Your search keyword '"Graham, Stephen M."' showing total 15 results

1. Efficacy and Safety of Memantine in Children with Autism Spectrum Disorder: Results from Three Phase 2 Multicenter Studies

Author

Hardan, Antonio Y., Hendren, Robert L., Aman, Michael G., Robb, Adelaide, Melmed, Raun D., Andersen, Kristen A., Luchini, Rachel, Rahman, Rezwanur, Ali, Sanjida, Jia, X Daniel, Mallick, Madhuja, Lateiner, Jordan E., Palmer, Robert H., and Graham, Stephen M.

Abstract

Three phase 2 trials were conducted to assess the efficacy and long-term safety of weight-based memantine extended release (ER) treatment in children with autism spectrum disorder. MEM-MD-91, a 50-week open-label trial, identified memantine extended-release treatment responders for enrollment into MEM-MD-68, a 12-week randomized, double-blind, placebo-controlled withdrawal trial. MEM-MD-69 was an open-label extension trial in which participants from MEM-MD-68, MEM-MD-91, and open-label trial MEM-MD-67 were treated ?48 weeks with memantine extended release. In MEM-MD-91, 517 (59.6%) participants were confirmed Social Responsiveness Scale responders at week 12; mean Social Responsiveness Scale total raw scores improved two to three times a minimal clinically important difference of 10 points. In MEM-MD-68, there was no difference between memantine and placebo on the primary efficacy parameter, the proportion of patients with a loss of therapeutic response (defined as ?10-point increase from baseline in Social Responsiveness Scale total raw score). MEM-MD-69 exploratory analyses revealed mean standard deviation improvement in Social Responsiveness Scale total raw score of 32.4 (26.4) from baseline of the first lead-in study. No new safety concerns were evident. While the a priori-defined efficacy results of the double-blind trial were not achieved, the considerable improvements in mean Social Responsiveness Scale scores from baseline in the open-label trials were presumed to be clinically important.

Published

2019

2. Reply to Holm et al

Author

Graham, Stephen M., Casenghi, Martina, Jean-Philippe, Patrick, Hatherill, Mark, Hesseling, Anneke C., Nachman, Sharon, Starke, Jeffrey R., Swaminathan, Soumya, and Cuevas, Luis E.

Published

2013

3. Importance of Antibody and Complement for Oxidative Burst and Killing of Invasive Nontyphoidal Salmonella by Blood Cells in Africans

Author

Gondwe, Esther N., Molyneux, Malcolm E., Goodall, Margaret, Graham, Stephen M., Mastroeni, Pietro, Drayson, Mark T., MacLennan, Caiman A., and Kasper, Dennis L.

Published

2010

4. Bacteremia in Malawian Children with Severe Malaria: Prevalence, Etiology, HIV Coinfection, and Outcome

Author

Bronzan, Rachel N., Taylon, Terrie E., Mwenechanya, James, Tembo, Madalitso, Kayira, Kondwani, Bwanaisa, Lloyd, Njobvu, Alfred, Kondowe, Wendy, Chalira, Chipo, Walsh, Amanda L., Phiri, Amos, Wilson, Lorna K., Molyneux, Malcolm E., and Graham, Stephen M.

Published

2007

5. Tuberculosis Infection in Children and Adolescents.

Author

Tchakounte Youngui, Boris, Tchounga, Boris Kevin, Graham, Stephen M., and Bonnet, Maryline

Subjects

MYCOBACTERIUM tuberculosis, TUBERCULOSIS, TEENAGERS, INFECTION

Abstract

The burden of tuberculosis (TB) in children and adolescents remains very significant. Several million children and adolescents are infected with TB each year worldwide following exposure to an infectious TB case and the risk of progression from TB infection to tuberculosis disease is higher in this group compared to adults. This review describes the risk factors for TB infection in children and adolescents. Following TB exposure, the risk of TB infection is determined by a combination of index case characteristics, contact features, and environmental determinants. We also present the recently recommended approaches to diagnose and treat TB infection as well as novel tests for infection. The tests for TB infection have limitations and diagnosis still relies on an indirect immunological assessment of cellular immune response to Mycobacterium tuberculosis antigens using immunodiagnostic testing. It is recommended that TB exposed children and adolescents and those living with HIV receive TB preventive treatment (TPT) to reduce the risk of progression to TB disease. Several TPT regimens of similar effectiveness and safety are now available and recommended by the World Health Organisation. [ABSTRACT FROM AUTHOR]

Published

2022

6. Detecting Mycobacterium tuberculosis Infection in Children Migrating to Australia.

Author

Laemmle-Ruff, Ingrid, Graham, Stephen M., Williams, Bridget, Horyniak, Danielle, Majumdar, Suman S., Paxton, Georgia A., Soares Caplice, Lila V., Hellard, Margaret E., and Trauer, James M.

Subjects

*TUBERCULOSIS epidemiology, *TUBERCULOSIS diagnosis, *INTERFERON gamma release tests, *MEDICAL screening, *MYCOBACTERIUM tuberculosis, *TUBERCULIN test

Abstract

In 2015, Australia updated premigration screening for tuberculosis (TB) disease in children 2-10 years of age to include testing for infection with Mycobacterium tuberculosis and enable detection of latent TB infection (LTBI). We analyzed TB screening results in children <15 years of age during November 2015-June 2017. We found 45,060 child applicants were tested with interferon-gamma release assay (IGRA) (57.7% of tests) or tuberculin skin test (TST) (42.3% of tests). A total of 21 cases of TB were diagnosed: 4 without IGRA or TST, 10 with positive IGRA or TST, and 7 with negative results. LTBI was detected in 3.3% (1,473/44,709) of children, for 30 applicants screened per LTBI case detected. LTBI-associated factors included increasing age, TB contact, origin from a higher TB prevalence region, and testing by TST. Detection of TB and LTBI benefit children, but the updated screening program's effect on TB in Australia is likely to be limited. [ABSTRACT FROM AUTHOR]

Published

2022

7. Diagnostic Challenges in Childhood Pulmonary Tuberculosis—Optimizing the Clinical Approach.

Author

Gunasekera, Kenneth S., Vonasek, Bryan, Oliwa, Jacquie, Triasih, Rina, Lancioni, Christina, Graham, Stephen M., Seddon, James A., and Marais, Ben J.

Subjects

DECISION making in children, SYMPTOMS, TUBERCULOSIS, HEALTH services accessibility, CHILD mortality, THERAPEUTICS, SPINAL tuberculosis

Abstract

The management of childhood tuberculosis (TB) is hampered by the low sensitivity and limited accessibility of microbiological testing. Optimizing clinical approaches is therefore critical to close the persistent gaps in TB case detection and prevention necessary to realize the child mortality targets of the End TB Strategy. In this review, we provide practical guidance summarizing the evidence and guidelines describing the use of symptoms and signs in decision making for children being evaluated for either TB preventive treatment (TPT) or TB disease treatment in high-TB incidence settings. Among at-risk children being evaluated for TPT, a symptom screen may be used to differentiate children who require further investigation for TB disease before receiving TPT. For symptomatic children being investigated for TB disease, an algorithmic approach can inform which children should receive TB treatment, even in the absence of imaging or microbiological confirmation. Though clinical approaches have limitations in accuracy, they are readily available and can provide valuable guidance for decision making in resource-limited settings to increase treatment access. We discuss the trade-offs in using them to make TB treatment decisions. [ABSTRACT FROM AUTHOR]

Published

2022

8. Tuberculous Meningitis in Children: A Forgotten Public Health Emergency.

Author

du Preez, Karen, Jenkins, Helen E., Donald, Peter R., Solomons, Regan S., Graham, Stephen M., Schaaf, H. Simon, Starke, Jeffrey R., Hesseling, Anneke C., and Seddon, James A.

Subjects

TUBERCULOUS meningitis, MYCOBACTERIUM tuberculosis, MYCOBACTERIAL diseases, PUBLIC health, INFECTION, SYMPTOMS

Abstract

Tuberculous meningitis (TBM) remains a major cause of morbidity and mortality in children with tuberculosis (TB), yet there are currently no estimates of the global burden of pediatric TBM. Due to frequent non-specific clinical presentation and limited and inadequate diagnostic tests, children with TBM are often diagnosed late or die undiagnosed. Even when diagnosed and treated, 20% of children with TBM die. Of survivors, the majority have substantial neurological disability with significant negative impact on children and their families. Surveillance data on this devastating form of TB can help to quantify the contribution of TBM to the overall burden, morbidity and mortality of TB in children and the epidemiology of TB more broadly. Pediatric TBM usually occurs shortly after primary infection with Mycobacterium tuberculosis and reflects ongoing TB transmission to children. In this article we explain the public health importance of pediatric TBM, discuss the epidemiology within the context of overall TB control and health system functioning and the limitations of current surveillance strategies. We provide a clear rationale for the benefit of improved surveillance of pediatric TBM using a TB care cascade framework to support monitoring and evaluation of pediatric TB, and TB control more broadly. Considering the public health implications of a diagnosis of TBM in children, we provide recommendations to strengthen pediatric TBM surveillance and outline how improved surveillance can help us identify opportunities for prevention, earlier diagnosis and improved care to minimize the impact of TBM on children globally. [ABSTRACT FROM AUTHOR]

Published

2022

9. Predictors of Unlikely Bacterial Pneumonia and Adverse Pneumonia Outcome in Children Admitted to a Hospital in Central Vietnam.

Author

Nguyen, Phuong T K, Tran, Hoang T, Tran, Thach S, Fitzgerald, Dominic A, Graham, Stephen M, and Marais, Ben J

Subjects

ANTIBIOTICS, ANTI-infective agents, C-reactive protein, CHEST X rays, HOSPITAL care of children, DRUG resistance in microorganisms, DRUG utilization, DRUG side effects, LONGITUDINAL method, HEALTH outcome assessment, PNEUMONIA, TREATMENT effectiveness, PREDICTIVE tests, CHILDREN

Abstract

Background Pneumonia is the leading cause of antibiotic use and hospitalization in Vietnam. There is a need for better prediction of unlikely bacterial pneumonia and adverse pneumonia outcome in order to guide hospital admission and improve rational antibiotic use. Methods All children under 5 admitted with pneumonia (per clinician assessment) to the Da Nang Hospital for Women and Children were prospectively enrolled. Children were classified as having likely or unlikely bacterial pneumonia and followed for outcome assessment. A Bayesian model averaging approach was used to identify predictors of unlikely bacterial pneumonia and adverse pneumonia outcome, which guided the development of a pragmatic management algorithm. Results Of 3817 patients assessed, 2199 (57.6%) met World Health Organization (WHO) pneumonia criteria. In total, 1594 (41.7%) children were classified as having unlikely and 129 (3.4%) as having likely bacterial pneumonia. The remainder (2399; 62.9%) were considered to have disease of uncertain etiology. Factors predictive of unlikely bacterial pneumonia were no fever, no consolidation on chest radiograph, and absolute neutrophil count <5 × 109/L at presentation, which had a negative predictive value (NPV) for likely bacterial pneumonia of 99.0%. Among those who met WHO pneumonia criteria, 8.6% (189/2199) experienced an adverse outcome. Not having any WHO danger sign or consolidation on chest radiograph had an NPV of 96.8% for adverse pneumonia outcome. Conclusions An algorithm that screens for predictors of likely bacterial pneumonia and adverse pneumonia outcome could reduce unnecessary antibiotic use and hospital admission, but its clinical utility requires validation in a prospective study. [ABSTRACT FROM AUTHOR]

Published

2020

10. Presentation of life-threatening invasive nontyphoidal Salmonella disease in Malawian children: A prospective observational study.

Author

Maclennan, Calman A., Msefula, Chisomo L., Gondwe, Esther N., Gilchrist, James J., Pensulo, Paul, Mandala, Wilson L., Mwimaniwa, Grace, Banda, Meraby, Kenny, Julia, Wilson, Lorna K., Phiri, Amos, Maclennan, Jenny M., Molyneux, Elizabeth M., Molyneux, Malcolm E., and Graham, Stephen M.

Subjects

SALMONELLA diseases, CHILDREN, ANTIBIOTICS, CHILD mortality, LOGISTIC regression analysis, MULTIDRUG resistance in bacteria, DIAGNOSIS

Abstract

Nontyphoidal Salmonellae commonly cause invasive disease in African children that is often fatal. The clinical diagnosis of these infections is hampered by the absence of a clear clinical syndrome. Drug resistance means that empirical antibiotic therapy is often ineffective and currently no vaccine is available. The study objective was to identify risk factors for mortality among children presenting to hospital with invasive Salmonella disease in Africa. We conducted a prospective study enrolling consecutive children with microbiologically-confirmed invasive Salmonella disease admitted to Queen Elizabeth Central Hospital, Blantyre, in 2006. Data on clinical presentation, co-morbidities and outcome were used to identify children at risk of inpatient mortality through logistic-regression modeling. Over one calendar year, 263 consecutive children presented with invasive Salmonella disease. Median age was 16 months (range 0–15 years) and 52/256 children (20%; 95%CI 15–25%) died. Nontyphoidal serovars caused 248/263 (94%) of cases. 211/259 (81%) of isolates were multi-drug resistant. 251/263 children presented with bacteremia, 6 with meningitis and 6 with both. Respiratory symptoms were present in 184/240 (77%; 95%CI 71–82%), 123/240 (51%; 95%CI 45–58%) had gastrointestinal symptoms and 101/240 (42%; 95%CI 36–49%) had an overlapping clinical syndrome. Presentation at <7 months (OR 10.0; 95%CI 2.8–35.1), dyspnea (OR 4.2; 95%CI 1.5–12.0) and HIV infection (OR 3.3; 95%CI 1.1–10.2) were independent risk factors for inpatient mortality. Invasive Salmonella disease in Malawi is characterized by high mortality and prevalence of multi-drug resistant isolates, along with non-specific presentation. Young infants, children with dyspnea and HIV-infected children bear a disproportionate burden of the Salmonella-associated mortality in Malawi. Strategies to improve prevention, diagnosis and management of invasive Salmonella disease should be targeted at these children. [ABSTRACT FROM AUTHOR]

Published

2017

11. Childhood tuberculosis: A roadmap towards zero deaths.

Author

Marais, Ben J and Graham, Stephen M

Subjects

*TUBERCULOSIS research, *TUBERCULOSIS in children, *CHILDREN, *DEATH

Abstract

'Every day, more than 200 children under the age of 15 die needlessly from tuberculosis (TB) - a disease that is preventable and curable. The World Health Organization estimates that as many as 1 in 10 TB cases globally (6-10% of all TB cases) are among this age group, but the number could be even higher because many children are simply undiagnosed.' Childhood TB is emerging from the shadows. This quote comes from the recently launched international roadmap towards zero TB deaths in children. We provide a brief update of new developments and remaining challenges related to childhood TB, with particular emphasis on the new roadmap. [ABSTRACT FROM AUTHOR]

Published

2016

12. The epidemiology of tuberculosis in children in Australia, 2003–2012.

Author

Teo, Stephen S., Tay, Ee Laine, Douglas, Paul, Krause, Vicki L., and Graham, Stephen M.

Subjects

TUBERCULOSIS in children, EPIDEMIOLOGY, CHILDREN, RETROSPECTIVE studies, DISEASE incidence, INDIGENOUS children, HEALTH

Abstract

Objective: To describe the burden of and trends in paediatric tuberculosis (TB) in Australia between 2003 and 2012. Design: A retrospective analysis of TB data from the National Notifiable Diseases Surveillance System (NNDSS) on TB in children (under 15 years of age) during the 10-year period, 2003–2012. Results: TB notifications in Australia during the study period included 538 children (range, 37–66 cases per year), representing 4.6% of the total TB case load during the period (range, 3.8%e5.8% each year). Place of birth was recorded for 524 patients (97.4%); of these, 230 (43.9%) were born in Australia, 294 (56.1%) overseas. The average annual notification rate was 1.31 (95% CI, 1.20e1.43) cases per 100000 child population. The rate was higher for overseas-born than for Australian-born children (9.57 [95% CI, 8.51–10.73] v 0.61 [95% CI, 0.53–0.69] cases per 100000 children. The overall rate was highest among those aged 0–4 years. The annual notification rate was three times higher for Indigenous children than for non- Indigenous Australian-born children. Of 427 patients (79.4% of total) for whom the method of case detection was recorded, 37.0% were detected by contact screening, 8.7% by post-arrival immigration screening, and 54.3% by passive case detection. Pulmonary TB was the most common diagnostic classification (64.7% of patients). The most common risk factors were close contact with a TB case and recent residence in a country with a high incidence of TB. Treatment outcomes were satisfactory; 89.4% of children had completed treatment or were cured. Conclusions: The burden of paediatric TB in Australia is low but has not changed over the past decade. The highest rates are among children born overseas, emphasising the important role of immigration screening as Australia aspires to eliminate TB. [ABSTRACT FROM AUTHOR]

Published

2015

13. Treatment of paediatric TB: revised WHO guidelines.

Author

Graham, Stephen M.

Subjects

TUBERCULOSIS in children, GUIDELINES, DRUG dosage, SERUM, DATA analysis, HIV-positive persons, THERAPEUTICS

Abstract

Summary: The World Health Organization has recently revised the recommended dosages of the main first-line anti-tuberculosis drugs for use in children. The recommended dosages and range of isoniazid, rifampicin, pyrazinamide and ethambutol have been increased from the previous recommended dosages. Ethambutol is now recommended for use in children of all ages including those of less than 5 years of age. This review explains the rationale for these recent revisions. Children require higher dosages than adults to achieve the same serum concentrations. Available data in HIV-uninfected children suggest that the revised dosages are within limits that have a very low risk of toxicity. An important challenge will be to examine the impact of higher dosages on clinical response, drug-drug interactions and risk of toxicity in HIV-infected children. [Copyright &y& Elsevier]

Published

2011

14. Childhood TB: can the End TB Strategy deliver?

Author

Seddon, James A. and Graham, Stephen M.

Subjects

TUBERCULOSIS in children, DISEASE incidence, BURDEN of care, FAMILY nursing, PREVENTION

Abstract

The accelerated reductions in global TB incidence required to achieve the End TB Strategy goal will result in reductions in the burden of childhood TB. Contact screening and preventive therapy have emerged as important components of TB burden reduction, and family-centered approaches could be an effective route in delivering these activities. Lack of accurate diagnostics for children remains a critical barrier and a need remains for better collaborative and supportive links between the child health and TB control sectors. Irrespective of whether the ambitious targets can be achieved, the unprecedented opportunities provided by the End TB Strategy must be embraced. [ABSTRACT FROM AUTHOR]

Published

2016

15. New and repurposed drugs for pediatric multidrug-resistant tuberculosis practice-based recommendations

Author

Jennifer Hughes, Ben J. Marais, Anthony J. Garcia-Prats, Lindsay McKenna, Stephen M. Graham, James A Seddon, Marina Tadolini, Elizabeth P. Harausz, Anneke C. Hesseling, Jonathan Bernheimer, Peyton Wilson, Sylvie Jonckheere, Giovanni Battista Migliori, Jay Achar, Lia D'Ambrosio, Jennifer Furin, Anne Detjen, Andrea T. Cruz, Alena Skrahina, H. Simon Schaaf, Harausz, Elizabeth P, Garcia-Prats, Anthony J., Seddon, James A., Schaaf, H. Simon, Hesseling, Anneke C., Achar, Jay, Bernheimer, Jonathan, Cruz, Andrea T., D'Ambrosio, Lia, Detjen, Anne, Graham, Stephen M., Hughes, Jennifer, Jonckheere, Sylvie, Marais, Ben J., Migliori, Giovanni Battista, Mckenna, Lindsay, Skrahina, Alena, Tadolini, Marina, Wilson, Peyton, and Furin, Jennifer

Subjects

Pediatrics, Respiratory System, Antitubercular Agents, CHILDREN, Mycobacterium tuberculosi, Critical Care and Intensive Care Medicine, Clofazimine, chemistry.chemical_compound, 0302 clinical medicine, Tuberculosis, Multidrug-Resistant, 030212 general & internal medicine, Child, Medicine (all), 11 Medical And Health Sciences, Multidrug-resistant tuberculosi, multidrug-resistant tuberculosis, Tolerability, Practice Guidelines as Topic, Delamanid, Life Sciences & Biomedicine, medicine.drug, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Tuberculosis, Nevirapine, REGIMEN, Adolescent, DELAMANID, 03 medical and health sciences, Critical Care Medicine, General & Internal Medicine, COMPASSIONATE USE, medicine, Humans, COHORT, XDR-TB, METAANALYSIS, Science & Technology, business.industry, Mycobacterium tuberculosis, medicine.disease, PROLONGATION, BEDAQUILINE, Regimen, pediatric, 030228 respiratory system, chemistry, Linezolid, TOLERABILITY, Bedaquiline, business

Abstract

It is estimated that 33,000 children develop multidrug-resistant tuberculosis (MDR-TB) each year. In spite of these numbers, children and adolescents have limited access to the new and repurposed MDR-TB drugs. There is also little clinical guidance for the use of these drugs and for the shorter MDR-TB regimen in the pediatric population. This is despite the fact that these drugs and regimens are associated with improved interim outcomes and acceptable safety profiles in adults. This review fills a gap in the pediatric MDR-TB literature by providing practice-based recommendations for the use of the new (delamanid and bedaquiline) and repurposed (linezolid and clofazimine) MDR-TB drugs and the new shorter MDR-TB regimen in children and adolescents.

Published

2016