caused clinical disease in dairy cattle in the Waikato district. It was found that 73% of the cows that aborted and 19% of other animals in the same herds had microscopic agglutination test titres to pomona of 1:2,000 or greater. By contrast, only 2% of cattle in herds without clinical evidence of leptospirosis had such titres. One cow retained a titre of 1:2,000 or greater to pomona for 7 months; titres of this order had a shorter duration in other cows. Leptospiruria occurred in 50% of cows that had aborted and in 9% of in-contact cows in the same herds. Only 0.7% of cows had leptospiruria in the herds with no clinical disease. Ten of 35 cows shedding pomona still had leptospiruria one month later. It was concluded that clinical leptospirosis should be diagnosed by testing a sample of the herd, rather than just individual cows, because of the variability and persistence of leptospiruria and serological titres in cows with and without clinical signs. Although hardjo is common in cattle in the Waikato district, it was not found to cause abortion in cattle.

Published
1982
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20. Three cases of post traumatic vascular headache treated by surgery.

Author

Holland JT

Subjects
Adult, Female, Humans, Male, Temporal Arteries surgery, Vascular Headaches etiology, Headache surgery, Temporal Arteries injuries, Vascular Headaches surgery
Abstract

Three cases are reported of vascular headache following trauma and which failed to respond adequately to standard therapy for migraine. In each case the effect of ligation of the arteries involved has been dramatic, with complete and lasting relief in two cases.

Published
1976

22. Opsoclonus with myoclonus.

Author

Holland JT

Subjects
Adult, Eye Diseases etiology, Female, Humans, Myoclonus etiology, Eye Diseases complications, Eye Movements, Myoclonus complications
Abstract

A further case of opsoclonus with myoclonus is described. When this syndrome occurs in childhood an associated neuroblastoma should be excluded. In the majority of cases at all ages no underlying disease will be found, although a preceding history of minor upper respiratory or gastrointestinal infection may be elicited, suggesting that a possible encephalitis affecting brain stem mechanisms may be the cause. The prognosis is, as a rule, excellent although full recovery may not occur for many months. Corticosteroids and nitrazepam may have a place in the treatment of severely affected patients with distressing symptoms.

Published
1975

24. The causalgia syndrome treated with regional intravenous guanethidine.

Author

Holland JT

Subjects
Adolescent, Causalgia etiology, Causalgia therapy, Female, Guanethidine administration & dosage, Humans, Injections, Intravenous, Middle Aged, Sympathectomy, Causalgia drug therapy, Guanethidine therapeutic use, Neuralgia drug therapy
Abstract

Two cases of the causalgia syndrome have been presented, one probably related to a mild peripheral neuropathy and the second, more classically, following trauma. The technique of regional infusion of guanethidine has been shown to be efficacious in relieving the pain, if only temporarily, but as it is largely without risk it may be repeated is necessary. It should probably be performed as a routine before consideration of surgical sympathectomy in order to assess whether surgical intervention is likely to be effective. Mechanisms of the causalgia syndrome itself are considered and a rationale for the efficacy of the procedure is suggested.

Published
1978

25. Convulsive status epilepsy: is there a role for thiopentone-induced narcosis?

Author

Burton K and Holland JT

Subjects
Adolescent, Adult, Child, Child, Preschool, Enema, Extravasation of Diagnostic and Therapeutic Materials, Humans, Infusions, Parenteral, Middle Aged, Respiratory Insufficiency chemically induced, Thiopental administration & dosage, Thiopental adverse effects, Status Epilepticus drug therapy, Thiopental therapeutic use
Abstract

Convulsive status epilepsy is a medical emergency with significant mortality and morbidity. This retrospective survey reports the use of non-anaesthetic doses of thiopentone, given either by intravenous or rectal infusion. The regime was effective in controlling convulsive status without significant complications. It is suggested that this regime can be used safely when standard doses of diazepam (or clonazepam), and/or phenytoin, fail to effect immediate control of convulsive status, and before anaesthetic agents are administered.

Published
1984

26. Leptospirosis: I. Clinical investigation of the infection in dairy cattle in the Waikato district of New Zealand.

Author

Cordes DO, Carter ME, Townsend KG, Lewis SF, and Holland JT

Abstract

An investigation was made into the prevalence of leptospiral infection in cattle. An area 50 km radius was selected in a region where leptospirosis was reputedly common. Farmers volunteered 250 herds with 39 500 cows for testing and 7 500 animals were selected and sampled. Twenty-nine cows (0.4%) on 14 (5.6%) of the farms had leptospiruria at the first examination. Leptospirae were cultured from the urines of nine of these animals and all were Leptospira interrogans serovar hardjo. Serologically 12.5% of cows had titres of 1:200 or greater to hardjo and 3.5% titres of 1:200 or greater to pomona. In the Spring of 1977, there was evidence of clinical leptospirosis in calves associated with only one of the herds and no clinical leptospirosis in the 250 lactating herds, although leptospiral titres were found in 88% of them. This indicated that clinical disease was much less common than infection. We concluded that leptospirosis was of minor economic importance in dairy cattle, although it could be significant in individual herds, and a health hazard to farm workers.

Published
1982
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29. Characterization of staphylococci associated with clinical and subclinical bovine mastitis.

Author

Hodges RT, Jones YS, and Holland JT

Abstract

Attempts were made to identify 900 species of staphylococci or micrococci recovered from samples of bovine milk examined for mastitis pathogens. The presence and identity of haemolysins was recorded together with results of disc diffusion antibiotic sensitivity tests. The occurrence of clinical mastitis was also noted and somatic cell counts (SCC) were performed on milk samples which were normal in appearance. Eight hundred and thirty-one coagulase positive staphylococci were obtained, of which 810 were S. aureus and 21 were S. intermedius. Of 65 coagulase negative staphylococci the species of 19 could not be determined by the identification systems used. The remainder were identified as S. hyicus sub sp. hyicus (1), S. hyicus sub sp. chromogenes (19), S. haemolyticus (17), S. hominis (3), S. epidermidis (4), S. capitis (1) and either S. hominis or S. warneri (1). Four other isolates could not clearly be assigned to the genus Staphylococcus or Micrococcus and were designated irregular strains. No micrococci were identified. The presence of alpha, beta, or delta haemolysins occurring singly or in various combinations was identified in 98.3% of coagulase positive staphylococci and in 60% of coagulase negative staphylococci. Epsilon haemolysin was detected in 47.6% of the coagulase negative staphylococci and in 9.5% of S. intermedius. All staphylococci were sensitive to tetracycline (30 microg), novobiocin (1.6 microg), nafcillin (30 microg), methicillin (10 microg) and cephalothin (30 microg) and variable numbers of each species were sensitive to penicillin (2 iu) and streptomycin (10 microg). One non-identified species of coagulase negative staphylococcus was sensitive to erythromycin (0.4 microg) the remaining staphylococci were resistant. Each of the four irregular strains was sensitive to erythromycin and novobiocin. Clinical mastitis was associated with 30.6% of coagulase positive staphylococci, 15.3% of coagulase negative staphylococci, and two of the four irregular strains (50%). Subclinical mastitis as determined by SCC of 500 x 10(3) or greater was associated with 92.7% of coagulase positive and 37.5% of coagulase negative staphylococci.

Published
1984
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30. Mycoplasma mastitis.

Author

Brookbanks EO, Carter ME, and Holland JT

Subjects
Animals, Cattle, Female, Mycoplasma isolation & purification, Mycoplasma Infections microbiology, New Zealand, Mastitis, Bovine microbiology, Mycoplasma Infections veterinary
Published
1969
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32. TREATMENT OF URINARY TRACT INFECTION WITH NALIDIXIC ACID.

Author

HOLLAND JT and MONTGOMERIE JZ

Subjects
Adolescent, Child, Biomedical Research, Escherichia coli Infections, Geriatrics, Nalidixic Acid, Naphthyridines, Pharmacology, Proteus Infections, Pseudomonas Infections, Toxicology, Urinary Tract Infections, Urine
Published
1964

34. A-mode echoencephalography (experience with 1300 midline echos).

Author

Holland JT and Kossoff G

Subjects
Cerebral Ventricles, Cerebrovascular Disorders diagnosis, Craniocerebral Trauma diagnosis, Hematoma, Epidural, Cranial diagnosis, Hematoma, Subdural diagnosis, Humans, Methods, Septum Pellucidum, Brain Diseases diagnosis, Echoencephalography
Published
1973

35. Serum-lipids and cerebrovascular disease.

Author

Cumings JN, Grundt IK, Holland JT, and Marshall J

Subjects
Adipose Tissue, Chromatography, Gas, Female, Humans, Male, Middle Aged, Skin, Triglycerides blood, Cholesterol, Fatty Acids blood, Glycerides blood, Intracranial Arteriosclerosis blood, Phospholipids blood
Published
1967
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