1,087 results on '"Brown JC"'
Search Results
2. NGOs, Turnout, and the Left: A Sub-national Analysis of Brazil
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Brown, DS, Brown, JC, and Desposato, SW
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NGOs ,voting ,Brazil ,democracy ,social capital ,Development Studies ,Urban and Regional Planning ,Anthropology ,Political Science - Abstract
This article is designed to examine the role non-governmental organizations (NGOs) play in politics. Previous evidence suggests that NGOs mobilize communities to challenge existing patterns of authority or that they serve hand in glove with existing elites. We reconcile these two contradictory findings by identifying an important contextual feature that helps determine the extent NGOs mobilize or anesthetize. We argue that a community’s level of education influences not only whether people vote but how they vote. We employ a cross-sectional data set from Brazilian municipalities that allows us to estimate the relationship between NGOs, voting turnout, and electoral results. We find that although there is a significant statistical interaction between literacy and NGOs when explaining voting turnout, the effect is not substantively important. The interaction between literacy and NGOs is, however, an important consideration in determining how people vote: in communities with relatively low literacy rates, a robust NGO presence significantly increases the left’s electoral fortunes. Our findings imply the influence NGOs have on society is more political than social.
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- 2014
3. Type I interferon receptor signalling deficiency results in dysregulated innate immune responses to SARS‐CoV‐2 in mice
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Ogger, PP, Garcia Martín, M, Michalaki, C, Zhou, J, Brown, JC, Du, Y, Miah, KM, Habib, O, Hyde, SC, Gill, DR, Barclay, WS, Johansson, C, Rosetrees Trust, Imperial College COVID-19 response fund, and UK Research and Innovation
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Science & Technology ,SARS-CoV-2 ,Immunology ,COVID-19 ,Receptor, Interferon alpha-beta ,SARS-CoV-2/ myeloid cells ,Immunity, Innate ,TRANSGENE EXPRESSION ,in vivo ,Mice ,Innate Immune Response/ type I IFN ,1107 Immunology ,myeloid cells ,Interferon Type I ,innate immune response ,Animals ,Immunology and Allergy ,Life Sciences & Biomedicine ,Pandemics ,type I IFN - Abstract
SARS-CoV-2 is a newly emerged coronavirus, causing the global pandemic of respiratory coronavirus disease (COVID-19). The type I interferon (IFN) pathway is of particular importance for anti-viral defense and recent studies identified that type I IFNs drive early inflammatory responses to SARS-CoV-2. Here, we use a mouse model of SARS-CoV-2 infection, facilitating viral entry by intranasal recombinant Adeno-Associated Virus (rAAV) transduction of hACE2 in wildtype (WT) and type I IFN receptor-1 deficient (Ifnar1–/–) mice, to study the role of type I IFN signalling and innate immune responses during SARS-CoV-2 infection. Our data show that type I IFN signalling is essential for inducing anti-viral effector responses to SARS-CoV-2, control of virus replication, and to prevent enhanced disease. Furthermore, hACE2-Ifnar1–/– mice had increased gene expression of the chemokine Cxcl1 and airway infiltration of neutrophils as well as reduced and delayed production of monocyte-recruiting chemokine CCL2. hACE2-Ifnar1–/– mice showed altered recruitment of inflammatory myeloid cells to the lung upon SARS-CoV-2 infection, with a shift from Ly6C+ to Ly6C– expressing cells. Together, our findings suggest that type I IFN signalling deficiency results in a dysregulated innate immune response to SARS-CoV-2 infection.
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- 2022
4. Validity of self-testing at home with rapid severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) antibody detection by lateral flow immunoassay
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Atchison, CJ, Moshe, M, Brown, JC, Whitaker, M, Wong, NCK, Bharath, AA, McKendry, RA, Darzi, A, Ashby, D, Donnelly, CA, Riley, S, Elliott, P, Barclay, WS, Cooke, GS, and Ward, H
- Abstract
Background We explore severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) antibody lateral flow immunoassay (LFIA) performance under field conditions compared to laboratory-based electrochemiluminescence immunoassay (ECLIA) and live virus neutralization. Methods In July 2021, 3758 participants performed, at home, a self-administered Fortress LFIA on finger-prick blood, reported and submitted a photograph of the result, and provided a self-collected capillary blood sample for assessment of immunoglobulin G (IgG) antibodies using the Roche Elecsys® Anti-SARS-CoV-2 ECLIA. We compared the self-reported LFIA result to the quantitative ECLIA and checked the reading of the LFIA result with an automated image analysis (ALFA). In a subsample of 250 participants, we compared the results to live virus neutralization. Results Almost all participants (3593/3758, 95.6%) had been vaccinated or reported prior infection. Overall, 2777/3758 (73.9%) were positive on self-reported LFIA, 2811/3457 (81.3%) positive by LFIA when ALFA-reported, and 3622/3758 (96.4%) positive on ECLIA (using the manufacturer reference standard threshold for positivity of 0.8 U mL–1). Live virus neutralization was detected in 169 of 250 randomly selected samples (67.6%); 133/169 were positive with self-reported LFIA (sensitivity 78.7%; 95% confidence interval [CI]: 71.8, 84.6), 142/155 (91.6%; 95% CI: 86.1, 95.5) with ALFA, and 169 (100%; 95% CI: 97.8, 100.0) with ECLIA. There were 81 samples with no detectable virus neutralization; 47/81 were negative with self-reported LFIA (specificity 58.0%; 95% CI: 46.5, 68.9), 34/75 (45.3%; 95% CI: 33.8, 57.3) with ALFA, and 0/81 (0%; 95% CI: 0, 4.5) with ECLIA. Conclusions Self-administered LFIA is less sensitive than a quantitative antibody test, but the positivity in LFIA correlates better than the quantitative ECLIA with virus neutralization.
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- 2023
5. Structures of bovine and human papillomaviruses. Analysis by cryoelectron microscopy and three-dimensional image reconstruction
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Baker, TS, Newcomb, WW, Olson, NH, Cowsert, LM, Olson, C, and Brown, JC
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Biological Sciences ,Chemical Sciences ,Physical Sciences ,Infectious Diseases ,Sexually Transmitted Infections ,Animals ,Bovine papillomavirus 1 ,Cattle ,Cattle Diseases ,Freezing ,Humans ,Microscopy ,Electron ,Models ,Structural ,Papillomaviridae ,Tumor Virus Infections ,Warts ,Biophysics ,Biological sciences ,Chemical sciences ,Physical sciences - Abstract
The structures of bovine papillomavirus type 1 (BPV-1) and human papillomavirus type 1 (HPV-1) were determined at 2.5 nm resolution by cryoelectron microscopy and three dimensional image reconstruction techniques. As expected, the reconstructions showed that both viruses consist of a T = 7 icosahedral capsid (approximately 60 nm in diameter) which surrounds a nucleohistone core. The capsid morphologies of the two viruses are nearly indistinguishable. Each capsid consists of a shell layer (approximately 2 nm thick) of nearly continuous density from which capsomers project radially to a maximum height of approximately 5.8 nm. The five-coordinate (pentavalent) and six-coordinate (hexavalent) capsomers both exhibit distinct five-fold axial symmetry as was observed for SV40 and polyoma viruses. Thus, both genera (papilloma and polyoma) of the papovavirus family have now been shown to have the characteristic "all-pentamer" capsid construction. BPV-1 and HPV-1 capsomers consist of a thick (8.6 nm diameter) trunk that broadens distally to form a regular five-pointed, star-shaped head, and proximally to create the shell layer where capsomers associate. A cylindrical channel (approximately 2.8 nm diameter) extends along the axis of each capsomer from the interior of the virus to a point approximately half way to the capsomer surface. Computationally sectioned views of individual capsomers displayed at decreasing radii show that each of the five capsomer subunits (in both pentavalent and hexavalent capsomers) makes a pronounced (30 degrees) left-handed twist just above the outer surface of the capsid shell. Similar views of the reconstructions also clarify the morphology of intercapsomer contacts. For example, they show how hexavalent capsomers coordinate six neighboring capsomers despite the fact that they contain only five subunits. The system of intercapsomer contacts is indistinguishable in BPV-1 and HPV-1, but quite different from that reported for polyoma virus capsids assembled in vitro from the major capsid protein, VP1 (D. M. Salunke, D. L. D. Caspar, and R. L. Garcea. 1989. Biophys. J. 56:887-900). Thus, because both polyoma and papilloma viruses have all-pentamer capsids, it appears that intracapsomer subunit-subunit interactions which stabilize pentameric capsomers are better preserved evolutionarily than those involved in capsomer-capsomer contacts.
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- 1991
6. Liquid-crystalline, phage-like packing of encapsidated DNA in herpes simplex virus
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Booy, FP, Newcomb, WW, Trus, BL, Brown, JC, Baker, TS, and Steven, AC
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Infectious Diseases ,Sexually Transmitted Infections ,Aetiology ,2.2 Factors relating to the physical environment ,Infection ,Animals ,Bacteriophages ,Capsid ,Cell Line ,Computer Graphics ,DNA ,Viral ,Freezing ,Microscopy ,Electron ,Models ,Structural ,Nucleic Acid Conformation ,Protein Conformation ,Simplexvirus ,X-Ray Diffraction ,Biological Sciences ,Medical and Health Sciences ,Developmental Biology - Abstract
The organization of DNA within the HSV-1 capsid has been determined by cryoelectron microscopy and image reconstruction. Purified C-capsids, which are fully packaged, were compared with A-capsids, which are empty. Unlike A-capsids, C-capsids show fine striations and punctate arrays with a spacing of approximately 2.6 nm. The packaged DNA forms a uniformly dense ball, extending radially as far as the inner surface of the icosahedral (T = 16) capsid shell, whose structure is essentially identical in A-capsids and C-capsids. Thus we find no evidence for the inner T = 4 shell previously reported by Schrag et al. to be present in C-capsids. Encapsidated HSV-1 DNA closely resembles that previously visualized in bacteriophages T4 and lambda, thus supporting the idea of a close parallelism between the respective assembly pathways of a major family of animal viruses (the herpesviruses) and a major family of bacterial viruses.
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- 1991
7. Three-dimensional structures of maturable and abortive capsids of equine herpesvirus 1 from cryoelectron microscopy.
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Baker, TS, Newcomb, WW, Booy, FP, Brown, JC, and Steven, AC
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Biological Sciences ,Ecology ,Animals ,Capsid ,Computer Simulation ,Freezing ,Herpesviridae ,Herpesvirus 1 ,Equid ,L Cells ,Mice ,Microscopy ,Electron ,Models ,Molecular ,Protein Conformation ,Agricultural and Veterinary Sciences ,Medical and Health Sciences ,Virology ,Agricultural ,veterinary and food sciences ,Biological sciences ,Biomedical and clinical sciences - Abstract
Cryoelectron microscopy and three-dimensional computer reconstruction techniques have been used to compare the structures of two types of DNA-free capsids of equine herpesvirus 1 at a resolution of 4.5 nm. "Light" capsids are abortive, whereas "intermediate" capsids are related to maturable intracellular precursors. Their T = 16 icosahedral outer shells, approximately 125 nm in diameter, are indistinguishable and may be described in terms of three layers of density, totalling 15 nm in thickness. The outermost layer consists of protruding portions of both the hexon and the penton capsomers, rising approximately 5 nm above a midlayer of density. The innermost layer, or "floor," is a 4-nm-thick sheet of virtually continuous density except for the orifices of the channels that traverse each capsomer. Hexon protrusions are distinctly hexagonal in shape, and penton protrusions are pentagonal. The structures of the three kinds of hexons (distinguished according to their positions on the surface lattice) are closely similar but differ somewhat in their respective orientations and in the shapes of their channels. The most prominent features of the midlayer are threefold nodules ("triplexes") at the trigonal lattice points. By analogy with other viral capsids, the triplexes may represent trimers of another capsid protein, possibly VP23 (36 kilodaltons [kDa]) or VP26 (12 kDa). Intermediate capsids differ from light capsids, which are empty, in having one or more internal components. In individual images from which the shell structure has been filtered away, these components are seen to have dimensions of 20 to 30 nm but to lack a visible substructure. This material--which is smeared out in the reconstruction, implying that its distribution is not icosahedrally symmetric or necessarily consistent from particle to particle--consists of aggregates of VP22 (46 kDa). From several lines of evidence, we conclude that this protein is located entirely within the capsid shell. These aggregates may be the remnants of morphogenetic cores retained in capsids interrupted in the process of DNA packaging.
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- 1990
8. The effect of trait self-control on dyspnoea and tolerance to a CO2 rebreathing challenge in healthy males and females
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Brown, JC, Boat, R, Williams, NC, Johnson, MA, and Sharpe, GR
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Behavioral Neuroscience ,Experimental and Cognitive Psychology - Abstract
Background: High trait self-control is associated with greater tolerance of unpleasant sensations including effort and pain. Dyspnoea and pain have several commonalities and this study aimed to investigate for the first time whether trait self-control influences responses to a hypercapnic rebreathing challenge designed to induce dyspnoea. As sex also influences tolerance to dyspnoea, we also sought to investigate whether this moderated the role of trait self-control.\ud \ud Methods: Participants (n = 65, 32 females) scoring high or low for trait self-control, performed a standardised rebreathing challenge, in which inspired carbon dioxide (CO2) gradually increased over a period of 6 min or until an intolerable level of dyspnoea. Air hunger (AH) intensity – a distinctive quality of dyspnoea, was measured every 30 s. The multidimensional dyspnoea profile (MDP) was completed after the rebreathing challenge for a more complete overview of breathing discomfort.\ud \ud Results: Males high in trait self-control (SCHIGH) (302 ± 42 s), tolerated the rebreathing challenge for longer than males low in self-control (SCLOW) (252 ± 66 s, P = 0.021), experienced slower increases in AH intensity during the rebreathing challenge (0.03 ± 0.01 cm.s − 1 vs. 0.04 ± 0.01 cm.s − 1, P = 0.045) and reported lower perceived mental effort on the MDP (4.94 ± 2.46 vs. 7.06 ± 1.60, P = 0.007). There was no difference between SCHIGH and SCLOW females for challenge duration. However, SCHIGH females (9.29 ± 0.66 cm) reported greater air hunger at the end of the challenge than SCLOW females (7.75 ± 1.75 cm, P = 0.003). It is possible that SCLOW females were unwilling to tolerate the same perceptual intensity of AH as the SCHIGH females.\ud \ud Conclusions: These results indicate that individuals high in trait self-control are more tolerant of dyspnoea during a CO2 rebreathing challenge than low self-control individuals. Tolerance of the stimulus was moderated by the sex of the participant, presenting an interesting opportunity for future research.
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- 2022
9. An Analysis of Diesel Locomotive Operator's Cab Vibration Isolation
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Conference on Railway Engineering (7th : 1993 : Newcastle, N.S.W.), Leonard, MJ, and Brown, JC
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- 1993
10. Locomotive Remanufacture
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Conference on Railway Engineering (6th : 1991 : Adelaide, S. Aust.) and Brown, JC
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- 1991
11. Mutations in Drosophila tRNA processing factors cause phenotypes similar to Pontocerebellar Hypoplasia
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Joseph D. Giusto, Brown Jc, Min Ly, Salzler Hr, Casey A. Schmidt, McVay Mh, and A G Matera
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Phenocopy ,RNA splicing ,Pontocerebellar hypoplasia ,medicine ,RNA ,TRNA processing ,Biology ,Kinase activity ,medicine.disease ,Gene ,Phenotype ,Cell biology - Abstract
Mature tRNAs are generated by multiple RNA processing events, which can include the excision of intervening sequences. The tRNA splicing endonuclease (TSEN) complex is responsible for cleaving these intron-containing pre-tRNA transcripts. In humans, TSEN copurifies with CLP1, an RNA kinase. Despite extensive work on CLP1, its in vivo connection to tRNA splicing remains unclear. Interestingly, mutations in CLP1 or TSEN genes cause neurological diseases in humans that are collectively termed Pontocerebellar Hypoplasia (PCH). In mice, loss of Clp1 kinase activity results in premature death, microcephaly and progressive loss of motor function. To determine if similar phenotypes are observed in Drosophila, we characterized mutations in crowded-by-cid (cbc), the CLP1 ortholog, as well as in the fly ortholog of human TSEN54. Analyses of organismal viability, larval locomotion and brain size revealed that mutations in both cbc and Tsen54 phenocopy those in mammals in several details. In addition to an overall reduction in brain lobe size, we also found increased cell death in mutant larval brains. Ubiquitous or tissue-specific knockdown of cbc in neurons and muscles reduced viability and locomotor function. These findings indicate that we can successfully model PCH in a genetically-tractable invertebrate.
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- 2021
12. Factors associated with parents' willingness to enroll their children in trials for COVID-19 vaccination
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Goldman RD, Staubli G, Parra C, Brown JC, Hoeffe J, Seiler M, Gelernter R, Hall JE, Griffiths MA, Davis AL, Manzano S, Mater A, Ahmed S, Sheridan D, Hansen M, Ali S, Thompson GC, Shimizu N, and Klein EJ
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parental attitudes ,decision-making ,Coronavirus ,vaccine trials ,global survey - Abstract
The coronavirus disease 2019 (COVID-19) pandemic has taken an unprecedented global toll and vaccination is needed to restore healthy living. Timely inclusion of children in vaccination trials is critical. We surveyed caregivers of children seeking care in 17 Emergency Departments (ED) across 6 countries during the peak of the pandemic to identify factors associated with intent to participate in COVID-19 vaccine trials. Questions about child and parent characteristics, COVID-19 expressed concerns and parental attitudes toward participation in a trial were asked.Of 2768 completed surveys, 18.4% parents stated they would enroll their child in a clinical trial for a COVID-19 vaccine and 14.4% would agree to a randomized placebo-controlled study. Factors associated with willingness to participate were parents agreeing to enroll in a COVID-19 vaccine trial themselves (Odds Ratio (OR) 32.9, 95% Confidence Interval (CI) (21.9-51.2)) having an older child (OR 1.0 (1.0-1.01)), having children who received all vaccinations based on their country schedule (OR 2.67 (1.35-5.71)) and parents with high school education or lower (OR 1.79 (1.18-2.74)). Mothers were less likely to enroll their child in a trial (OR 0.68 (0.47-0.97)). Only one fifth of families surveyed will consider enrolling their child in a vaccine trial. Parental interest in participation, history of vaccinating their child, and the child being older all are associated with parents allowing their child to participate in a COVID vaccine trial. This information may help decision-makers and researchers shape their strategies for trial design and participation engagement in upcoming COVID19 vaccination trials.
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- 2021
13. Caregiver-reported delay in presentation to pediatric emergency departments for fear of contracting COVID-19: a multi-national cross-sectional study
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Davis AL, Sunderji A, Marneni SR, Seiler M, Hall JE, Parra C, Klein EJ, Brown JC, Gelernter R, Griffiths MA, Hoeffe J, Gualco G, Mater A, Manzano S, Thompson GC, Ahmed S, Ali S, Goldman RD, and International COVID-19 Parental Attitude Study (COVIPAS) Group
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Children ,Emergency department ,Caregivers ,Presentation delay ,COVID-19 - Abstract
OBJECTIVE: To determine if caregivers of children presenting to pediatric emergency departments (EDs) during the COVID-19 pandemic are delaying presenting to care for fear of contracting COVID-19. METHODS: This was a pre-planned secondary analysis of a cross-sectional survey study of caregivers accompanying their children aged 0-19 years to 16 pediatric EDs in 5 countries from May to June 2020. An anonymous online survey, completed by caregivers via RedCAP, included caregiver and child demographics, presenting complaints, if they delayed presentation and whether symptoms worsened during this interval, as well as caregiver concern about the child or caregiver having COVID-19 at the time of ED visit. RESULTS: Of 1543 caregivers completing the survey, 287 (18.6%) reported a delay in seeking ED care due to concerns of contracting COVID-19 in the hospital. Of those, 124 (43.2%) stated their child's symptoms worsened during the waiting interval. Caregiver relationship to child [mother] (OR 1.85, 95% CI 1.27-2.76), presence of chronic illness in child (OR 1.78. 95% CI 1.14-2.79), younger age of caregiver (OR 0.965, 95% CI 0.943-0.986), and caregiver concerns about lost work during the pandemic (OR 1.08, 95% CI 1.04-1.12) were independently associated with a COVID-19-related delayed presentation in multivariable regression analysis. CONCLUSIONS: Almost one in five caregivers reported delaying ED presentation for their ill or injured child specifically due to fear of contracting COVID-19 while in hospital, with mothers, younger caregivers, caregivers of children with chronic illness, and those concerned about lost work more likely to report delaying ED presentation.
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- 2021
14. Declining prevalence of antibody positivity to SARS-CoV-2: a community study of 365,000 adults
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Ward, H, Cooke, G, Atchison, C, Whitaker, M, Elliott, J, Moshe, M, Brown, JC, Flower, B, Daunt, A, Ainslie, K, Ashby, D, Donnelly, C, Riley, S, Darzi, A, Barclay, W, and Elliott, P
- Abstract
Background The prevalence and persistence of antibodies following a peak SARS-CoV-2 infection provides insights into its spread in the community, the likelihood of reinfection and potential for some level of population immunity.Methods Prevalence of antibody positivity in England, UK (REACT2) with three cross-sectional surveys between late June and September 2020. 365104 adults used a self-administered lateral flow immunoassay (LFIA) test for IgG. A laboratory comparison of LFIA results to neutralization activity in panel of sera was performed.Results There were 17,576 positive tests over the three rounds. Antibody prevalence, adjusted for test characteristics and weighted to the adult population of England, declined from 6.0% [5.8, 6.1], to 4.8% [4.7, 5.0] and 4.4% [4.3, 4.5], a fall of 26.5% [-29.0, −23.8] over the three months of the study. There was a decline between rounds 1 and 3 in all age groups, with the highest prevalence of a positive result and smallest overall decline in positivity in the youngest age group (18-24 years: −14.9% [-21.6, −8.1]), and lowest prevalence and largest decline in the oldest group (75+ years: −39.0% [-50.8, −27.2]); there was no change in antibody positivity between rounds 1 and 3 in healthcare workers (+3.45% [-5.7, +12.7]).The decline from rounds 1 to 3 was largest in those who did not report a history of COVID-19, (−64.0% [-75.6, −52.3]), compared to −22.3% ([-27.0, −17.7]) in those with SARS-CoV-2 infection confirmed on PCR.Discussion These findings provide evidence of variable waning in antibody positivity over time such that, at the start of the second wave of infection in England, only 4.4% of adults had detectable IgG antibodies using an LFIA. Antibody positivity was greater in those who reported a positive PCR and lower in older people and those with asymptomatic infection. These data suggest the possibility of decreasing population immunity and increasing risk of reinfection as detectable antibodies decline in the population.Competing Interest StatementThe authors have declared no competing interest.Funding StatementThis work was funded by the Department of Health and Social Care in England. We thank key collaborators on this work -- Ipsos MORI: Stephen Finlay, John Kennedy, Kevin Pickering, Duncan Peskett, Sam Clemens and Kelly Beaver; Institute of Global Health Innovation at Imperial College: Gianluca Fontana, Dr Hutan Ashrafian, Sutha Satkunarajah and Lenny Naar; Imperial College Healthcare NHS Trust: Robert Klaber; the Patient Experience Research Centre and the REACT Public Advisory Panel; NHS Digital for access to the NHS Register. HW is a NIHR Senior Investigator and acknowledges support from NIHR Biomedical Research Centre of Imperial College NHS Trust, NIHR School of Public Health Research, NIHR Applied Research Collaborative North West London, Wellcome Trust 205456/Z/16/Z. GC is supported by an NIHR Professorship. WSB is the Action Medical Research Professor, AD is an NIHR senior investigator and DA is an Emeritus NIHR Senior Investigator. SR acknowledges support from MRC Centre for Global Infectious Disease Analysis, National Institute for Health Research (NIHR) Health Protection Research Unit (HPRU), Wellcome Trust (200861/Z/16/Z, 200187/Z/15/Z), and Centres for Disease Control and Prevention (US, U01CK0005-01-02) PE is Director of the MRC Centre for Environment and Health (MR/L01341X/1, MR/S019669/1). PE acknowledges support from the NIHR Imperial Biomedical Research Centre and the NIHR HPRUs in Environmental Exposures and Health and Chemical and Radiation Threats and Hazards, the British Heart Foundation Centre for Research Excellence at Imperial College London (RE/18/4/34215) and the UK Dementia Research Institute at Imperial (MC_PC_17114). We thank the Huo Family Foundation for support of our work on COVID-19. Author DeclarationsI confirm all relevant ethical guidelines have been followed, and any necessary IRB and/or ethics committee approvals have been obtained.YesThe details of the IRB/oversight body that provided approval or exemption for the research described are given below:We obtained research ethics approval from the South Central-Berkshire B Research Ethics Committee (IRAS ID: 283787) All necessary patient/participant consent has been obtained and the appropriate institutional forms have been archived.All necessary patient/participant consent has been obtained and the appropriate institutional forms have been archived.YesI understand that all clinical trials and any other prospective interventional studies must be registered with an ICMJE-approved registry, such as ClinicalTrials.gov. I confirm that any such study reported in the manuscript has been registered and the trial registration ID is provided (note: if posting a prospective study registered retrospectively, please provide a statement in the trial ID field explaining why the study was not registered in advance).YesI have followed all appropriate research reporting guidelines and uploaded the relevant EQUATOR Network research reporting checklist(s) and other pertinent material as supplementary files, if applicable.YesThe original datasets generated or analysed, or both, during this study are not publicly available because of governance restrictions and the identifiable nature of the data.
- Published
- 2020
15. Caregivers' Willingness to Accept Expedited Vaccine Research During the COVID-19 Pandemic: A Cross-sectional Survey
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Goldman RD, Marneni SR, Seiler M, Brown JC, Klein EJ, Parra C, Gelernter R, Yan TD, Hoeffe J, Davis AL, Griffiths MA, Hall JE, Gualco G, Mater A, Manzano S, Thompson GC, Ahmed S, Ali S, Shimizu N, and International COVID-19 Parental Attitude Study (COVIPAS) Group
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parental attitudes ,drug approval ,COVID-19 ,vaccine - Abstract
PURPOSE: This study determined the predictors of caregivers' willingness to accept an accelerated regulatory process for the development of vaccines against coronavirus disease 2019 (COVID-19). METHODS: An international cross-sectional survey was administered to 2557 caregivers of children in 17 pediatric emergency departments (EDs) across 6 countries from March 26, 2020, to June 30, 2020. Caregivers were asked to select 1 of 4 choices with which they most agreed regarding a proposed COVID-19 vaccine-approval process, in addition to questions regarding demographic characteristics, the ED visit, and attitudes about COVID-19. Univariate analyses were conducted using the Mann-Whitney U test for comparing non-normally distributed continuous variables, an independent t test for comparing normally distributed continuous variables, and a ?(2) or Fisher exact test for categorical variables. Multivariate logistic regression analysis was used for determining independent factors associated with caregivers' willingness to accept abridged development of a COVID-19 vaccine. A P value of
- Published
- 2020
16. The Steroid Metabolome in the Isolated Ovarian Follicle and Its Response to Androgen Exposure and Antagonism
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Lebbe, M, Taylor, AE, Visser, Jenny, Kirkman-Brown, JC, Woodruff, TK, Arlt, W, and Internal Medicine
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Reproduction, Sex, and Gender ,Dehydroepiandrosterone ,urologic and male genital diseases ,Mice ,Ovarian Follicle ,Androgen Receptor Antagonists ,Androgens ,Metabolome ,Animals ,Female ,Steroids ,Gonadal Steroid Hormones ,Research Articles ,Cells, Cultured ,Metabolic Networks and Pathways - Abstract
The ovarian follicle is a major site of steroidogenesis, crucially required for normal ovarian function and female reproduction. Our understanding of androgen synthesis and metabolism in the developing follicle has been limited by the sensitivity and specificity issues of previously used assays. Here we used liquid chromatography–tandem mass spectrometry to map the stage-dependent endogenous steroid metabolome in an encapsulated in vitro follicle growth system, from murine secondary through antral follicles. Furthermore, follicles were cultured in the presence of androgen precursors, nonaromatizable active androgen, and androgen receptor (AR) antagonists to assess effects on steroidogenesis and follicle development. Cultured follicles showed a stage-dependent increase in endogenous androgen, estrogen, and progesterone production, and incubations with the sex steroid precursor dehydroepiandrosterone revealed the follicle as capable of active androgen synthesis at early developmental stages. Androgen exposure and antagonism demonstrated AR–mediated effects on follicle growth and antrum formation that followed a biphasic pattern, with low levels of androgens inducing more rapid follicle maturation and high doses inhibiting oocyte maturation and follicle growth. Crucially, our study provides evidence for an intrafollicular feedback circuit regulating steroidogenesis, with decreased follicle androgen synthesis after exogenous androgen exposure and increased androgen output after additional AR antagonist treatment. We propose that this feedback circuit helps maintain an equilibrium of androgen exposure in the developing follicle. The observed biphasic response of follicle growth and function in increasing androgen supplementations has implications for our understanding of polycystic ovary syndrome pathophysiology and the dose-dependent utility of androgens in in vitro fertilization settings., Steroid metabolome analysis by mass spectrometry in the isolated ovarian follicle revealed early developmental capacity for androgen synthesis, which was upregulated by androgen receptor antagonists.
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- 2017
17. Three-Dimensional reconstructions of ’light’ and ’intermediate’ capsids of equine herpes virus
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Baker, TS, Newcomb, WW, Booy, FP, Brown, JC, and Steven, AC
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Infectious Diseases ,Infection ,Condensed Matter Physics ,Biochemistry and Cell Biology ,Materials Engineering ,Microscopy - Abstract
Equine herpes virus type 1 (EHV-1) belongs to an extensive family of large, genetically complex, and medically important animal viruses. The virion consists of an icosahedral nucleocapsid (T=16) separated from the viral envelope by a proteinaceous tegument layer. Assembly occurs in the nucleus of infected cells where capsids assemble, are packaged with DNA, then bud through the nuclear membrane. Two morphological species of EHV-1 capsids have been distinguished: “lights” which are abortive particles incapable of packaging DNA and “intermediates” which are precursors in the assembly of mature virions. Purified “intermediates” contain an additional proteinP22 (46 kDa), which is not present in “lights” and accounts for ˜10% of the total particle mass. In order to characterize the capsid structures of the two particle types and explore differences between them, we have applied three-dimensional reconstruction techniques to electron micrographs of frozen-hydrated specimens.The Kentucky A strain of EHV-1 was propagated in L-929 cells, and the two types of capsids were obtained as separate fractions from Renografin-76 density gradients. Neither fraction contained any significant amount of DNA. Cryo-electron microscopy of capsids on carbon film substrates was performed as described earlier. Micrographs were recorded at a nominal magnification of x36,000 at 2-3μm underfocus and digitized with a 50/μn step size (˜1.38nm sampling at the specimen). Three-dimensional reconstructions of the two particle types were computed to 4.5nm resolution using modified “common-lines” procedures. Images of 37 “light” and 39 “intermediate” particles were separately combined to compute three-dimensional density distributions.
- Published
- 1989
18. A technical skill training framework and skill load measurements for the Rugby Union tackle
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Hendricks, S, Till, KA, Oliver, J, Johnston, R, Attwood, M, Brown, JC, Drake, D, Macleod, S, Mellalieu, S, Treu, P, Grant, R, and Jones, B
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- 2018
19. The global burden of tuberculosis: results from the Global Burden of Disease Study 2015
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Kyu, HH, Maddison, ER, Henry, NJ, Mumford, JE, Barber, R, Shields, C, Brown, JC, Nguyen, G, Carter, A, Wolock, TM, Wang, H, Liu, PY, Reitsma, M, Ross, JM, Abajobir, AA, Abate, KH, Abbas, K, Abera, M, Abera, SF, Hareri, HA, Ahmed, M, Alene, KA, Alvis-Guzman, N, Amo-Adjei, J, Andrews, J, Ansari, H, Antonio, CA, Anwari, P, Asayesh, H, Atey, TM, Atre, S, Barac, A, Beardsley, J, Bedi, N, Bensenor, I, Beyene, AS, Butt, ZA, Cardona, PJ, Christopher, DJ, Dandona, L, Dandona, R, Deribe, K, Deribew, A, Ehrenkranz, R, El Sayed Zaki, M, Endries, A, Feyissa, Tesfaye, Fischer, F, Gai, R, Garcia-Basteiro, AL, Gebrehiwot, TT, Gesesew, H, Getahun, B, Gona, P, Goodridge, A, Gugnani, H, Haghparast-Bidgoli, H, Hailu, GB, Hassen, HY, Hilawe, E, Horita, N, Jacobsen, KH, Jonas, JB, Kasaeian, A, Sano Kedir, M, Kemmer, L, Khader, Y, Khan, E, Khang, YH, Khoja, AT, Kim, YJ, Koul, P, Koyanagi, A, Krohn, KJ, Anil Kumar, G, Kutz, M, Lodha, R, Magdy Abd El Razek, H, Majdzadeh, R, Manyazewal, T, Memish, Z, Mendoza, W, Mezgebe, HB, Mohammed, S, Ogbo, FA, Oh, IH, Oren, E, Osgood-Zimmerman, A, Pereira, D, Plass, D, Pourmalek, F, Qorbani, M, Rafay, A, Rahman, M, Rai, RK, Rao, PC, Ray, SE, Reiner, R, Reinig, N, Safiri, S, Kyu, HH, Maddison, ER, Henry, NJ, Mumford, JE, Barber, R, Shields, C, Brown, JC, Nguyen, G, Carter, A, Wolock, TM, Wang, H, Liu, PY, Reitsma, M, Ross, JM, Abajobir, AA, Abate, KH, Abbas, K, Abera, M, Abera, SF, Hareri, HA, Ahmed, M, Alene, KA, Alvis-Guzman, N, Amo-Adjei, J, Andrews, J, Ansari, H, Antonio, CA, Anwari, P, Asayesh, H, Atey, TM, Atre, S, Barac, A, Beardsley, J, Bedi, N, Bensenor, I, Beyene, AS, Butt, ZA, Cardona, PJ, Christopher, DJ, Dandona, L, Dandona, R, Deribe, K, Deribew, A, Ehrenkranz, R, El Sayed Zaki, M, Endries, A, Feyissa, Tesfaye, Fischer, F, Gai, R, Garcia-Basteiro, AL, Gebrehiwot, TT, Gesesew, H, Getahun, B, Gona, P, Goodridge, A, Gugnani, H, Haghparast-Bidgoli, H, Hailu, GB, Hassen, HY, Hilawe, E, Horita, N, Jacobsen, KH, Jonas, JB, Kasaeian, A, Sano Kedir, M, Kemmer, L, Khader, Y, Khan, E, Khang, YH, Khoja, AT, Kim, YJ, Koul, P, Koyanagi, A, Krohn, KJ, Anil Kumar, G, Kutz, M, Lodha, R, Magdy Abd El Razek, H, Majdzadeh, R, Manyazewal, T, Memish, Z, Mendoza, W, Mezgebe, HB, Mohammed, S, Ogbo, FA, Oh, IH, Oren, E, Osgood-Zimmerman, A, Pereira, D, Plass, D, Pourmalek, F, Qorbani, M, Rafay, A, Rahman, M, Rai, RK, Rao, PC, Ray, SE, Reiner, R, Reinig, N, and Safiri, S
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- 2018
20. Forecasting life expectancy, years of life lost, and all-cause and cause-specific mortality for 250 causes of death: reference and alternative scenarios for 2016-40 for 195 countries and territories
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Foreman, KJ, Marquez, N, Dolgert, A, Fukutaki, K, Fullman, N, McGaughey, M, Pletcher, MA, Smith, AE, Tang, K, Yuan, C-W, Brown, JC, Friedman, J, He, J, Heuton, KP, Holmberg, M, Patel, DJ, Reidy, P, Carter, A, Cercy, K, Capin, A, Douwes-Schultz, D, Frank, T, Goettsch, F, Liu, PY, Nandakumar, V, Reitsma, MB, Reuter, V, Sadat, N, Sorensen, RJD, Srinivasan, V, Updike, RL, York, H, Lopez, AD, Lozano, R, Lim, SS, Mokdad, AH, Vollset, SE, Murray, CJL, Foreman, KJ, Marquez, N, Dolgert, A, Fukutaki, K, Fullman, N, McGaughey, M, Pletcher, MA, Smith, AE, Tang, K, Yuan, C-W, Brown, JC, Friedman, J, He, J, Heuton, KP, Holmberg, M, Patel, DJ, Reidy, P, Carter, A, Cercy, K, Capin, A, Douwes-Schultz, D, Frank, T, Goettsch, F, Liu, PY, Nandakumar, V, Reitsma, MB, Reuter, V, Sadat, N, Sorensen, RJD, Srinivasan, V, Updike, RL, York, H, Lopez, AD, Lozano, R, Lim, SS, Mokdad, AH, Vollset, SE, and Murray, CJL
- Abstract
Background Understanding potential trajectories in health and drivers of health is crucial to guiding long-term investments and policy implementation. Past work on forecasting has provided an incomplete landscape of future health scenarios, highlighting a need for a more robust modelling platform from which policy options and potential health trajectories can be assessed. This study provides a novel approach to modelling life expectancy, all-cause mortality and cause of death forecasts —and alternative future scenarios—for 250 causes of death from 2016 to 2040 in 195 countries and territories. Methods We modelled 250 causes and cause groups organised by the Global Burden of Diseases, Injuries, and Risk Factors Study (GBD) hierarchical cause structure, using GBD 2016 estimates from 1990–2016, to generate predictions for 2017–40. Our modelling framework used data from the GBD 2016 study to systematically account for the relationships between risk factors and health outcomes for 79 independent drivers of health. We developed a three-component model of cause-specific mortality: a component due to changes in risk factors and select interventions; the underlying mortality rate for each cause that is a function of income per capita, educational attainment, and total fertility rate under 25 years and time; and an autoregressive integrated moving average model for unexplained changes correlated with time. We assessed the performance by fitting models with data from 1990–2006 and using these to forecast for 2007–16. Our final model used for generating forecasts and alternative scenarios was fitted to data from 1990–2016. We used this model for 195 countries and territories to generate a reference scenario or forecast through 2040 for each measure by location. Additionally, we generated better health and worse health scenarios based on the 85th and 15th percentiles, respectively, of annualised rates of change across location-years for all the GBD risk factors, income per perso
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- 2018
21. Technical determinants of tackle and ruck performance in International rugby union.
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Hendricks, S, van Niekerk, T, Sin, DW, Lambert, M, den Hollander, S, Brown, JC, Maree, W, Treu, P, Till, K, Jones, B, Hendricks, S, van Niekerk, T, Sin, DW, Lambert, M, den Hollander, S, Brown, JC, Maree, W, Treu, P, Till, K, and Jones, B
- Abstract
The most frequently occurring contact events in rugby union are the tackle and ruck. The ability repeatedly to engage and win the tackle and ruck has been associated with team success. To win the tackle and ruck, players have to perform specific techniques. These techniques have not been studied at the highest level of rugby union. Therefore, the purpose of this study was to identify technical determinants of tackle and ruck performance at the highest level of rugby union. A total of 4479 tackle and 2914 ruck events were coded for the Six Nations and Championship competitions. Relative risk ratio (RR), the ratio of the probability of an outcome occurring when a characteristic was observed (versus the non-observed characteristic), was determined using multinomial logistic regression. Executing front-on tackles reduced the likelihood of offloads and tackle breaks in both competitions (Six Nations RR 3.0 Behind tackle, 95% confidence interval [95% CI]: 1.9-4.6, effect size [ES] = large, P < 0.001); Championship RR 2.9 Jersey tackle, 95% CI: 1.3-6.4, ES = moderate, P = 0.01). Fending during contact increased the chances of offloading and breaking the tackle in both competitions (Six Nations RR 4.5 Strong, 95% CI: 2.2-9.2, ES = large, P = P < 0.001; Championship RR 5.1 Moderate, 95% CI: 3.5-7.4, ES = large, P < 0.001). For the ruck, actively placing the ball increased the probability of maintaining possession (Six Nations RR 2.2, 95% CI: 1.1-4.3, ES = moderate, P = 0.03); Championship RR 4.0, 95% CI: 1.3-11.8, ES = large, P = 0.01). The techniques identified in this study should be incorporated and emphasised during training to prepare players for competition. Furthermore, these techniques need to be added to coaching manuals for the tackle and ruck.
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- 2017
22. Global and National Burden of Diseases and Injuries Among Children and Adolescents Between 1990 and 2013 Findings From the Global Burden of Disease 2013 Study
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Kyu, HH, Pinho, C, Wagner, JA, Brown, JC, Bertozzi-Villa, A, Charlson, FJ, Coffeng, LE, Dandona, L, Erskine, HE, Ferrari, AJ, Fitzmaurice, C, Fleming, TD, Forouzanfar, MH, Graetz, N, Guinovart, C, Haagsma, J, Higashi, H, Kassebaum, NJ, Larson, HJ, Lim, SS, Mokdad, AH, Moradi-Lakeh, M, Odell, SV, Roth, GA, Serina, PT, Stanaway, JD, Misganaw, A, Whiteford, HA, Wolock, TM, Hanson, SW, Abd-Allah, F, Abera, SF, Abu-Raddad, LJ, AlBuhairan, FS, Amare, AT, Antonio, CAT, Artaman, A, Barker-Collo, SL, Barrero, LH, Benjet, C, Bensenor, IM, Bhutta, ZA, Bikbov, B, Brazinova, A, Campos-Nonato, I, Castaneda-Orjuela, CA, Catala-Lopez, F, Chowdhury, R, Cooper, C, Crump, JA, Dandona, R, Degenhardt, L, Dellavalle, RP, Dharmaratne, SD, Faraon, EJA, Feigin, VL, Fuerst, T, Geleijnse, JM, Gessner, BD, Gibney, KB, Goto, A, Gunnell, D, Hankey, GJ, Hay, RJ, Hornberger, JC, Hosgood, HD, Hu, G, Jacobsen, KH, Jayaraman, SP, Jeemon, P, Jonas, JB, Karch, A, Kim, D, Kim, S, Kokubo, Y, Defo, BK, Bicer, BK, Kumar, GA, Larsson, A, Leasher, JL, Leung, R, Li, Y, Lipshultz, SE, Lopez, AD, Lotufo, PA, Lunevicius, R, Lyons, RA, Majdan, M, Malekzadeh, R, Mashal, T, Mason-Jones, AJ, Melaku, YA, Memish, ZA, Mendoza, W, Miller, TR, Mock, CN, Murray, J, Nolte, S, Oh, I-H, Olusanya, BO, Ortblad, KF, Park, E-K, Paternina Caicedo, AJ, Patten, SB, Patton, GC, Pereira, DM, Perico, N, Piel, FB, Polinder, S, Popova, S, Pourmalek, F, Quistberg, DA, Remuzzi, G, Rodriguez, A, Rojas-Rueda, D, Rothenbacher, D, Rothstein, DH, Sanabria, J, Santos, IS, Schwebel, DC, Sepanlou, SG, Shaheen, A, Shiri, R, Shiue, I, Skirbekk, V, Sliwa, K, Sreeramareddy, CT, Stein, DJ, Steiner, TJ, Stovner, LJ, Sykes, BL, Tabb, KM, Terkawi, AS, Thomson, AJ, Thorne-Lyman, AL, Towbin, JA, Ukwaja, KN, Vasankari, T, Venketasubramanian, N, Vlassov, VV, Vollset, SE, Weiderpass, E, Weintraub, RG, Werdecker, A, Wilkinson, JD, Woldeyohannes, SM, Wolfe, CDA, Yano, Y, Yip, P, Yonemoto, N, Yoon, S-J, Younis, MZ, Yu, C, Zaki, MES, Naghavi, M, Murray, CJL, Vos, T, Kyu, HH, Pinho, C, Wagner, JA, Brown, JC, Bertozzi-Villa, A, Charlson, FJ, Coffeng, LE, Dandona, L, Erskine, HE, Ferrari, AJ, Fitzmaurice, C, Fleming, TD, Forouzanfar, MH, Graetz, N, Guinovart, C, Haagsma, J, Higashi, H, Kassebaum, NJ, Larson, HJ, Lim, SS, Mokdad, AH, Moradi-Lakeh, M, Odell, SV, Roth, GA, Serina, PT, Stanaway, JD, Misganaw, A, Whiteford, HA, Wolock, TM, Hanson, SW, Abd-Allah, F, Abera, SF, Abu-Raddad, LJ, AlBuhairan, FS, Amare, AT, Antonio, CAT, Artaman, A, Barker-Collo, SL, Barrero, LH, Benjet, C, Bensenor, IM, Bhutta, ZA, Bikbov, B, Brazinova, A, Campos-Nonato, I, Castaneda-Orjuela, CA, Catala-Lopez, F, Chowdhury, R, Cooper, C, Crump, JA, Dandona, R, Degenhardt, L, Dellavalle, RP, Dharmaratne, SD, Faraon, EJA, Feigin, VL, Fuerst, T, Geleijnse, JM, Gessner, BD, Gibney, KB, Goto, A, Gunnell, D, Hankey, GJ, Hay, RJ, Hornberger, JC, Hosgood, HD, Hu, G, Jacobsen, KH, Jayaraman, SP, Jeemon, P, Jonas, JB, Karch, A, Kim, D, Kim, S, Kokubo, Y, Defo, BK, Bicer, BK, Kumar, GA, Larsson, A, Leasher, JL, Leung, R, Li, Y, Lipshultz, SE, Lopez, AD, Lotufo, PA, Lunevicius, R, Lyons, RA, Majdan, M, Malekzadeh, R, Mashal, T, Mason-Jones, AJ, Melaku, YA, Memish, ZA, Mendoza, W, Miller, TR, Mock, CN, Murray, J, Nolte, S, Oh, I-H, Olusanya, BO, Ortblad, KF, Park, E-K, Paternina Caicedo, AJ, Patten, SB, Patton, GC, Pereira, DM, Perico, N, Piel, FB, Polinder, S, Popova, S, Pourmalek, F, Quistberg, DA, Remuzzi, G, Rodriguez, A, Rojas-Rueda, D, Rothenbacher, D, Rothstein, DH, Sanabria, J, Santos, IS, Schwebel, DC, Sepanlou, SG, Shaheen, A, Shiri, R, Shiue, I, Skirbekk, V, Sliwa, K, Sreeramareddy, CT, Stein, DJ, Steiner, TJ, Stovner, LJ, Sykes, BL, Tabb, KM, Terkawi, AS, Thomson, AJ, Thorne-Lyman, AL, Towbin, JA, Ukwaja, KN, Vasankari, T, Venketasubramanian, N, Vlassov, VV, Vollset, SE, Weiderpass, E, Weintraub, RG, Werdecker, A, Wilkinson, JD, Woldeyohannes, SM, Wolfe, CDA, Yano, Y, Yip, P, Yonemoto, N, Yoon, S-J, Younis, MZ, Yu, C, Zaki, MES, Naghavi, M, Murray, CJL, and Vos, T
- Abstract
IMPORTANCE: The literature focuses on mortality among children younger than 5 years. Comparable information on nonfatal health outcomes among these children and the fatal and nonfatal burden of diseases and injuries among older children and adolescents is scarce. OBJECTIVE: To determine levels and trends in the fatal and nonfatal burden of diseases and injuries among younger children (aged <5 years), older children (aged 5-9 years), and adolescents (aged 10-19 years) between 1990 and 2013 in 188 countries from the Global Burden of Disease (GBD) 2013 study. EVIDENCE REVIEW: Data from vital registration, verbal autopsy studies, maternal and child death surveillance, and other sources covering 14,244 site-years (ie, years of cause of death data by geography) from 1980 through 2013 were used to estimate cause-specific mortality. Data from 35,620 epidemiological sources were used to estimate the prevalence of the diseases and sequelae in the GBD 2013 study. Cause-specific mortality for most causes was estimated using the Cause of Death Ensemble Model strategy. For some infectious diseases (eg, HIV infection/AIDS, measles, hepatitis B) where the disease process is complex or the cause of death data were insufficient or unavailable, we used natural history models. For most nonfatal health outcomes, DisMod-MR 2.0, a Bayesian metaregression tool, was used to meta-analyze the epidemiological data to generate prevalence estimates. FINDINGS: Of the 7.7 (95% uncertainty interval [UI], 7.4-8.1) million deaths among children and adolescents globally in 2013, 6.28 million occurred among younger children, 0.48 million among older children, and 0.97 million among adolescents. In 2013, the leading causes of death were lower respiratory tract infections among younger children (905.059 deaths; 95% UI, 810,304-998,125), diarrheal diseases among older children (38,325 deaths; 95% UI, 30,365-47,678), and road injuries among adolescents (115,186 deaths; 95% UI, 105,185-124,870). Iron defici
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- 2016
23. Video analysis of concussion injury mechanism in Under-18 Rugby
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Hendricks, MS, O’ Connor, S, Lambert, M, Brown, JC, McFie, S, Burger, N, Readhead, C, Viljoen, W, Hendricks, MS, O’ Connor, S, Lambert, M, Brown, JC, McFie, S, Burger, N, Readhead, C, and Viljoen, W
- Abstract
Background Understanding the mechanism of injury is necessary for the development of effective injury prevention strategies. Video analysis of injuries provides valuable information on the playing situation and athlete-movement patterns, which can be used to formulate these strategies. Therefore, we conducted a video analysis of the mechanism of concussion injury in junior-level rugby union and compared it with a representative and matched non-injury sample. Methods Injury reports for 18 concussion events were collected from the 2011 to 2013 under-18 Craven Week tournaments. Also, video footage was recorded for all 3 years. On the basis of the injury events, a representative ‘control’ sample of matched non-injury events in the same players was identified. The video footage, which had been recorded at each tournament, was then retrospectively analysed and coded. 10 injury events (5 tackle, 4 ruck, 1 aerial collision) and 83 non-injury events were analysed. Results All concussions were a result of contact with an opponent and 60% of players were unaware of the impending contact. For the measurement of head position on contact, 43% had a ‘down’ position, 29% the ‘up and forward’ and 29% the ‘away’ position (n=7). The speed of the injured tackler was observed as ‘slow’ in 60% of injurious tackles (n=5). In 3 of the 4 rucks in which injury occurred (75%), the concussed player was acting defensively either in the capacity of ‘support’ (n=2) or as the ‘jackal’ (n=1). Conclusions Training interventions aimed at improving peripheral vision, strengthening of the cervical muscles, targeted conditioning programmes to reduce the effects of fatigue, and emphasising safe and effective playing techniques have the potential to reduce the risk of sustaining a concussion injury.
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- 2016
24. Skills Associated with Line Breaks in Elite Rugby Union
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den Hollander, S, Brown, JC, Lambert, M, Treu, P, Hendricks, MS, den Hollander, S, Brown, JC, Lambert, M, Treu, P, and Hendricks, MS
- Abstract
The ability of the attacking team to break through the defensive line is a key indicator of success as it creates opportunities to score tries. The aim of this study was to analyse line breaks and identify the associated skills and playing characteristics. The 2013 Super Rugby season (125 games) was analysed, in which 362 line breaks were identified and coded using variables that assessed team patterns and non-contact attacking skills in the phases preceding the line break. There was an average of 3 line breaks per game, with 39% of line breaks resulting in a try. Line breaks occurred when the ball-carrier was running fast [61%, x 2 (4) = 25.784, p = 0.000, Cramer’s v = 0.1922, weak]. At a moderate distance, short lateral passes (19%) and skip passes (15%) attributed to the highest percentage of line breaks [x 2 (26) = 50.899, p = 0.036, Cramer’s v = 0.2484, moderate]. Faster defensive line speeds resulted in more line breaks [x 2 (12) = 61.703, p < 0.001, Cramer’s v = 0.3026, moderate]. Line breaks are associated with overall team success and try scoring opportunities. Awareness of the defenders line speed and depth, fast running speed when receiving the ball and quick passing between attackers to the outside backs creates line break opportunities. During training, coaches should emphasise the movement speed of the ball between attackers and manipulate the speed and distance of the defenders.
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- 2016
25. Global, regional, and national disability-adjusted life years (DALYs) for 306 diseases and injuries and healthy life expectancy (HALE) for 188 countries, 1990-2013: Quantifying the epidemiological transition
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Murray, CJL, Barber, RM, Foreman, KJ, Ozgoren, AA, Abd-Allah, F, Abera, SF, Aboyans, V, Abraham, JP, Abubakar, I, Abu-Raddad, LJ, Abu-Rmeileh, NM, Achoki, T, Ackerman, IN, Ademi, Z, Adou, AK, Adsuar, JC, Afshin, A, Agardh, EE, Alam, SS, Alasfoor, D, Albittar, MI, Alegretti, MA, Alemu, ZA, Alfonso-Cristancho, R, Alhabib, S, Ali, R, Alla, F, Allebeck, P, Almazroa, MA, Alsharif, U, Alvarez, E, Alvis-Guzman, N, Amare, AT, Ameh, EA, Amini, H, Ammar, W, Anderson, HR, Anderson, BO, Antonio, CAT, Anwari, P, Arnlöv, J, Arsenijevic, VSA, Artaman, A, Asghar, RJ, Assadi, R, Atkins, LS, Avila, MA, Awuah, B, Bachman, VF, Badawi, A, Bahit, MC, Balakrishnan, K, Banerjee, A, Barker-Collo, SL, Barquera, S, Barregard, L, Barrero, LH, Basu, A, Basu, S, Basulaiman, MO, Beardsley, J, Bedi, N, Beghi, E, Bekele, T, Bell, ML, Benjet, C, Bennett, DA, Bensenor, IM, Benzian, H, Bernabé, E, Bertozzi-Villa, A, Beyene, TJ, Bhala, N, Bhalla, A, Bhutta, ZA, Bienhoff, K, Bikbov, B, Biryukov, S, Blore, JD, Blosser, CD, Blyth, FM, Bohensky, MA, Bolliger, IW, Başara, BB, Bornstein, NM, Bose, D, Boufous, S, Bourne, RRA, Boyers, LN, Brainin, M, Brayne, CE, Brazinova, A, Breitborde, NJK, Brenner, H, Briggs, AD, Brooks, PM, Brown, JC, Brugha, TS, Buchbinder, R, Buckle, GC, Murray, CJL, Barber, RM, Foreman, KJ, Ozgoren, AA, Abd-Allah, F, Abera, SF, Aboyans, V, Abraham, JP, Abubakar, I, Abu-Raddad, LJ, Abu-Rmeileh, NM, Achoki, T, Ackerman, IN, Ademi, Z, Adou, AK, Adsuar, JC, Afshin, A, Agardh, EE, Alam, SS, Alasfoor, D, Albittar, MI, Alegretti, MA, Alemu, ZA, Alfonso-Cristancho, R, Alhabib, S, Ali, R, Alla, F, Allebeck, P, Almazroa, MA, Alsharif, U, Alvarez, E, Alvis-Guzman, N, Amare, AT, Ameh, EA, Amini, H, Ammar, W, Anderson, HR, Anderson, BO, Antonio, CAT, Anwari, P, Arnlöv, J, Arsenijevic, VSA, Artaman, A, Asghar, RJ, Assadi, R, Atkins, LS, Avila, MA, Awuah, B, Bachman, VF, Badawi, A, Bahit, MC, Balakrishnan, K, Banerjee, A, Barker-Collo, SL, Barquera, S, Barregard, L, Barrero, LH, Basu, A, Basu, S, Basulaiman, MO, Beardsley, J, Bedi, N, Beghi, E, Bekele, T, Bell, ML, Benjet, C, Bennett, DA, Bensenor, IM, Benzian, H, Bernabé, E, Bertozzi-Villa, A, Beyene, TJ, Bhala, N, Bhalla, A, Bhutta, ZA, Bienhoff, K, Bikbov, B, Biryukov, S, Blore, JD, Blosser, CD, Blyth, FM, Bohensky, MA, Bolliger, IW, Başara, BB, Bornstein, NM, Bose, D, Boufous, S, Bourne, RRA, Boyers, LN, Brainin, M, Brayne, CE, Brazinova, A, Breitborde, NJK, Brenner, H, Briggs, AD, Brooks, PM, Brown, JC, Brugha, TS, Buchbinder, R, and Buckle, GC
- Abstract
Background The Global Burden of Disease Study 2013 (GBD 2013) aims to bring together all available epidemiological data using a coherent measurement framework, standardised estimation methods, and transparent data sources to enable comparisons of health loss over time and across causes, age-sex groups, and countries. The GBD can be used to generate summary measures such as disability-adjusted life-years (DALYs) and healthy life expectancy (HALE) that make possible comparative assessments of broad epidemiological patterns across countries and time. These summary measures can also be used to quantify the component of variation in epidemiology that is related to sociodemographic development. Methods We used the published GBD 2013 data for age-specific mortality, years of life lost due to premature mortality (YLLs), and years lived with disability (YLDs) to calculate DALYs and HALE for 1990, 1995, 2000, 2005, 2010, and 2013 for 188 countries. We calculated HALE using the Sullivan method; 95% uncertainty intervals (UIs) represent uncertainty in age-specific death rates and YLDs per person for each country, age, sex, and year. We estimated DALYs for 306 causes for each country as the sum of YLLs and YLDs; 95% UIs represent uncertainty in YLL and YLD rates. We quantified patterns of the epidemiological transition with a composite indicator of sociodemographic status, which we constructed from income per person, average years of schooling after age 15 years, and the total fertility rate and mean age of the population. We applied hierarchical regression to DALY rates by cause across countries to decompose variance related to the sociodemographic status variable, country, and time. Findings Worldwide, from 1990 to 2013, life expectancy at birth rose by 6·2 years (95% UI 5·6-6·6), from 65·3 years (65·0-65·6) in 1990 to 71·5 years (71·0-71·9) in 2013, HALE at birth rose by 5·4 years (4·9-5·8), from 56·9 years (54·5-59·1) to 62·3 years (59·7-64·8), total DALYs fell by 3·6% (0·3
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- 2015
26. Weight Lifting and Physical Function among Breast Cancer Survivors: A Post Hoc Analysis of a Randomized Controlled Trial
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Brown, JC, primary and Schmitz, KH, additional
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- 2015
- Full Text
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27. A regularization approach for the analysis of X-ray solar spectra: blind tests and applications
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Brown, Jc, Emslie, Ag, Holman, G, Johns Krull, C, Kontar, Ep, Massone, Am, and Piana, Michele
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- 2005
28. The incidence and severity of injuries at the 2011 South African Rugby Union (SARU) Youth Week tournaments
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Brown, JC, Verhagen, JC, Viljoen, W, Readhead, C, Van Mechelen, W, Hendricks, MS, Lambert, MI, Brown, JC, Verhagen, JC, Viljoen, W, Readhead, C, Van Mechelen, W, Hendricks, MS, and Lambert, MI
- Abstract
Background. Rugby Union, compared with other popular team sports, presents an above-average risk of injury to players that may increase with age and level of play. Elite schoolboy rugby players have been competing at the South African Rugby Union (SARU) Youth tournaments at the under-13 (CW13), under-16 (GK16) and under-18 (AW18 and CW18) tournaments annually since 1964. The injury epidemiology of these tournaments has yet to be established. Objectives. To determine the injury incidence densities (IIDs) and severity of SARU Youth Week tournament injuries, if the IID increases with age, and the types of injuries at the different age group levels, in 2011. Methods. All match-related injuries presenting to the Tournament Doctor during these tournaments were recorded and classified for severity and type, using the injury collection Consensus Statement for Rugby. Injury incidence per 1 000 match hours and 95% confidence intervals were calculated using overall player exposure time. Results. Match-related IIDs for ‘all’ (combined: 47.9 injuries/1000 match hours) and time-loss injuries (combined: 23.1 injuries/1000 match hours) were not significantly different by age group, despite a strong tendency to indicate differences. The absolute number of injuries per match increased with age. In general, there was a higher proportion of concussions at the GK16, AW18, and CW18 compared with the CW13 tournament(s). Conclusions. Time-loss IIDs at SARU Youth Weeks are similar to other elite junior rugby data. The absolute number and type/ classification of injuries per match may be more informative than IIDs alone for medical planning purposes.
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- 2012
29. Conserved features in papillomavirus and polyomavirus capsids
- Author
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Belnap, DM, Olson, NH, Cladel, NM, Newcomb, WW, Brown, JC, Kreider, JW, Christensen, ND, and Baker, TS
- Subjects
Biochemistry & Molecular Biology ,cryoelectron microscopy ,Simian virus 40 ,Cottontail rabbit papillomavirus ,Microbiology ,handedness ,Medicinal and Biomolecular Chemistry ,Capsid ,papovaviridae ,three-dimensional image reconstruction ,enantiomer ,Animals ,Humans ,2.2 Factors relating to the physical environment ,Viral ,Antigens ,Aetiology ,Papillomaviridae ,Bovine papillomavirus 1 ,Viral Structural Proteins ,Infectious Diseases ,Sexually Transmitted Infections ,HIV/AIDS ,Capsid Proteins ,Rabbits ,Biochemistry and Cell Biology ,Polyomavirus ,Infection ,Sequence Alignment - Abstract
Capsids of papilloma and polyoma viruses (papovavirus family) are composed of 72 pentameric capsomeres arranged on a skewed icosahedral lattice (triangulation number of seven, T = 7). Cottontail rabbit papillomavirus (CRPV) was reported previously to be a T = 7laevo (left-handed) structure, whereas human wart virus, simian virus 40, and murine polyomavirus were shown to be T = 7dextro (right-handed). The CRPV structure determined by cryoelectron microscopy and image reconstruction was similar to previously determined structures of bovine papillomavirus type 1 (BPV-1) and human papillomavirus type 1 (HPV-1). CRPV capsids were observed in closed (compact) and open (swollen) forms. Both forms have star-shaped capsomeres, as do BPV-1 and HPV-1, but the open CRPV capsids are approximately 2 nm larger in radius. The lattice hands of all papillomaviruses examined in this study were found to be T = 7dextro. In the region of maximum contact, papillomavirus capsomeres interact in a manner similar to that found in polyomaviruses. Although papilloma and polyoma viruses have differences in capsid size (approximately 60 versus approximately 50 nm), capsomere morphology (11 to 12 nm star-shaped versus 8 nm barrel-shaped), and intercapsomere interactions (slightly different contacts between capsomeres), papovavirus capsids have a conserved, 72-pentamer, T = 7dextro structure. These features are conserved despite significant differences in amino acid sequences of the major capsid proteins. The conserved features may be a consequence of stable contacts that occur within capsomeres and flexible links that form among capsomeres.
- Published
- 1996
30. The incidence and severity of injuries at the 2011 South African Rugby Union (SARU) Youth Week tournaments
- Author
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Brown, JC, primary, Verhagen, E, additional, Viljoen, W, additional, Readhead, C, additional, Van Mechelen, W, additional, Hendricks, S, additional, and Lambert, MI, additional
- Published
- 2012
- Full Text
- View/download PDF
31. Evolution of treatment of paralytic scoliosis at Rancho Los Amigos Hospital
- Author
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Bonnett, C, Brown, JC, Perry, J, Nickel, VL, Walinski, T, Brooks, L, Hoffer, M, Stiles, C, and Brooks, R
- Published
- 1975
32. Thoracolumbar scoliosis in cerebral palsy. Results of surgical treatment
- Author
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Bonnett, C, Brown, JC, and Grow, T
- Published
- 1976
33. A comparison of the response of equine heart rate to different equine exercise regimes
- Author
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Barratt, CES, primary, Litten-Brown, JC, additional, and Reynolds, CK, additional
- Published
- 2010
- Full Text
- View/download PDF
34. Undergraduate and diploma students' motives for training as mathematics and science teachers
- Author
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Nyaumwe, LJ, primary, Brown, JC, additional, and Dhliwayo, L, additional
- Published
- 2007
- Full Text
- View/download PDF
35. Visualization of the HSV-1 Portal Complex in situ by Cryo-Electron Tomography
- Author
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Cardone, G, primary, Winkler, D, additional, Trus, BL, additional, Newcomb, WW, additional, Brown, JC, additional, and Steven, AC, additional
- Published
- 2006
- Full Text
- View/download PDF
36. DIRECT EVIDENCE OF FUNCTIONAL L-type Ca2+ CHANNELS IN HUMAN SPERMATOZOA
- Author
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Kirkman-Brown, JC, primary, Barratt, CLR, additional, and Publicover, SJ, additional
- Published
- 2000
- Full Text
- View/download PDF
37. Qualification for practice as a sole practitioner.
- Author
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BROWN, JC
- Published
- 1982
38. Influence of the physical form of barley grain on the digestion of its starch in the human small intestine and implications for health
- Author
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Livesey, G, primary, Wilkinson, JA, additional, Roe, M, additional, Faulks, R, additional, Clark, S, additional, Brown, JC, additional, Kennedy, H, additional, and Elia, M, additional
- Published
- 1995
- Full Text
- View/download PDF
39. Energy balance and expenditure while consuming guar gum at various fat intakes and ambient temperatures
- Author
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Brown, JC, primary and Livesey, G, additional
- Published
- 1994
- Full Text
- View/download PDF
40. Perceptual cues in the regulation of exercise performance - physical sensations of exercise and awareness of effort interact as separate cues.
- Author
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Swart J, Lindsay TR, Lambert MI, Brown JC, and Noakes TD
- Abstract
It has been argued that the physical sensations induced by exercise, measured as the ratings of perceived exertion (RPE), are distinct from the sense of effort. This study aimed to determine whether a new measure of task effort - the Task Effort and Awareness (TEA) score - is able to measure sensations distinct from those included in the conventional RPE scale. Seven well-trained cyclists completed a maximal effort 100 km time trial (TT) and a submaximal trial at 70% of the power sustained during the TT (70% TT). Five maximal 1 km sprints were included in both trials. Both the RPE related solely to physical sensation (P-RPE) and the TEA score increased during the TT and were linearly related. During the 70% TT, both P-RPE and TEA scores increased, but TEA increased significantly less than P-RPE (p<0.001). TEA scores reached maximal values in all 1 km sprints in both the maximal TT and 70% TT, whereas the RPE increased progressively, reaching a maximal value only in the final 1 km sprints in both the TT and the 70% TT. These results indicate that the physical sensations of effort measured as the P-RPE act as the template regulating performance during exercise and that deviation from that template produces an increase in the sense of effort measured by the TEA score. Together, these controls ensure that the chosen exercise intensity does not threaten bodily homeostasis. Our findings also explain why submaximal exercise conducted within the constraints of the template P-RPE does not produce any conscious awareness of effort. [ABSTRACT FROM AUTHOR]
- Published
- 2012
41. Surgical and functional results of spine fusion in spinal muscular atrophy.
- Author
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Brown JC, Zeller JL, Swank SM, Furumasu J, Warath SL, Brown, J C, Zeller, J L, Swank, S M, Furumasu, J, and Warath, S L
- Published
- 1989
42. Functional activities in spinal muscular atrophy patients after spinal fusion.
- Author
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Furumasu J, Swank SM, Brown JC, Gilgoff I, Warath S, Zeller J, Furumasu, J, Swank, S M, Brown, J C, Gilgoff, I, Warath, S, and Zeller, J
- Published
- 1989
43. Diagnostic difficulties encountered in the myasthenic syndrome sometimes associated with carcinoma
- Author
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Brown Jc and Johns Rj
- Subjects
Adult ,Male ,Pathology ,medicine.medical_specialty ,Concentric needle electromyography ,Neural Conduction ,Action Potentials ,Electromyography ,Guanidines ,Synaptic Transmission ,Diagnosis, Differential ,Muscular Diseases ,medicine ,Carcinoma ,Humans ,Carcinoma, Small Cell ,Myopathy ,Electrodes ,Evoked Potentials ,Electric stimulation ,Aged ,medicine.diagnostic_test ,business.industry ,Bronchial Neoplasms ,Articles ,Middle Aged ,medicine.disease ,Dermatology ,Electric Stimulation ,Psychiatry and Mental health ,Female ,Surgery ,Neurology (clinical) ,Differential diagnosis ,medicine.symptom ,business - Abstract
Six patients with the physiological features of the myasthenic syndrome associated with carcinoma are presented. The clinical features encountered in this group, including age, mode of onset, and duration of symptom indicate that it may escape detection owing to its resemblance to other neuromuscular disorders. Conventional concentric needle electromyography may lead to the disorder being confused with a myopathy. The association with carcinoma is by no means constant. Clinical and physiological improvement with guanidine is described in each case.
- Published
- 1974
44. Muscle weakness after rest in myotonic disorders: an electrophysiological study
- Author
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Brown Jc
- Subjects
Adult ,Weakness ,Time Factors ,Myotonia Congenita ,genetic structures ,Rest ,Myotonic Disorder ,Neuromuscular Junction ,Action Potentials ,Electromyography ,Edrophonium ,Guanidines ,Myotonic dystrophy ,medicine ,Humans ,Myotonic Dystrophy ,medicine.diagnostic_test ,business.industry ,Myotonia congenita ,Muscles ,Temperature ,Muscle weakness ,Articles ,Middle Aged ,Myotonia ,medicine.disease ,Electric Stimulation ,Psychiatry and Mental health ,Phenytoin ,Anesthesia ,Surgery ,Neurology (clinical) ,medicine.symptom ,business ,Muscle Contraction ,Muscle contraction - Abstract
Changes in amplitude of the evoked muscle action potential (MAP) have been observed in four patients with myotonia congenita and two with dystrophia myotonica. A fade in the response occurred in every case with stimulus frequencies of 10 per second or less, provided that the muscle was in a rested state and that long enough stimulus trains were used. Intramuscular stimulation and recording techniques show that the myotonic muscle fibre is the site of this defect. The MAP fade is thought to represent the transient weakness from which such patients may suffer, particularly after rest. Since neither this weakness nor the fade was related to the severity of the myotonia, nor were they significantly influenced by cooling or hydantoins, they may well be due to a separate defect in the myotonic muscle from that which causes the hyperexcitability of the fibre membrane.
- Published
- 1974
45. The Differential Diagnosis of Hip Pain using Radionuclide Imaging
- Author
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Brown Jc, Forrester Dm, and Fogel Jp
- Subjects
medicine.medical_specialty ,Rheumatology ,business.industry ,medicine ,Radionuclide imaging ,Hip pain ,Radiology ,Differential diagnosis ,Nuclear medicine ,business - Published
- 1983
46. The Use of Gallium-67 Citrate to Distinguish between Infectious and Non-Infectious Arthritis
- Author
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Brown Jc, Hensel Al, and Forrester Dm
- Subjects
Rheumatology ,business.industry ,Immunology ,Medicine ,Arthritis ,Gallium 67 citrate ,business ,medicine.disease ,Non infectious - Published
- 1983
47. Nonreversibility in the Reductive Denaturation of Chymotrypsinogen A
- Author
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Brown Jc and Horton Hr
- Subjects
chemistry.chemical_classification ,Chromatography ,Chymotrypsin ,biology ,Chemistry ,Chymotrypsinogen ,Polypeptide chain ,Trypsin ,General Biochemistry, Genetics and Molecular Biology ,CHYMOTRYPSINOGEN A ,Enzyme ,Biochemistry ,biology.protein ,medicine ,Denaturation (biochemistry) ,Chemical stability ,medicine.drug - Abstract
SummaryInvestigation of the air-reoxidation of denatured, fully reduced chymotrypsinogen A resulted in a maximum recovery of 1.4% of enzymatically active chymotrypsin upon treatment with trypsin. Under the same conditions, urea-denatured chymotrypsinogen, which had not been reduced, yielded 100% recovery of enzymatic activity. Thus the biologically functional conformation of the polypeptide chain comprising chymotrypsinogen may not be that of greatest thermodynamic stability.
- Published
- 1972
48. Relationship between Electrical and Spontaneous Thrombosis
- Author
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Lavelle Sm, Brown Jc, and Sawyer Pn
- Subjects
medicine.medical_specialty ,Chemistry ,Internal medicine ,medicine ,Cardiology ,Coagulation (water treatment) ,Hematology ,Spontaneous thrombosis - Abstract
SummaryThe triggering of electrical thrombosis on electrodes depends on the coagulation steps prior to factor IX activation. Factor XII may be responsible for this phenomenon. The platelet may also play a role. It has been shown that platelet deposition is visible at potentials more positive than +0.3 V versus the normal hydrogen electrode. The same compounds which inhibit intravascular thrombosis will also impair electrical thrombosis.
- Published
- 1969
49. Stress management training for dental students
- Author
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Tisdelle, DA, Hansen, DJ, St Lawrence, JS, and Brown, JC
- Abstract
Dental school and professional practice are well‐documented sources of stress. Although students and dentists risk developing stress‐related disorders, no empirically evaluated method for helping dental students cope with stress has been reported. A group of 17 dental students participated in a six‐session program that included instruction in self‐relaxation and time management; exercise and leisure planning; and cognitive modification techniques. From pre‐ to post‐training, subjects showed improvement on a variety of self‐report and physiological measures relative to a waiting‐list control group. A three‐month follow‐up assessment revealed continued reductions in stress‐related behavior. The importance of stress‐management training for dental students is discussed as well as suggestions for future research.
- Published
- 1984
- Full Text
- View/download PDF
50. Autoregulation of an antibody response via network-induced auto-anti-idiotype
- Author
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Brown, JC and Rodkey, LS
- Abstract
The antibody response of a single outbred rabbit was studied throughout three rounds of injections with Micrococcus lysodeikticus vaccine over a 31-mo period. The first-round response was characterized by a vigorous anti- micrococcus response and a strong anti-IgG rheumatoid factor response. The second-round response consisted of a triad of interacting molecules: anti- micrococcal antibodies, autoanti-idiotypic antibodies specific for distinct clonotypes of the first-round anti-micrococcal antibodies, and Fc-specific anti-IgG rheumatoid factor. The interacting triple complex was detected because of the formation of an immune complex that became insoluble upon dilution of the serum. Complex formation was inhibited in the presence of saccharide compounds known to be major immunodominant determinants of the micrococcal cell-wall carbohydrate polymer. The same saccharides did not affect the reaction of rheumatoid factor with IgG. Direct-binding radioimmunoassays ruled out mediation of the dilution-precipitation reaction by soluble micrococcal antigens. Specific absorption of rheumatoid factor inhibited the dilution-precipitation reaction. Auto-anti-idiotypic antibodies were specifically purified from second-round sera, directly confirming the presence of these antibodies. Suppressive effects of auto-anti-idiotypic antibodies on distinct antibody clonotypes were shown by gel isoelectric focusing of first-, second-, and third-round sera. Clonotypes expressed in the first round of immunizations were reduced in quantity or absent when auto-anti-idiotypic antibodies were detectable. Greatly enhanced levels or initial synthesis of new clonotypes of anti-micrococcal antibodies were detected during the period of auto-anti-idiotype synthesis. The third-round sera, devoid of detectable auto-anti-idiotype, contained clonotypes characteristic of both first- and second-round antisera. Thus, auto-anti- idiotypic-mediated suppression appeared to be reversible. The data are interpreted as lending strong support for concepts of autoregulation of immune processes in normal outbred animals via an idiotypic network.
- Published
- 1979
- Full Text
- View/download PDF
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