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428 results on '"Reardon C"'

1. The cholinergic anti‐inflammatory pathway revisited

Author

Murray, K and Reardon, C

Subjects
Biomedical and Clinical Sciences, Immunology, Neurosciences, Digestive Diseases, Autoimmune Disease, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Animals, Humans, Inflammatory Bowel Diseases, Receptors, Cholinergic, Signal Transduction, Vagus Nerve Stimulation, autonomic nervous system, cholinergic anti-inflammatory pathway, colitis, inflammation, vagal nerve stimulation, Clinical Sciences, Medical Physiology, Gastroenterology & Hepatology, Clinical sciences, Medical physiology
Abstract

Inflammatory bowel disease negatively affects the quality of life of millions of patients around the world. Although the precise etiology of the disease remains elusive, aberrant immune system activation is an underlying cause. As such, therapies that selectively inhibit immune cell activation without broad immunosuppression are desired. Inhibition of immune cell activation preventing pro-inflammatory cytokine production through neural stimulation has emerged as one such treatment. These therapeutics are based on the discovery of the cholinergic anti-inflammatory pathway, a reflex arc that induces efferent vagal nerve signaling to reduce immune cell activation and consequently mortality during septic shock. Despite the success of preclinical and clinical trials, the neural circuitry and mechanisms of action of these immune-regulatory circuits are controversial. At the heart of this controversy is the protective effect of vagal nerve stimulation despite an apparent lack of neuroanatomical connections between the vagus and target organs. Additional studies have further emphasized the importance of sympathetic innervation of these organs, and that alternative neural circuits could be involved in neural regulation of the immune system. Such controversies also extend to the regulation of intestinal inflammation, with the importance of efferent vagus nerve signals in question. Experiments that better characterize these pathways have now been performed by Willemze et al. in this issue of Neurogastroenterology & Motility. These continued efforts will be critical to the development of better neurostimulator based therapeutics for inflammatory bowel disease.

Published
2018

2. Effect of lithographically-induced strain relaxation on the magnetic domain configuration in microfabricated epitaxially grown Fe81Ga19

Author

Beardsley, R. P., Parkes, D. E., Zemen, J., Bowe, S., Edmonds, K. W., Reardon, C., Maccherozzi, F., Isakov, I., Warburton, P. A., Campion, R. P., Gallagher, B. L., Cavill, S. A., and Rushforth, A. W.

Subjects
Condensed Matter - Mesoscale and Nanoscale Physics
Abstract

We investigate the role of lithographically-induced strain relaxation in a micron-scaled device fabricated from epitaxial thin films of the magnetostrictive alloy Fe81Ga19. The strain relaxation due to lithographic patterning induces a magnetic anisotropy that competes with the magnetocrystalline and shape induced anisotropies to play a crucial role in stabilising a flux-closing domain pattern. We use magnetic imaging, micromagnetic calculations and linear elastic modelling to investigate a region close to the edges of an etched structure. This highly-strained edge region has a significant influence on the magnetic domain configuration due to an induced magnetic anisotropy resulting from the inverse magnetostriction effect. We investigate the competition between the strain-induced and shape-induced anisotropy energies, and the resultant stable domain configurations, as the width of the bar is reduced to the nanoscale range. Understanding this behaviour will be important when designing hybrid magneto-electric spintronic devices based on highly magnetostrictive materials.

Published
2016
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3. Characterization of idiopathic chronic diarrhea and associated intestinal inflammation and preliminary observations of effects of vagal nerve stimulation in a non-human primate

Author

Populin, LC, Rajala, AZ, Matkowskyj, KA, Saha, S, Zeng, W, Christian, B, Mcvea, A, Tay, EX, Mueller, EM, Malone, ME, Brust-Mascher, I, Mcmillan, AB, Ludwig, KA, Suminski, AJ, Reardon, C, Furness, JB, Populin, LC, Rajala, AZ, Matkowskyj, KA, Saha, S, Zeng, W, Christian, B, Mcvea, A, Tay, EX, Mueller, EM, Malone, ME, Brust-Mascher, I, Mcmillan, AB, Ludwig, KA, Suminski, AJ, Reardon, C, and Furness, JB

Abstract

BACKGROUND: Diarrhea is commonly associated with irritable bowel syndrome, inflammatory bowel disease, microscopic colitis, and other gastrointestinal dysfunctions. Spontaneously occurring idiopathic chronic diarrhea is frequent in rhesus macaques, but has not been used as a model for the investigation of diarrhea or its treatment. We characterized this condition and present preliminary data demonstrating that left vagal nerve stimulation provides relief. METHODS: Stool consistency scores were followed for up to 12 years. Inflammation was assessed by plasma C-reactive protein, [18F]fluorodeoxyglucose (FDG) uptake, measured by positron emission tomography (PET), multiplex T cell localization, endoscopy and histology. The vagus was stimulated for 9 weeks in conscious macaques, using fully implanted electrodes, under wireless control. KEY RESULTS: Macaques exhibited recurrent periods of diarrhea for up to 12 years, and signs of inflammation: elevated plasma C-reactive protein, increased bowel FDG uptake and increased mucosal T helper1 T-cells. The colon and distal ileum were endoscopically normal, and histology revealed mild colonic inflammation. Application of vagal nerve stimulation to conscious macaques (10 Hz, 30 s every 3 h; 24 h a day for 9 weeks) significantly reduced severity of diarrhea and also reduced inflammation, as measured by FDG uptake and C-reactive protein. CONCLUSIONS AND INFERENCES: These macaques exhibit spontaneously occurring diarrhea with intestinal inflammation that can be reduced by VNS. The data demonstrate the utility of this naturally occurring primate model to study the physiology and treatments for chronic diarrhea and the neural control circuits influencing diarrhea and inflammation that are not accessible in human subjects.

Published
2024

5. Unique lamina propria stromal cells imprint the functional phenotype of mucosal dendritic cells

Author

Vicente-Suarez, I, Larange, A, Reardon, C, Matho, M, Feau, S, Chodaczek, G, Park, Y, Obata, Y, Gold, R, Wang-Zhu, Y, Lena, C, Zajonc, DM, Schoenberger, SP, Kronenberg, M, and Cheroutre, H

Subjects
Biomedical and Clinical Sciences, Immunology, Nutrition, Digestive Diseases, Underpinning research, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Cell Communication, Cell Differentiation, Cell Movement, Cells, Cultured, Dendritic Cells, Diet, Granulocyte-Macrophage Colony-Stimulating Factor, Immunity, Mucosal, Immunomodulation, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Mice, Knockout, Mucous Membrane, Stromal Cells, T-Lymphocytes, Tretinoin, Biological Sciences, Medical and Health Sciences
Abstract

Mucosal dendritic cells (DCs) in the intestine acquire the unique capacity to produce retinoic acid (RA), a vitamin A metabolite that induces gut tropism and regulates the functional differentiation of the T cells they prime. Here, we identified a stromal cell (SC) population in the intestinal lamina propria (LP), which is capable of inducing RA production in DCs in a RA- and granulocyte-macrophage colony-stimulating factor (GM-CSF)-dependent fashion. Unlike DCs, LP SCs constitutively expressed the enzymatic machinery to produce RA even in the absence of dietary vitamin A, but were not able to do so in germ-free mice implying regulation by microbiota. Interestingly, DCs promoted GM-CSF production by the SCs indicating a two-way cross-talk between both cell types. Furthermore, RA-producing LP SCs and intestinal DCs localized closely in vivo suggesting that the interactions between both cell types might have an important role in the functional education of migratory DCs and therefore in the regulation of immune responses toward oral and commensal antigens.

Published
2015

7. Mutation in protein disulfide isomerase A3 causes neurodevelopmental defects by disturbing endoplasmic reticulum proteostasis

Author

Medinas, D. B. (Danilo Bilches), Malik, S. (Sajid), Yıldız-Bölükbaşı, E. (Esra), Borgonovo, J. (Janina), Saaranen, M. J. (Mirva J), Urra, H. (Hery), Pulgar, E. (Eduardo), Afzal, M. (Muhammad), Contreras, D. (Darwin), Wright, M. T. (Madison T), Bodaleo, F. (Felipe), Quiroz, G. (Gabriel), Rozas, P. (Pablo), Mumtaz, S. (Sara), Díaz, R. (Rodrigo), Rozas, C. (Carlos), Cabral-Miranda, F. (Felipe), Piña, R. (Ricardo), Valenzuela, V. (Vicente), Uyan, O. (Ozgun), Reardon, C. (Christopher), Woehlbier, U. (Ute), Brown, R. H. (Robert H), Sena-Esteves, M. (Miguel), Gonzalez-Billault, C. (Christian), Morales, B. (Bernardo), Plate, L. (Lars), Ruddock, L. W. (Lloyd W), Concha, M. L. (Miguel L), Hetz, C. (Claudio), Tolun, A. (Aslıhan), Medinas, D. B. (Danilo Bilches), Malik, S. (Sajid), Yıldız-Bölükbaşı, E. (Esra), Borgonovo, J. (Janina), Saaranen, M. J. (Mirva J), Urra, H. (Hery), Pulgar, E. (Eduardo), Afzal, M. (Muhammad), Contreras, D. (Darwin), Wright, M. T. (Madison T), Bodaleo, F. (Felipe), Quiroz, G. (Gabriel), Rozas, P. (Pablo), Mumtaz, S. (Sara), Díaz, R. (Rodrigo), Rozas, C. (Carlos), Cabral-Miranda, F. (Felipe), Piña, R. (Ricardo), Valenzuela, V. (Vicente), Uyan, O. (Ozgun), Reardon, C. (Christopher), Woehlbier, U. (Ute), Brown, R. H. (Robert H), Sena-Esteves, M. (Miguel), Gonzalez-Billault, C. (Christian), Morales, B. (Bernardo), Plate, L. (Lars), Ruddock, L. W. (Lloyd W), Concha, M. L. (Miguel L), Hetz, C. (Claudio), and Tolun, A. (Aslıhan)

Abstract

Recessive gene mutations underlie many developmental disorders and often lead to disabling neurological problems. Here, we report identification of a homozygous c.170G>A (p.Cys57Tyr or C57Y) mutation in the gene coding for protein disulfide isomerase A3 (PDIA3, also known as ERp57), an enzyme that catalyzes formation of disulfide bonds in the endoplasmic reticulum, to be associated with syndromic intellectual disability. Experiments in zebrafish embryos show that PDIA3C57Y expression is pathogenic and causes developmental defects such as axonal disorganization as well as skeletal abnormalities. Expression of PDIA3C57Y in the mouse hippocampus results in impaired synaptic plasticity and memory consolidation. Proteomic and functional analyses reveal that PDIA3C57Y expression leads to dysregulation of cell adhesion and actin cytoskeleton dynamics, associated with altered integrin biogenesis and reduced neuritogenesis. Biochemical studies show that PDIA3C57Y has decreased catalytic activity and forms disulfide-crosslinked aggregates that abnormally interact with chaperones in the endoplasmic reticulum. Thus, rare disease gene variant can provide insight into how perturbations of neuronal proteostasis can affect the function of the nervous system.

Published
2022

9. Identifying, Replicating, and Spreading Health care Innovations across a Nation‐Wide Health care System: VHA Diffusion of Excellence

Author

Jackson, G., primary, Cutrona, S., additional, White, B., additional, Reardon, C., additional, Orvek, E., additional, Nevedal, A., additional, Lindquist, J., additional, Gifford, A., additional, King, H., additional, DeLaughter, K., additional, Henderson, B., additional, Vega, R., additional, and Damschroder, L., additional

Published
2020
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12. One thousand plant transcriptomes and the phylogenomics of green plants

Author

Leebens, Mack J.H., Graham, S.W, Wong, G.K-S., DeGironimo, L., Edger, P.P., Jordon-Thaden, I.E., Joya, S., Melkonian, B., Miles, N.W., Pokorny Montero, L., Quigley, C., Thomas, P., Villarreal, J.C., Augustin, M.M., Barrett, M.D., Baucom, R.S., Beerling, D.J., Benstein, R.M., Biffin, E., Brockington, S.F., Burge, D.O., Burris, J.N., Burris, K.P., Burtet-Sarramegna, V., Caicedo, A.L., Cannon, S.B., Çebi, Z., Chang, Y., Chater, C., Cheeseman, J.M., Chen, T., Clarke, N.D., Clayton, H., Covshoff, S., Crandall-Stotler, B.J., Cross, H., Determann, R., Dickson, R.C., Di Stilio, V.S., Ellis, S., Fast, E., Feja, N., Field, K.J., Filatov, D.A., Finnegan, P.M., Floyd, S.K., Fogliani, B., GarcÍa, N., Gâteblé, G., Godden, G.T., Goh, Q., Greiner, S., Harkess, A., Heaney, Mike J., Helliwell, K.E., Heyduk, K., Hibberd, J.M., Hodel, R.G.J., Hollingsworth, P.M., Johnson, M.T.J., Jost, R., Joyce, B., Kapralov, M.V., Kazamia, E., Kellogg, E.A., Koch, M.A., Von Konrat, M., Könyves, K., Kutchan, T.M., Lam, V., Larsson, A., Leitch, A.R., Lentz, R., Li, F.-W., Lowe, A.J., Ludwig, M., Manos, P.S., Mavrodiev, E., McCormick, M.K., McKain, M, McLellan, T., McNeal, J., Miller, R., Nelson, M.N., Peng, Y., Ralph, P., Real, D., Riggins, C.W., Ruhsam, M., Sage, R.F., Sakai, A.K., Scascitella, M., Schilling, E.E., Schlösser, E., Sederoff, H., Servick, S., Shaw, A.J., Shaw, S.W., Sigel, E.M., Skema, C., Smith, A.G., Smithson, A., NeilStewart, C., Stinchcombe, J.R., Szövényi, P., Tate, J.A., Tiebel, H., Trapnell, D., Villegente, M., Wang, C., Weller, S.G., Wenzel, M., Weststrand, S., Westwood, J.H., Whigham, D.F., Wulff, A.S., Yang, Y., Zhu, D., Zhuang, C., Zuidof, J., Chase, M.W., Deyholos, M.K., Graham, S.W., Pires, J. Chris, Rothfels, C.J., Chen, C., Chen, L., Cheng, S., Li, J., Li, R., Li, X., Lu, H., Ou, Y., Tan, X., Tang, J., Tian, Z., Wang, F., Wang, J., Wei, X., Wong, G. K.-S., Xu, X., Yan, Z., Yang, F., Zhong, X., Zhou, F., Zhu, Y., Zhang, Y., Yu, J., Barkman, T. J., Carpenter, E. J., Liu, T., Sun, X., Wu, S., Mirarab, S., Nguyen, N., Gitzendanner, M. A., Ayyampalayam, S., Der, J., Matasci, N., Sayyari, E., Soltis, D. E., Soltis, P. S., Stevenson, D. W., Wafula, E. K., Walls, R., Wickett, N. J., De Pamphilis, C. W., Graham, S. W, Leebens-Mack, J. H., Warnow, T., Li, Z., An, H., Arrigo, N., Baniaga, A. E., Galuska, S., Jorgensen, S. A., Kidder, T. I., Kong, H., Lu-Irving, P., Marx, H. E., Qi, X., Reardon, C. R., Sessa, E. B., Sutherland, B. L., Tiley, G. P., Welles, S. R., Yu, R., Zhan, S., Barker, M. S., Porsch, M., Ullrich, K. K., Gramzow, L., Melkonian, M., Nelson, D. R., Theißen, G., Wong, G. K. S., Grosse, I., Rensing, S. A., Quint, M., Institut de sciences exactes et appliquées (ISEA), Université de la Nouvelle-Calédonie (UNC), Apollo - University of Cambridge Repository, National Key Research and Development Program (China), Ministry of Science and Technology of the People's Republic of China, Filatov, D, One Thousand Plant Transcriptomes Initiative, and School of Plant and Environmental Sciences

Subjects
0106 biological sciences, Genome evolution, Nuclear gene, 631/208/212/2306, [SDV]Life Sciences [q-bio], Viridiplantae, 01 natural sciences, Genome, Article, Evolution, Molecular, 03 medical and health sciences, Plant evolution, Phylogenomics, Databases, Genetic, Glaucophyta, 631/449/2669, 631/181/735, Plastid, Phylogeny, 45/90, 030304 developmental biology, 45/91, Adaptive radiation, 0303 health sciences, 631/181/759/2467, Multidisciplinary, biology, Archaeplastida, fungi, Botany, food and beverages, Botanik, 15. Life on land, biology.organism_classification, Biological Evolution, Evolutionary biology, Molecular evolution, Transcriptome, Genome, Plant, 010606 plant biology & botany
Abstract

Green plants (Viridiplantae) include around 450,000–500,000 species1,2 of great diversity and have important roles in terrestrial and aquatic ecosystems. Here, as part of the One Thousand Plant Transcriptomes Initiative, we sequenced the vegetative transcriptomes of 1,124 species that span the diversity of plants in a broad sense (Archaeplastida), including green plants (Viridiplantae), glaucophytes (Glaucophyta) and red algae (Rhodophyta). Our analysis provides a robust phylogenomic framework for examining the evolution of green plants. Most inferred species relationships are well supported across multiple species tree and supermatrix analyses, but discordance among plastid and nuclear gene trees at a few important nodes highlights the complexity of plant genome evolution, including polyploidy, periods of rapid speciation, and extinction. Incomplete sorting of ancestral variation, polyploidization and massive expansions of gene families punctuate the evolutionary history of green plants. Notably, we find that large expansions of gene families preceded the origins of green plants, land plants and vascular plants, whereas whole-genome duplications are inferred to have occurred repeatedly throughout the evolution of flowering plants and ferns. The increasing availability of high-quality plant genome sequences and advances in functional genomics are enabling research on genome evolution across the green tree of life., The One Thousand Plant Transcriptomes Initiative provides a robust phylogenomic framework for examining green plant evolution that comprises the transcriptomes and genomes of diverse species of green plants.

Published
2019

13. Hybrid plasmonic waveguide coupling of photons from a single molecule

Author

Grandi, S, Nielsen, MP, Cambiasso, J, Boissier, S, Major, KD, Reardon, C, Krauss, TF, Oulton, RF, Hinds, EA, and Clark, AS

Subjects
quant-ph, Physics::Optics, physics.optics
Abstract

We demonstrate the emission of photons from a single molecule into a hybrid gap plasmon waveguide (HGPW). Crystals of anthracene, doped with dibenzoterrylene (DBT), are grown on top of the waveguides. We investigate a single DBT molecule coupled to the plasmonic region of one of the guides, and determine its in-plane orientation, excited state lifetime and saturation intensity. The molecule emits light into the guide, which is remotely out-coupled by a grating. The second-order auto-correlation and cross-correlation functions show that the emitter is a single molecule and that the light emerging from the grating comes from that molecule. The coupling efficiency is found to be $\beta_{WG}=11.6(1.5)\%$. This type of structure is promising for building new functionality into quantum-photonic circuits, where localised regions of strong emitter-guide coupling can be interconnected by low-loss dielectric guides.

Published
2019

14. 19th Sir peter freyer memorial lecture and surgical symposium 16th and 17th September 1994: Session I General (Parallel with Oncology / Immunology)

Author

McEvoy, D. A., Connolly, B., Donohue, V., O’Halpin, D., Rowley, H., O’Dywer, T. P., Timon, C., McKeever, J. A., Stokes, M. A., Bannigan, J. G., Early, M. J., Baker, D. M., Nguyen, Van-Tam, Bush, D., Jones, J., Bourke, J. B., Cross, K. S., Durkan, G., Stokes, M., Carroll, T., Gorey, T., O’Malley, K., Mulcahy, D., McCormack, D., McElwain, J., Natin, S. C., Walsh, T. N., Hennessy, T. P. J., Carson, K., Page, R., Blunnie, W., Moriarty, D. C., Watson, R. W. G., Bouchier-Hayes, D. M., Abdih, H., Kelly, C. J., Barry, M., Burke, P., Tanner, A., Bouchier-Hayes, D. J., O’Sullivan, T., Horgan, A. F., Chin, D. H. L., Mannick, J. A., Rodrick, M. L., Finnegan, N., O’Sullivan, S. T., Wolf, S. F., Barry, M. C., Condron, C., Watson, R. G. K., Evans, J. D., Maxwell-Armstrong, C. A., Barry, M. K., Singh, K. K., Ralston, P., Auld, C. D., Henderson, M., McCormick, J., Walls, A. D. F., Keogh, I., Kerin, M., O’Hanlon, D., Walsh, S., Kent, P., Callaghan, J., Given, H. F., Madhavan, P., Golden, B., Khan, F., Murphy, E., Couse, N., Burke, G., Delaney, P. V., McLoughlin, R., Kenny, P., O’Hanlon, D ., Grimes, H., Reid, S., Neary, P., Nassralla, M., Neelamekam, T. K., Horgan, P., Traynor, O., Horgan, P. G., Hyland, J., O’Hanlon, D. M., O’Boyle, C., Duffy, M. J., McDermott, E. W. M., Reilly, D., Fennelly, J. J., O’Higgins, N. J., McNamara, A., Mullett, H., O’Riordan, D., McDermott, E., Sharp, M., O’Higgins, N., Murphy, M., Little, M., Maher, D., Khalid, A., McCarthy, P., Given, I. F., Bolger, C., Phillips, J. P., Gilligan, C., Zareb, S., Roake, C., O’Riordain, D. S., Farley, D., Grant, C., van Heerden, J., O’Brien, D. P., Flynn, M. J., Keane, F. B. V., Sweeney, B., O’Riordain, D., Curran, A. J., Joyce, W., Smith, D., Gallagher, H., Walsh, M. A., Bouchier-Hayes, D., Phillips, J., O’Brien, T., Yusuf, S. W., Perkins, A. C., Frier, M., Wenham, P. W., Hopkinson, B. R., Makin, G. S., Hind, R., Yusuf, W., Whitaker, S. C., Hind, R. E., Chuter, T. A. M., Durkan, G. C., Grenell, M. J., Regan, M. C., Gorey, T. F., Castineira, C. F., Sheehan, S. J., Wali, M., Colgan, M. P., Moore, D. J., Shanik, G. D., McGreal, G., Kelly, J., Hehir, D., Brady, M. P., Sibbering, D. M., Holland, P. A. M., Wilson, A. R. M., Blarney, R. W., Khurrum Baig, M., Mulligan, N., Farrell, B., Cunningham, F. O., Magd-Eldin, M., Keeling, P., Gul, Y. A., Yeo, S. W., Khan, U. D., Lennon, F., Shine, M. F., Kalidasan, V., Fulena, O., Guiney, E. J., Fitzgerald, R. J., Corbally, M., Wood, A. E., Horgan, P. G., O’Sullivan, S. T., Reardon, C. M., McGreal, G. T., Hehir, D. J., O’Donnell, J. A., Brady, M. P., Kirwan, W. O., Mahomed, A. A., Keshgar, A., Surna, R., Corbally, M. T., O’Rourke, S., Beckingham, I., Bishop, M. C., Blarney, R. W., Husain, J., Hegarty, N., Calleary, J., Rafi, I., Gilmore, M., Saleem, S. M., Singh, H. P., Aherne, T., Redmond, H. P., McCarthy, J., Mulcahy, D. M., Nicholson, P., Harrington, P., Sharif, T., Smyth, H., Fenelon, G., Pegum, J., Corrigan, J., Jenkinson, A., El-Magbri, A. A., Gussail, M. A., Smew, M. A., Martin, A., Bennett, M., Farrell, M. A., Curran, C., Kerin, M. J., Caldwell, M. T. P., Byrne, P. J., Chin, D. H. L., Rodrick, M. L., Mannick, J. A., Duggan, S., Jones, A. S., Field, J. K., O’Hanlon, D. M., Monaghan, D., Barry, M. C., Condren, C., Redmond, H. P., Crerand, S., Kavanagh, M., Dervan, P., Hurson, B., Aiyaswami, K., Hurson, B., Evoy, D., Walsh, M., Garrihy, B., Kaf Al-Ghazal, S., O’Donoghue, J., McCann, J., Wagstaff, S., Conroy, C., Dolan, M., Smith, L., Klenerman, L., Noel, J., Waide, V., O’Sullivan, D., Biyani, C., Powell, C., Heal, M., Surana, R., Khan, A., Fitzgerald, R. J., Lynch, T., Sami, T., Baluch, W., Hickey, D., Donovan, M., McLean, P., Murphy, D., Johnston, S., Rastogi, V., Doyle, J., Flynn, J. R., Kelly, P., Neligan, M. F., MacGowan, S. W., Sharkey, O., Wood, A. E., Bhojwani, A., Lynch, T., Barry Walsh, C., Kay, E., Walsh, M., Milbum, C., McLean, P., Hickey, D., Murphy, D., Leader, M., McDermott, J., Moriarty, D., Caushaj, P., Fitzpatrick, J. M., Byrne, D., Hederman, W. P., O’Malley, N. K., Chan, K. H., Fleming, P., O’Sullivan, G. C., Horgan, P. G., Aizaz, K., O’Donnell, A. F., Luke, D. A., McGovern, E. M., Patil, N., Gormley, P., and McCarthy, P. M.

Published
1994
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16. Seventeenth Sir Peter Freyer memorial lecture and surgical symposium: September 23rd & 24th, 1993

Author

O’Broin, E., Donohoe, J., Mealy, K., Kerin, M., Gillen, P., Tanner, W. A., Keane, F. B. V., McCarthy, P., Rubesin, S., Herlinger, H., Laufer, I., Caldwell, M. T. P., Lawlor, P., Byrne, P. J., Walsh, T. N., Hennessy, T. P. J., Curran, A. J., Gormley, P., Barry, K., McGuire, M., Marks, P., Asad, A. Syed, Lane, B., Browne, H. I., Keeling, P., Barry, M. K., Yeo, C. J., Sauter, P. K., Lillemoe, K. D., Pitt, H. A., Cameron, J. L., Sostre, S., O’Donovan, D. A., Kelly, C. J., Bouchier-Hayes, D. M., Redmond, H. P., Burke, P., Monkhouse, W. S., Burke, J., Williams, N., Gorey, T., Afdhal, N. H., Butt, A. I., Vazir, M. H., Sullivan, R., Connolly, C. E., Bredin, H. C., Sweeney, J. P., Greene, D., Harkin, R., Thornton, J., Butler, M. R., McDermott, T. E. D., Grainger, R., Thornhill, J., Kerin, M. J., Wilkie, J., Monson, J. R. T., Duggan, S., McCarthy, J., Watson, R. G. W., Croke, D. T., McDermott, M., Croke, D., Keane, P. B. V., Watson, R. W. G., O’Donnell, R., Horgan, A. F., O’Riordain, D. S., Saporoschetz, I., Mannick, J. A., Rodrick, M. L., Baker, D. M., Jones, J. A., Nguyen-Van-Tam, J. S., Morris, D. L., Hardcastle, J. D., Steele, R. J. C., Bourke, J. B., Lloyd, J. H., Brown, S., Attwood, S. E. A., McGrath, J., Regan, M., McCann, S., Stephens, R. B., Devitt, A. T., O’Sullivan, T. J., Hurson, B. J., Regan, M. C., Hurson, M., Kirk, S. J., Wasserkrug, H. L., Barbul, A., Naidu, E. R., Sullivan, Tracy, Colreavy, M., Al-Ghazal, S. Kaf, McCann, J., Rodrick, M., Cronin, K. J., Butler, P., McHugh, M., Edwards, G., Geoghegan, J. G., Hehir, D. J., Kirwan, W. O., Brady, M. P., O’Donnell, J. A., Evoy, D., O’Sullivan, S. T., Reardon, C. M., Stokes, M. A., Bergin, F., Mercer, P., Murphy, D., O’Higgins, N., Cannon, P. M., Robertson, J. F. R., Ellis, I. O., Blarney, R. W., Manning, D. L., Nicolson, R. I., Mulligan, E., Kent, P., Ennis, J., Dowling, M., Dervan, P., Fitzpatrick, J. M., Gorey, T. F., Sibbering, D. M., Galea, M. H., Morgan, D. A. L., Locker, A. P., Elston, C. W., Blamey, R. W., Cannon, S. P. M., Sibbering, D. M., O’Rourke, S., Galea, M., Evans, A., Ellis, I., Johnston, S., Byrne, J., Horgan, P., Kennedy, M., Callaghan, J., Given, H. F., Mooney, E., Donohue, S., O’Hanlon, D. M., Waldron, R., Johnston, J., Stokes, M., MeDermott, E., Sharp, M., Duffy, M., Murphy, J., McGreal, G. T., Kealy, W., Neligan, M., O’Malley, K., McEntee, G., Khan, F., Morrin, M., Delaney, P., Brindley, N., Dudeney, S., Drebin, J., Geraghty, J., Broe, P., Fynes, M., Horgan, P. G., O’Connell, P. R., Golden, B., Loughnane, F., Baldota, S., O’Donnell, M., Chen, S., Eustace, P. W., Johnston, J. G., Gaffney, T., Tawil, S. El, Cunningham, F., Brazil, E., Reynolds, J., Ireland, A., Traynor, O., Little, D., Barry, M., Thornton, F., Sheehan, S., Bouchier-Hayes, D. J., Fitzgerald, P., Grace, P., Gul, Y., Waldron, D., Wali, M., Colgan, M. P., Moore, D. J., Shanik, D. G., MacNamara, J., Lynch, V. P., Abdih, H., Watson, W., Aloisi, J. D., Boyle, T. J., Lyerly, H. Kim, Kelly, C., O’Donovan, D., Monkhouse, W., O’Donoghue, J. M., Curran, C., O’Hanlon, D., Maher, D., Homer, C., O’Brien, M., Caldwell, M., Sheehan, R., Crean, P., O’Brien, T., Grant, C., Van Heerden, J. A., Lynn, J. A., O’Donovan, B. G., Quill, D. S., Delaney, C. P., Phillips, J., McKeever, J. A., Earley, M. J., Hooper, A. C. B., Al-Ghazal, S. K., Khan, K., McKiernan, M., McQuillan, R., McCabe, J. R., O’Farrell, D., O’Byrne, J., O’Donovan, B., Rafi, I., Gilmore, M., Fitzgerald, F., Moran, R., O’Brien, D., Pidgeon, C., Young, S., Allcutt, D., Rawluk, D., O’Brien, D. P., Phillips, J. P., Beckingham, I., Hinwood, M., Rigg, K., Bishop, M., Rowley, H., O’Dwyer, T. P., Beckingham, I. J., O’Rourke, J. S., Dennis, M. J. S., Bell, P. R. F., Nicholson, M. L., Akhtar, N., Corcoran, M. O., Lynch, T. H., Connellan, G., Mulvin, D., Boyle, B., O’Donoghue, M., El-Tayeb, Y., O’Donoghue, J., Parke, L., Evoy, D. A., Attwood, S. E., Keeling, P. W. N., O’Hanlon, D. M., Doyle, J., Flynn, J. R., Hurley, J., Wood, A. E., Duncan, C., Quershi, A., Leahy, A., Hayes, D., Osborne, H., Mashali, H., and Watson, R. G. K.

Published
1994
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17. Irish society of gastroenterology: Proceedings of Winter Meeting held 4th/5th December 1992in Beaumont hospital, Dublin

Author

O’Sullivan, M., Thornton, G., O’Sullivan, G., O’Mahony, A. M., O’Connell, J., Hanvajanawong, C., Phelan, D., O’Sullivan, G. C., Collins, J. K., Bamford, K. B., Lutton, D. A., Collins, J. S. A., O’Loughlin, B., Johnston, B. T., McFarland, R. J., Love, A. H. G., Buchanan, K. D., Fillmore, D., Ardill, J. E. S., Clyne, M., Drumm, B., Cyne, M., Tham, T. C. K., McLaughlin, N., Hughes, D. F., Ferguson, M., Crosbie, J. J., Madden, M., Namnyak, S., O’Connor, F. A., Magbri, Awad El, Stevens, F. M., McCarthy, C. F., Lynch, M., O’Brien, M., Ryan, E., MacMathuna, P., Kelly, P., Lennon, J., Crowe, J., Mulvey, S., Maguire, C., Clarke, E., Cronin, K. J., Kent, P., Mooney, E., Corrigan, T., O’Connell, R., Fitzpatrick, J. M., Gorey, T. F., Prabhaker, M. C., Bannon, C. A., Delaney, C., Duggan, M., Gorey, T., Abuzakouk, M., Lynch, S., Casey, E., Weir, D., Feighery, C., O’Farrelly, C., Fan, X. J., Chua, A., Shahi, C. N., Kelleher, D., Keeling, P. W. N., Parks, R. W., Diamond, T., McCrory, D. C., Johnston, G. W., Clements, W. D. B., Ennis, M., Campbell, G. R., Halliday, M. I., Rowlands, B. J., Wilson, R. H., Williamson, K., McLoughlin, J., Moorehead, R. J., O’Connor, A. M., Johnston, C. F., Gillmore, D., Boreham, C., Caldwell, M. T. P., Jazrawi, S., Byrne, P. J., Walsh, T. N., Hennessy, T. P. J., Li, H., Kay, E. W., Mulcahy, H., Curran, B., O’Donoghue, D., Leader, M., Walsh, C. Barry, O’Sullivan, S. T., Reardon, C. M., Hardiman, C., O’Donnell, J. A., Kirwan, W. O., Brady, M. P., McGreal, G., Hehir, D. J., Brady, M. P., O’Donnell, J., Pender, S. M., Courtney, M. G., Fielding, J. F., Swan, N., Chong, A., Denesh, T. G., Coll, D., McElearney, C., Kay, E., Sant, S., Doyle, J. S., Buckley, M., Cahill, R. J., Beattie, S., Hamilton, H., O’Morain, C., O’Sullivan, K., Forde, A. M., Gilvarry, J., Jackson, J., Alvi, R., Leahy, A., Lynch, G., Lane, B., Browne, H. Y., Keeling, P., Stafford-Johnson, D., Kee, S., Carr, J., Ryan, M. J., Sheehan, S., Broe, P., Deasy, J., O’Donovan, D. A., Bouchier-Hayes, D. M., Kelly, C., Grace, P., Redmond, H. P, Burke, P., Bouchier-Hayes, D. J., O’Malley, K., Qureshi, A., Osborne, H., Monkhouse, W. S., Bouchier-Hayes, D., Goggin, M., Joyce, W. P., Traynor, O., Hyland, J., Beausang, E., Mealy, K., Prendergast, C., Joyce, L., McNicholas, M. M. J., Gibney, R. G., Dolan, J., MacErlean, D. P., Hyland, J. M., Fenlon, H. M., Mulcahy, H. E., Stack, W. A., Skelly, M. M., Hegarty, J. E., Stack, W., O’Donoghue, D. P., Norris, S. M., McNicholas, M., Murray, F. E., Williams, N., Burke, J., Lamort, W., Fitzpatrick, J., Afdhal, N., Gibney, R., McLoughlin, R. F., Mourad, F. H., O’Donnell, L. J. D., Dias, J., Ogutu, E., Farthing, M. J. G., Hoyle, C. H. V., Hill, A. D. K., Darzi, A., Carey, P. D., Menzies-Gow, N., Monson, J. R. T., Goggins, M. G., O’Broin, S., Kelleher, B., Scott, J. M., Weir, D. D., Watson, R. G. P., Goss, B., Angus, P. W., Duckham, N., Sewell, R. B., and Smallwood, R. A.

Published
1993
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18. Proceedings of meeting held November 6th & 7th, 1992 in the Sir Charles Parsons Theatre, University of Limerick

Author

O’Sullivan, S. T., Reardon, C. M., Hardiman, C., O’Donnell, J. A., Kirwan, W. O., Brady, M. P., Kelly, I., Attwood, S. E. A., Corrigan, T. P., Burke, P., Fitzgerald, P., Keeling, F., Grace, P., Bouchier-Hayes, D., Creagh, T. A., Williams, N. N., Kerin, M. K., Cronin, K., Smith, J., Fitzpatrick, J. M., Syed, S., Surana, R., Guiney, E. J., Malone, F., Reynolds, J., Ellias, Y., Traynor, O., O’Donnell, B., Samsunden, R., Humphreys, W. G., Khan, K., Al-Ghazal, S. K., Al-Ghazal, S., McKiernan, M., McCann, J., McAvinchey, D., Fitzgerald, M., McDermott, S., Murphy, A., Mooney, E. F., Geraghty, J., O’Connell, M., Kent, P., Sarazen, A., Angerson, W., Reynolds, J. V., Murchan, P., Keane, F. B. V., Tanner, W. A., McCarthy, J., Watson, W., O’Donnell, R., Brindley, N., Creagh, T., Dolan, J., Leader, M., Monkhouse, S., Qureshi, A., Clements, B., Halliday, I., Irwin, P., McCaigue, M., Barclay, R., Rowlands, B. J., Watson, R. W. G., Redmond, H. P., McCarthy, J. C., Dudley, M. S., Croke, D. T., Kelly, C. J., Grace, P. A., Burke, P. E., Bouchier-Hayes, D. J., Morrin, M., Khan, F., Barrett, N., Pembroke, T., Williams, N., Delaney, P., Gerghty, J., Kay, E., Leahy, A., Tanner, W. A., Refsum, S. E., Norwood, W., Boston, V. E., O’Mahony, A., Collins, J. K., O’Sullivan, G., Ramsbottom, D., Collins, P. B., Anderson, A. H., Johnston, S., Byrne, J., Horgan, P. G., Kennedy, M., Callaghan, J., Given, H. F., Delaney, C., Couse, N., Horgan, P., Fitzpatrick, J., Gorey, T., Solomon, I., Stokes, N., Bohan, A., Young, A., Murphy, D., Mercer, P., O’Higgins, N., Kerin, M. J., Murray, J., Dowling, M., Dervan, P., Ennis, J., Gorey, T. F., Ahmed, M., Cunningham, F. O., Smyth, P. P. A., Hetherton, A. M., Murray, M., O’Higgins, N. J., Alvi, R., Lane, B., Lynch, G., Browne, H., Keeling, P., Joyce, W. P., Hyland, J. M., Rehman, L., O’Leary, B., Hamdy, A., Watson, R. G. K., Hegarty, J., Breslin, D., Delaney, C. P., Istarabadi, M., O’Donnell, A., Hussain, R., Luke, D. A., McGovern, E., O’Neill, J., Stokes, M. A., Keaveney, T. V., Rasheed, R., Khan, F. H., Egan, T. J., Drumm, J., O’Domhnaill, S., Delaney, P. V., Hill, G. L., Hill, A. D. K., Darzi, A., Menzies-Gow, N., Donnelly, M. J., Timon, C. I., McShane, D. P., Ninan, G. K., Rasheed, K., Puri, P., Coveney, E. C., Moloney, R., Fitzgerald, R. J., Geoghegan, J. G., Branch, M. S., Pappas, T. N., Cotton, P. B., and Ryan, D.

Published
1993
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19. Nod-like receptors are critical for gut-brain axis signalling in mice

Author

Universitat Rovira i Virgili, Pusceddu, MM; Barboza, M; Keogh, CE; Schneider, M; Stokes, P; Sladek, JA; Kim, HJD; Torres-Fuentes, C; Goldfild, LR; Gillis, SE; Brust-Mascher, I; Rabasa, G; Wong, KA; Lebrilla, C; Byndloss, MX; Maisonneuve, C; Bäumler, AJ; Philpott, DJ; Ferrero, RL; Barrett, KE; Reardon, C; Gareau, MG, Universitat Rovira i Virgili, and Pusceddu, MM; Barboza, M; Keogh, CE; Schneider, M; Stokes, P; Sladek, JA; Kim, HJD; Torres-Fuentes, C; Goldfild, LR; Gillis, SE; Brust-Mascher, I; Rabasa, G; Wong, KA; Lebrilla, C; Byndloss, MX; Maisonneuve, C; Bäumler, AJ; Philpott, DJ; Ferrero, RL; Barrett, KE; Reardon, C; Gareau, MG

Abstract

Gut-brain axis signalling is critical for maintaining health and homeostasis. Stressful life events can impact gut-brain signalling, leading to altered mood, cognition and intestinal dysfunction. In the present study, we identified nucleotide binding oligomerization domain (Nod)-like receptors (NLR), Nod1 and Nod2, as novel regulators for gut-brain signalling. NLR are innate immune pattern recognition receptors expressed in the gut and brain, and are important in the regulation of gastrointestinal physiology. We found that mice deficient in both Nod1 and Nod2 (NodDKO) demonstrate signs of stress-induced anxiety, cognitive impairment and depression in the context of a hyperactive hypothalamic-pituitary-adrenal axis. These deficits were coupled with impairments in the serotonergic pathway in the brain, decreased hippocampal cell proliferation and immature neurons, as well as reduced neural activation. In addition, NodDKO mice had increased gastrointestinal permeability and altered serotonin signalling in the gut following exposure to acute stress. Administration of the selective serotonin reuptake inhibitor, fluoxetine, abrogated behavioural impairments and restored serotonin signalling. We also identified that intestinal epithelial cell-specific deletion of Nod1 (VilCre(+)Nod1(f/f)), but not Nod2, increased susceptibility to stress-induced anxiety-like behaviour and cognitive impairment following exposure to stress. Together, these data suggest that intestinal epithelial NLR are novel modulators of gut-brain communication and may serve as potential novel therapeutic targets for the treatment of gut-brain disorders.

Published
2019

30. Effect of lithographically-induced strain relaxation on the magnetic domain configuration in microfabricated epitaxially grown Fe81Ga19

Author

Beardsley, R. P., primary, Parkes, D. E., additional, Zemen, J., additional, Bowe, S., additional, Edmonds, K. W., additional, Reardon, C., additional, Maccherozzi, F., additional, Isakov, I., additional, Warburton, P. A., additional, Campion, R. P., additional, Gallagher, B. L., additional, Cavill, S. A., additional, and Rushforth, A. W., additional

Published
2017
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34. Toso controls encephalitogenic immune responses by dedritic cells and regulatory T cells

Author

Brenner, Dirk, Bruestle, Anne, Lin, G. H, Lang, P. A, Duncan, G. S, Knobbe-Thomson, C. B, St Paul, M, Reardon, C, Tusche, M. W, Snow, B, Hamilton, S. R, Pfefferle, C. B, Gilani, S. O, Ohashi, Pamela, Lang, Karl S, Mak, T. W, Brenner, Dirk, Bruestle, Anne, Lin, G. H, Lang, P. A, Duncan, G. S, Knobbe-Thomson, C. B, St Paul, M, Reardon, C, Tusche, M. W, Snow, B, Hamilton, S. R, Pfefferle, C. B, Gilani, S. O, Ohashi, Pamela, Lang, Karl S, and Mak, T. W

Published
2014

35. GRACE.

Author

REARDON, C. S.

Subjects
*MURDER
Published
2017

38. Where are we short and who are we short of? A review of the human resources for health in South Africa

Author

George, G., Quinlan, T.K.C., Reardon, C., Aguilera, J., George, G., Quinlan, T.K.C., Reardon, C., and Aguilera, J.

Abstract

This review showed that thinking about the shortage of health care personnel merely in terms of insufficient numbers prevents sound strategic interventions to solve the country's human resources for health (HRH) problem. It revealed that the numbers shortage was one facet of a broader problem that included the mal distribution of HRH, production of the wrong skills in the nursing care, the attrition of staff from the public health services and, contextually, the ever-changing demands on the health services. The challenge in South Africa was furthermore to train and retain health care personnel with skills and expertise that are commensurate with the changing demands on the public health services. © 2012. The Authors.

Published
2012
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