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3. Capturing the Value of Vaccination within Health Technology Assessment and Health Economics—Practical Considerations for Expanding Valuation by Including Key Concepts.

Author

Biundo, Eliana, Dronova, Mariia, Chicoye, Annie, Cookson, Richard, Devlin, Nancy, Doherty, T. Mark, Garcia, Stephanie, Garcia-Ruiz, Antonio J., Garrison, Louis P., Nolan, Terry, Postma, Maarten, Salisbury, David, Shah, Hiral, Sheikh, Shazia, Smith, Richard, Toumi, Mondher, Wasem, Jurgen, and Beck, Ekkehard

Subjects
MENINGOCOCCAL vaccines, ROTAVIRUS vaccines, HEALTH equity, MACROECONOMIC models, VALUE capture
Abstract

Following the development of a value of vaccination (VoV) framework for health technology assessment/cost-effectiveness analysis (HTA/CEA), and identification of three vaccination benefits for near-term inclusion in HTA/CEA, this final paper provides decision makers with methods and examples to consider benefits of health systems strengthening (HSS), equity, and macroeconomic gains. Expert working groups, targeted literature reviews, and case studies were used. Opportunity cost methods were applied for HSS benefits of rotavirus vaccination. Vaccination, with HSS benefits included, reduced the incremental cost-effectiveness ratio (ICER) by 1.4–50.5% (to GBP 11,552–GBP 23,016) depending on alternative conditions considered. Distributional CEA was applied for health equity benefits of meningococcal vaccination. Nearly 80% of prevented cases were among the three most deprived groups. Vaccination, with equity benefits included, reduced the ICER by 22–56% (to GBP 7014–GBP 12,460), depending on equity parameters. Macroeconomic models may inform HTA deliberative processes (e.g., disease impact on the labour force and the wider economy), or macroeconomic outcomes may be assessed for individuals in CEAs (e.g., impact on non-health consumption, leisure time, and income). These case studies show how to assess broader vaccination benefits in current HTA/CEA, providing decision makers with more accurate and complete VoV assessments. More work is needed to refine inputs and methods, especially for macroeconomic gains. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Healthy ageing: Herpes zoster infection and the role of zoster vaccination.

Author

Curran, Desmond, Doherty, T. Mark, Lecrenier, Nicolas, and Breuer, Thomas

Subjects
HERPES zoster, QUALITY of life, ACTIVE aging, OLDER people, HERPES zoster vaccines
Abstract

Populations are ageing worldwide, with considerable time lived in ill-health, putting upwards pressure on healthcare budgets. Healthy ageing is defined as maintaining functional ability, including the ability to: meet basic needs; learn, grow and make decisions; be mobile; build and maintain relationships; and contribute to society. The risk and impact of infectious diseases increase with age due to immunosenescence. Vaccination can help to prevent disease in older adults, promoting healthy ageing and active lives. Herpes zoster (HZ) occurs when the varicella zoster virus is reactivated due to declining immunity. HZ is common, with a lifetime risk of one-third, and increases in incidence with age. HZ is associated with severe and intense pain, substantially affecting the functional status of patients as well as their overall health-related quality of life. HZ and its complications may result in prolonged morbidity, including persistent pain (post-herpetic neuralgia, PHN), hearing impairment, vision loss and increased risk of stroke and myocardial infarction. HZ and PHN are difficult to treat, substantiating the benefits of prevention. Vaccines to prevent HZ include a recombinant zoster vaccine (RZV). RZV has shown efficacy against the HZ burden of disease and HZ burden of interference on activities of daily living of over 90% in immunocompetent adults aged ≥50 years. Vaccine efficacy against HZ was maintained at over 70% at 10 years post-vaccination. Adult vaccination, including against HZ, has the potential to reduce burden of disease, thus helping to maintain functioning and quality of life to support healthy ageing in older adults. [ABSTRACT FROM AUTHOR]

Published
2023
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13. Maintaining a 'fit' immune system: the role of vaccines.

Author

Laupèze, Béatrice and Doherty, T. Mark

Subjects
IMMUNE system, COVID-19 pandemic, INFECTION prevention, VACCINES, DISEASE susceptibility
Abstract

Conventionally, vaccines are thought to induce a specific immune response directed against a target pathogen. Long recognized but poorly understood nonspecific benefits of vaccination, such as reduced susceptibility to unrelated diseases or cancer, are now being investigated and may be due in part to "trained immunity'. We discuss 'trained immunity' and whether vaccine-induced 'trained immunity' could be leveraged to prevent morbidity due to a broader range of causes. The prevention of infection i.e. maintaining homeostasis by preventing the primary infection and resulting secondary illnesses, is the pivotal strategy used to direct vaccine design and may have long-term, positive impacts on health at all ages. In the future, we anticipate that vaccine design will change to not only prevent the target infection (or related infections) but to generate positive modifications to the immune response that could prevent a wider range of infections and potentially reduce the impact of immunological changes associated with aging. Despite changing demographics, adult vaccination has not always been prioritized. However, the SARS-CoV-2 pandemic has demonstrated that adult vaccination can flourish given the right circumstances, demonstrating that harnessing the potential benefits of life-course vaccination is achievable for all. [ABSTRACT FROM AUTHOR]

Published
2023
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18. Resistance to Murine Acquired Immunodeficiency Syndrome (MAIDS)

Author

Gilmore, Gary L., Morawetz, Renate A., Doherty, T. Mark, Giese, Nathalia A., Hartley, Janet W., Müller, Werner, Kühn, Ralf, Rajewsky, Klaus, Coffman, Robert, Morse, Herbert C., Kanagawa, Osami, Vaupel, Barbara A., Gayama, Shinyo, Koehler, Georges, and Kipf, Manfred

Published
1994

19. Lifting non-pharmaceutical interventions following the COVID-19 pandemic – the quiet before the storm?

Author

Oh, Kyu-Bin, Doherty, T. Mark, Vetter, Volker, and Bonanni, Paolo

Subjects
COVID-19 pandemic, INFLUENZA, COMMUNICABLE diseases, SARS-CoV-2, TRAVEL restrictions
Abstract

In the first months of the novel coronavirus (COVID-19) pandemic that begun in 2020, non-pharmaceutical interventions (NPIs) have been adopted worldwide. However, the effects of NPI implementation go beyond slowing the spread of COVID-19. Here, we review the non-intended effects that may have arisen from prolonged application of NPIs. NPIs also affected the epidemiology of other infectious diseases, with unprecedentedly low circulation of several respiratory and gastrointestinal viruses being observed worldwide in 2020. While this was a welcome effect for already strained health-care systems, prolonged low exposure to pathogens may result in an increased pool of individuals susceptible to certain diseases. Out-of-season or unusually intense outbreaks of non-vaccine preventable diseases have already been documented as NPIs were gradually eased. In the context of widespread and important disruptions in national vaccination programs during the early phase of the pandemic, the risk of vaccine-preventable disease resurgence after NPIs are lifted cannot be excluded either. Awareness must be raised of the risk of vaccine-preventable disease resurgence, and efforts need to be made to mitigate this risk, where possible, by increasing vaccination coverage. Research and regulatory opportunities brought on by the COVID-19 pandemic should be seized. In the first months of the COVID-19 pandemic, the only methods available to slow the spread of the disease were non-pharmaceutical interventions, such as lockdowns, mask wearing, social distancing, school closures, and travel bans. Even after vaccines against COVID-19 became available, combinations of non-pharmaceutical interventions continued to be implemented by most countries, to various extents. Although these measures lowered the number of people who got sick before vaccines and therapies against COVID-19 were available, they also had other consequences for public health. The non-pharmaceutical interventions implemented worldwide have slowed or even stopped the spread of several infectious diseases: since 2020, fewer cases of flu, bronchiolitis, gastroenteritis, and other diseases were recorded compared to pre-pandemic times. This relatively long 2-year period during which people, especially children, were exposed to fewer infections might mean that their immune systems are less prepared to fight these diseases. In addition, vaccination against diseases other than COVID-19 dropped in the early months of the pandemic, meaning that the number of children and adults who are not protected against vaccine-preventable disease has potentially increased. Easing of COVID-19 restrictions has caused a comeback of some diseases against which no vaccine is available, sometimes with more cases than during the pre-pandemic years; there is a risk that this might happen with vaccine-preventable diseases as well. To prevent outbreaks, routine and catch-up vaccinations against other diseases besides COVID-19 should be encouraged and promoted. [ABSTRACT FROM AUTHOR]

Published
2022
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20. Immunological outcomes of new tuberculosis vaccine trials: WHO panel recommendations

Author

Hanekom, Willem A., Dockrell, Hazel M., Ottenhoff, Tom H.M., Doherty, T. Mark, Fletcher, Helen, McShane, Helen, Weichold, Frank F., Hoft, Dan F., Parida, Shreemanta K., and Fruth, Uli J.

Subjects
Immunological research -- Standards -- Physiological aspects, Tuberculosis vaccines -- Physiological aspects -- Standards, Clinical trials -- Standards -- Physiological aspects, Biological sciences, World Health Organization -- Standards
Abstract

The mechanisms of immune protection against human TB, a disease that causes 2 million deaths world-wide each year, are not fully known. T cell immunity is critical for protection [1,2]; [...]

Published
2008

21. Evaluation of Mycobacterium tuberculosis - specific antibody responses in populations with different levels of exposure from Tanzania, Ethiopia, Brazil, and Denmark

Author

Hoff, Soren T., Abebe, Markos, Ravn, Pernille, Range, Nyagosya, Malenganisho, Wabyahe, Rodriques, Denise S., Kallas, Esper G., Soborg, Christian, Doherty, T. Mark, Andersen, Peter, and Weldingh, Karin

Subjects
Tuberculosis -- Diagnosis, Tuberculosis -- Care and treatment, Tuberculosis -- Statistics, Tuberculosis -- Demographic aspects, Mycobacterium tuberculosis -- Research, Mycobacterium tuberculosis -- Physiological aspects, Mycobacterium tuberculosis -- Demographic aspects, Serodiagnosis -- Methods, Health, Health care industry
Published
2007

24. Precision Medicine and Vaccination of Older Adults: From Reactive to Proactive (A Mini-Review).

Author

Doherty, T. Mark, Di Pasquale, Alberta, Michel, Jean-Pierre, Del Giudice, Giuseppe, Doherty, T Mark, Di Pasquale, Alberta, and Del Giudice, Giuseppe

Subjects
*OLDER people, *INDIVIDUALIZED medicine, *VACCINATION, *NON-communicable diseases, *RESPIRATORY diseases, *PATIENT refusal of treatment, *ADULTS, *PREVENTION of chronic diseases, *IMMUNIZATION
Abstract

As populations age globally, the health of older adults is looming larger on the agendas of public health bodies. In particular, the priority is to ensure that older adults remain healthy, independent, and engaged in their communities. In other words, ensuring that increasing life spans are matched by increasing "health spans," meaning years spent in good health. Chronic conditions such as cancer or respiratory and cardiovascular diseases account for the bulk of the disease burden in older adults, and the consensus is that these can best be tackled by effective primary prevention. However, given the diverse nature of older populations, whose prior health experiences can be complicated by multi-morbidity and poly-pharmacy, effective primary prevention can be challenging. One approach that is gaining momentum is what is called "precision" or P4 medicine. The acronym stands for "predictive, personalized, preventive, participatory" medicine, and is based on the premise that preventing disease is better than treating it. However, effective prevention requires the ability to predict disease risk for a given patient, the tailoring of treatment to their circumstances, and their consent for or participation in the offered treatment. A P4 approach may seem counter-intuitive, given that vaccination is generally considered a public health intervention. However, in this article, we discuss the application of P4 medicine as a complement to planning the vaccination of older individuals, with a special focus on the important role that vaccine-preventable infections play in the burden of non-communicable disease. [ABSTRACT FROM AUTHOR]

Published
2020
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30. Potential of novel Mycobacterium tuberculosis infection phase-dependent antigens in the diagnosis of TB disease in a high burden setting

Author

Chegou Novel N, Black Gillian F, Loxton Andre G, Stanley Kim, Essone Paulin N, Klein Michel R, Parida Shreemanta K, Kaufmann Stefan HE, Doherty T Mark, Friggen Annemieke H, Franken Kees L, Ottenhoff Tom H, and Walzl Gerhard

Subjects
Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Confirming tuberculosis (TB) disease in suspects in resource limited settings is challenging and calls for the development of more suitable diagnostic tools. Different Mycobacterium tuberculosis (M.tb) infection phase-dependent antigens may be differentially recognized in infected and diseased individuals and therefore useful as diagnostic tools for differentiating between M.tb infection states. In this study, we assessed the diagnostic potential of 118 different M.tb infection phase-dependent antigens in TB patients and household contacts (HHCs) in a high-burden setting. Methods Antigens were evaluated using the 7-day whole blood culture technique in 23 pulmonary TB patients and in 19 to 21 HHCs (total n = 101), who were recruited from a high-TB incidence community in Cape Town, South Africa. Interferon-gamma (IFN-γ) levels in culture supernatants were determined by ELISA. Results Eight classical TB vaccine candidate antigens, 51 DosR regulon encoded antigens, 23 TB reactivation antigens, 5 TB resuscitation promoting factors (rpfs), 6 starvation and 24 other stress response-associated TB antigens were evaluated in the study. The most promising antigens for ascertaining active TB were the rpfs (Rv0867c, Rv2389c, Rv2450c, Rv1009 and Rv1884c), with Areas under the receiver operating characteristics curves (AUCs) between 0.72 and 0.80. A combination of M.tb specific ESAT-6/CFP-10 fusion protein, Rv2624c and Rv0867c accurately predicted 73% of the TB patients and 80% of the non-TB cases after cross validation. Conclusions IFN-γ responses to TB rpfs show promise as TB diagnostic candidates and should be evaluated further for discrimination between M.tb infection states.

Published
2012
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31. Effect of vaccination on the use of antimicrobial agents: a systematic literature review.

Author

Doherty, T. Mark, Hausdorff, William P., and Kristinsson, Karl G.

Subjects
ANTI-infective agents, DRUG resistance in microorganisms, VACCINATION, META-analysis, INFLUENZA
Abstract

Antimicrobial resistance is a growing global health threat. To preserve the effectiveness of antimicrobials, it is important to reduce demand for antimicrobials. The objective of the study was to screen the existing peer-reviewed literature to identify articles that addressed the potential impact of influenza or Pneumococcus vaccination on antibiotic usage. Data sources: PubMed, Embase Study eligibility criteria: Clinical studies where antimicrobial prescribing was assessed in both vaccinated and unvaccinated populations. Participants and interventions: All patient populations were included (infants, children, adults and elderly), where the effects of the intervention (vaccination) was assessed We identified unique 3638 publications, of which 26 were judged to be of sufficiently high quality to allow the calculation of the potential impact of vaccination. Of these studies 23/26 found a significant reduction in antibiotic use by at least one of the parameters assessed. Different measures used to define anti-microbial use, studies typically focus on specific risk groups and most studies are from high-income countries. Conclusions and implications of key findings: Despite the limitations of the review, the evidence indicates that improved coverage with existing vaccines may significantly reduce antimicrobial demand. This suggests it may be a valuable tool for antimicrobial stewardship. While vaccines against a number of pathogens have been studied for their ability to reduce antimicrobial use, currently only vaccination against influenza or pneumococcus has generated sufficient data for analysis Vaccination against either influenza or pneumococcus significantly reduced overall antimicrobial prescribing rates, both in vaccinated individuals and at a population level Maintaining and expanding vaccination coverage thus appears to be a key tool for antimicrobial stewardship [ABSTRACT FROM AUTHOR]

Published
2020
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32. Adult vaccination as part of a healthy lifestyle: moving from medical intervention to health promotion.

Author

Doherty, T. Mark, Del Giudice, Giuseppe, and Maggi, Stefania

Subjects
VACCINATION, HEALTH promotion, OLDER people, AUTONOMY (Psychology), VACCINE refusal, RISK perception
Abstract

As the global population ages, there is concern about the effect of an increased proportion of older individuals on the economic sustainability of healthcare systems and the social effects of an older society. Health authorities and advocacy groups in countries at the forefront of this trend are now developing strategies to ameliorate the social and financial effects of an ageing population. There is broad agreement that for both society and for the individuals, it is important to ensure that increasing lifespans are matched with increased "healthspans" – the number of years spent in good health. There is also growing consensus that vaccination is one of the tools that can play an important role in improving adult health – though currently vaccination coverage is often poor. This review focuses on two issues that consistently appear to be associated with under-vaccination: the low awareness of risk (and potential consequences) for vaccine-preventable diseases and a poor understanding of the value of improved vaccination coverage for adults. We suggest that understanding of vaccination as a health-promoting activity, rather than a medical intervention designed to prevent the spread of a specific pathogen – is a crucial step to improve vaccination uptake among adults (see ). As populations age globally, we are seeing an increasing burden of vaccine-preventable disease in adults. Adult vaccination against some common diseases has been shown to dramatically improve health and quality of life for older people. Despite the attested benefits, vaccination coverage is almost always poor in adults, even in countries where access is free at point of care. In this article, we discuss what appears to a neglected issue in adult vaccination, that of personal autonomy. We argue that adult vaccination will only be successful if it respects individual autonomy and that this requires treating the choice to vaccinate as a public health issue akin to smoking cessation, exercise and healthy diet. [ABSTRACT FROM AUTHOR]

Published
2019
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35. Response letter Re: The burden of seasonal influenza: improving vaccination coverage to mitigate morbidity and its impact on healthcare systems.

Author

Oh, Kyu-Bin, Doherty, T. Mark, Vetter, Volker, and Bonanni, Paolo

Subjects
SEASONAL influenza, VACCINATION coverage, INFLUENZA vaccines, MEDICAL personnel, COVID-19 pandemic
Abstract

The article discusses the impact of the COVID-19 pandemic on infectious diseases and healthcare systems. It highlights the "tripledemic" of respiratory syncytial virus, influenza, and COVID-19 during the winter of 2022/2023, which overwhelmed hospitals in several countries. The article emphasizes the need to improve vaccination coverage for influenza and other infectious diseases, as well as the importance of integrating the lessons learned from the pandemic. It also acknowledges the strain on healthcare systems due to COVID-19 deaths, burnout among healthcare workers, and the demographic pressure of an aging population. The authors argue that increasing vaccination coverage is crucial for public health and the preservation of healthcare system capacity. [Extracted from the article]

Published
2023
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36. Vaccination programs for older adults in an era of demographic change.

Author

Doherty, T. Mark, Connolly, Mark P., Del Giudice, Giuseppe, Flamaing, Johan, Goronzy, Jorg J., Grubeck-Loebenstein, Beatrix, Lambert, Paul-Henri, Maggi, Stefania, McElhaney, Janet E., Nagai, Hideaki, Schaffner, William, Schmidt-Ott, Ruprecht, Walsh, Edward, and Di Pasquale, Alberta

Abstract

Objectives: Populations are aging worldwide. This paper summarizes some of the challenges and opportunities due to the increasing burden of infectious diseases in an aging population.Results: Older adults typically suffer elevated morbidity from infectious disease, leading to increased demand for healthcare resources and higher healthcare costs. Preventive medicine, including vaccination can potentially play a major role in preserving the health and independence of older adults. However, this potential of widespread vaccination is rarely realized. Here, we give a brief overview of the problem, discuss concrete obstacles and the potential for expanded vaccination programs to promote healthy aging.Conclusion: The increasing healthcare burden of infectious diseases expected in aging populations could, to a large extent, be reduced by achieving higher vaccination coverage among older adults. Vaccination can thus contribute to healthy aging, alongside healthy diet and physical exercise. The available evidence indicates that dedicated programs can achieve substantial improvements in vaccination coverage among older adults, but more research is required to assess the generalizability of the results achieved by specific interventions (see Additional file 1). [ABSTRACT FROM AUTHOR]

Published
2018
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37. Maternal immunization: where are we now and how to move forward?

Author

Vojtek, Ivo, Dieussaert, Ilse, Doherty, T. Mark, Franck, Valentine, Hanssens, Linda, Miller, Jacqueline, Bekkat-Berkani, Rafik, Kandeil, Walid, Prado-Cohrs, David, and Vyse, Andrew

Abstract

Pregnancy and the postpartum period are associated with elevated risks to both mother and infant from infectious disease. Vaccination of pregnant women, also called maternal immunization, has the potential to protect pregnant women, foetuses and infants from several vaccine-preventable diseases. Maternal immunoglobulin G antibodies are actively transferred through the placenta to provide passive immunity to new-borns during the first months of life, until the time for infant vaccinations or until the period of greatest susceptibility has passed. Currently, inactivated influenza, tetanus, and pertussis vaccines are recommended during pregnancy in many countries, but other vaccines may also be administered to pregnant women when risk factors are present. Several new vaccines with a specific indication for use during pregnancy are under development (e.g. respiratory syncytial virus and group B streptococcus vaccines). Years of experience suggest that maternal immunization against influenza, tetanus or pertussis has an acceptable safety profile, is well tolerated, effective and confers significant benefits to pregnant women and their infants. This review describes the principles of maternal immunization and provides an update of the recent evidence regarding the use and timing of maternal immunization. Finally, the barriers preventing wider vaccination coverage and the current limitations in addressing these are also described (Supplementary Material). Key messages: Maternal immunization gives pregnant women greater protection against infectious diseases; induces high levels of maternal antibodies that can be transferred to the foetus; and helps protect new-borns during their first months of life, until they are old enough to be vaccinated. Pregnant women and new-borns are more vulnerable to infectious diseases than the overall population; nevertheless, vaccination rates are often low in pregnant women. This review provides an update of the recent evidence regarding the use and timing of maternal immunization and describes the barriers preventing wider vaccination uptake and the current limitations in addressing these. [ABSTRACT FROM AUTHOR]

Published
2018
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38. Challenges in adult vaccination.

Author

de Gomensoro, Eduardo, Del Giudice, Giuseppe, and Doherty, T. Mark

Abstract

Life-long primary prevention interventions beginning and continuing throughout an individual’s lifetime are increasingly seen as key to meeting the global healthcare challenges that accompany demographic changes - a concept referred to as “Healthy aging”. In this perspective, vaccination is seen as part of a triad, together with healthy diet and exercise. Current adult vaccine coverage is lower than target vaccination rates in most developed countries, and so vaccine preventable diseases continue to present a substantial burden on health and healthcare resources, especially in older individuals. In part, this is due to lack of knowledge and understanding of the benefits of vaccination, inconsistent recommendations by providers and uncertainties about cost benefits. However, lower vaccine effectiveness in older adults plays a part, and new vaccines with novel characteristics to improve effectiveness in older adults are required. A life-course immunization approach to ensure optimal vaccine uptake across adults of all ages can be expected to reduce morbidity and mortality in later life. To achieve this, greater emphasis on public and healthcare provider education is necessary, based on appropriate economic analyses that demonstrate the overall value of vaccination. This article introduces the technical, economic, political and demographic issues that make establishing effective adult vaccination programs such a difficult, but pressing issue, and outlines some of the steps that are now being taken to address them. Key messages: Life-long preventive activities that start and continue throughout life are essential, especially as the world’s population is “getting older”. This “Healthy aging” approach includes not only healthy diet and physical exercise; vaccination is critical in reducing some infectious diseases and their complications. Many adults, especially older adults (who have lower immunity than younger people) develop infections such as influenza and shingles that could potentially be prevented through vaccination. This review provides a perspective on the challenges in delivering a life-course immunization program. While some vaccines are less effective in older people, newer vaccines have been developed which provide stronger and longer protection in older patients than standard existing vaccines. However, the benefits of vaccination can only be realized if the vaccines are recommended and used. For that purpose, greater education of patients and their healthcare providers is necessary. Better knowledge of vaccines and making sure that all adults are up to date with all their recommended vaccines is an essential part of “Healthy aging”. This should prevent not only vaccine-preventable diseases but also reduce the risk of complications in later life. [ABSTRACT FROM AUTHOR]

Published
2018
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39. A phase I, open-label trial on the safety and immunogenicity of the adjuvanted tuberculosis subunit vaccine H1/IC31® in people living in a TB-endemic area.

Author

Hussein, Jemal, Zewdie, Martha, Yamuah, Lawrence, Bedru, Ahmed, Abebe, Markos, Dagnew, Alemnew F., Chanyalew, Menberework, Yohannes, Asfawesen G., Ahmed, Jemal, Engers, Howard, Doherty, T. Mark, Bang, Peter, Kromann, Ingrid, Hoff, Søren T., and Aseffa, Abraham

Subjects
IMMUNOLOGICAL adjuvants, IMMUNOMODULATORS, TUBERCULOSIS treatment, CHIMERIC proteins, TUBERCULIN test, SKIN tests, THERAPEUTICS, BACTERIAL vaccines, CLINICAL trials, COMPARATIVE studies, IMMUNOGLOBULINS, RESEARCH methodology, MEDICAL cooperation, RESEARCH, VACCINES, EVALUATION research, BACTERIAL antibodies, PHARMACODYNAMICS
Abstract

Background: H1/IC31® is a tuberculosis (TB) subunit vaccine candidate consisting of the fusion protein of Ag85B and ESAT-6 (H1) formulated with the IC31® adjuvant. Previous trials have reported on the H1/IC31® vaccine in M. tuberculosis (Mtb)-naïve, BCG-vaccinated and previously Mtb-infected individuals. In this trial, conducted between December 2008 and April 2010, the safety and immunogenicity of H1/IC31® was assessed in participants living in Ethiopia - a highly TB-endemic area.Methods: Healthy male participants aged 18-25 years were recruited into four groups. Participants in group 1 (N = 12) and group 2 (N = 12) were Tuberculin Skin Test (TST) negative and QuantiFERON-TB Gold in-tube test (QFT) negative (Mtb-naïve groups), participants in group 3 (N = 3) were TST positive and QFT negative (BCG group), and participants in group 4 (N = 12) were both TST and QFT positive (Mtb-infected group). H1 vaccine alone (group 1) or H1 formulated with the adjuvant IC31® (groups 2, 3 and 4) was administered intramuscularly on day 0 and day 56. Safety and immunogenicity parameters were evaluated for up to 32 weeks after day 0.Results: The H1/IC31®vaccine was safe and generally well tolerated. There was little difference among the four groups, with a tendency towards a higher incidence of adverse events in Mtb-infected compared to Mtb-naïve participants. Two serious adverse events were reported in the Mtb-infected group where a relationship to the vaccine could not be excluded. In both cases the participants recovered without sequelae within 72 h. Immunogenicity assays, evaluated in the 29 participants who received both vaccinations, showed a stronger response to TB antigens in the Mtb-naïve group vaccinated with the adjuvant.Conclusion: The trial confirmed the need for an adjuvant for the vaccine to be immunogenic and highlighted the importance of early phase testing of a novel TB vaccine candidate in TB-endemic areas.Trial Registration: ClinicalTrials.gov, ID: NCT01049282. Retrospectively registered on 14 January 2010. [ABSTRACT FROM AUTHOR]

Published
2018
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40. Incidence of tuberculosis among school-going adolescents in South India.

Author

Uppada, Dharma Rao, Selvam, Sumithra, Jesuraj, Nelson, Lau, Esther L., Doherty, T. Mark, Grewal, Harleen M. S., Vaz, Mario, Lindtjørn, Bernt, and TB Trials Study Group

Subjects
TUBERCULOSIS in children, TUBERCULOSIS vaccines, TUBERCULOSIS diagnosis, RANDOMIZED controlled trials, SPUTUM microbiology, TUBERCULOSIS epidemiology, LONGITUDINAL method, MYCOBACTERIUM, PUBLIC health surveillance, SCHOOLS, DISEASE incidence
Abstract

Background: Tuberculosis (TB) incidence data in vaccine target populations, particularly adolescents, are important for designing and powering vaccine clinical trials. Little is known about the incidence of tuberculosis among adolescents in India. The objective of current study is to estimate the incidence of pulmonary tuberculosis (PTB) disease among adolescents attending school in South India using two different surveillance methods (active and passive) and to compare the incidence between the two groups.Methods: The study was a prospective cohort study with a 2-year follow-up period. The study was conducted in Palamaner, Chittoor District of Andhra Pradesh, South India from February 2007 to July 2010. A random sampling procedure was used to select a subset of schools to enable approximately 8000 subjects to be available for randomization in the study. A stratified randomization procedure was used to assign the selected schools to either active or passive surveillance. Participants who met the criteria for being exposed to TB were referred to the diagnostic ward for pulmonary tuberculosis confirmation. A total number of 3441 males and 3202 females between the ages 11 and less than 18 years were enrolled into the study.Results: Of the 3102 participants in the active surveillance group, four subjects were diagnosed with definite tuberculosis, four subjects with probable tuberculosis, and 71 subjects had non-tuberculous Mycobacteria (NTM) isolated from their sputum. Of the 3541 participants in the passive surveillance group, four subjects were diagnosed with definite tuberculosis, two subjects with probable tuberculosis, and 48 subjects had non-tuberculosis Mycobacteria isolated from their sputum. The incidence of definite + probable TB was 147.60 / 100,000 person years in the active surveillance group and 87 / 100,000 person years in the passive surveillance group.Conclusion: The incidence of pulmonary tuberculosis among adolescents in our study is lower than similar studies conducted in South Africa and Eastern Uganda - countries with a higher incidence of tuberculosis and human immunodeficiency virus (HIV) than India. The study data will inform sample design for vaccine efficacy trials among adolescents in India. [ABSTRACT FROM AUTHOR]

Published
2016
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42. Effect of Non-tuberculous Mycobacteria on Host Biomarkers Potentially Relevant for Tuberculosis Management.

Author

Dhanasekaran, S., Jenum, Synne, Stavrum, Ruth, Wiker, Harald G., Kenneth, John, Vaz, Mario, Doherty, T. Mark, and Grewal, Harleen M. S.

Subjects
MYCOBACTERIA, MYCOBACTERIUM tuberculosis, TUBERCULOSIS, VACCINE trials, JUVENILE diseases, MYCOBACTERIUM avium paratuberculosis, BURULI ulcer
Abstract

Background: Non-tuberculous mycobacteria (NTM) are different from Mycobacterium tuberculosis (MTB) both in their ubiquitous environmental distribution and in their reduced capacity to cause disease. While often neglected in favour of other infectious diseases, NTM may interfere with important aspects of TB control and management, namely the efficacy of new anti-tuberculosis (TB) vaccines; the immuno-diagnostic Tuberculin skin test (TST) and QuantiFERON TB Gold In Tube assay (QFTGIT); and immune biomarkers explored for their diagnostic and/or predictive potential. Our objective was therefore to explore host immune biomarkers in children who had NTM isolated from respiratory and/or gastric specimens. Methodology and Principle Findings: The present study was nested within a prospective cohort study of BCG-vaccinated neonates in Southern India. In this setting, immune biomarkers from peripheral blood were analyzed in 210 children aged <3 years evaluated for TB using dual-colour-Reverse-Transcriptase-Multiple-Ligation-dependent-Probe-Amplification (dcRT-MLPA) and Bio-Plex assays. The children were classified based on clinical examination, chest X-rays and mycobacterial culture reports as either: 1) TB disease, 2) NTM present and 3) controls. The study shows a down-regulation of RAB33A (p<0.001) and up-regulation of TGFβ1, IL-2 and IL-6 (all p<0.05) in children with TB disease, and that RAB33A, TGFBR2 and IL-10 (all p<0.05) were differentially expressed in children with NTM present when compared to children that were culture negative for MTB and NTM (controls). Conclusions and Significance: Carriage of NTM may reduce the specificity of future diagnostic and predictive immune biomarkers relevant to TB management. Author Summary: Non-tuberculous mycobacteria (NTM) are a ubiquitous group of mycobacteria found in the environment. They are opportunistic pathogens causing human disease, especially in immunocompromised individuals. Differentiation between NTM infection and tuberculosis (TB) can be difficult. Data on incidence of NTM in TB endemic countries is limited due to resource intensive methods required for identification and a considerable workload due to other diseases. The present study was based on children investigated for TB and classified according to chest X-rays and mycobacterial culture reports. We explored host immune biomarkers which are potentially relevant to TB management, in children with confirmed NTM exposure. The findings from the present study suggest that NTM exposure modulates TB-relevant immune biomarkers in the host by eliciting some of the same immune responses as MTB infection. This is may be of importance when evaluating immunological correlates of protection in the setting of TB vaccine trials and potential TB diagnostic biomarkers. [ABSTRACT FROM AUTHOR]

Published
2014
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43. Combination of Cytokine Responses Indicative of Latent TB and Active TB in Malawian Adults.

Author

Hur, Yun-Gyoung, Gorak-Stolinska, Patricia, Ben-Smith, Anne, Lalor, Maeve K., Chaguluka, Steven, Dacombe, Russell, Doherty, T. Mark, Ottenhoff, Tom H., Dockrell, Hazel M., and Crampin, Amelia C.

Subjects
MYCOBACTERIUM tuberculosis, CYTOKINES, MALAWIANS, INTERLEUKINS, BACTERIAL antigens, BACTERIAL cultures
Abstract

Background: An IFN-γ response to M. tuberculosis-specific antigens is an effective biomarker for M. tuberculosis infection but it cannot discriminate between latent TB infection and active TB disease. Combining a number of cytokine/chemokine responses to M. tuberculosis antigens may enable differentiation of latent TB from active disease. Methods: Asymptomatic recently-exposed individuals (spouses of TB patients) were recruited and tuberculin skin tested, bled and followed-up for two years. Culture supernatants, from a six-day culture of diluted whole blood samples stimulated with M. tuberculosis-derived PPD or ESAT-6, were measured for IFN-γ, IL-10, IL-13, IL-17, TNF-α and CXCL10 using cytokine ELISAs. In addition, 15 patients with sputum smear-positive pulmonary TB were recruited and tested. Results: Spouses with positive IFN-γ responses to M. tuberculosis ESAT-6 (>62.5 pg/mL) and TB patients showed high production of IL-17, CXCL10 and TNF-α. Higher production of IL-10 and IL-17 in response to ESAT-6 was observed in the spouses compared with TB patients while the ratios of IFN-γ/IL-10 and IFN-γ/IL-17 in response to M. tuberculosis-derived PPD were significantly higher in TB patients compared with the spouses. Tuberculin skin test results did not correlate with cytokine responses. Conclusions: CXCL10 and TNF-α may be used as adjunct markers alongside an IFN-γ release assay to diagnose M. tuberculosis infection, and IL-17 and IL-10 production may differentiate individuals with LTBI from active TB. [ABSTRACT FROM AUTHOR]

Published
2013
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44. Expression of TNF-Alpha-Dependent Apoptosis-Related Genes in the Peripheral Blood of Malagasy Subjects with Tuberculosis.

Author

Rakotosamimanana, Niaina, Doherty, T. Mark, Andriamihantasoa, Lova H., Richard, Vincent, Gicquel, Brigitte, Soares, Jean-Louis, Zumla, Alimuddin, and Razanamparany, Voahangy Rasolofo

Subjects
*GENE expression, *MYCOBACTERIUM tuberculosis, *APOPTOSIS, *DISEASE progression, *POLYMERASE chain reaction, *FOLLOW-up studies (Medicine), *IMMUNE response
Abstract

The majority of Mycobacterium tuberculosis (Mtb) infections remain asymptomatic with only up to 10% progressing to clinical tuberculosis. However, the constituents of the effective “protective immunity” against tuberculosis responsible for containing most infections remain unknown. Evaluating gene transcriptional profiles in tuberculosis clinical cohorts is one approach to understanding the spectrum of tuberculosis progression. It is clear that apoptosis plays a role in the control of tuberculosis but the utility of apoptosis-related genes as surrogate markers of protection against tuberculosis has not been well investigated. To characterize potential surrogate markers that could discriminate different phases of the clinical tuberculosis spectrum, we investigated gene expression of several TNF-alpha dependent apoptotic genes (TNFR1, TNFR2, FLICE, FLIPs) by real-time RT-PCR of peripheral blood cells from cohorts of individuals with active tuberculosis or potential exposure to tuberculosis. Newly diagnosed tuberculosis patients (n = 23), their close household contacts (n = 80), and community controls (n = 46) were tested at intervals over a period of up to two years. Latent infection or previous Mtb contact was assessed by ELISPOT and TST and complete blood counts were performed during the follow up. Results showed significant upregulation of FLIPs expression by infected individuals regardless of clinical status at entry to the study. A higher percentage of lymphocytes was found in the infected household contacts that remained healthy. In contrast, in individuals with active TB, a significant upregulation of TNFR2 expression, a significantly higher percentage of monocytes and a significantly decreased lymphocyte count were seen, compared to subjects that remained healthy. Moreover, the household contacts who subsequently developed signs of TB also had a significantly high number of monocytes. These data suggest tuberculosis may be associated with decreased T-cell survival (perhaps due to apoptosis) while inhibition of apoptosis in monocytes could lead to a relative increase in these cells: a situation predicted to favour Mtb. [ABSTRACT FROM AUTHOR]

Published
2013
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45. Relationships between Inflammation, Adiponectin, and Oxidative Stress in Metabolic Syndrome.

Author

Shu-Ju Chen, Chi-Hua Yen, Yi-Chia Huang, Bor-Jen Lee, Simon Hsia, Ping-Ting Lin, and Doherty, T. Mark

Subjects
METABOLIC disorders, HUMAN abnormalities, INFLAMMATION, OXIDATIVE stress, INTERLEUKIN-6, ENZYMES
Abstract

Metabolic syndrome (MS) represents a cluster of physiological and anthropometric abnormalities. The purpose of this study was to investigate the relationships between the levels of inflammation, adiponectin, and oxidative stress in subjects with MS. The inclusion criteria for MS, according to the Taiwan Bureau of Health Promotion, Department of Health, were applied to the case group (n = 72). The control group (n = 105) comprised healthy individuals with normal blood biochemical values. The levels of inflammatory markers [high sensitivity C-reactive protein (hs-CRP) and interleukin-6 (IL-6), adiponectin, an oxidative stress marker (malondialdehyde), and antioxidant enzymes activities [catalase (CAT), superoxide dismutase (SOD), and glutathione peroxidase (GPx)] were measured. Subjects with MS had significantly higher concentrations of inflammatory markers and lower adiponectin level, and lower antioxidant enzymes activities than the control subjects. The levels of inflammatory markers and adiponectin were significantly correlated with the components of MS. The level of hs-CRP was significantly correlated with the oxidative stress marker. The IL-6 level was significantly correlated with the SOD and GPx activities, and the adiponectin level was significantly correlated with the GPx activity. A higher level of hs-CRP (≥1.00 mg/L), or IL-6 (≥1.50 pg/mL) or a lower level of adiponectin (<7.90 µg/mL) were associated with a significantly greater risk of MS. In conclusion, subjects suffering from MS may have a higher inflammation status and a higher level of oxidative stress. A higher inflammation status was significantly correlated with decreases in the levels of antioxidant enzymes and adiponectin and an increase in the risk of MS. [ABSTRACT FROM AUTHOR]

Published
2012
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46. Ontogeny of Toll-Like Receptor Mediated Cytokine Responses of South African Infants throughout the First Year of Life.

Author

Reikie, Brian A., Adams, Rozanne C. M., Ruck, Candice E., Ho, Kevin, Leligdowicz, Aleksandra, Pillay, Santoshan, Naidoo, Shalena, Fortuno III, Edgardo S., De Beer, Corena, Preiser, Wolfgang, Cotton, Mark F., Speert, David P., Esser, Monika, Kollmann, Tobias R., and Doherty, T. Mark

Subjects
DISEASE susceptibility, INFECTION, NATURAL immunity, IMMUNE response, ONTOGENY
Abstract

The first year of life represents a time of marked susceptibility to infections; this is particularly true for regions in sub-Saharan Africa. As innate immunity directs the adaptive immune response, the observed increased risk for infection as well as a suboptimal response to vaccination in early life may be due to less effective innate immune function. In this study, we followed a longitudinal cohort of infants born and raised in South Africa over the first year of life, employing the most comprehensive analysis of innate immune response to stimulation published to date. Our findings reveal rapid changes in innate immune development over the first year of life. This is the first report depicting dramatic differences in innate immune ontogeny between different populations in the world, with important implications for global vaccination strategies. [ABSTRACT FROM AUTHOR]

Published
2012
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47. Transcript and Protein Analysis Reveals Better Survival Skills of Monocyte-Derived Dendritic Cells Compared to Monocytes during Oxidative Stress.

Author

Van Brussel, Ilse, Schrijvers, Dorien M., Martinet, Wim, Pintelon, Isabel, Deschacht, Maartje, Schnorbusch, Kathy, Maes, Louis, Bosmans, Johan M., Vrints, Christiaan J., Adriaensen, Dirk, Cos, Paul, Bult, Hidde, and Doherty, T. Mark

Subjects
DENDRITIC cells, ATHEROSCLEROSIS, OXIDATIVE stress, ANTIOXIDANTS, FLOW cytometry, GENE expression
Abstract

Background: Dendritic cells (DCs), professional antigen-presenting cells with the unique ability to initiate primary T-cell responses, are present in atherosclerotic lesions where they are exposed to oxidative stress that generates cytotoxic reactive oxygen species (ROS). A large body of evidence indicates that cell death is a major modulating factor of atherogenesis. We examined antioxidant defence systems of human monocyte-derived (mo)DCs and monocytes in response to oxidative stress. Methods: Oxidative stress was induced by addition of tertiary-butylhydroperoxide (tert-BHP, 30 min). Cellular responses were evaluated using flow cytometry and confocal live cell imaging (both using 5-(and-6)-chloromethyl-2,7-dichlorodihydrofluorescein diacetate, CM- H2DCFDA). Viability was assessed by the neutral red assay. Total RNA was extracted for a PCR profiler array. Five genes were selected for confirmation by Taqman gene expression assays, and by immunoblotting or immunohistochemistry for protein levels. Results: Tert-BHP increased CM-H2DCFDA fluorescence and caused cell death. Interestingly, all processes occurred more slowly in moDCs than in monocytes. The mRNA profiler array showed more than 2-fold differential expression of 32 oxidative stress-related genes in unstimulated moDCs, including peroxiredoxin-2 (PRDX2), an enzyme reducing hydrogen peroxide and lipid peroxides. PRDX2 upregulation was confirmed by Taqman assays, immunoblotting and immunohis- tochemistry. Silencing PRDX2 in moDCs by means of siRNA significantly increased CM-DCF fluorescence and cell death upon tert-BHP-stimulation. Conclusions: Our results indicate that moDCs exhibit higher intracellular antioxidant capacities, making them better equipped to resist oxidative stress than monocytes. Upregulation of PRDX2 is involved in the neutralization of ROS in moDCs. Taken together, this points to better survival skills of DCs in oxidative stress environments, such as atherosclerotic plaques. [ABSTRACT FROM AUTHOR]

Published
2012
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48. Risk Stratification of Latent Tuberculosis Defined by Combined Interferon Gamma Release Assays.

Author

Corbière, Véronique, Pottier, Gaelle, Bonkain, Florence, Schepers, Kinda, Verscheure, Virginie, Lecher, Sophie, Doherty, T. Mark, Locht, Camille, Mascart, Françoise, and Dieli, Francesco

Subjects
INTERLEUKIN-18, MYCOBACTERIUM tuberculosis, MYCOBACTERIAL diseases, TUBERCULOSIS patients, ANTIGENS, PREVENTIVE medicine
Abstract

Background: Most individuals infected with Mycobacterium tuberculosis develop latent tuberculosis infection (LTBI). Some may progress to active disease and would benefit from preventive treatment yet no means currently exists to predict who will reactivate. Here, we provide an approach to stratify LTBI based on IFN-γ responses to two antigens, the recombinant Early- Secreted Antigen Target-6 (rESAT-6) and the latency antigen Heparin-Binding Haemagglutinin (HBHA). Methods: We retrospectively analyzed results from in- house IFN-γ-release assays with HBHA (HBHA-IGRA) and rESAT-6 (rESAT-6- IGRA) performed during a 12-year period on serial blood samples (3 to 9) collected from 23 LTBI subjects in a low-TB incidence country. Both the kinetics of the absolute IFN-γ concentrations secreted in response to each antigen and the dynamics of HBHA/rESAT-6-induced IFN-γ concentrations ratios were examined. Results: This analysis allowed the identification among the LTBI subjects of three major groups. Group A featured stable HBHA and rESAT-6-IGRA profiles with an HBHA/rESAT-6 ratio persistently higher than 1, and with high HBHA- and usually negative rESAT-6-IGRA responses throughout the study. Group B had changing HBHA/rESAT-6 ratios fluctuating from 0.0001 to 10,000, with both HBHA and rESAT-6 responses varying over time at least once during the follow-up. Group C was characterized by a progressive disappearance of all responses. Conclusions: By combining the measures of IFN-γ concentrations secreted in response to an early and a latency antigens, LTBI subjects can be stratified into different risk groups. We propose that disappearing responses indicate cure, that persistent responses to HBHA with HBHA/rESAT-6 ratios ≥1 represent stable LTBI subjects, whereas subjects with ratios varying from ≥1 to <1 should be closely monitored as they may represent the highest-risk group, as illustrated by a case report, and should therefore be prioritized for preventive treatment. [ABSTRACT FROM AUTHOR]

Published
2012
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49. Toll-Like Receptor (TLR2 and TLR4) Polymorphisms and Chronic Obstructive Pulmonary Disease.

Author

Budulac, Simona E., Boezen, H. Marike, Hiemstra, Pieter S., Lapperre, Therese S., Vonk, Judith M., Timens, Wim, Postma, Dirkje S., and Doherty, T. Mark

Subjects
TOLL-like receptors, BACTERIAL diseases, OBSTRUCTIVE lung diseases, SPUTUM microbiology, REGRESSION analysis, CELLS
Abstract

Toll-like receptors (TLRs) participate in the defence against bacterial infections that are common in patients with Chronic Obstructive Pulmonary Disease (COPD). We studied all tagging SNPs in TLR2 and TLR4 and their associations with the level and change over time of both FEV1 and sputum inflammatory cells in moderate-to-severe COPD. Nine TLR2 SNPs and 17 TLR4 SNPs were genotyped in 110 COPD patients. Associations of SNPs with lung function and inflammatory cells in induced sputum were analyzed cross- sectionally with linear regression and longitudinally with linear mixed-effect models. Two SNPs in TLR2 (rs1898830 and rs1 1938228) were associated with a lower level of FEV1 and accelerated decline of FEV1 and higher numbers of sputum inflammatory cells. None of the TLR4 SNPs was associated with FEV1 level. Eleven out of 17 SNPs were associated with FEV1 decline, including rs12377632 and rs10759931, which were additionally associated with higher numbers of sputum inflammatory cells at baseline and with increase over time. This is the first longitudinal study showing that tagging SNPs in TLR2 and TLR4 are associated with the level and decline of lung function as well as with inflammatory cell numbers in induced sputum in COPD patients, suggesting a role in the severity and progression of COPD. [ABSTRACT FROM AUTHOR]

Published
2012
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50. Proof-of-Concept, Randomized, Controlled Clinical Trial of Bacillus- Calmette-Guerin for Treatment of Long-Term Type 1 Diabetes.

Author

Faustman, Denise L., Limei Wang, Okubo, Yoshiaki, Burger, Douglas, Liqin Ban, Guotong Man, Hui Zheng, Schoenfeld, David, Pompei, Richard, Avruch, Joseph, Nathan, David M., and Doherty, T. Mark

Subjects
IMMUNOTHERAPY, DIABETES, LABORATORY mice, BCG vaccines, INSULIN, IMMUNITY, TUMOR necrosis factors
Abstract

Background: No targeted immunotherapies reverse type 1 diabetes in humans. However, in a rodent model of type 1 diabetes, Bacillus Calmette-Guerin (BCG) reverses disease by restoring insulin secretion. Specifically, it stimulates innate immunity by inducing the host to produce tumor necrosis factor (TNF), which, in turn, kills disease-causing autoimmune cells and restores pancreatic beta-cell function through regeneration. Methodology/Principal Findings: Translating these findings to humans, we administered BCG, a generic vaccine, in a proof-of-principle, double-blind, placebo-controlled trial of adults with long-term type 1 diabetes (mean: 15.3 years) at one clinical center in North America. Six subjects were randomly assigned to BCG or placebo and compared to self, healthy paired controls (n = 6) or reference subjects with (n = 57) or without (n = 16) type 1 diabetes, depending upon the outcome measure. We monitored weekly blood samples for 20 weeks for insulin-autoreactive T cells, regulatory T cells (Tregs), glutamic acid decarboxylase (GAD) and other autoantibodies, and C-peptide, a marker of insulin secretion. BCG-treated patients and one placebo-treated patient who, after enrollment, unexpectedly developed acute Epstein-Barr virus infection, a known TNF inducer, exclusively showed increases in dead insulin-autoreactive T cells and induction of Tregs. C- peptide levels (pmol/L) significantly rose transiently in two BCG-treated subjects (means: 3.49 pmol/L [95% CI 2.95-3.8], 2.57 [95% CI 1.65-3.49]) and the EBV-infected subject (3.16 [95% CI 2.54-3.69]) vs.1.65 [95% CI 1.55-3.2] in reference diabetic subjects. BCG-treated subjects each had more than 50% of their C-peptide values above the 95th percentile of the reference subjects. The EBV-infected subject had 18% of C-peptide values above this level. Conclusions/Significance: We conclude that BCG treatment or EBV infection transiently modified the autoimmunity that underlies type 1 diabetes by stimulating the host innate immune response. This suggests that BCG or other stimulators of host innate immunity may have value in the treatment of long-term diabetes. [ABSTRACT FROM AUTHOR]

Published
2012
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