Your search keyword '"Fitzgerald SP"' showing total 35 results

1. Thrombomodulin Expression in Bladder Cancer Tissue and Its Association with Prognosis and Patient Survival

Author

Watt J, Maguire DG, Reid CN, Lamont JV, Fitzgerald SP, and Ruddock MW

Subjects

transitional urothelial carcinoma, tissue microarrays, immunohistochemistry, bladder cancer., Diseases of the genitourinary system. Urology, RC870-923

Abstract

Joanne Watt, Daniel G Maguire, Cherith N Reid, John V Lamont, Stephen P Fitzgerald, Mark W Ruddock Randox Laboratories Ltd, Molecular Biology, Crumlin, County Antrim BT29 4QY, Northern Ireland, UKCorrespondence: Mark W RuddockRandox Laboratories Ltd, Molecular Biology, 55 Diamond Road, Crumlin, County Antrim BT29 4QY, Northern Ireland, United KingdomTel +44 28 9442 2413Fax +44 28 9445 2912Email Mark.Ruddock@randox.comBackground: Decreased expression of thrombomodulin (TM) in bladder cancer tissue has been shown to be associated with cell proliferation, increased malignancy and a poor prognosis. The aim of this study was to investigate the immunoexpression of TM in bladder tissue cores by immunohistochemistry (IHC) and the relationship between TM score and patient survival for the following pathologies: transitional cell papillary carcinoma (TCPC), transitional cell carcinoma (non-papillary) (TCC), squamous cell carcinoma (SCC), adenocarcinoma, and sarcoma. TM immunoexpression was also evaluated in normal adjacent bladder tissue cores.Methods: TM immunoexpression was assessed in n=185 formalin-fixed paraffin-embedded (FFPE) bladder tissue cores from n=98 patients by IHC. Tissue cores included TCPC (n=29), TCC (n=85), SCC (n=21), adenocarcinoma (n=12), sarcoma (n=4), and normal tissue cores (n=34).Results: TM immunoexpression scores are stronger in TCPC, TCC and SCC bladder cancer tissue cores with respect to adenocarcinoma and sarcoma (mean TM immunoexpression scores: 3.04, 2.57, 2.55, 1.55 and 1.19, respectively) (Kruskal–Wallis p< 0.001). TM immunoexpression scores significantly decreased in bladder cancer tissue cores across both stage (p< 0.001) and grade (p< 0.001) (Kruskal–Wallis). Survival data were available for n=45 bladder cancer patients (mean follow-up of 34 months). Applying a TM immunoexpression cut-off score of 3.0 demonstrated that patients with bladder cancer who had a TM immunoexpression score < 3.0 had lower survival rates (median survival 23.5 months). In contrast, patients with TM immunoexpression scores ≥ 3.0 had longer survival rates (median survival 40 months) (log-rank; p=0.045).Conclusion: TM immunoexpression in bladder cancer tissue may be a clinically relevant predictor of tumor progression and survival. Low expression of TM in bladder cancer biopsies or in recurrent bladder cancer may be indicative of a poor prognosis. TM immunoexpression could be used to guide clinical decision making.Keywords: transitional urothelial carcinoma, tissue microarrays, immunohistochemistry, bladder cancer

Published

2020

2. Interstitial-mediated dislocation climb and the weakening of particle-reinforced alloys under irradiation

Author

Thompson, DH, Tarleton, E, Roberts, SG, and Fitzgerald, SP

Subjects

Condensed Matter - Materials Science, Condensed Matter - Mesoscale and Nanoscale Physics

Abstract

Dislocations can climb out of their glide plane by absorbing (or emitting) point defects (vacancies and self-interstitial atoms (SIAs)). In contrast with conservative glide motion, climb relies on the point defects' thermal diffusion and hence operates on much longer timescales, leading to some forms of creep. Whilst equilibrium point defect concentrations allow dislocations to climb to relieve non-glide stresses, point defect supersaturations also lead to osmotic forces, driving dislocation motion even in the absence of external stresses. Self-interstitial atoms typically have significantly higher formation energies than vacancies, so their contribution to climb is usually ignored. However, under irradiation conditions, both types of defect are athermally created in equal numbers. In this letter, we use simple thermodynamic arguments to show that the contribution of interstitials cannot be neglected in irradiated materials, and that the osmotic force they induce on dislocations is many orders of magnitude larger than that caused by vacancies. This explains why the prismatic dislocation loops observed by {\it in situ} transmission electron microscope irradiations are more often of interstitial rather than vacancy character. Using discrete dislocation dynamics simulations, we investigate the effect on dislocation-obstacle interactions, and find reductions in the depinning time of many orders of magnitude. This has important consequences for the strength of particle-reinforced alloys under irradiation., Comment: 10 pages, 3 figures

Published

2018

3. Effect of collision cascades on dislocations in tungsten: A molecular dynamics study

Author

Fu, BQ, Fitzgerald, SP, Hou, Q, Wang, J, and Li, M

Subjects

Condensed Matter::Materials Science

Abstract

Tungsten (W) is the prime candidate material for the divertor and other plasma-facing components in DEMO. The point defects (i.e. vacancies and self-interstitials) produced in collision cascades caused by incident neutrons aggregate into dislocation loops (and voids), which strongly affect the mechanical properties. The point defects also interact with existing microstructural features, and understanding these processes is crucial for modelling the long term microstructural evolution of the material under fusion conditions. In this work, we performed molecular dynamics simulations of cascades interacting with initially straight edge dislocation dipoles. It was found that the residual vacancy number usually exceeds the residual interstitial number for cascades interacting with vacancy type dipoles, but for interstitial type dipoles these are close. We observed that a cascade near a dislocation promotes climb, i.e. it facilitates the movement of point defects along the climb direction. We also observed that the dislocations move easily along the glide direction, and that kinks are formed near the centre of the cascade, which then facilitate the movement of the dipoles. Some dipoles are sheared off by the cascade, and this is dependent on PKA energy, position, direction, and the width of dipole.

Published

2017

4. Kink pair production and dislocation motion

Author

Fitzgerald, SP

Abstract

The motion of extended defects called dislocations controls the mechanical properties of crystalline materials such as strength and ductility. Under moderate applied loads, this motion proceeds via the thermal nucleation of kink pairs. The nucleation rate is known to be a highly nonlinear function of the applied load, and its calculation has long been a theoretical challenge. In this article, a stochastic path integral approach is used to derive a simple, general, and exact formula for the rate. The predictions are in excellent agreement with experimental and computational investigations, and unambiguously explain the origin of the observed extreme nonlinearity. The results can also be applied to other systems modelled by an elastic string interacting with a periodic potential, such as Josephson junctions in superconductors.

Published

2016

5. Structure and dynamics of crowdion defects in bcc metals

Author

Fitzgerald, SP

Subjects

Condensed Matter - Materials Science, Microstructural evolution, Materials science, Polymers and Plastics, Dynamics (mechanics), Materials Science (cond-mat.mtrl-sci), FOS: Physical sciences, 02 engineering and technology, 021001 nanoscience & nanotechnology, 01 natural sciences, Crystallographic defect, Multiscale modeling, Atomic and Molecular Physics, and Optics, Mechanics of Materials, Chemical physics, 0103 physical sciences, Ceramics and Composites, 010306 general physics, 0210 nano-technology

Abstract

Crowdion defects are produced in body-centered-cubic metals under irradiation. Their structure and diffusive dynamics play a governing role in microstructural evolution, and hence the mechanical properties of nuclear materials. In this paper, we apply the analytical Frenkel-Kontorova model to crowdions and clusters thereof (prismatic dislocation loops) and show that the Peierls potential in which these defects diffuse is remarkably small (in the micro eV range as compared to the eV range for other defects). We also develop a coarse-grained statistical methodology for simulating these fast-diffusing objects in the context of object kinetic Monte Carlo, which is less vulnerable to the low barrier problem than naïve stochastic simulation.

Published

2018

6. Immunodetection of Cytoplasmatic Membrane-Bound Thrombomodulin in Formalin-Fixed Paraffin-Embedded Human Tissue Microarrays

Author

Fitzgerald Sp, Lamont Jv, McReynolds D, Williamson Ke, Reid Cn, and Ruddock Mw

Subjects

Pathology, medicine.medical_specialty, Tissue microarray, Biology, urologic and male genital diseases, medicine.disease, Thrombomodulin, female genital diseases and pregnancy complications, Transitional cell carcinoma, cardiovascular system, medicine, Adenocarcinoma, Sarcoma, Teratoma, Urothelium, Immunostaining

Abstract

Background: Loss of thrombomodulin immunoreactivity denotes a poor prognosis for patients presenting with malignant disease. Objectives: Immunodetection for cytoplasmatic membrane-bound thrombomodulin in formalin-fixed paraffinembedded (FFPE) tissue microarrays. Methods: Thrombomodulin immunoreactivity was assessed in 97 FFPE tissue cores representing bladder, kidney, prostate, testis, penis, ovary, cervix, vulva, endometriosis, and myometrium, from 84 patients arrayed on three TMAs (64 (66%) cancers, 22 (23%) normal controls, and 11 (11%) benign pathologies). Human bladder tissue lysate from matched normal urothelium and TCC biopsies were also examined by western blot analysis for thrombomodulin expression. Results: Thrombomodulin immunoreactivity was strongest in the TCC cores where ≥60% of the tissue sections scored +3, or greater. By contrast, SCCs, adenocarcinomas, CCCs, papillary carcinoma, sarcomas, seminomas, teratoma and all other tissue sections scored ≤ +2. Thrombomodulin expression was also detected by western blot analysis in the human bladder tumour lysate. No signal was detected in adjacent normal control. Conclusion: Cytoplasmatic membrane-bound thrombomodulin immunostaining is strongest in TCC sections with respect to SCC, adenocarcinoma, sarcoma, seminoma, teratoma, papillary carcinoma, CCC, and is independent of both grade and stage. Thrombomodulin immunostaining in tumour tissue sections are predominately membranous.

Published

2014

7. Dynamics and simulations of shifting in a dual clutch transmission

Author

Walker, PD, Zhang, N, Tamba, RT, Fitzgerald, SP, Teh, K, Davies, I, and Howard, I

Abstract

In this paper a finite element model of a dual clutch transmission (DCT) equipped rear wheel drive powertrain is developed for the study of transient dynamics during clutch-to-clutch shifting. Damped free vibration analysis is performed to identify natural frequencies and damping ratios. These results indicate that damping in the DCT is significantly lower than in comparable automatic transmissions. Clutch pressure signals are employed from a constant torque shift control algorithm with engine throttle angle control for transient simulations. These simulations demonstrate inadequacy of the sole use of torque control for providing high quality gear shifts in DCTs. To rectify this issue the torque phase of shifting was restricted by applying a ramp increase in clutch torque to reduce pressure overshoot during simulations. Results demonstrate a reduction in post lockup transients; however it is suggested that inclusion of time delay in shift control must be considered to achieve best possible performance.

Published

2010

8. Dynamics and simulations of shifting in a dual clutch transmission

Author

Teh, K, Davies, I, Howard, I, Walker, PD, Zhang, N, Tamba, RT, Fitzgerald, SP, Teh, K, Davies, I, Howard, I, Walker, PD, Zhang, N, Tamba, RT, and Fitzgerald, SP

Abstract

In this paper a finite element model of a dual clutch transmission (DCT) equipped rear wheel drive powertrain is developed for the study of transient dynamics during clutch-to-clutch shifting. Damped free vibration analysis is performed to identify natural frequencies and damping ratios. These results indicate that damping in the DCT is significantly lower than in comparable automatic transmissions. Clutch pressure signals are employed from a constant torque shift control algorithm with engine throttle angle control for transient simulations. These simulations demonstrate inadequacy of the sole use of torque control for providing high quality gear shifts in DCTs. To rectify this issue the torque phase of shifting was restricted by applying a ramp increase in clutch torque to reduce pressure overshoot during simulations. Results demonstrate a reduction in post lockup transients; however it is suggested that inclusion of time delay in shift control must be considered to achieve best possible performance.

Published

2010

9. Synchroniser modeling with application specific to the dual clutch transmission

Author

Committee, CT, Walker, PD, Zhang, N, Tamba, RT, Fitzgerald, SP, Committee, CT, Walker, PD, Zhang, N, Tamba, RT, and Fitzgerald, SP

Abstract

The synchromesh type synchroniser has been introduced to dual clutch transmission applications for gear selection prior to shifting. Historical research into this type of mechanism has targeted the application to manual transmission systems only. Such work targets the phenomena associated with driver feel such as shift effort and âdouble bumpâ . Now automated, the control of the synchroniser is less concerned with such aspects of the actuation, focus not trends towards repeatability of the process as well as speed of engagement. The actuation of this type of mechanism relies on the balancing of torques derived from engagement chamfers, the cone clutch and losses experienced in the transmission. These torques affect the displacement of sleeve, asynchronisation of the target gear, as well as the unblocking of synchroniser ring and indexing of the gear to the locked position. Thus a simplified model of the synchroniser mechanism and associated gear is developed for the purpose of simulating its operation in a dual clutch transmission. Unlike similar simulations this model targets the actuation of the mechanism using input forces from the controller, rather than using the control of sleeve displacement to determine maximum forces experience by the driver. To assess how operating characteristics have varied the mechanism has been modelled in the Matlab® environment. This paper presents the techniques used to model the mechanism, including the governing principles of synchroniser actuation and drag torque. Simulation results demonstrate that the primary variation in the mechanism is through the indexing chamfers. Additionally the influence of temperature variation is demonstrated for a fifth gear upshift, and the detrimental effects of cold starts demonstrated.

Published

2009

10. The application of new concepts of the assessment of the thyroid state to pregnant women.

Author

Fitzgerald SP, Bean NG, Fitzgerald SP, and Falhammar H

Subjects

Female, Humans, Pregnancy, Pregnancy Outcome, Pregnant Women, Thyroid Hormones, Thyrotropin, Thyroid Gland, Thyroxine

Abstract

Recently proposed concepts regarding the nature and assessment of the thyroid state have provided a model more consistent with empiric evidence. It now appears likely that there are no such entities as thyroid set points and individual euthyroidism. Rather than there being discrete thyroid states, peripheral organ parameters are associated with thyroid function in a continuous manner. Thyroid hormone levels and, in particular, levels of free thyroxine now appear to be superior to thyrotropin levels as indicators of the thyroid state. Complicating the assessment of the correlations of the thyroid state with pregnancy outcomes are the contribution of the placenta to maternal thyroid function, fetal thyroid development, the multiple potential pathways to any particular outcome, the likely presence of small critical periods of time, the differing genetics of fetal and maternal tissues, and the unreliability of thyroid hormone assays. Nevertheless, there is no apparent reason for there to be a change in pregnancy to the basic principles of thyroid hormone action. The relationships between mild abnormalities of the thyroid state and pregnancy outcomes and the value of treating such mild abnormalities remain uncertain and controversial. The evidence suggests that further investigation of these clinical questions might better be based on thyroid hormone, particularly free thyroxine, levels. In the investigation of borderline low thyroid states, the categories of subclinical hypothyroidism and isolated hypothyroxinemia might both be abandoned with attention being directed to low free thyroxine levels regardless of the thyroid-stimulating hormone (TSH) levels. For these changes to occur, there would ideally be improvements in the assays for free thyroxine in pregnancy. The evidence suggests that, just as in the non-pregnant situation, pregnancy guidelines based on thyrotropin levels may need revision., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Fitzgerald, Bean, Fitzgerald and Falhammar.)

Published

2022

11. Inhibition of IRE1α RNase activity sensitizes patient-derived acute myeloid leukaemia cells to proteasome inhibitors.

Author

Creedican S, Robinson CM, Mnich K, Islam MN, Szegezdi E, Clifford R, Krawczyk J, Patterson JB, FitzGerald SP, Summers M, Richardson C, Martin K, Gorman AM, and Samali A

Subjects

Endoplasmic Reticulum Stress, Humans, Proteasome Inhibitors pharmacology, Protein Serine-Threonine Kinases, Endoribonucleases, Leukemia, Myeloid, Acute drug therapy, Leukemia, Myeloid, Acute genetics

Published

2022

12. Redefinition of Successful Treatment of Patients With Hypothyroidism. Is TSH the Best Biomarker of Euthyroidism?

Author

Fitzgerald SP and Falhammar H

Subjects

Biomarkers, Humans, Thyroid Function Tests, Thyroid Hormones therapeutic use, Thyrotropin, Hypothyroidism diagnosis, Hypothyroidism drug therapy

Abstract

In recent years evidence has accumulated supporting a revised view of the nature of euthyroidism and the biomarkers of thyroid function. Within the normal range, variations in thyroid hormone levels are associated with variations in clinical parameters and outcomes. There are therefore no readily identified individually specific optimum levels of thyroid hormones for any individual. Levels around the middle of the normal population range may best reflect euthyroidism. These levels may have evolutionary advantages on the basis that adverse outcomes often increase with divergence from such levels, and physiological processes tend to minimise such inter-individual and intra-individual divergence. In populations of predominantly untreated individuals, levels of thyroid hormones and in particular levels of free thyroxine (FT4) correlate more often with clinical parameters than do levels of thyrotropin (TSH). Levels of thyroid hormones may therefore be regarded as the best available biomarkers of euthyroidism and dysthyroidism. It follows that 'subclinical hypothyroidism' (normal FT4/raised TSH levels), rather than being an accurate marker of peripheral tissue hypothyroidism is more a marker of decreased thyroid reserve and prognosis. The recent evidence suggests that treatment of hypothyroxinemia, regardless of the TSH level, and monitoring therapy using FT4 and/or triiodothyronine levels, depending on the replacement regime, may result in more successful treatment of hypothyroidism than relying on thyrotropin levels for patient selection and subsequent treatment monitoring. The equivalents of mid-range levels of thyroid hormones (especially FT4), adjusted by individual comorbidity concerns, may be rational general replacement targets. These implications of the new evidence may create opportunities for novel trials of thyroid replacement therapy., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Fitzgerald and Falhammar.)

Published

2022

13. Integrating inflammatory serum biomarkers into a risk calculator for prostate cancer detection.

Author

Jalali A, Kitching M, Martin K, Richardson C, Murphy TB, FitzGerald SP, Watson RW, and Perry AS

Subjects

Adult, Aged, Aged, 80 and over, Biopsy, Early Detection of Cancer, Humans, Liquid Biopsy, Male, Middle Aged, Neoplasm Grading, Neoplasm Staging, Prostatic Neoplasms epidemiology, ROC Curve, Risk Assessment, Risk Factors, Biomarkers blood, Inflammation Mediators blood, Prostatic Neoplasms blood, Prostatic Neoplasms diagnosis

Abstract

Improved prostate cancer detection methods would avoid over-diagnosis of clinically indolent disease informing appropriate treatment decisions. The aims of this study were to investigate the role of a panel of Inflammation biomarkers to inform the need for a biopsy to diagnose prostate cancer. Peripheral blood serum obtained from 436 men undergoing transrectal ultrasound guided biopsy were assessed for a panel of 18 inflammatory serum biomarkers in addition to Total and Free Prostate Specific Antigen (PSA). This panel was integrated into a previously developed Irish clinical risk calculator (IPRC) for the detection of prostate cancer and high-grade prostate cancer (Gleason Score ≥ 7). Using logistic regression and multinomial regression methods, two models (Logst-RC and Multi-RC) were developed considering linear and nonlinear effects of the panel in conjunction with clinical and demographic parameters for determination of the two endpoints. Both models significantly improved the predictive ability of the clinical model for detection of prostate cancer (from 0.656 to 0.731 for Logst-RC and 0.713 for Multi-RC) and high-grade prostate cancer (from 0.716 to 0.785 for Logst-RC and 0.767 for Multi-RC) and demonstrated higher clinical net benefit. This improved discriminatory power and clinical utility may allow for individualised risk stratification improving clinical decision making.

Published

2021

14. A comparison of methods for the isolation and separation of extracellular vesicles from protein and lipid particles in human serum.

Author

Brennan K, Martin K, FitzGerald SP, O'Sullivan J, Wu Y, Blanco A, Richardson C, and Mc Gee MM

Subjects

Adult, Biomarkers metabolism, Blood Proteins metabolism, Blotting, Western methods, Centrifugation, Density Gradient methods, Chromatography, Gel methods, Electrophoresis, Polyacrylamide Gel methods, Humans, Lipid Droplets metabolism, Lipoproteins metabolism, Blood Proteins isolation & purification, Extracellular Vesicles metabolism, Lipoproteins isolation & purification

Abstract

Extracellular vesicles (EVs) are nano-sized vesicles containing nucleic acid and protein cargo that are released from a multitude of cell types and have gained significant interest as potential diagnostic biomarkers. Human serum is a rich source of readily accessible EVs; however, the separation of EVs from serum proteins and non-EV lipid particles represents a considerable challenge. In this study, we compared the most commonly used isolation techniques, either alone or in combination, for the isolation of EVs from 200 µl of human serum and their separation from non-EV protein and lipid particles present in serum. The size and yield of particles isolated by each method was determined by nanoparticle tracking analysis, with the variation in particle size distribution being used to determine the relative impact of lipoproteins and protein aggregates on the isolated EV population. Purification of EVs from soluble protein was determined by calculating the ratio of EV particle count to protein concentration. Finally, lipoprotein particles co-isolated with EVs was determined by Western blot analysis of lipoprotein markers APOB and APOE. Overall, this study reveals that the choice of EV isolation procedure significantly impacts EV yield from human serum, together with the presence of lipoprotein and protein contaminants.

Published

2020

15. Application of a New Multiplexed Array for Rapid, Sensitive, Simultaneous and Quantitative Assessment of Spliced and Unspliced XBP1.

Author

Creedican S, Talty A, Fitzgerald SP, Samali A, Richardson C, Gorman AM, and Martin K

Abstract

Background: IRE1α-mediated unconventional splicing of XBP1 is emerging as a biomarker in several disease states and is indicative of activation of the unfolded protein response sensor IRE1. Splicing of XBP1 mRNA results in the translation of two distinct XBP1 protein isoforms (XBP1s and XBP1u) which, due to post-translational regulation, do not correlate with mRNA levels. As both XBP1 isoforms are implicated in pathogenic or disease progression mechanisms there is a need for a reliable, clinically applicable method to detect them., Methods: A multiplexed isoform-specific XBP1 array utilising Biochip array technology (BAT™) was assessed for specificity and suitability when using cell protein lysates. The array was applied to RIPA protein lysates from several relevant pre-clinical models with an aim to quantify XBP1 isoforms in comparison with RT-PCR or immunoblot reference methods., Results: A novel reliable, specific and sensitive XBP1 biochip was successfully utilised in pre-clinical research. Application of this biochip to detect XBP1 splicing at the protein level in relevant breast cancer models, under basal conditions as well as pharmacological inhibition and paclitaxel induction, confirmed the findings of previous studies. The biochip was also applied to non-adherent cells and used to quantify changes in the XBP1 isoforms upon activation of the NLRP3 inflammasome., Conclusions: The XBP1 biochip enables isoform specific quantification of protein level changes upon activation and inhibition of IRE1α RNase activity, using a routine clinical methodology. As such it provides a research tool and potential clinical tool with a quantified, simultaneous, rapid output that is not available from any other published method., Competing Interests: Competing interestsAG and AS are cofounders of Cell Stress Discoveries, Ltd., there no conflicting interests. CR, KM are employed by Randox Teoranta, SPF is employed by Randox Holdings. The funding organization played no role in the study design; in the collection, analysis, and interpretation of data; in the writing of the report; or in the decision to submit the report for publication., (© The Author(s). 2019.)

Published

2019

16. Population data provide evidence against the presence of a set point for hemoglobin levels or tissue oxygen delivery.

Author

Fitzgerald SP, Grote Beverborg N, Beguin Y, Artunc F, Falhammar H, and Bean NG

Subjects

Erythropoietin blood, Humans, Reference Values, Sex Characteristics, Hemoglobins metabolism, Oxygen Consumption physiology, Proteostasis physiology

Abstract

Hemoglobin levels are believed to be regulated as per a set point model of regulation. This model of regulation, by which specific levels of a parameter are targeted and defended by physiological systems, implies a particular population correlation between the parameter and its controlling hormone. Empirical population correlations of other parameters and their controlling hormones, have denied the presence of such set point-based regulation. To assess if hemoglobin is regulated according to a set point model we performed a systematic search of PubMed/MEDLINE and Web of Science identifying relevant reports published up to November 2018. Population hemoglobin/erythropoietin level correlations were retrieved, and these empirically derived correlations were compared with the positive correlation implied by a set point model of regulation. Authors of papers containing potentially suitable data were contacted with requests for further analyses, and a meta-analysis was performed. Twelve correlations between hemoglobin and erythropoietin levels from eleven papers were analyzed. None of these correlations were significantly positive, three, restricted to the normal range of hemoglobin, were significantly negative. All but one of the other correlations showed a negative trend. New analyses of previously published data sets resulted in similar findings. In particular a new analysis of large data sets of males (n = 2417) and females (n = 2592) with normal range hemoglobin levels, revealed significantly negative correlations. A meta-analysis of our results indicated that the data overall are not consistent with a positive relationship between hemoglobin and erythropoietin (P < 0.0001). Population data indicate that individuals do not have set point levels of hemoglobin., (© 2019 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of The Physiological Society and the American Physiological Society.)

Published

2019

17. Thyroid stimulating hormone (TSH) autoregulation reduces variation in the TSH response to thyroid hormones.

Author

Fitzgerald SP and Bean NG

Abstract

The physiological functions of Thyroid Stimulating Hormone (TSH) autoregulation, the ultra-short feedback loop inhibition of TSH by TSH itself, have not been determined. In this work we explored the role of TSH autoregulation in thyroid homeostasis. We synthesized the known physiology of autoregulation with theknown physiological relationships between thyroid hormones; in particular between free thyroxine and TSH. We analysed the implications of TSH autoregulation, on the generation of the TSH response to free thyroxine (the 'TSH curve'), and on the variation inthis response, which might result from variations in hypothalamopituitary or thyroid gland function. Our analysis demonstrated that, in the circumstances of inter-individual and intra-individual variations to hypothalamo-pituitary function TSH autoregulation lessens variation in the TSH curve. This in turn enhances the probability of generating and maintaining a euthyroid free thyroxine value. This contribution of TSH autoregulation to the stabilisation of thyroid physiology offers a logical explanation for the evolutionary selection of this physiological process.

Published

2018

18. Population correlations do not support the existence of set points for blood levels of calcium or glucose - a new model for homeostasis.

Author

Fitzgerald SP and Bean NG

Subjects

Correlation of Data, Female, Humans, Male, Thyroid Hormones blood, Blood Glucose metabolism, Calcium blood, Homeostasis, Models, Biological, Population

Abstract

The prevailing teaching regarding homeostasis, and in particular endocrine homeostasis, includes the fundamental concept of a "set point," which represents a target or optimum level defended by physiological control mechanisms. Analogies for the description and teaching of this concept have included thermostats and cruise controls. We previously demonstrated that such a set-point model of regulation implies that in population data of parameter set point/controlling hormone levels, correlations between the parameter and its controlling hormone must be in the direction of the response of the parameter to its controlling hormone, and that in thyroid homeostasis this relationship is not observed. In this work we similarly examined population correlations, extracted from the literature, for the parameters glucose and calcium, and their controlling hormones. We found 10 correlations. Most were highly significant (P < 0.01). All were in the direction of the response of the controlling hormone to the parameter. Therefore, none were consistent with the pattern implied by a set-point model of regulation. Instead all were consistent with an "equilibrium point" model of regulation, whereby ambient levels have no particular connotation to the individual, and result passively from the interplay of physiological processes. We conclude that glucose and calcium regulation, like thyroid regulation, are not centered on set points. This may reflect a general property of homeostasis. We provide an alternative mechanistic analogy, without a set point, for the heuristic description and teaching, of homeostasis., (© 2018 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of The Physiological Society and the American Physiological Society.)

Published

2018

19. A method of decision analysis quantifying the effects of age and comorbidities on the probability of deriving significant benefit from medical treatments.

Author

Fitzgerald SP, Bean NG, and Ruberu RP

Abstract

Background: The external validity, or generalizability, of trials and guidelines has been considered poor in the context of multiple morbidity. How multiple morbidity might affect the magnitude of benefit of a given treatment, and thereby external validity, has had little study., Objective: To provide a method of decision analysis to quantify the effects of age and comorbidity on the probability of deriving a given magnitude of treatment benefit., Design: We developed a method to calculate probabilistically the effect of all of a patient's comorbidities on their underlying utility, or well-being, at a future time point. From this, we derived a distribution of possible magnitudes of treatment benefit at that future time point. We then expressed this distribution as the probability of deriving at least a given magnitude of treatment benefit. To demonstrate the applicability of this method of decision analysis, we applied it to the treatment of hypercholesterolaemia in a geriatric population of 50 individuals. We highlighted the results of four of these individuals., Results: This method of analysis provided individualized quantifications of the effect of age and comorbidity on the probability of treatment benefit. The average probability of deriving a benefit, of at least 50% of the magnitude of benefit available to an individual without comorbidity, was only 0.8%., Conclusion: The effects of age and comorbidity on the probability of deriving significant treatment benefits can be quantified for any individual. Even without consideration of other factors affecting external validity, these effects may be sufficient to guide decision-making., Competing Interests: The authors have no conflicts of interest to declare.

Published

2017

20. Population data indicate that thyroid regulation is consistent with an equilibrium-point model, but not with a set-point model.

Author

Fitzgerald SP, Bean NG, and Fitzgerald LN

Published

2017

21. Corrigendum to "The Relationship between Population T4/TSH Set Point Data and T4/TSH Physiology".

Author

Fitzgerald SP and Bean NG

Abstract

[This corrects the article DOI: 10.1155/2016/6351473.].

Published

2017

22. The Relationship between Population T4/TSH Set Point Data and T4/TSH Physiology.

Author

Fitzgerald SP and Bean NG

Abstract

Context. Population studies of the distribution of T4/TSH set points suggest a more complex inverse relationship between T4 and TSH than that suggested by physiological studies. The reasons for the similarities and differences between the curves describing these relationships are unresolved. Methods. We subjected the curve, derived from empiric data, describing the TSH suppression response to T4, and the more mathematically derived curve describing the T4 response to TSH, to the different possible models of population variation. The implied consequences of these in terms of generating a population distribution of T4/TSH equilibrium points (a "population curve") were generated and compared to the empiric population curve. The physiological responses to primary hypothyroidism and hyperthyroidism were incorporated into the analysis. Conclusions. Though the population curve shows a similarly inverse relationship, it is describing a different relationship than the curve describing the suppression of TSH by T4. The population curve is consistent with the physiological studies of the TSH response to T4 and implies a greater interindividual variation in the positive thyroid T4 response to TSH than in the central inhibitory TSH response to T4. The population curve in the dysthyroid states is consistent with known physiological responses to these states.

Published

2016

23. The Role of Serine Proteases and Antiproteases in the Cystic Fibrosis Lung.

Author

Twigg MS, Brockbank S, Lowry P, FitzGerald SP, Taggart C, and Weldon S

Subjects

Cathepsin G physiology, Elafin physiology, Humans, Leukocyte Elastase physiology, Myeloblastin physiology, Neutrophils enzymology, Secretory Leukocyte Peptidase Inhibitor physiology, alpha 1-Antitrypsin physiology, Cystic Fibrosis metabolism, Protease Inhibitors metabolism, Serine Proteases physiology

Abstract

Cystic fibrosis (CF) lung disease is an inherited condition with an incidence rate of approximately 1 in 2500 new born babies. CF is characterized as chronic infection of the lung which leads to inflammation of the airway. Sputum from CF patients contains elevated levels of neutrophils and subsequently elevated levels of neutrophil serine proteases. In a healthy individual these proteases aid in the phagocytic process by degrading microbial peptides and are kept in homeostatic balance by cognate antiproteases. Due to the heavy neutrophil burden associated with CF the high concentration of neutrophil derived proteases overwhelms cognate antiproteases. The general effects of this protease/antiprotease imbalance are impaired mucus clearance, increased and self-perpetuating inflammation, and impaired immune responses and tissue. To restore this balance antiproteases have been suggested as potential therapeutics or therapeutic targets. As such a number of both endogenous and synthetic antiproteases have been trialed with mixed success as therapeutics for CF lung disease.

Published

2015

24. Investigation and verification of a bioluminescent biosensor for the quantitation of ara-CTP generation: a biomarker for cytosine arabinoside sensitivity in acute myeloid leukaemia.

Author

Anderson E, Conway M, Alloush H, O'Malley K, Smith MA, Martin A, Ruddock M, Reid C, Lamont J, Fitzgerald SP, Smith JG, Mehta P, and Salisbury V

Subjects

Arabinofuranosylcytosine Triphosphate blood, Biomarkers, Tumor blood, Humans, Leukemia, Myeloid, Acute pathology, Limit of Detection, Luminescent Measurements, Arabinofuranosylcytosine Triphosphate isolation & purification, Biosensing Techniques, Cytarabine isolation & purification, Leukemia, Myeloid, Acute blood

Abstract

A novel whole cell bacterial biosensor, which emits light in response to the active metabolite of cytosine arabinoside (ara-C, cytarabine), ara-CTP, has been investigated and verified. The biosensor has been formulated as an ex vivo assay, designed for peripheral blood or bone marrow cells, which can produce a clinical result within a working day. The nucleoside analogue ara-C is a key agent for treatment of acute myeloid leukaemia (AML); treatment decisions are made rapidly with AML, patients often receiving same-day commencement of chemotherapy. Currently no rapid predictive test is available to select appropriate therapy for patients prior to treatment. Experiments were designed to determine optimal assay conditions using leukaemic cell lines. We observed a significant increase (~15 fold) in bioluminescence signal compared to control after 8-h incubation of the biosensor with ara-C. This corresponded to a >2-log increase in light output per bacterial cell. Interestingly, bioluminescence conferred a survival advantage to the bacteria following ara-C treatment. The assay is sensitive (lower limit of quantitation of 0.05 µM), selective, accurate (≤ 15% RE) and precise (≤ 15% coefficient of variation) over a linear concentration range of ara-CTP (0.05-0.5 µM), and detection is independent of reaction volume. Recovery of added standard was tested using ex vivo patient leukaemic cells (n=5). Stability studies on lyophilized bacterial biosensor were performed to ensure maintenance of performance over 12 months. The biosensor assay could be invaluable to the clinician, assisting with treatment selection, and potentially mitigating the risks of resistance and toxicity observed with this drug., (© 2013 Elsevier B.V. All rights reserved.)

Published

2014

25. A new PCR-based method shows that blue crabs (Callinectes sapidus (Rathbun)) consume winter flounder (Pseudopleuronectes americanus (Walbaum)).

Author

Collier JL, Fitzgerald SP, Hice LA, Frisk MG, and McElroy AE

Subjects

Animals, DNA analysis, DNA genetics, Gastrointestinal Tract metabolism, Molecular Sequence Data, Seasons, Brachyura physiology, Feeding Behavior physiology, Flounder physiology, Polymerase Chain Reaction methods

Abstract

Winter flounder (Pseudopleuronectes americanus) once supported robust commercial and recreational fisheries in the New York (USA) region, but since the 1990s populations have been in decline. Available data show that settlement of young-of-the-year winter flounder has not declined as sharply as adult abundance, suggesting that juveniles are experiencing higher mortality following settlement. The recent increase of blue crab (Callinectes sapidus) abundance in the New York region raises the possibility that new sources of predation may be contributing to juvenile winter flounder mortality. To investigate this possibility we developed and validated a method to specifically detect winter flounder mitochondrial control region DNA sequences in the gut contents of blue crabs. A survey of 55 crabs collected from Shinnecock Bay (along the south shore of Long Island, New York) in July, August, and September of 2011 showed that 12 of 42 blue crabs (28.6%) from which PCR-amplifiable DNA was recovered had consumed winter flounder in the wild, empirically supporting the trophic link between these species that has been widely speculated to exist. This technique overcomes difficulties with visual identification of the often unrecognizable gut contents of decapod crustaceans, and modifications of this approach offer valuable tools to more broadly address their feeding habits on a wide variety of species.

Published

2014

26. A novel multiplex-protein array for serum diagnostics of colorectal cancer: impact of pre-analytical storage conditions.

Author

Bünger S, Klempt-Giessing K, Toner V, Kelly M, FitzGerald SP, Brenner H, von Eggeling F, and Habermann JK

Subjects

Aged, Aged, 80 and over, Colorectal Neoplasms diagnosis, Female, Freezing, High-Throughput Screening Assays, Humans, Male, Middle Aged, Specimen Handling standards, Time Factors, Biomarkers blood, Colorectal Neoplasms blood, Molecular Diagnostic Techniques methods, Protein Array Analysis methods, Specimen Handling methods

Abstract

Introduction: Biomarker discovery studies seldom report on pre-analytical effects. We used a novel multiplex protein biochip for colorectal cancer screening to investigate effects of different storage temperatures and repeated freeze-thaw cycles., Methods: This biochip, composed of CEA, IL-8, VEGF, M-CSF, S100A11, C3adesArg, CD26, and CRP, was applied to twenty highly standardized preserved serum samples., Results: Aliquot comparison of long-term storage at -80°C (n=20) versus -170°C (n=20) did not show significant differences for any of the eight markers. In contrast, three freeze-thaw cycles (3 × 20 aliquots) detected changes in the serum level for all markers (p<0.05) but S100A11 and CD26: levels of CEA, IL-8, C3adesArg, and CRP increased, while VEGF and M-CSF levels decreased. However, applying diagnostic thresholds for CEA, IL-8, and CRP revealed that freeze-thaw cycles did not affect diagnostic performance. In contrast, analysis of samples stored at -80°C compared to -170°C failed to detect one out of three detectable malignancies., Conclusion: We conclude that three freeze-thaw cycles modulated serum marker levels significantly, but do not compromise biochip diagnostic performance. For our marker panel, serum preservation at -80°C seems comparable to -170°C; however, storage at -80°C could lead to misdiagnosis. Our findings emphasize the need for standardized sample collection, processing, storage, and reporting.

Published

2013

27. A novel multiplex-protein array for serum diagnostics of colon cancer: a case-control study.

Author

Bünger S, Haug U, Kelly M, Posorski N, Klempt-Giessing K, Cartwright A, Fitzgerald SP, Toner V, McAleer D, Gemoll T, Laubert T, Büning J, Fellermann K, Bruch HP, Roblick UJ, Brenner H, von Eggeling F, and Habermann JK

Subjects

Adenoma blood, Adenoma diagnosis, Adult, Aged, Aged, 80 and over, Algorithms, C-Reactive Protein metabolism, Carcinoembryonic Antigen blood, Case-Control Studies, Colonic Neoplasms diagnosis, Computational Biology, Female, High-Throughput Screening Assays, Humans, Interleukin-8 blood, Male, Middle Aged, Protein Array Analysis methods, ROC Curve, Biomarkers, Tumor blood, Colonic Neoplasms blood, Molecular Diagnostic Techniques methods

Abstract

Background: More than 1.2 million new cases of colorectal cancer are reported each year worldwide. Despite actual screening programs, about 50% of the patients are diagnosed at advanced tumor stages presenting poor prognosis. Innovative screening tools could aid the detection at early stages and allow curative treatment interventions., Methods: A nine target multiplex serum protein biochip was generated and evaluated using a training- and validation-set of 317 highly standardized, liquid nitrogen preserved serum samples comprising controls, adenomas, and colon cancers., Results: Serum levels of CEA, IL-8, VEGF, S100A11, MCSF, C3adesArg, CD26, and CRP showed significant differences between cases and controls. The largest areas under the receiver operating characteristics curve were observed for CEA, IL-8, and CRP. At threshold levels yielding 90% specificity, sensitivities for CEA, IL-8 and CRP were 26%, 22%, and 17%, respectively. The most promising marker combinations were CEA + IL-8 reaching 37% sensitivity at 83% specificity and CEA + CRP with 35% sensitivity at 81% specificity. In an independent validation set CEA + IL-8 reached 47% sensitivity at 86% specificity while CEA + CRP obtained 39% sensitivity at 86% specificity. Early carcinomas were detected with 33% sensitivity for CEA + IL-8 and 28% for CEA + CRP., Conclusions: Apart from CEA, IL-8, and CRP, the screening value of additional blood markers and the potential advantage of combining serum biochip testing with fecal occult blood testing needs to be studied. Multiplex biochip array technology utilizing serum samples offers an innovative approach to colorectal cancer screening.

Published

2012

28. Development of an Evidence biochip array kit for the multiplex screening of more than 20 anthelmintic drugs.

Author

Porter J, O'Loan N, Bell B, Mahoney J, McGarrity M, McConnell RI, and Fitzgerald SP

Subjects

Animals, Cattle, Immunoassay methods, Indicators and Reagents, Luminescent Measurements methods, Milk chemistry, Anthelmintics analysis, Drug Evaluation, Preclinical methods, Microarray Analysis methods

Abstract

Anthelmintic drugs are used in clinical and veterinary practice for the treatment of infections caused by parasitic worms. Their extensive use in food-producing animals can cause the presence of residues in food. For consumer protection it is necessary to monitor the levels of anthelmintic residues to ensure that they remain within the legally permitted maximum acceptable concentrations. For this purpose, the use of multiplex screening methods is advantageous. Biochip array technology allows the simultaneous determination of multiple analytes from a single sample at a single point in time. This study reports the development of an Evidence biochip array for the multiplex screening of anthelmintic drugs. Simultaneous competitive chemiluminescent immunoassays are employed. The solid support and vessel is the biochip, which contains an array of discrete test sites. The assays were applied to the semiautomated bench-top analyser Evidence Investigator. The aminobenzimidazoles assay detected aminomebendazole, albendazole 2-aminosulphone and aminoflubendazole, the avermectins assay detected emamectin benzoate, eprinomectin, abamectin, ivermectin and doramectin, the benzimidazoles assay detected albendazole sulphone, albendazole, albendazole sulphoxide, oxibendazole, oxfendazole and flubendazole, the thiabendazole assay detected cambendazole, thiabendazole and 5-hydroxythiabendazole and the triclabendazole assay detected ketotriclabendazole, triclabendazole and triclabendazole sulphoxide. The limits of detection ranged from 0.3 ppb (aminobenzimidazoles) to 2.0 ppb (levamisole) in milk and from 0.15 ppb (aminobenzimidazoles) to 6.5 ppb (levamisole) in tissue. The average recovery range was 71-135 %. This multianalytical approach on a biochip platform is applicable to the screening of more than 20 anthelmintic drugs in different food matrices, leading to consolidation of tests and enhancement of the test result output.

Published

2012

29. Toward standardized high-throughput serum diagnostics: multiplex-protein array identifies IL-8 and VEGF as serum markers for colon cancer.

Author

Bünger S, Haug U, Kelly FM, Klempt-Giessing K, Cartwright A, Posorski N, Dibbelt L, Fitzgerald SP, Bruch HP, Roblick UJ, von Eggeling F, Brenner H, and Habermann JK

Subjects

Adult, Aged, Aged, 80 and over, CA-19-9 Antigen blood, Carcinoembryonic Antigen blood, Colonic Neoplasms pathology, Female, Humans, Male, Middle Aged, Neoplasm Staging, Sensitivity and Specificity, Biomarkers, Tumor blood, Colonic Neoplasms blood, Colonic Neoplasms diagnosis, High-Throughput Screening Assays standards, Interleukin-8 blood, Protein Array Analysis, Vascular Endothelial Growth Factor A blood

Abstract

Development and progression of colon cancer may be related to cytokines. Cytokines with diagnostic value have been identified individually but have not been implemented into clinical praxis. Using a multiplex protein array, the authors explore a panel of cytokines simultaneously and compared its performance to carcinoembryonic antigen (CEA) and carbohydrate antigen 19-9 (CA 19-9). Serum concentrations of 12 cytokines were simultaneously determined by multiplex biochip technology in 50 colon cancer patients and 50 healthy controls. Serum levels of interleukin-8 (IL-8) and CEA were significantly higher in cancer patients than in healthy controls. Areas under the receiver operating characteristic curves (AUCs) were largest for IL-8, followed by CEA, vascular endothelial growth factor (VEGF), and CA 19-9. Analyses regarding marker combinations showed an advantage over single marker performance for CEA, VEGF, and CA 19-9 but not for IL-8. Multiplex biochip array technology represents a practical tool in cytokine and cancer research when simultaneous determination of different biomarkers is of interest. The results suggest that the assessment of IL-8, CEA, VEGF, and possibly CA 19-9 serum levels could be useful for colon cancer screening with the potential of also detecting early stage tumors. Further validation studies using these and additional markers on a multiplex array format are encouraged.

Published

2011

30. Lack of association between EGF 61A>G polymorphism and plasma EGF concentration in the STANISLAS family study.

Author

Berrahmoune H, Herbeth B, Lamont JV, Masson C, FitzGerald SP, and Visvikis-Siest S

Subjects

Adenine, Guanine, Humans, Osmolar Concentration, Prognosis, Epidermal Growth Factor blood, Epidermal Growth Factor genetics, Melanoma blood, Melanoma genetics, Polymorphism, Genetic, Skin Neoplasms blood, Skin Neoplasms genetics

Published

2007

31. Development of a high-throughput automated analyzer using biochip array technology.

Author

Fitzgerald SP, Lamont JV, McConnell RI, and Benchikh el O

Subjects

Autoanalysis, Biomarkers analysis, Cytokines analysis, Humans, Luminescent Measurements, Reproducibility of Results, Spectrometry, Mass, Electrospray Ionization, Spectrometry, X-Ray Emission, Protein Array Analysis methods

Abstract

Background: Use of protein array technology over conventional assay methods has advantages that include simultaneous detection of multiple analytes, reduction in sample and reagent volumes, and high output of test results. The susceptibility of ligands to denaturation, however, has impeded production of a stable, reproducible biochip platform, limiting most array assays to manual or, at most, semiautomated processing techniques. Such limitations may be overcome by novel biochip fabrication procedures., Methods: After selection of a suitable biochip substrate, biochip surfaces were chemically modified and assessed to enable optimization of biochip fabrication procedures for different test panels. The assay procedure was then automated on a dedicated instrument, and assay performance was determined for a panel of cytokine markers. Assay results were then compared with a commercial method for measurement of cytokine markers., Results: Secondary ion mass spectrometry and x-ray photoelectron spectroscopy demonstrated appropriate and reproducible modification of the biochip surface. Contact-angle studies also confirmed generation of hydrophobic surfaces that enabled containment of droplets for fabrication of discrete test regions. Automation of the biochip assays on a dedicated instrument produced excellent cytokine marker performance with intra- and interassay imprecision <10% for most analytes. Comparison studies showed good agreement with other methods (r = 0.95-0.99) for cytokines., Conclusion: Performance data from this automated biochip array analyzer provide evidence that it is now possible to produce stable and reproducible biochips for output of more than 2000 test results per hour.

Published

2005

32. Familial corticosteroid-binding globulin deficiency due to a novel null mutation: association with fatigue and relative hypotension.

Author

Torpy DJ, Bachmann AW, Grice JE, Fitzgerald SP, Phillips PJ, Whitworth JA, and Jackson RV

Subjects

Adrenocorticotropic Hormone, Adult, Amino Acid Sequence, Australia, Base Sequence, Blood Pressure, Codon, Terminator, Exons, Fatigue blood, Female, Genetic Carrier Screening, Homozygote, Humans, Hydrocortisone blood, Hypotension blood, Italy ethnology, Male, Middle Aged, Pedigree, Polymerase Chain Reaction, Radioimmunoassay, Restriction Mapping, Transcortin analysis, White People, alpha 1-Antitrypsin genetics, alpha 1-Antitrypsin metabolism, Fatigue genetics, Hypotension genetics, Mutation, Transcortin deficiency, Transcortin genetics

Abstract

Corticosteroid-binding globulin is a 383-amino acid glycoprotein that serves a hormone transport role and may have functions related to the stress response and inflammation. We describe a 39-member Italian-Australian family with a novel complete loss of function (null) mutation of the corticosteroid-binding globulin gene. A second, previously described, mutation (Lyon) segregated independently in the same kindred. The novel exon 2 mutation led to a premature termination codon corresponding to residue -12 of the procorticosteroid-binding globulin molecule (c.121G-->A). Among 32 family members there were 3 null homozygotes, 19 null heterozygotes, 2 compound heterozygotes, 3 Lyon heterozygotes, and 5 individuals without corticosteroid-binding globulin mutations. Plasma immunoreactive corticosteroid-binding globulin was undetectable in null homozygotes, and mean corticosteroid-binding globulin levels were reduced by approximately 50% at 18.7 +/- 1.3 microg/ml (reference range, 30-52 microg/ml) in null heterozygotes. Morning total plasma cortisol levels were less than 1.8 microg/dl in homozygotes and were positively correlated to the plasma corticosteroid-binding globulin level in heterozygotes. Homozygotes and heterozygote null mutation subjects had a high prevalence of hypotension and fatigue. Among 19 adults with the null mutation, the systolic blood pressure z-score was 12.1 +/- 3.5; 11 of 19 subjects (54%) had a systolic blood pressure below the third percentile. The mean diastolic blood pressure z-score was 18.1 +/- 3.4; 8 of 19 subjects (42%) had a diastolic blood pressure z-score below 10. Idiopathic chronic fatigue was present in 12 of 14 adult null heterozygote subjects (86%) and in 2 of 3 null homozygotes. Five cases met the Centers for Disease Control criteria for chronic fatigue syndrome. Fatigue questionnaires revealed scores of 25.1 +/- 2.5 in 18 adults with the mutation vs. 4.2 +/- 1.5 in 23 healthy controls (P < 0.0001). Compound heterozygosity for both mutations resulted in plasma cortisol levels comparable to those in null homozygotes. Abnormal corticosteroid-binding globulin concentrations or binding affinity may lead to the misdiagnosis of isolated ACTH deficiency. The mechanism of the association between fatigue and relative hypotension is not established by these studies. As idiopathic fatigue disorders are associated with relatively low plasma cortisol, abnormalities of corticosteroid-binding globulin may be pathogenic.

Published

2001

33. Bacteriostatic effect of serum: role of antibody to lipopolysaccharide.

Author

Fitzgerald SP and Rogers HJ

Subjects

Animals, Escherichia coli immunology, Escherichia coli Infections immunology, Lactoferrin physiology, Mice, Transferrin physiology, Antibodies, Bacterial physiology, Blood Physiological Phenomena, Deoxy Sugars immunology, Escherichia coli growth & development, Lipopolysaccharides immunology

Abstract

Previous work has shown that antibody and transferrin, acting together, exert a bacteriostatic effect on certain pathogenic Escherichia coli. This effect may be due to the ability of the antibody to interfere with the release of the iron chelator, enterochelin, from the bacterial cell. Enterochelin is essential for the transport of iron from transferrin to the bacterial cell. The nature of the bacterial antigen against which the antibody is directed has now been determined by means of adsorption experiments. It was found that absorption of serum either with hear-killed cells of E. coli O111 or with Boivin antigen abolished the bacteriostatic effect. A monosaccharide, which proved to be colitose (3,6-dideoxy-L-galactose), was isolated after acetic acid hydrolysis of the Boivin antigen. Colitose is the terminal monosaccharide of the O-specific side chain of the lipopolysaccharide from E. coli O111. This monosaccharide abolished the bacteriostatic effect of both whole serum and mixtures of antibody and iron-binding proteins. When administered by the intraperitoneal route, it reduced the resistance of mice to subsequent infection with E. coli O111. This ability of colitose to interfere with antibacterial mechanisms is in accord with published immunochemical studies.

Published

1980

34. Neuronal cell killing by the envelope protein of HIV and its prevention by vasoactive intestinal peptide.

Author

Brenneman DE, Westbrook GL, Fitzgerald SP, Ennist DL, Elkins KL, Ruff MR, and Pert CB

Subjects

Animals, Antibodies, Monoclonal, Antigens, Differentiation, T-Lymphocyte immunology, Cells, Cultured, Dose-Response Relationship, Drug, HIV Envelope Protein gp120, Hippocampus cytology, Mice, Recombinant Proteins pharmacology, Neurons drug effects, Retroviridae Proteins pharmacology, Vasoactive Intestinal Peptide pharmacology

Abstract

The clinical manifestations of AIDS (acquired immune deficiency syndrome) often include neuropsychiatric and neurological deficits, including early memory loss and progressive dementia. HIV (human immunodeficiency virus), the aetiological agent of AIDS, is probably carried by infected macrophages in the central nervous system. The virus enters cells by binding its envelope glycoprotein gp120 to the CD4 antigen present on brain and immune cells. From the data reported in this paper, we now suggest that the neuronal deficits associated with HIV may not be entirely a result of infectivity, but that gp120 shed from HIV could directly produce the neuropathology as a result of its interference with endogenous neurotrophic substances. It is known that an analogue of a sequence contained in vasoactive intestinal peptide (VIP) occurs in all known sequenced gp120 isolates and that VIP is important for neuronal survival in cell culture. Here we show that purified gp120 from two diverse HIV isolates and a recombinant gp120 from a third isolate were all potent in specifically producing significant neuronal cell death in dissociated hippocampal cultures derived from fetal mice, and that this could be reduced by monoclonal antibodies against the murine CD4 antigen and completely antagonized by VIP.

Published

1988

35. The isolation of large and small plaque canine distemper viruses which differ in their neurovirulence for hamsters.

Author

Cosby SL, Lyons C, Fitzgerald SP, Martin SJ, Pressdee S, and Allen IV

Subjects

Animals, Antibodies, Viral biosynthesis, Antigens, Viral, Cell Line, Chlorocebus aethiops, Cricetinae, Cytopathogenic Effect, Viral, Distemper Virus, Canine growth & development, Distemper Virus, Canine immunology, Dogs, Mesocricetus, Temperature, Viral Plaque Assay, Viral Proteins biosynthesis, Central Nervous System Diseases etiology, Distemper microbiology, Distemper Virus, Canine pathogenicity

Abstract

Large and small plaque-forming viruses were isolated from the Onderstepoort strain of canine distemper virus (CDV). Small plaque virus, which was released more slowly from infected cells than large plaque virus, readily established persistent infections in Vero cells, whereas large plaque virus required undilute passage to do so. All persistently infected cultures eventually released small plaque virus. No difference was found in the size of polypeptides induced by either plaque-purified viruses or virus released from persistent cultures. Both dilute and undilute passage, large plaque virus produced an acute neurological illness in weanling hamsters. whereas small plaque virus failed to produce any clinical signs of disease for 3 months after inoculation. After this period 50% of the animals infected with small plaque virus showed a general deterioration in their condition and lesions were observed in the brain which resembled those found in cases of large plaque virus infection. Serum-neutralizing antibody titres to CDV rapidly increased after infection with small plaque virus, whereas animals infected with large plaque virus had low or undetectable levels. All hamsters infected with small plaque virus and a small number which survived large plaque virus infection had elevated titres of antibody over a test period of 15 months.

Published

1981