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2. Disseminated tuberculosis presenting as bilateral neuro-retinitis

Author

Anton-Vazquez, V, Parthasarathi, P, Grimaldi, G, Dhanes, T, Rees, A, Singh, M, Macallan, D, and Arias, M

Subjects
genetic structures, eye diseases
Abstract

Disseminated tuberculosis presenting with intraocular involvement is a rare condition which can lead to profound visual loss if misdiagnosed. We report a case of a 24-year-old Nepalese male with disseminated tuberculosis who presented primarily with bilateral vision loss.

Published
2022

5. Directly measured kinetics of circulating T lymphocytes in normal and HIV-1-infected humans

Author

Hellerstein, M., Hanley, M.B., Cesar, D., Siler, S., Papageorgopoulos, C., Wieder, E., Schmidt, D., Hoh, R., Neese, R., Macallan, D., Deeks, S., and McCune, J.M.

Subjects
HIV infection -- Development and progression, T cells -- Physiological aspects
Abstract

The authors report on investigation as to the reason for depletion of T-cells in persons infected with HIV-1 virus. They attribute this occurrence to a combination of shortened survival time of the cells along with a lack of increase in T-cell production.

Published
1999

8. An observational cohort study to evaluate the clinical utilty of current and second-generation interferon-gamma release-assays in diagnostic evaluation of tuberculosis

Author

Whitworth, HS, Badhan, A, Boakye, AA, Takwoingi, Y, Rees-Roberts, M, Partlett, C, Lambie, H, Innes, J, Cooke, G, Lipman, M, Conlon, C, Macallan, D, Chua, F, Post, F, Wiselka, M, Woltmann, G, Deeks, JJ, Kon, OM, Lalvani, A, and Diagnostic Evaluation of Active TB (IDEA) Study Group

Subjects
1108 Medical Microbiology, 1103 Clinical Sciences, Microbiology
Abstract

Background The role of interferon-gamma release assays (IGRAs) in diagnosis of active tuberculosis (TB) is unclear, yet they are commonly used in low-TB-incidence countries. This study sought to resolve this clinical uncertainty by determining the diagnostic accuracy and role of current and second-generation IGRAs in the diagnostic assessment of suspected TB in a low-incidence setting. Methods This was a prospective cohort study of 1,060 adults with suspected TB, conducted in routine secondary care in England. Patients were tested for M. tuberculosis (Mtb) infection at baseline using current and second-generation IGRAs, the latter incorporating novel Mtb antigens, and followed up for 6-12m to establish definitive diagnoses. Sensitivity, specificity and positive and negative likelihood ratios (LRs) and predictive values (PVs) of the tests for TB were determined. Findings TB was diagnosed in 363 (43%) of 845 patients included in analyses. Sensitivity of T-SPOT.TB was 81.4% (95%CI 76.6-85.3%), higher than Quantiferon-Gold In-Tube at 67.3% (95%CI 62.0-72.1%). Second-generation IGRA had higher sensitivity than current tests, at 94.0% (95%CI 90.0–96.4%) for culture-confirmed TB and 89.2% (95%CI 85.2–92.2%) when including highly-probable TB, giving a negative LR for all TB of 0.13 (95%CI 0.10-0.19). Specificity ranged from 86.2% (95%CI 82.3-89.4%) for T-SPOT.TB to 80.0% (95%CI 75.6-83.8%) for second-generation IGRA. Interpretation Currently-available IGRAs lack sufficient accuracy for diagnostic evaluation of suspected TB. Second-generation tests, however, may have sufficiently high sensitivity, low negative LR and correspondingly high negative PV in low-incidence settings to facilitate prompt rule-out of TB.

Published
2018

11. Human cytomegalovirus-specific CD8(+) T-cell expansions contain long-lived cells that retain functional capacity in both young and elderly subjects

Author

Wallace, D, Masters, J, De Lara, C, Henson, S, Worth, A, Zhang, Y, Kumar, SR, Beverley, P, Akbar, A, and Macallan, D

Abstract

The immune response to human cytomegalovirus (HCMV) infection is characterized by the accumulation of HCMV-specific CD8(+) T cells, particularly in the elderly; such expansions may impair immune responses to other pathogens. We investigated mechanisms underlying HCMV-specific expansions in 12 young and 21 old healthy subjects (although not all analyses were performed on all subjects). Phenotypically, HCMV-pentamer(+) CD8(+) T cells were characterized by marked Vβ restriction, advanced differentiation (being predominantly CD27(-) CD28(-) ), and variable CD45RO/RA expression. Although more common and larger in older subjects, expansions had similar phenotypic characteristics in the young. In one old subject, repeated studies demonstrated stability in size and Vβ distribution of pentamer(+) populations over 6 years. We tested whether HCMV-specific CD8(+) T-cell expansions arose from accelerated proliferation or extended lifespan by in vivo labelling with deuterated glucose and ex vivo Ki-67 expression. Uptake of deuterated glucose was lower in pentamer(+) cells than in pentamer(-) CD8(+) CD45RO(+) or CD8(+) CD45RA(+) cells in three old subjects, consistent with reduced proliferation and extended lifespan. Similarly Ki-67 labelling showed no evidence for increased proliferation in HCMV-specific CD8(+) expansions in older subjects, although pentamer(-) CD45RA(+) cells from young donors expressed very little Ki-67. We investigated Bcl-2 and CD95 as possible anti-apoptotic mediators, but neither was associated with pentamer-positivity. To investigate whether expansion represents a compensatory response to impaired functionality, we performed two tests of functionality, peptide-stimulated proliferation and CD107 expression; both were intact in pentamer(+) cells. Our data suggest that HCMV-specific CD8(+) expansions in older subjects accumulate by extended lifespan, rather than accelerated proliferation.

Published
2011

14. Report from the second cytomegalovirus and immunosenescence workshop

Author

Wills, M, Akbar, A, Beswick, M, Bosch, JA, Caruso, C, Colonna-Romano, G, Dutta, A, Franceschi, C, Fulop, T, Gkrania-Klotsas, E, Goronzy, J, Griffiths, SJ, Henson, SM, Herndler-Brandstetter, D, Hill, A, Kern, F, Klenerman, P, Macallan, D, Macaulay, R, Maier, AB, Mason, G, Melzer, D, Morgan, M, Moss, P, Nikolich-Zugich, J, Pachnio, A, Riddell, N, Roberts, R, Sansoni, P, Sauce, D, Sinclair, J, Solana, R, Strindhall, J, Trzonkowski, P, van Lier, R, Vescovini, R, Wang, G, Westendorp, R, Pawelec, G, Wills, M, Akbar, A, Beswick, M, Bosch, JA, Caruso, C, Colonna-Romano, G, Dutta, A, Franceschi, C, Fulop, T, Gkrania-Klotsas, E, Goronzy, J, Griffiths, SJ, Henson, SM, Herndler-Brandstetter, D, Hill, A, Kern, F, Klenerman, P, Macallan, D, Macaulay, R, Maier, AB, Mason, G, Melzer, D, Morgan, M, Moss, P, Nikolich-Zugich, J, Pachnio, A, Riddell, N, Roberts, R, Sansoni, P, Sauce, D, Sinclair, J, Solana, R, Strindhall, J, Trzonkowski, P, van Lier, R, Vescovini, R, Wang, G, Westendorp, R, and Pawelec, G

Abstract

The Second International Workshop on CMV & Immunosenescence was held in Cambridge, UK, 2-4th December, 2010. The presentations covered four separate sessions: cytomegalovirus and T cell phenotypes; T cell memory frequency, inflation and immunosenescence; cytomegalovirus in aging, mortality and disease states; and the immunobiology of cytomegalovirus-specific T cells and effects of the virus on vaccination. This commentary summarizes the major findings of these presentations and references subsequently published work from the presenter laboratory where appropriate and draws together major themes that were subsequently discussed along with new areas of interest that were highlighted by this discussion.

Published
2011

15. Immunosenescence and Cytomegalovirus: where do we stand after a decade?

Author

Pawelec, G, Akbar, A, Beverley, P, Caruso, C, Derhovanessian, E, Fülöp, T, Griffiths, P, Grubeck-Loebenstein, B, Hamprecht, K, Jahn, G, Kern, F, Koch, SD, Larbi, A, Maier, AB, Macallan, D, Moss, P, Samson, S, Strindhall, J, Trannoy, E, Wills, M, Pawelec, G, Akbar, A, Beverley, P, Caruso, C, Derhovanessian, E, Fülöp, T, Griffiths, P, Grubeck-Loebenstein, B, Hamprecht, K, Jahn, G, Kern, F, Koch, SD, Larbi, A, Maier, AB, Macallan, D, Moss, P, Samson, S, Strindhall, J, Trannoy, E, and Wills, M

Published
2010

16. Immunosenescence and Cytomegalovirus:where do we stand after a decade?

Author

Pawelec, G, Akbar, A, Beverly, P, Caruso, C, Derhovanessian, E, Fülöp, T, Griffiths, P, Grubeck-Loebenstein, B, Hamprecht, K, Jahn, G, Kern, F, Koch, SD, Larbi, A, Maier, AB, Macallan, D, Moss, P, Samson, S, Strindhall, Jan, Trannoy, E, Wills, M, Pawelec, G, Akbar, A, Beverly, P, Caruso, C, Derhovanessian, E, Fülöp, T, Griffiths, P, Grubeck-Loebenstein, B, Hamprecht, K, Jahn, G, Kern, F, Koch, SD, Larbi, A, Maier, AB, Macallan, D, Moss, P, Samson, S, Strindhall, Jan, Trannoy, E, and Wills, M

Published
2010
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17. High Production Rates Sustain In Vivo Levels of PD-1high Simian Immunodeficiency Virus-Specific CD8 T Cells in the Face of Rapid Clearance

Author

Petrovas, C., primary, Yamamoto, T., additional, Price, D. A., additional, Rao, S. S., additional, Klatt, N. R., additional, Brenchley, J. M., additional, Douek, D. C., additional, Gostick, E., additional, Angermann, B. R., additional, Grossman, Z., additional, Macallan, D. C., additional, Meier-Schellersheim, M., additional, and Koup, R. A., additional

Published
2013
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25. Wasting in HIV infection and AIDS.

Author

Macallan, Derek C. and Macallan, D C

Abstract

AIDS wasting is not characterized by a single pathophysiological process but by a variety of processes that operate at different times. Acute wasting tends to be associated with secondary infections; chronic wasting is associated with gastrointestinal disease. Although resting energy expenditure is increased, total energy expenditure is reduced in individuals who are losing weight and it is usually reduced intake that commonly drives wasting. However, reduced intake is not an adequate explanation for the metabolic abnormalities that are seen in HIV infection. In particular, protein metabolism and lipid metabolism are abnormal, possibly representing inappropriate utilization of substrates. The response to nutrition may be impaired, particularly in terms of accrual of lean tissue but nutritional support may prolong survival. The impact of protease inhibitors on wasting in HIV infection is yet to be fully ascertained but despite antiviral therapy it seems that wasting is likely to remain a problem at least in some patients. [ABSTRACT FROM AUTHOR]

Published
1999
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26. Nutrition and immune function in human immunodeficiency virus infection.

Author

Macallan, D C

Abstract

The triad of human immunodeficiency virus (HIV) infection, nutritional status and immune function are intimately related, each factor having effects on the others. The dominant effect in this three-way relationship is the effect of HIV infection on nutritional status, an effect which, until the advent of potent anti-retroviral drugs, has been manifest primarily as wasting. Recently, more complex metabolic abnormalities have become apparent, particularly fat redistribution syndromes, hyperlipidaemia and hypercholesterolaemia. For the converse effect, the effect of nutritional state on HIV disease progression, there is good evidence that clinical outcome is poorer in individuals with compromised nutrition. However, the beneficial effects of nutritional support have been more difficult to demonstrate. For macronutrients, effective macronutrient supply improves survival in severely-malnourished individuals and may have beneficial effects in less-severely-affected individuals. Micronutrient deficiencies appear to be involved in modifying clinical HIV disease and may also be associated with enhanced mother-to-child transmission of virus, particularly in developing countries. Intervention trials in this setting are currently under way. In conclusion, the interaction of HIV infection and nutrition is of great importance not just because of the major impact that HIV infection has on nutritional state, but also because strategies to improve nutritional status, both quantitatively and qualitatively, may have a beneficial effect on the clinical and immunological course of the disease. [ABSTRACT FROM AUTHOR]

Published
1999
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28. SELF ASSESSMENT QUESTIONS: A Mauritian woman with fever, abdominal pain and facial palsy.

Author

Gyawali, P., Agranoff, D., and Macallan, D. C.

Subjects
FEVER, DISEASES in women, ABDOMINAL pain, NAUSEA, VOMITING, FACIAL paralysis
Abstract

This article studies the case of al 43 year old woman of Mauritian origin presented to the surgeons with abdominal pain, nausea, and vomiting occurring over a period of eight weeks. There were no respiratory symptoms. She had been exposed to tuberculosis at the age of 2 before immigrating to Great Britain. On examination she had a low grade fever and was tender in the epigastrium. She had altered sensation to light touch and pinprick in the lower thoracic and upper abdominal dermatomes. She had modestly deranged liver function tests.

Published
2001
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29. Report from the second cytomegalovirus and immunosenescence workshop

Author

Wills Mark, Akbar Arne, Beswick Mark, Bosch Jos A, Caruso Calogero, Colonna-Romano Giuseppina, Dutta Ambarish, Franceschi Claudio, Fulop Tamas, Gkrania-Klotsas Effrossyni, Goronzy Joerg, Griffiths Stephen J, Henson Sian M, Herndler-Brandstetter Dietmar, Hill Ann, Kern Florian, Klenerman Paul, Macallan Derek, Macaulay Richard, Maier Andrea B, Mason Gavin, Melzer David, Morgan Matthew, Moss Paul, Nikolich-Zugich Janko, Pachnio Annette, Riddell Natalie, Roberts Ryan, Sansoni Paolo, Sauce Delphine, Sinclair John, Solana Rafael, Strindhall Jan, Trzonkowski Piotr, van Lier Rene, Vescovini Rosanna, Wang George, Westendorp Rudi, and Pawelec Graham

Subjects
Immunologic diseases. Allergy, RC581-607, Geriatrics, RC952-954.6
Abstract

Abstract The Second International Workshop on CMV & Immunosenescence was held in Cambridge, UK, 2-4th December, 2010. The presentations covered four separate sessions: cytomegalovirus and T cell phenotypes; T cell memory frequency, inflation and immunosenescence; cytomegalovirus in aging, mortality and disease states; and the immunobiology of cytomegalovirus-specific T cells and effects of the virus on vaccination. This commentary summarizes the major findings of these presentations and references subsequently published work from the presenter laboratory where appropriate and draws together major themes that were subsequently discussed along with new areas of interest that were highlighted by this discussion.

Published
2011
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30. Immunosenescence and Cytomegalovirus: where do we stand after a decade?

Author

Pawelec Graham, Akbar Arne, Beverley Peter, Caruso Calogero, Derhovanessian Evelyna, Fülöp Tamas, Griffiths Paul, Grubeck-Loebenstein Beatrix, Hamprecht Klaus, Jahn Gerhard, Kern Florian, Koch Sven D, Larbi Anis, Maier Andrea B, Macallan Derek, Moss Paul, Samson Sandrine, Strindhall Jan, Trannoy Emanuelle, and Wills Mark

Subjects
Immunologic diseases. Allergy, RC581-607, Geriatrics, RC952-954.6
Published
2010
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31. Report from the second cytomegalovirus and immunosenescence workshop

Author

Jan Strindhall, Natalie E. Riddell, Arne N. Akbar, Graham Pawelec, George C. Wang, Mark Beswick, Gavin M. Mason, Claudio Franceschi, Tamas Fulop, René A. W. van Lier, Calogero Caruso, Delphine Sauce, Annette Pachnio, Goronzy Joerg J, Rafael Solana, Florian Kern, Piotr Trzonkowski, Andrea B. Maier, Janko Nikolich-Zugich, Mark R. Wills, Dietmar Herndler-Brandstetter, Derek C. Macallan, Ryan Roberts, Ambarish Dutta, Matthew D. Morgan, David Melzer, Giuseppina Colonna-Romano, Sian M. Henson, Jos A. Bosch, Rosanna Vescovini, Stephen J. Griffiths, John Sinclair, Paul Klenerman, Rudi G. J. Westendorp, Paolo Sansoni, Paul Moss, Ann B. Hill, Effrossyni Gkrania-Klotsas, Richard Macaulay, Department of Medicine, University of Cambridge [UK] (CAM), Division of Infection and Immunity, University College of London [London] (UCL), School of Cancer Sciences, University of Birmingham [Birmingham], College of Life and Environmental Sciences, Social and Preventive Medicine, Universität Heidelberg [Heidelberg]-Mannheim Institute of Public Health, Department of Pathobiology and Medical and Forensic Biotechnologies, Università degli studi di Palermo - University of Palermo, Epidemiology and Public Health Group, University of Exeter, Dept. Experimental Pathology, Alma Mater Studiorum Università di Bologna [Bologna] (UNIBO), Research Centre on Aging, Université de Sherbrooke (UdeS), Addenbrooke's Hospital, Cambridge University NHS Trust, Stanford School of Medicine [Stanford], Stanford Medicine, Stanford University-Stanford University, School of Immunity and Infection, Dept Microbiology and Immunology, Oregon Health and Science University [Portland] (OHSU), BSMS, University of Sussex, Nuffield Dept of Clinical Medicine, University of Oxford [Oxford]-NIHR Biomedical Research Centre, Centre for Infection, St George's, University of London, Department of Gerontology and Geriatrics, Leiden University Medical Center (LUMC), Department of Immunobiology and the Arizona Center on Aging, University of Arizona, Department of Internal Medicine and Biomedical Sciences, University of Parma = Università degli studi di Parma [Parme, Italie], Immunité et Infection, Institut National de la Santé et de la Recherche Médicale (INSERM)-IFR113-Université Pierre et Marie Curie - Paris 6 (UPMC), Instituto Maimonides de Investigación Biomédica de Cordoba (IMIBIC), Universidad de Córdoba [Cordoba]-Hospital Universitario Reina Sofía, Department of Natural Science and Biomedicine, School of Health Sciences-Jönköping University [Sweden], Department of Clinical Immunology and Transplantology, Medical University of Gdansk, Department of Experimental Immunology, Sanquin Blood Supply Foundation, Division of Geriatric Medicine and Gerontology, Johns Hopkins University School of Medicine, Department of Public Health and Primary Care, Department of Internal Medicine II, Eberhard Karls Universität Tübingen = Eberhard Karls University of Tuebingen, Wills1, M, Akbar, A, Beswick, M, Bosch, JA, Caruso, C, Colonna-Romano, G, Dutta, A, Franceschi, C, Fulop, T, Gkrania-Klotsas, E, Goronzy, G, Griffiths, SJ, Henson, SM, Herndler-Brandstetter, D, Hill, A, Kern, F, Klenerman, P, Macallan, D, Macaulay, R, Maier, AB, Mason, G, Melzer, D, Morgan, M, Moss, P, Nikolich-Zugich, J, Pachnio, A, Riddell, N, Roberts, R, Sansoni, P, Sauce, D, Sinclair, J, Solana, R, Strindhall, J, Trzonkowski, P, van Lier, R, Vescovini, R, Wang, G, Westendorp, R, Pawelec, G., University of Cambridge [UK] (CAM)-Addenbrooke's Hospital, Cancer Sciences School, Advisory Board of OA Cancer, University of Amsterdam [Amsterdam] (UvA), Department of Pathobiology and Biomedical Methodologies, University of Exeter Medical School, Centro Interdipartimentale Galvani (CIG), Semmelweis University [Budapest, Hungary], Department of Molecular Microbiology and Immunology, Brighton and Sussex Medical School (BSMS), NIHR Biomedical Research Centre [London], Guy's and St Thomas' NHS Foundation Trust-King‘s College London, Department of Immunobiology, University of Arizona-College of Medicine, Department of Internal Medicine, Centre d'Immunologie et de Maladies Infectieuses (CIMI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Immunology Unit, Instituto Maimónides de Investigación Biomédica de Córdoba (IMIBIC)-Reina Sofia University-Hospital-University of Cordoba, Health Sciences School, Jönköping University [Sweden], Medical University of Gdańsk, Experimental Immunology, Academic Medical Center - Academisch Medisch Centrum [Amsterdam] (AMC), University of Amsterdam [Amsterdam] (UvA)-University of Amsterdam [Amsterdam] (UvA), Dipartimento di Medicina Interna e Scienze Biomediche, Section for Transplantation Immunology and Immunohaematology, University Hospital Tübingen, Wills M., Akbar A., Beswick M., Bosch J.A., Caruso C., Colonna-Romano G., Dutta A., Franceschi C., Fulop T., Gkrania-Klotsas E., Goronzy J., Griffiths S.J., Henson S., Herndler-Brandstetter D., Hill A., Kern F., Klenerman P., Macallan D., Macualay R., Maier A.B., Mason G., Melzer D., Morgan M., Moss P., Nikolich-Zugich J., Pachnio A., Riddell N., Roberts R., Sansoni P., Sauce D., Sinclair J., Solana R., Strindhall J., Trzonkowski P., van Lier R., Vescovini R., Wang G., Westendorp R., Pawelec G., Neuromechanics, BMC, Ed., University of Oxford-NIHR Biomedical Research Centre, Università degli studi di Parma = University of Parma (UNIPR), Université Pierre et Marie Curie - Paris 6 (UPMC)-IFR113-Institut National de la Santé et de la Recherche Médicale (INSERM), Universidad de Córdoba = University of Córdoba [Córdoba]-Hospital Universitario Reina Sofía, Wills, Mark [0000-0001-8548-5729], Gkrania-Klotsas, Effrossyni [0000-0002-0930-8330], Sinclair, John [0000-0002-2616-9571], Apollo - University of Cambridge Repository, Universität Heidelberg [Heidelberg] = Heidelberg University-Mannheim Institute of Public Health, and Universiteit Leiden-Universiteit Leiden

Subjects
lcsh:Immunologic diseases. Allergy, Gerontology, Aging, [SDV.IMM] Life Sciences [q-bio]/Immunology, [SDV]Life Sciences [q-bio], Immunology, Congenital cytomegalovirus infection, Disease, Ageing, CMV, immunity, lcsh:Geriatrics, 0601 Biochemistry and Cell Biology, Vaccine Related, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Medicine, cytomegalovirus, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, immunosenescence, 0303 health sciences, business.industry, Geriatrics gerontology, Immunosenescence, medicine.disease, 3. Good health, lcsh:RC952-954.6, Ageing, HCMV Infection, Infectious Diseases, Commentary, [SDV.IMM]Life Sciences [q-bio]/Immunology, Immunization, lcsh:RC581-607, business, 030215 immunology
Abstract

This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.; International audience; The Second International Workshop on CMV & Immunosenescence was held in Cambridge, UK, 2-4th December, 2010. The presentations covered four separate sessions: cytomegalovirus and T cell phenotypes; T cell memory frequency, inflation and immunosenescence; cytomegalovirus in aging, mortality and disease states; and the immunobiology of cytomegalovirus-specific T cells and effects of the virus on vaccination. This commentary summarizes the major findings of these presentations and references subsequently published work from the presenter laboratory where appropriate and draws together major themes that were subsequently discussed along with new areas of interest that were highlighted by this discussion.

Published
2011

32. Immunosenescence and Cytomegalovirus

Author

Beatrix Grubeck-Loebenstein, Tamas Fulop, Derek C. Macallan, Arne N. Akbar, Jan Strindhall, Sven D. Koch, Paul Moss, Gerhard Jahn, Calogero Caruso, Emanuelle Trannoy, Evelyna Derhovanessian, Peter C. L. Beverley, Andrea B. Maier, Graham Pawelec, Mark R. Wills, Klaus Hamprecht, Paul D. Griffiths, Florian Kern, Anis Larbi, Sandrine I. Samson, Neuromechanics, AMS - Ageing and Morbidity, Wills, Mark [0000-0001-8548-5729], Apollo - University of Cambridge Repository, Pawelec, G, Akbar,A, Beverley,P, Caruso, C, Derhovanessian, E, Fülöp, T, Griffiths, P, Grubeck-Loebenstein, B, Hamprecht,K, Jahn, G, Kern,F, Koch, SD, Larbi,A, Maier, AB, Macallan,D, Moss,P, Samson, S, Strindhall, J, Trannoy, E, and Wills, M.

Subjects
lcsh:Immunologic diseases. Allergy, Aging, CMV, Immunosenescence,ageing, T cell, Immunology, Congenital cytomegalovirus infection, Yellow fever vaccine, 32 Biomedical and Clinical Sciences, lcsh:Geriatrics, Virus, Immune system, Medicine, 3202 Clinical Sciences, biology, business.industry, virus diseases, Immunosenescence, Biological Sciences, medicine.disease, 3204 Immunology, lcsh:RC952-954.6, Ageing, medicine.anatomical_structure, T cell subset, QR180, biology.protein, Commentary, Antibody, lcsh:RC581-607, business, medicine.drug
Abstract

Since Looney at al. published their seminal paper a decade ago [1] it has become clear that many of the differences in T cell immunological parameters observed between young and old people are related to the age-associated increasing prevalence of infection with the persistent β-herpesvirus HHV-5 (Cytomegalovirus). Ten years later, studies suggest that hallmark age-associated changes in peripheral blood T cell subset distribution may not occur at all in people who are not infected with this virus [[2]; Derhovanessian et al., in press]. Whether the observed changes are actually caused by CMV is an open question, but very similar, rapid changes observed in uninfected patients receiving CMV-infected kidney grafts are consistent with a causative role [3]. This meeting intensively discussed these and other questions related to the impact of CMV on human immune status and its relevance for immune function in later life.

Published
2010

33. Chromoblastomycosis Treated With Posaconazole and Adjunctive Imiquimod: Lending Innate Immunity a Helping Hand.

Author

Logan C, Singh M, Fox N, Brown G, Krishna S, Gordon K, Macallan D, and Bicanic T

Abstract

Chromoblastomycosis (CBM) is a difficult-to-treat, chronic fungal infection of the skin and subcutaneous tissue. The evidence base for treatment is scarce, with no standardized therapeutic approach. Chronicity of CBM infection is postulated to be due in part to a failure of host cell-mediated immunity to generate a proinflammatory response sufficient for fungal clearance. We present a case of a chronic chromoblastomycosis lesion of the hand present for nearly 4 decades, previously refractory to itraconazole monotherapy, that was successfully treated with a combination of posaconazole and adjunctive immunotherapy with topical imiquimod, a Toll-like receptor 7 agonist. Serial biopsies and images demonstrate the clinical and histopathological improvement of the lesion. Randomized trials of antifungal therapy with adjunctive imiquimod are warranted to determine whether a combination of antifungal and host-directed therapy improves outcomes for this neglected tropical mycosis., Competing Interests: Potential conflicts of interest. C.L. has received conference sponsorship from Gilead Sciences. T.B. reports research funding support from Gilead Sciences, Pfizer, and Merck Sharp & Dohme, advisory board fees from Gilead Sciences, and speaker fees from Gilead Sciences and Pfizer. M.S., N.F., G.B., S.K., K.G., and D.M. have nothing to declare. All other authors report no potential conflicts., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published
2023
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34. Redefining WILD syndrome: a primary lymphatic dysplasia with congenital multisegmental lymphoedema, cutaneous lymphovascular malformation, CD4 lymphopaenia and warts.

Author

Mansour S, Josephs KS, Ostergaard P, Gordon K, Van Zanten M, Pearce J, Jeffery S, Keeley V, Riches K, Kreuter A, Wieland U, Hägerling R, Ratnam L, Sackey E, Grigoriadis D, Ho B, Smith F, Rauter E, Mortimer P, and Macallan D

Subjects
Humans, Warts diagnosis, Warts genetics, Lymphedema diagnosis, Lymphedema genetics, Immunologic Deficiency Syndromes
Abstract

Background: Primary lymphoedema (PL) syndromes are increasingly recognised as presentations of complex genetic disease, with at least 20 identified causative genes. Recognition of clinical patterns is key to diagnosis, research and therapeutics. The defining criteria for one such clinical syndrome, 'WILD syndrome' ( W arts, I mmunodeficiency, L ymphoedema and anogenital D ysplasia), have previously depended on a single case report., Methods and Results: We present 21 patients (including the first described case) with similar clinical and immunological phenotypes. All had PL affecting multiple segments, with systemic involvement (intestinal lymphangiectasia/pleural or pericardial effusions) in 70% (n=14/20). Most (n=20, 95%) had a distinctive cutaneous lymphovascular malformation on the upper anterior chest wall. Some (n=10, 48%) also had hyperpigmented lesions resembling epidermal naevi (but probably lymphatic in origin). Warts were common (n=17, 81%) and often refractory. In contrast to the previous case report, anogenital dysplasia was uncommon-only found in two further cases (total n=3, 14%). Low CD4 counts and CD4:CD8 ratios typified the syndrome (17 of 19, 89%), but monocyte counts were universally normal, unlike GATA2 deficiency., Conclusion: WILD syndrome is a previously unrecognised, underdiagnosed generalised PL syndrome. Based on this case series, we redefine WILD as ' W arts, I mmunodeficiency, and L ymphatic D ysplasia' and suggest specific diagnostic criteria. The essential criterion is congenital multisegmental PL in a 'mosaic' distribution. The major diagnostic features are recurrent warts, cutaneous lymphovascular malformations, systemic involvement (lymphatic dysplasia), genital swelling and CD4 lymphopaenia with normal monocyte counts. The absence of family history suggests a sporadic condition, and the random distribution of swelling implicates mosaic postzygotic mutation as the cause., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2023. Re-use permitted under CC BY. Published by BMJ.)

Published
2023
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35. Images of the month: Cavernous sinus venous thrombosis secondary to Streptococcus milleri maxillary sinusitis: An unusual cause of diplopia and headache.

Author

Anton-Vazquez V, Dru R, Rich P, Arias M, and Macallan D

Subjects
Diplopia, Headache, Humans, Male, Middle Aged, Streptococcus milleri Group, Cavernous Sinus, Maxillary Sinusitis diagnosis, Maxillary Sinusitis diagnostic imaging, Venous Thrombosis diagnostic imaging, Venous Thrombosis etiology
Abstract

Cavernous sinus venous thrombosis is an uncommon condition associated with high mortality rates if not recognised early. Symptoms include headache, visual loss, ophthalmoplegia, altered consciousness, proptosis and periorbital oedema. High-quality imaging is critical in early diagnosis and successful management. Primary infection (such as sinusitis) and possible complications (including meningitis) should be considered as potential aetiologies of cavernous sinus venous thrombosis, especially in those with a preceding history of localised infection. We present a case of a 50-year-old man with a bilateral cavernous sinus venous thrombosis with associated meningitis caused by Streptococcus milleri , secondary to maxillary sinusitis and otomastoiditis. He was successfully treated with antimicrobial treatment, surgical drainage and anticoagulation., (© Royal College of Physicians 2020. All rights reserved.)

Published
2020
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36. The Rules of Human T Cell Fate in vivo .

Author

Costa Del Amo P, Debebe B, Razavi-Mohseni M, Nakaoka S, Worth A, Wallace D, Beverley P, Macallan D, and Asquith B

Subjects
Cell Death immunology, Cell Differentiation immunology, Cell Division immunology, Humans, Models, Theoretical, T-Lymphocytes immunology
Abstract

The processes governing lymphocyte fate (division, differentiation, and death), are typically assumed to be independent of cell age. This assumption has been challenged by a series of elegant studies which clearly show that, for murine cells in vitro , lymphocyte fate is age-dependent and that younger cells (i.e., cells which have recently divided) are less likely to divide or die. Here we investigate whether the same rules determine human T cell fate in vivo . We combined data from in vivo stable isotope labeling in healthy humans with stochastic, agent-based mathematical modeling. We show firstly that the choice of model paradigm has a large impact on parameter estimates obtained using stable isotope labeling i.e., different models fitted to the same data can yield very different estimates of T cell lifespan. Secondly, we found no evidence in humans in vivo to support the model in which younger T cells are less likely to divide or die. This age-dependent model never provided the best description of isotope labeling; this was true for naïve and memory, CD4 + and CD8 + T cells. Furthermore, this age-dependent model also failed to predict an independent data set in which the link between division and death was explored using Annexin V and deuterated glucose. In contrast, the age-independent model provided the best description of both naïve and memory T cell dynamics and was also able to predict the independent dataset., (Copyright © 2020 Costa del Amo, Debebe, Razavi-Mohseni, Nakaoka, Worth, Wallace, Beverley, Macallan and Asquith.)

Published
2020
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37. Diagnostic challenges in Mycobacteria chimaera infection.

Author

Hall H, Cosgrove C, Houston A, Macallan DC, and Aul R

Subjects
Adult, Anti-Bacterial Agents therapeutic use, Female, Humans, Mycobacterium avium-intracellulare Infection drug therapy, Surgical Equipment microbiology, Surgical Wound Infection epidemiology, Cardiopulmonary Bypass adverse effects, Equipment Contamination, Mycobacterium avium Complex isolation & purification, Mycobacterium avium-intracellulare Infection diagnosis
Published
2018
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38. Human TSCM cell dynamics in vivo are compatible with long-lived immunological memory and stemness.

Author

Costa Del Amo P, Lahoz-Beneytez J, Boelen L, Ahmed R, Miners KL, Zhang Y, Roger L, Jones RE, Marraco SAF, Speiser DE, Baird DM, Price DA, Ladell K, Macallan D, and Asquith B

Subjects
Adult, Aged, 80 and over, CD4-Positive T-Lymphocytes cytology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes cytology, CD8-Positive T-Lymphocytes immunology, Humans, Kinetics, Mathematical Concepts, Middle Aged, Models, Immunological, T-Lymphocyte Subsets cytology, Telomere Homeostasis immunology, Yellow fever virus immunology, Cell Self Renewal immunology, Immunologic Memory, T-Lymphocyte Subsets immunology
Abstract

Adaptive immunity relies on the generation and maintenance of memory T cells to provide protection against repeated antigen exposure. It has been hypothesised that a self-renewing population of T cells, named stem cell-like memory T (TSCM) cells, are responsible for maintaining memory. However, it is not clear if the dynamics of TSCM cells in vivo are compatible with this hypothesis. To address this issue, we investigated the dynamics of TSCM cells under physiological conditions in humans in vivo using a multidisciplinary approach that combines mathematical modelling, stable isotope labelling, telomere length analysis, and cross-sectional data from vaccine recipients. We show that, unexpectedly, the average longevity of a TSCM clone is very short (half-life < 1 year, degree of self-renewal = 430 days): far too short to constitute a stem cell population. However, we also find that the TSCM population is comprised of at least 2 kinetically distinct subpopulations that turn over at different rates. Whilst one subpopulation is rapidly replaced (half-life = 5 months) and explains the rapid average turnover of the bulk TSCM population, the half-life of the other TSCM subpopulation is approximately 9 years, consistent with the longevity of the recall response. We also show that this latter population exhibited a high degree of self-renewal, with a cell residing without dying or differentiating for 15% of our lifetime. Finally, although small, the population was not subject to excessive stochasticity. We conclude that the majority of TSCM cells are not stem cell-like but that there is a subpopulation of TSCM cells whose dynamics are compatible with their putative role in the maintenance of T cell memory., Competing Interests: The authors have declared that no competing interests exist.

Published
2018
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39. The fate and lifespan of human monocyte subsets in steady state and systemic inflammation.

Author

Patel AA, Zhang Y, Fullerton JN, Boelen L, Rongvaux A, Maini AA, Bigley V, Flavell RA, Gilroy DW, Asquith B, Macallan D, and Yona S

Subjects
Animals, Cell Survival immunology, Cells, Cultured, Deuterium metabolism, Endotoxemia blood, Endotoxemia immunology, Flow Cytometry, Homeostasis immunology, Humans, Inflammation blood, Isotope Labeling methods, Mice, Time Factors, Bone Marrow Cells immunology, Cell Differentiation immunology, Inflammation immunology, Monocytes immunology
Abstract

In humans, the monocyte pool comprises three subsets (classical, intermediate, and nonclassical) that circulate in dynamic equilibrium. The kinetics underlying their generation, differentiation, and disappearance are critical to understanding both steady-state homeostasis and inflammatory responses. Here, using human in vivo deuterium labeling, we demonstrate that classical monocytes emerge first from marrow, after a postmitotic interval of 1.6 d, and circulate for a day. Subsequent labeling of intermediate and nonclassical monocytes is consistent with a model of sequential transition. Intermediate and nonclassical monocytes have longer circulating lifespans (∼4 and ∼7 d, respectively). In a human experimental endotoxemia model, a transient but profound monocytopenia was observed; restoration of circulating monocytes was achieved by the early release of classical monocytes from bone marrow. The sequence of repopulation recapitulated the order of maturation in healthy homeostasis. This developmental relationship between monocyte subsets was verified by fate mapping grafted human classical monocytes into humanized mice, which were able to differentiate sequentially into intermediate and nonclassical cells., (© 2017 Patel et al.)

Published
2017
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40. Physiologically Based Simulations of Deuterated Glucose for Quantifying Cell Turnover in Humans.

Author

Lahoz-Beneytez J, Schaller S, Macallan D, Eissing T, Niederalt C, and Asquith B

Abstract

In vivo [6,6- 2 H 2 ]-glucose labeling is a state-of-the-art technique for quantifying cell proliferation and cell disappearance in humans. However, there are discrepancies between estimates of T cell proliferation reported in short (1-day) versus long (7-day) 2 H 2 -glucose studies and very-long (9-week) 2 H 2 O studies. It has been suggested that these discrepancies arise from underestimation of true glucose exposure from intermittent blood sampling in the 1-day study. Label availability in glucose studies is normally approximated by a "square pulse" (Sq pulse). Since the body glucose pool is small and turns over rapidly, the availability of labeled glucose can be subject to large fluctuations and the Sq pulse approximation may be very inaccurate. Here, we model the pharmacokinetics of exogenous labeled glucose using a physiologically based pharmacokinetic (PBPK) model to assess the impact of a more complete description of label availability as a function of time on estimates of CD4+ and CD8+ T cell proliferation and disappearance. The model enabled us to predict the exposure to labeled glucose during the fasting and de-labeling phases, to capture the fluctuations of labeled glucose availability caused by the intake of food or high-glucose beverages, and to recalculate the proliferation and death rates of immune cells. The PBPK model was used to reanalyze experimental data from three previously published studies using different labeling protocols. Although using the PBPK enrichment profile decreased the 1-day proliferation estimates by about 4 and 7% for CD4 and CD8+ T cells, respectively, differences with the 7-day and 9-week studies remained significant. We conclude that the approximations underlying the "square pulse" approach-recently suggested as the most plausible hypothesis-only explain a component of the discrepancy in published T cell proliferation rate estimates.

Published
2017
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41. Human neutrophil kinetics: modeling of stable isotope labeling data supports short blood neutrophil half-lives.

Author

Lahoz-Beneytez J, Elemans M, Zhang Y, Ahmed R, Salam A, Block M, Niederalt C, Asquith B, and Macallan D

Subjects
Adult, Deuterium chemistry, Female, Glucose chemistry, Glucose metabolism, Glucose pharmacology, Granulocyte Precursor Cells cytology, Half-Life, Humans, Isotope Labeling methods, Kinetics, Male, Middle Aged, Neutrophils cytology, Granulocyte Precursor Cells metabolism, Models, Biological, Neutrophils metabolism
Abstract

Human neutrophils have traditionally been thought to have a short half-life in blood; estimates vary from 4 to 18 hours. This dogma was recently challenged by stable isotope labeling studies with heavy water, which yielded estimates in excess of 3 days. To investigate this disparity, we generated new stable isotope labeling data in healthy adult subjects using both heavy water (n = 4) and deuterium-labeled glucose (n = 9), a compound with more rapid labeling kinetics. To interpret results, we developed a novel mechanistic model and applied it to previously published (n = 5) and newly generated data. We initially constrained the ratio of the blood neutrophil pool to the marrow precursor pool (ratio = 0.26; from published values). Analysis of heavy water data sets yielded turnover rates consistent with a short blood half-life, but parameters, particularly marrow transit time, were poorly defined. Analysis of glucose-labeling data yielded more precise estimates of half-life (0.79 ± 0.25 days; 19 hours) and marrow transit time (5.80 ± 0.42 days). Substitution of this marrow transit time in the heavy water analysis gave a better-defined blood half-life of 0.77 ± 0.14 days (18.5 hours), close to glucose-derived values. Allowing the ratio of blood neutrophils to mitotic neutrophil precursors (R) to vary yielded a best-fit value of 0.19. Reanalysis of the previously published model and data also revealed the origin of their long estimates for neutrophil half-life: an implicit assumption that R is very large, which is physiologically untenable. We conclude that stable isotope labeling in healthy humans is consistent with a blood neutrophil half-life of less than 1 day., (© 2016 by The American Society of Hematology.)

Published
2016
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42. Accelerated in vivo proliferation of memory phenotype CD4+ T-cells in human HIV-1 infection irrespective of viral chemokine co-receptor tropism.

Author

Zhang Y, de Lara C, Worth A, Hegedus A, Laamanen K, Beverley P, and Macallan D

Subjects
Adult, CD4 Lymphocyte Count, CD4-Positive T-Lymphocytes metabolism, Cell Proliferation, Female, HIV Infections virology, Humans, Leukocyte Common Antigens metabolism, Male, Viral Tropism, Young Adult, CD4-Positive T-Lymphocytes immunology, HIV Infections immunology, HIV-1 immunology, Immunologic Memory, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism
Abstract

CD4(+) T-cell loss is the hallmark of HIV-1 infection. CD4 counts fall more rapidly in advanced disease when CCR5-tropic viral strains tend to be replaced by X4-tropic viruses. We hypothesized: (i) that the early dominance of CCR5-tropic viruses results from faster turnover rates of CCR5(+) cells, and (ii) that X4-tropic strains exert greater pathogenicity by preferentially increasing turnover rates within the CXCR4(+) compartment. To test these hypotheses we measured in vivo turnover rates of CD4(+) T-cell subpopulations sorted by chemokine receptor expression, using in vivo deuterium-glucose labeling. Deuterium enrichment was modeled to derive in vivo proliferation (p) and disappearance (d*) rates which were related to viral tropism data. 13 healthy controls and 13 treatment-naive HIV-1-infected subjects (CD4 143-569 cells/ul) participated. CCR5-expression defined a CD4(+) subpopulation of predominantly CD45R0(+) memory cells with accelerated in vivo proliferation (p = 2.50 vs 1.60%/d, CCR5(+) vs CCR5(-); healthy controls; P<0.01). Conversely, CXCR4 expression defined CD4(+) T-cells (predominantly CD45RA(+) naive cells) with low turnover rates. The dominant effect of HIV infection was accelerated turnover of CCR5(+)CD45R0(+)CD4(+) memory T-cells (p = 5.16 vs 2.50%/d, HIV vs controls; P<0.05), naïve cells being relatively unaffected. Similar patterns were observed whether the dominant circulating HIV-1 strain was R5-tropic (n = 9) or X4-tropic (n = 4). Although numbers were small, X4-tropic viruses did not appear to specifically drive turnover of CXCR4-expressing cells (p = 0.54 vs 0.72 vs 0.44%/d in control, R5-tropic, and X4-tropic groups respectively). Our data are most consistent with models in which CD4(+) T-cell loss is primarily driven by non-specific immune activation.

Published
2013
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43. Severe Guillain-Barré syndrome following primary infection with varicella zoster virus in an adult.

Author

Cresswell F, Eadie J, Longley N, and Macallan D

Subjects
Adult, Chickenpox diagnosis, Chickenpox virology, Guillain-Barre Syndrome drug therapy, Guillain-Barre Syndrome virology, Humans, Male, Chickenpox complications, Guillain-Barre Syndrome etiology, Herpesvirus 3, Human
Abstract

Varicella zoster virus (VZV) infection may trigger Guillain-Barré syndrome (GBS), but this is rare and almost always in the context of reactivation disease from latent VZV, 'shingles'. We report here a case of severe GBS following primary VZV infection in an adult. A 40-year-old man of Indian origin developed features of GBS including quadriplegia, bulbar paralysis, and bilateral facial nerve palsies 14 days after primary VZV infection contracted from a known case in a family member. Nerve conduction studies confirmed acute inflammatory demyelinating polyneuropathy. Anti-ganglioside antibodies were negative. The mechanism of Schwann cell attack following VZV infection is poorly understood but this case suggests that primary VZV infection may be a sufficient stimulus to drive antibody generation and precipitate severe clinical symptomatology. The morbidity associated with the complications of VZV infection in adulthood could be avoided if patients who are seronegative for VZV (frequently from the Asian subcontinent) are offered prophylaxis after an exposure in adulthood., (Copyright 2009 International Society for Infectious Diseases. Published by Elsevier Ltd. All rights reserved.)

Published
2010
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44. Pharmacokinetic interactions between efavirenz and rifampicin in the treatment of HIV and tuberculosis: one size does not fit all.

Author

Brennan-Benson P, Lyus R, Harrison T, Pakianathan M, and Macallan D

Subjects
AIDS-Related Opportunistic Infections complications, Adult, Aged, Alkynes, Anti-HIV Agents administration & dosage, Anti-HIV Agents adverse effects, Antibiotics, Antitubercular administration & dosage, Antibiotics, Antitubercular adverse effects, Benzoxazines, Cyclopropanes, Drug Interactions, Drug Therapy, Combination, Female, Humans, Male, Middle Aged, Oxazines administration & dosage, Oxazines adverse effects, Rifampin administration & dosage, Rifampin adverse effects, Tuberculosis complications, AIDS-Related Opportunistic Infections drug therapy, Anti-HIV Agents pharmacokinetics, Antibiotics, Antitubercular pharmacokinetics, Oxazines pharmacokinetics, Rifampin pharmacokinetics, Tuberculosis drug therapy
Abstract

The concomitant treatment of HIV-tuberculosis co-infection is complicated by pharmacological interactions between drugs, resulting in unpredictable drug levels. We monitored efavirenz levels in all tuberculosis-HIV-treated patients over 2 years. Using 800 mg/day of efavirenz, high levels and toxicity were detected in seven out of nine patients, necessitating reduction or discontinuation. Polymorphisms in cytochrome P450 2B6 may account for this. Therapeutic drug monitoring, dose reduction or a lower starting dose may be appropriate in some patients to abrogate toxicity.

Published
2005
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45. Wasting and obesity in HIV outpatients.

Author

Hodgson LM, Ghattas H, Pritchitt H, Schwenk A, Payne L, and Macallan DC

Subjects
Adult, Antiretroviral Therapy, Highly Active adverse effects, Body Mass Index, Female, HIV Infections drug therapy, Humans, Male, Prevalence, United Kingdom epidemiology, HIV Infections complications, HIV Wasting Syndrome epidemiology, Obesity epidemiology, Outpatients
Published
2001
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46. Short-term growth hormone administration at the time of opportunistic infections in HIV-positive patients.

Author

Paton NI, Newton PJ, Sharpstone DR, Ross HM, Cotton J, Calder AG, Milne E, Elia M, Shah S, Engrand P, Macallan DC, Gazzard BG, and Griffin GE

Subjects
AIDS-Related Opportunistic Infections metabolism, Adult, Body Composition, Double-Blind Method, Growth Hormone administration & dosage, HIV Wasting Syndrome complications, HIV Wasting Syndrome metabolism, Hand Strength, Human Growth Hormone, Humans, Male, Proteins metabolism, Quality of Life, Treatment Outcome, AIDS-Related Opportunistic Infections complications, Growth Hormone adverse effects, Growth Hormone therapeutic use, HIV Wasting Syndrome drug therapy
Abstract

Objectives: A 12-week course of recombinant human growth hormone is an effective but expensive therapy for established HIV-related wasting. Wasting in HIV disease is often episodic, coinciding with bouts of acute opportunistic infection. We hypothesized that a short course of growth hormone, targeted at the time of opportunistic infection, might improve protein metabolism thereby reducing lean tissue loss., Methods: HIV-infected men with acute opportunistic infections, who received standard antimicrobial treatment for their infection as well as intensive nutritional counselling and oral energy supplements, were randomized to receive growth hormone or placebo for 14 days. Principal assessments were protein metabolism (measured by 13C-leucine infusion), body composition (measured by DEXA) and safety., Results: There were no significant changes in outcome parameters in the placebo group (n = 11). In the growth hormone group (n = 9), protein catabolic rate decreased by 60% in the fasted state (P = 0.02 versus placebo), lean body mass increased by 2.2 kg (P = 0.03 versus baseline) and fat mass decreased by 0.7 kg (P = 0.002 versus baseline). There was no increase in adverse or serious adverse events in the growth hormone as compared with the placebo group., Conclusions: A two-week course of growth hormone at the time of acute opportunistic infection in HIV-infected patients improves protein metabolism and body composition during therapy and appears to be safe. This may represent a rational and economical approach to the use of growth hormone therapy.

Published
1999
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48. Measurement of cell proliferation by labeling of DNA with stable isotope-labeled glucose: studies in vitro, in animals, and in humans.

Author

Macallan DC, Fullerton CA, Neese RA, Haddock K, Park SS, and Hellerstein MK

Subjects
Animals, Cell Division, DNA biosynthesis, Glucose, Humans, Isotope Labeling, Radioisotopes, Cytological Techniques, DNA analysis, DNA Replication
Abstract

A method for measuring DNA synthesis and, thus, cell proliferation, in vivo is presented. The technique consists of administering [6,6-2H2]Glc or [U-13C]Glc, isolating genomic DNA, hydrolyzing enzymatically to free deoxyribonucleosides, and derivatizing for GC-MS analysis of dA or dG isotopic enrichments, or both. Comparison of dA or dG to extracellular Glc enrichment (with a correction for intracellular dilution) reveals the fraction of newly synthesized DNA, by application of the precursor-product relationship. Thus, the technique differs from the widely used [3H]thymidine or BrdUrd techniques in that the de novo nucleotide synthesis pathway, rather than the nucleoside salvage pathway, is used to label DNA; the deoxyribose rather than the base moiety is labeled; purine rather than pyrimidine deoxyribonucleosides are analyzed; and stable isotopes rather than radioisotopes are used. The method is applied here in vitro to the growth of HepG2 and H9 cells in culture; in animals to proliferation of intestinal epithelium, thymus, and liver; and in humans to granulocyte turnover in blood. In all instances, measured cell proliferation kinetics were consistent with expected or independently measured kinetics. The method has several advantages over previously available techniques for measuring cell turnover, involves no radioactivity or potentially toxic metabolites, and is suitable for use in humans. The availability of a reliable and safe method for measuring cell proliferation in humans opens up a number of fundamental questions to direct experimental testing, including basic problems related to cancer, AIDS, and other pathologic states.

Published
1998
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49. Longitudinal changes in body composition measured with a variety of methods in patients with AIDS.

Author

Paton NI, Macallan DC, Jebb SA, Noble C, Baldwin C, Pazianas M, and Griffin GE

Subjects
Absorptiometry, Photon, Adult, Body Water metabolism, Electric Impedance, Humans, Longitudinal Studies, Male, Prospective Studies, Regression Analysis, Skinfold Thickness, Weight Loss physiology, Acquired Immunodeficiency Syndrome metabolism, Body Composition, HIV Wasting Syndrome metabolism
Abstract

We test the hypothesis that human immunodeficiency virus (HIV)-related weight loss is accompanied by inappropriately large losses of fat-free mass (FFM). Our secondary aims were to examine whether FFM increases during weight gain and to compare several techniques for measuring FFM change. FFM was measured at intervals averaging 5 months in 21 AIDS patients by means of skinfold thickness (SF), dual-energy x-ray absorptiometry (DEXA), total body water (TBW), and bioelectrical impedance using the equation of the manufacturer of the equipment (BIA(EZComp)) and a published prediction equation (BIA(Segal)). The FFM content of weight loss was similar for SF (57%), DEXA (60%), TBW (55%) and BIA(EZComp) (65%), but the result from BIA(Segal) (78%) was higher. The results were close to predicted starvation values apart from the results with BIA(Segal), which were significantly higher than predicted values. Weight gain was also composed of a large proportion of FFM. There were large intermethod differences in measurements of absolute FFM, but for measuring changes in FFM, the bias between SF, DEXA, and TBW was minimal. The results of BIA vary with the prediction equation used. In this group of patients with the acquired immune deficiency syndrome (AIDS), weight loss was composed of a large proportion of FFM, but in general this is compatible with undernutrition as the underlying cause and does not support the hypothesis of excessive FFM catabolism in HIV disease. SF, DEXA, TBW, and BIA(Segal) show reasonable agreement for measuring body composition changes. This information should be considered in the design of future intervention studies for HIV-related wasting.

Published
1997
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50. Lyme arthritis in southern England.

Author

Macallan DC, Hughes CA, and Bradlow A

Subjects
Female, Humans, Insect Bites and Stings complications, Lyme Disease drug therapy, Middle Aged, Penicillin V therapeutic use, Arthritis etiology, Lyme Disease complications
Published
1987
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