18 results on '"Nerys Roberts"'
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2. Tornadoes, transformers and time to imagine: Increasing opportunities for creative thinking with a class of young children
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Nerys Roberts-Law
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Class (computer programming) ,Mathematics education ,Sociology ,Creative thinking ,Transformer (machine learning model) - Abstract
This article looks at a specific intervention carried out with forty young children over the course of an academic year. The aim of the intervention was to give opportunities for creative thinking, with the ultimate goal of promoting learning free from preconceptions and judgements of ability. The intervention resulted in learning through co-agency, opportunities for the teacher to deepen their understanding of the pupils and their learning and, ultimately, it empowered pupils to become better learners.
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- 2021
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3. Clinical manifestations of coxsackievirus A6: what a dermatologist needs to know
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Khawar Hussain, Sumir Chawla, David Muir, and Nerys Roberts
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Dermatology - Published
- 2022
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4. Panton-Valentine leucocidin-producing Staphylococcus aureus: a clinical review
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Khawar Hussain, Anisha Bandyopadhyay, Nerys Roberts, Nabeela Mughal, Luke S. P. Moore, and Lucinda Claire Fuller
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Staphylococcus aureus ,Leukocidins ,Dermatology & Venereal Diseases ,Soft Tissue Infections ,Prevalence ,Humans ,Exotoxins ,1103 Clinical Sciences ,Dermatology ,Staphylococcal Infections - Abstract
Panton–Valentine leucocidin (PVL) is a virulence factor produced by certain strains of Staphylococcus aureus (SA). Through its cytolytic action on the cell membranes of human polymorphonuclear neutrophils, PVL causes a range of pathologies collectively known as PVL-SA disease. The hallmark clinical signs of PVL-SA are recurrent boils and necrotizing skin and soft tissue infections (SSTIs) in otherwise healthy patients; however, it can lead to more severe and invasive presentations, including necrotizing haemorrhagic pneumonia, necrotizing fasciitis and purpura fulminans. Young adults with minimal previous exposure to healthcare settings tend to be at highest risk for acquiring PVL-SA disease, with close physical contact playing a central role in disease transmission. The prevalence of PVL-SA varies globally; however, this is often underestimated owing to a lack of routine PVL testing. In the UK, PVL-positive SA isolates have been rising over the past decade alongside an increasing prevalence of multidrug resistance in larger cities. This review article aims to raise awareness of the PVL toxin, to aid clinicians with diagnostic pointers and to provide guidance with treatment, with an emphasis on the need for further population-based studies.
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- 2022
5. Visual impairment, severe visual impairment, and blindness in children in Britain (BCVIS2): a national observational study
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Lucinda J Teoh, Ameenat Lola Solebo, Jugnoo S Rahi, Joe Abbott, Wajda Abdullah, Gill Adams, Louise Allen, Christopher Anderson, Karen Ansell, Samira Anwar, Isabel Ash, Jane Ashworth, Sher Aslam, Majunath Astagi, Colin Ball, Rajesh Balu, Victoria Barrett, Zahabiyah Bassi, Adam Bates, Dushyant Batra, Sarah Bell, Linda Belmour, James Benzimra, Ginny Birrell, Susmito Biswas, Andrew Blaikie, Michael Blundell, Kate Bolton, Ewoud Bos, Pamela Bowen, Richard Bowman, Natalie Boyle, John Bradbury, Maria Bredow, Marsel Bregu, Nicholas Brennan, Rosie Brennan, Paul Brittain, Charles Buchanan, Catey Bunce, Howard Bunting, Priscilla Burgess, Cathie Burke, Alexandra Kate Bush, Jeremy Butcher, Lucilla Butler, Clare Cane, Cathryn Chadwick, Ruth Charlton, Anne-Marie Childs, Jessy Choi, Vivi Choleva, Amanda Churchill, Michael Clarke, Peter Clayton, Luke Clifford, Alan Connor, Rachel Cox, Lyn Cresswell, Annegret Dahlmann-Noor, Angela D'Amore, Mehul Dattani, Fiona Dean, Anita Devlin, Luna Dhir, Cora Doherty, Suzanne Dorey, Fiona Drimmie, Tina Duke, Gordon Dutton, Fiona Eaton, Megan Eaton, Danielle Eckersley, Clive Edelsten, Rachel Elderkin, Julia Ennis, Julia Escardo-Paton, Ziad Estephen, Onajite Etuwewe, Anthony Evans, Adjoa Ezekwe, Jenny Fairfield, Kevin Falzon, Allison Ferguson, Brian Fleck, Mary Gainsborough, Alexandra Galloway, Naomi Gerson-Sofer, Caspar Gibbon, Patricia Gibson, Kevin Goss, Katherine Graham-Evans, Judith Gray, Anna Gregory, Arun Gulati, Deniz Gurtin-Zorkun, Emma Guy, Diab Haddad, Helen Haggerty, Paul Haigh, Julia Hale, Samer Hamada, Joanne Hancox, Kerry Hanna, Sian Harris, Christine Harrison, Phillip Harvey, Sophie Headland, Dominic Heath, Paul Heaton, Robert Henderson, Melanie Hingorani, Zoe Hirst, Claire Hogg, Wolfgang Hogler, Roger Holden, Janice Hoole, Karen Horridge, Delyth Howard, Rachel Howells, Vanessa Irvine, Clare Irving, Nicola Johnson, Ian Johnston, Alice Jollands, David Jones, Annie Joseph, Archana Joshi, Pugazhvendan Kandaswamy, Charles Kattakayam, Joseph Keenan, Anne Kelly, James Kersey, Awais Khan, Peng Khaw, Tina Kipioti, Sadia Kiran, Lesley Kneen, Ajay Kotagiri, Richa Kulshrestha, Rosemary Lambley, Tim Lavy, Joanna Lawson, Vicki Lee, Jane Leitch, Julie Lennon, Gabi Lipshen, Chris Lloyd, John Loftus, Tom Lomas, Vernon Long, Jane Mackinnon, Mary MacRae, Usman Mahmood, Anna Maino, Sarah Maling, David Mansfield, Elizabeth Marder, Richard Markham, Jane Marr, Catherine Marsh, Anna Maw, Eleanor McCartney, Helen McCullagh, Anna McDonald, Derek McPhee, Lawrence Miall, Shila Mistry, Benjamin Moate, Meyyammai Mohan, Helen Moore, Will Moore, Nicola Morgan, Claire Morton, Alan Mulvihill, Ranjit Nair, Bill Newman, Christiane Nitsch, Katy O'Connell, Ngozi Oluonye, Vittaldas Pai, Helen Palmer, Maria Papadopoulos, Shelagh Parkinson, Bina Parmar, Manoj Parulekar, Madhavi Parvathareddy, Dipesh Patel, Himanshu Patel, Kamal Patel, Philippa Pennefather, Flaudia Petrone, Marcus Pierrepoint, Rachel Pilling, Sally Pollard, Renata Puertas, Karen Pysden, Anthony Quinn, Philip Quinn, Diyaa Rachdan, Jyoti Raina, Saul Rajak, Laura Ramm, Catherine Rands, Tekki Rao, Mary Ray, Ashwin Reddy, Sheilla Reilly, Maralla Rekha, Greg Richardson, Andrew Riordan, Nerys Roberts, Helen Robertson, Gillian Robinson, Neil Rogers, Shakir Saeed, Caroline Salmon, Jenefer Sargent, Nagini Sarvananthan, Conrad Schmoll, James Self, P Sellar, Elaine Service, Ayad Shafiq, Shilpa Shah, Vinod Sharma, Jemima Sharp, Julia Shaw, Manjula Shenoy, Tamsin Sleep, Elisa Smit, Katherine Smyth, Lynne Speedwell, Katherine Spowart, P Standring, Paulo Stanga, Alison Stanley, Alan Stanton, David Steel, John Stephen, Catherine Stewart, Jessica Street, Sally Stucke, Shona Sutherland, Katya Tambe, Anamika Tandon, Alison Tappin, Kate Taylor, Robert Taylor, Katherine Teasdale, Maria Theodorou, Gareth Thomas, Megan Thomas, Paula Thomas, Dorothy Thompson, Stephen Thomson, Indrajit Thopte, Peter Tiffin, Angela Tillett, Heidi Traunecker, Maria Tsimpida, Vivienne Van Someren, Udupa Venkatesh, Zoe Vermaak, Michael Vincent, David Walker, Simon Walker, Deidre Walsh, Bronwyn Walters, Martin Ward Platt, Louise Watson, Patrick Watts, Siobhan West, Stephanie West, Cathy White, Joy White, Gabriel Whitlingum, Cathy Williams, Sophie Wilne, Janice Wilson, Chien Wong, Tamsin Woodbridge, Paul Wright, Martha Wyles, and Philip Wylie
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Male ,medicine.medical_specialty ,Pediatrics ,Adolescent ,genetic structures ,Cross-sectional study ,Visual impairment ,Vision Disorders ,Blindness ,03 medical and health sciences ,0302 clinical medicine ,030225 pediatrics ,Epidemiology ,Health care ,Ethnicity ,Developmental and Educational Psychology ,medicine ,Humans ,Cumulative incidence ,030212 general & internal medicine ,Child ,business.industry ,Incidence ,Incidence (epidemiology) ,Infant, Newborn ,Childhood blindness ,Infant ,medicine.disease ,United Kingdom ,eye diseases ,Cross-Sectional Studies ,Socioeconomic Factors ,Child, Preschool ,Pediatrics, Perinatology and Child Health ,Female ,Observational study ,medicine.symptom ,business - Abstract
Summary Background The WHO VISION 2020 global initiative against blindness, launched in 2000, prioritised childhood visual disability by aiming to end avoidable childhood blindness by 2020. However, progress has been hampered by the global paucity of epidemiological data concerning childhood visual disability. The British Childhood Visual Impairment and Blindness Study 2 (BCVIS2) was done to address this evidence gap. Methods BCVIS2 was a prospective UK-wide, cross-sectional, observational study to establish an inception cohort of children newly diagnosed with visual impairment. Ophthalmologists and paediatricians reported cases from 89 hospitals and community centres across the UK. We included children aged 18 years or younger who were newly diagnosed with any condition causing impaired visual acuity to a level of 0·5 logMAR or worse (worse than 6/18 Snellen) in each eye, or equivalent vision as assessed by standard qualitative measures, between Oct 1, 2015, and Nov 1, 2016. Eligible children were notified simultaneously but independently by their managing ophthalmologists and paediatricians via the two national active surveillance schemes, the British Ophthalmological Surveillance Unit and the British Paediatric Surveillance Unit. Standardised detailed demographic, socioeconomic, and clinical data about detection, management, and treatment were collected at diagnosis and 1 year later. We calculated incidence estimates and relative rates by key sociodemographic factors. We did descriptive analyses of underlying ophthalmic disorders and non-ophthalmic comorbidities. Findings 61 (7%) of 845 eligible children initially notified were ineligible at follow-up because of improved vision after treatment. Thus, the study sample comprised 784 children with permanent newly-diagnosed all-cause visual impairment, severe visual impairment, or blindness. 559 (72%) of 778 children had clinically significant non-ophthalmic impairments or conditions. 28 (4%) of 784 children died within a year after diagnosis of visual disability (all had underlying systemic disorders). Incidence of visual disability in the first year of life was 5·19 per 10 000 children (95% CI 4·71–5·72), almost ten times higher than among 1-to-4-year-olds and between 20 times and 100 times higher than in the older age groups. The overall cumulative incidence (or lifetime risk) of visual impairment, severe visual impairment, or blindness was 10·03 per 10 000 children (9·35–10·76). Incidence rates were higher for those from any ethnic minority group, the lowest quintile of socioeconomic status, and those born preterm or with low birthweight. 345 (44%) of 784 children had a single affected anatomical site. Disorders of the brain and visual pathways affected 378 (48%) of 784 children. Interpretation BCVIS2 provides a contemporary snapshot of the heterogeneity, multi-morbidity, and vulnerability associated with childhood visual disability in a high-income country. These findings could facilitate developing and delivering health care and planning of interventional research. Our findings highlight the importance of including childhood visual disability as a sentinel event and metric in global child health initiatives. Funding Fight for Sight, National Institute for Health Research, and Ulverscroft Foundation.
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- 2021
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6. Athena Speciality Certificate Examination case for formulation and systemic therapy
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Khawar Hussain, Louise Fearfield, and Nerys Roberts
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Diagnosis, Differential ,Blister ,Immunoglobulin G ,Humans ,Dermatology ,Immunohistochemistry - Abstract
This Athena case describes possible differential diagnoses in a patient with multiple blisters. Histopathology showed subepidermal clefting and superficial dermal inflammation, while immunohistochemistry showed linear deposition of IgG and C3 along the basement membrane zone.
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- 2022
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7. Mentorship in dermatology: a necessity in difficult times
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Khawar Hussain, Neil Patel, Louise Fearfield, Nerys Roberts, and Richard Staughton
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Mentors ,COVID-19 ,Humans ,Dermatology ,Pandemics ,United Kingdom - Published
- 2022
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8. Hypereosinophilic Disorders
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Eirini E. Merika and Nerys Roberts
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- 2019
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9. Monoclonal gammopathy of cutaneous significance
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Khawar Hussain, Dipal Mehta, Priyank Patel, and Nerys Roberts
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Paraproteinemias ,Humans ,Dermatology ,Monoclonal Gammopathy of Undetermined Significance ,Skin - Published
- 2022
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10. Epithelial inflammation resulting from an inherited loss-of-function mutation in EGFR
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Penny E. Morton, Jemima E. Mellerio, Sachin N Patil, Michael A. Simpson, Lu Liu, Cheryl Wellington, Masashi Akiyama, James R. McMillan, Takuya Takeichi, Alya Abdul-Wahab, Sophia Aristodemou, John I. Harper, Maddy Parsons, Akemi Ishida-Yamamoto, Nerys Roberts, Amr Salam, Patrick Campbell, Gabriela Petrof, Laura E. Proudfoot, Sarawin Harnchoowong, Kristina L. Stone, W.H. Irwin McLean, Kingi Aminu, Kenneth Fong, and John A. McGrath
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Keratinocytes ,Male ,Pathology ,medicine.medical_specialty ,MAP Kinase Signaling System ,Cellular differentiation ,Biopsy ,Mutation, Missense ,Inflammation ,Dermatitis ,Dermatology ,In Vitro Techniques ,Biochemistry ,Epithelium ,Fatal Outcome ,Downregulation and upregulation ,medicine ,Humans ,Epidermal growth factor receptor ,Molecular Biology ,Tissue homeostasis ,EGFR inhibitors ,Skin ,biology ,medicine.diagnostic_test ,Homozygote ,Cell Differentiation ,Cell Biology ,3. Good health ,ErbB Receptors ,Child, Preschool ,Skin biopsy ,biology.protein ,Signal transduction ,medicine.symptom ,Proto-Oncogene Proteins c-akt ,Signal Transduction - Abstract
Epidermal growth factor receptor (EGFR) signaling is fundamentally important for tissue homeostasis through EGFR/ligand interactions that stimulate numerous signal transduction pathways. Aberrant EGFR signaling has been reported in inflammatory and malignant diseases, but thus far no primary inherited defects in EGFR have been recorded. Using whole-exome sequencing, we identified a homozygous loss-of-function missense mutation in EGFR (c.1283 G>A; p.Gly428Asp) in a male infant with lifelong inflammation affecting the skin, bowel, and lungs. During the first year of life, his skin showed erosions, dry scale, and alopecia. Subsequently, there were numerous papules and pustules--similar to the rash seen in patients receiving EGFR inhibitor drugs. Skin biopsy demonstrated an altered cellular distribution of EGFR in the epidermis with reduced cell membrane labeling, and in vitro analysis of the mutant receptor revealed abrogated EGFR phosphorylation and EGF-stimulated downstream signaling. Microarray analysis on the patient's skin highlighted disturbed differentiation/premature terminal differentiation of keratinocytes and upregulation of several inflammatory/innate immune response networks. The boy died at the age of 2.5 years from extensive skin and chest infections as well as electrolyte imbalance. This case highlights the major mechanism of epithelial dysfunction following EGFR signaling ablation and illustrates the broader impact of EGFR inhibition on other tissues.
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- 2014
11. Anthropological locations. Boundaries and grounds of a field science. EDITED BY AKHIL GUPTA AND JAMES FERGUSON. London: University of California Press. 1997. viii + 449 pp. Pb: £13.95. ISBN 0 520 20680 0
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Nerys Roberts
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History ,Sociology and Political Science ,Arts and Humanities (miscellaneous) ,Anthropology ,Developmental and Educational Psychology ,Environmental ethics ,Field science - Published
- 1999
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12. Infantile haemangioma: harmless 'strawberry' or life-threatening vascular anomaly?
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Nerys Roberts
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medicine.medical_specialty ,Skin Neoplasms ,Critically ill ,Vascular disease ,business.industry ,Vascular Malformations ,Incidence ,Infant ,General Medicine ,medicine.disease ,Dermatology ,Vascular anomaly ,Surgery ,CME Dermatology ,Angioma ,Diagnosis, Differential ,Infantile haemangioma ,medicine ,Humans ,Birthmark ,business ,Hemangioma - Abstract
Vascular birthmark classification was updated in 1996 ([Table 1][1])[1][2],[2][3] and has gained widespread recognition as a clinically useful framework. Haemangiomas are differentiated from vascular malformations by their clinical presentation, radiology and pathology, particularly by their
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- 2009
13. Pieces of mosaic. An essay on the making of Makedonija. By Jonathan Matthew Schwartz. Højbjerg: Intervention Press. 1996. ix + 149 pp. Pb.: £6.99. ISBN 87 89825 16 0
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Nerys Roberts
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History ,Sociology and Political Science ,Arts and Humanities (miscellaneous) ,Anthropology ,Intervention (counseling) ,Developmental and Educational Psychology ,Mosaic (geodemography) ,Theology ,Making-of ,Law and economics - Published
- 2001
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14. Cardiac responses to head up tilt during early extrauterine life: relevance of active acquisition of erect posture
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Fabio Magrini, R. Meazza, C. Mondadori, Michele M. Ciulla, Paolo Reggiani, Nerys Roberts, and Giovanna Branzi
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Tachycardia ,Supine position ,Physiology ,Cardiac Volume ,Posture ,Hemodynamics ,Blood Pressure ,Cardiovascular System ,Cardiovascular Physiological Phenomena ,Heart Rate ,Physiology (medical) ,Heart rate ,Intravascular volume status ,Humans ,Medicine ,business.industry ,Infant ,Head up tilt ,Adaptation, Physiological ,Blood pressure ,Anesthesia ,End-diastolic volume ,Vascular Resistance ,medicine.symptom ,Cardiology and Cardiovascular Medicine ,business ,Head - Abstract
Mammals must adapt to gravity on passing from the intrauterine to the extrauterine environment. In order to evaluate the cardiovascular effects of gravity in the first phases of extrauterine life, the effects of passive orthostatism on the cardiac filling volume were investigated through longitudinal haemodynamic studies in 14 normal healthy males before (6 months) and after (18 months) acquiring the ability to stand. Left ventricular diameter (by echocardiographic measurement), arterial blood pressure (by sphygmomanometry) and heart rate were measured in the supine and upright position at both ages. At 6 months the left ventricular end diastolic volume was not modified by a change in posture [supine 6(SEM 3) ml, upright 6(3) ml], so heart rate was minimally altered [supine 128(9), upright 130(11) beats.min-1] and blood pressure remained stable [supine 74(6), upright 73(5) mm Hg]. After the acquisition of the erect posture (18 months) left ventricular end diastolic volume was reduced [supine 14(3), upright 8(2) ml], heart rate increased [supine 110(11), upright 127(12) beats.min-1] and blood pressure remained constant [supine 80(6), upright 79(7) mm Hg]. The assumption of the erect posture therefore represents a phase when, for the first time in the natural history of the cardiovascular system, translocation of intravascular volume from the cardiopulmonary area to the periphery stimulates nervous and humoral responses to control the dynamics of body fluids and arterial blood pressure in a gravitational environment.
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- 1989
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15. Cardiogenic hypertension in maturing dogs
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Giovanna Branzi, Michele M. Ciulla, C. Mondadori, Nerys Roberts, R. Meazza, Paolo Reggiani, and Fabio Magrini
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Aging ,medicine.medical_specialty ,Mean arterial pressure ,Cardiac output ,Time Factors ,Hemodynamics ,Blood Pressure ,Femoral artery ,Veins ,Dogs ,Heart Rate ,Reference Values ,Internal medicine ,medicine.artery ,Heart rate ,Internal Medicine ,medicine ,Animals ,Cardiac Output ,biology ,business.industry ,Body Weight ,Fissipedia ,Cardiac Pacing, Artificial ,Heart ,Arteries ,biology.organism_classification ,Surgery ,Oxygen ,medicine.anatomical_structure ,Blood pressure ,Animals, Newborn ,Hypertension ,Vascular resistance ,Cardiology ,Vascular Resistance ,business - Abstract
The purpose of this study was to evaluate whether the heart can induce high blood pressure by maintaining an inappropriately elevated cardiac output/body weight ratio during growth. Direct (femoral artery) mean arterial pressure (MAP), heart rate, cardiac output/body weight ratio (as defined by M-mode echocardiography), and total peripheral vascular resistance were measured and calculated every 2 months in nine conscious dogs during development from 2 to 10 months of age. In four dogs a J-shaped catheter for atrial pacing was chronically implanted at the age of 3 months, and their hearts were permanently paced at 130 beats/min until maturity. The aim of atrial pacing was to prevent the natural slowing of the heart rate and, consequently, to maintain a cardiac output/body weight ratio that was inappropriately high in relation to age during growth. Five dogs were studied as controls. No hemodynamic differences were observed until the age of 4 months. From the age of 5 to 10 months heart rate was kept at 130 beats/min by atrial pacing in the atrially paced group, and the mean cardiac output/body weight ratio did not decrease (196 +/- 24 vs 191 +/- 34 [SE] ml/min/kg). MAP rose from 62 +/- 4 to 116 +/- 8 mm Hg, and total peripheral resistance increased from 0.34 +/- 0.07 to to 0.61 +/- 0.09 mm Hg/ml/min/kg.(ABSTRACT TRUNCATED AT 250 WORDS)
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- 1988
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16. Human renovascular effects of dopexamine hydrochloride: A novel agonist of peripheral dopamine and beta2-adreno-receptors
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Fabio Magrini, Giovanna Macchi, Alberto Zanchetti, R. Foulds, C. Mondadori, and Nerys Roberts
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Adult ,Male ,Agonist ,medicine.medical_specialty ,medicine.drug_class ,Dopamine ,Dopexamine ,Vasodilation ,urologic and male genital diseases ,Dopamine agonist ,Receptors, Dopamine ,Renal Circulation ,Heart Rate ,Internal medicine ,medicine ,Humans ,Pharmacology (medical) ,Cardiac Output ,Pharmacology ,Kidney ,Renal circulation ,business.industry ,Hemodynamics ,General Medicine ,Adrenergic beta-Agonists ,Middle Aged ,Endocrinology ,medicine.anatomical_structure ,Renal blood flow ,Hypertension ,cardiovascular system ,Vascular Resistance ,business ,medicine.drug - Abstract
The effects of dopexamine on the renal circulation have been examined to show whether any augmentation of renal blood flow (RBF) was secondary to the effect of the drug on cardiac output (CO) or whether it had any additional direct renal vasodilator activity. Eight male patients with mild to moderate hypertension, who were undergoing renal vein catheterization for renin estimation, were studied. Dose related increments in RBF (baseline (B) = 504 ml X min-1; after treatment (D) = 605 ml X min-1), CO (B = 5.9 l X min-1; D = 6.7 l X min-1), heart rate (B = 77 beats/min; D = 100 beats/min) and systolic blood pressure (B = 143 mmHg; D = 166 mmHg) were observed on administration of dopexamine 3 micrograms X kg-1 X min-1, with insignificant changes in diastolic blood pressure (B = 84.4 mmHg; D = 90 mmHg) and total peripheral resistance (B = 17.85; D = 17.25 Units). There was a slight but significant reduction in renal vascular resistance (B = 20.59, D = 18.75). The ratio of RBF to CO (%) confirmed that the increase in RBF due to dopexamine hydrochloride was greater that attributable to the increase in CO or perfusion pressure alone (RBF/CO B = 8.5%, D = 9%), consistent with selective renal vasodilatation. The fall in renin activity and lack of systemic vasodilatation suggest that this was a DA1-receptor mediated effect.
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- 1987
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17. A percutaneous approach to cardiac haemodynamics in anaesthetised rats
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Giovanna Branzi, Nerys Roberts, Fabio Magrini, R. Meazza, and Michele M. Ciulla
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Male ,Cardiac function curve ,medicine.medical_specialty ,Physiology ,Biplane angiography ,Hemodynamics ,Blood Pressure ,Rats, Inbred WKY ,Electrocardiography ,Physiology (medical) ,Internal medicine ,Methods ,Animals ,Ventricular Function ,Medicine ,Fluoroscopy ,Histological examination ,medicine.diagnostic_test ,business.industry ,Heart ,Stroke Volume ,Percutaneous approach ,Rats ,Radiography ,Cardiac haemodynamics ,Anesthesia ,Anesthesia, Intravenous ,Left ventricular cavity ,Cardiology ,Cardiology and Cardiovascular Medicine ,business - Abstract
Established methods for evaluating cardiac function in small animals involve surgical manoeuvres. We describe a method for evaluating left ventricular volume (LVV) and pressure (LVP) in anaesthetised adult rats. Under fluoroscopic control a 23 G needle was inserted into the left ventricular cavity of anaesthetised normotensive WKY rats. LVV was determined by biplane angiography and LVP was measured directly. Surface electrocardiograms were recorded throughout the procedure. In 8 animals the study was repeated three times, one week apart. Animals were then sacrificed and tissues harvested for histological examination. In 8 rats, the technique was found to be reproducible and there was no evidence of functional (ECG) or pathological myocardial damage following repeated measurements. In conclusion this technique provides a reproducible method of measuring LVV and LVP, allowing longitudinal haemodynamic studies in anaesthetised rats.
18. Renal hemodynamic effects of dopexamine hydrochloride
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Alberto Zanchetti, Fabio Magrini, Giovanna Macchi, Richard Foulds, C. Mondadori, and Nerys Roberts
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Cardiac output ,medicine.medical_specialty ,Renal circulation ,business.industry ,Plasma renin activity ,medicine.anatomical_structure ,Blood pressure ,Internal medicine ,Renal blood flow ,Vascular resistance ,medicine ,Cardiology ,Renal vein ,Cardiology and Cardiovascular Medicine ,business ,Perfusion - Abstract
The effects of dopexamine hydrochloride on the renal circulation have been examined to discover whether augmentation of renal blood flow is secondary to the effect of the drug on cardiac output (CO) or whether there is an additional direct renal vasodilator activity. Eight male patients with mild to moderate hypertension, who were undergoing renal vein catheterization for renin estimation, were studied. Dose-related increments in renal blood flow (baseline [B] = 504 ml/min; after treatment [D] = 605 ml/min), CO (B = 5.9 liters/min; D = 6.7 liters/min), heart rate (B = 77 beats/min; D = 100 beats/min) and systolic blood pressure (B = 143 mm Hg; D = 166 mm Hg) were observed after administration of dopexamine hydrochloride (3 μg/kg/min), with insignificant changes in diastolic blood pressure (B = 84.4 mm Hg; D = 90 mm Hg) and total peripheral resistance (B = 17.85; D = 17.25 units). There was a small but significant reduction in renal vascular resistance (B = 20.59; D = 18.75 units). The ratio of renal blood flow to CO confirmed that the increase in renal blood flow due to dopexamine hydrochloride was greater than that attributable to the increase in CO or perfusion pressure alone (renal blood flow/CO B = 8.5%; D = 9%), and this is consistent with selective renal vasodilatation. The decrease in renin activity and lack of systemic vasodilatation suggest that this was a DA 1 receptor-mediated effect.
- Published
- 1988
- Full Text
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