33 results on '"Amaya L. Bustinduy"'
Search Results
2. A 14-year follow-up of ultrasound-detected urinary tract pathology associated with urogenital schistosomiasis in women living in the Msambweni region of coastal Kenya
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Elizabeth Joekes, Kate McMonnies, Andrew Blanshard, Francis M Mutuku, Edmund Ireri, Peter Mungai, J Russell Stothard, Amaya L Bustinduy, and Charles H King
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Infectious Diseases ,Public Health, Environmental and Occupational Health ,Parasitology ,General Medicine - Abstract
Background Complications of urogenital schistosomiasis include acute inflammatory and chronic fibrotic changes within the urogenital tract. Disease burden of this neglected tropical disease is often underestimated, as only active, urine egg-patent Schistosoma infection is formally considered. Previous studies have focussed on short-term effects of praziquantel treatment on urinary tract pathology, demonstrating that acute inflammation is reversible. However, the reversibility of chronic changes is less well studied. Methods Our study compared, at two time points 14 y apart, urine egg-patent infection and urinary tract pathology in a cohort of women living in a highly endemic area having intermittent praziquantel treatment(s). In 2014 we matched 93 women to their findings in a previous study in 2000. Results Between 2000 and 2014 the rate of egg-patent infection decreased from 34% (95% confidence interval [CI] 25 to 44) to 9% (95% CI 3 to 14). However, urinary tract pathology increased from 15% (95% CI 8 to 22) to 19% (95% CI 11 to 27), with the greatest increase seen in bladder thickening and shape abnormality. Conclusions Despite praziquantel treatment, fibrosis from chronic schistosomiasis outlasts the presence of active infection, continuing to cause lasting morbidity. We suggest that future efforts to eliminate persistent morbidity attributable to schistosomiasis should include intensified disease management.
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- 2023
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3. The Presence of Hemoglobin in Cervicovaginal Lavage Is Not Associated With Genital Schistosomiasis in Zambian Women From the BILHIV Study
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Amy S Sturt, Emily L Webb, Comfort R Phiri, Joyce Mapani, Maina Mudenda, Lisa Himschoot, Eyrun F Kjetland, Tobias Mweene, Bruno Levecke, Govert J van Dam, Paul L A M Corstjens, Helen Ayles, Richard J Hayes, Suzanna C Francis, Lisette van Lieshout, Piet Cools, Isaiah Hansingo, and Amaya L Bustinduy
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TOOLS ,hematuria ,PCR ,Infectious Diseases ,Oncology ,female genital schistosomiasis ,Medicine and Health Sciences ,cervicovaginal lavage ,Schistosoma haematobium ,URINE SAMPLES ,hemoglobin ,HAEMATOBIUM INFECTION - Abstract
Background Female genital schistosomiasis (FGS) occurs when Schistosoma haematobium eggs are deposited in reproductive tissue. Female genital schistosomiasis in the cervical mucosa is associated with increased vascularity. If FGS is associated with the presence of hemoglobin in cervicovaginal lavage (CVL), the use of urinary reagent strips to detect hemoglobin in CVL could supplement FGS diagnosis. Methods Nonmenstruating, nonpregnant, sexually active women aged 18–31 participating in the HPTN 071 (PopART) Population-Cohort were invited in 2 Zambian communities. Genital self-swabs and a urine specimen were collected at a home visit, and CVL and hand-held colposcopy were performed at a midwife led clinic visit. Urinary reagent strips were used to identify hemoglobin in CVL. Eggs and circulating anodic antigen (CAA) were detected from urine. Visual-FGS was defined as the presence of sandy patches, rubbery papules, or abnormal blood vessels. Polymerase chain reaction (PCR)-FGS was defined as Schistosoma deoxyribonucleic acid detected by real-time PCR on CVL or cervical or vaginal swab. Results Of 209 women with home genital swabs and companion CVL specimens, 66% (138 of 209) had detectable CVL hemoglobin, 13.4% (28 of 209) had PCR-defined FGS, and 17.2% (36 of 209) had visual-FGS. Active Schistosoma infection, diagnosed by CAA or urine microscopy, was present in 21.0% (44 of 209) participants. Active Schistosoma infection (P = .4), PCR-FGS (P = 0.7), and visual-FGS (P = 0.3) were not associated with CVL hemoglobin presence. Results did not differ in subgroups with high infection burden (cycle threshold < 35 or 2–3 positive genital PCR). Conclusions Polymerase chain reaction-FGS, visual-FGS, and active Schistosoma infection were not associated with the presence of CVL hemoglobin. Further research is needed to establish accessible community-based FGS diagnostics.
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- 2022
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4. A review of the genetic determinants of praziquantel resistance in Schistosoma mansoni: Is praziquantel and intestinal schistosomiasis a perfect match?
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Shannan Summers, Tapan Bhattacharyya, Fiona Allan, J Russell Stothard, Andrew Edielu, Bonnie L. Webster, Michael A. Miles, and Amaya L. Bustinduy
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Schistosomiasis is a neglected tropical disease (NTD) caused by parasitic trematodes belonging to the Schistosoma genus. The mainstay of schistosomiasis control is the delivery of a single dose of praziquantel (PZQ) through mass drug administration (MDA) programs. These programs have been successful in reducing the prevalence and intensity of infections. Due to the success of MDA programs, the disease has recently been targeted for elimination as a public health problem in some endemic settings. The new World Health Organization (WHO) treatment guidelines aim to provide equitable access to PZQ for individuals above two years old in targeted areas. The scale up of MDA programs may heighten the drug selection pressures on Schistosoma parasites, which could lead to the emergence of PZQ resistant schistosomes. The reliance on a single drug to treat a disease of this magnitude is worrying should drug resistance develop. Therefore, there is a need to detect and track resistant schistosomes to counteract the threat of drug resistance to the WHO 2030 NTD roadmap targets. Until recently, drug resistance studies have been hindered by the lack of molecular markers associated with PZQ resistance. This review discusses recent significant advances in understanding the molecular basis of PZQ action in S. mansoni and proposes additional genetic determinants associated with PZQ resistance. PZQ resistance will also be analyzed in the context of alternative factors that may decrease efficacy within endemic field settings, and the most recent treatment guidelines recommended by the WHO.
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- 2022
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5. Meningococcal carriage among Hajj pilgrims, risk factors for carriage and records of vaccination: a study of pilgrims to Mecca
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Amaya L. Bustinduy, Abrar K Alasmari, David L Heymann, Fathia Ben-Rached, Arnab Pain, Ron H Behrens, Heidi J. Larson, Brian Greenwood, Joanna Houghton, Abdullah M. Assiri, and Phil Edwards
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Male ,Vaccination Coverage ,Self Medication ,Neisseria meningitidis ,medicine.disease_cause ,0302 clinical medicine ,Risk Factors ,antibiotic ,Hajj ,Neisseria meningitides ,Prevalence ,Medicine ,meningococcal ,Travel ,Vaccination ,Middle Aged ,Anti-Bacterial Agents ,Infectious Diseases ,Carrier State ,Original Article ,Female ,Adult ,Adolescent ,030231 tropical medicine ,Saudi Arabia ,Meningococcal Vaccines ,Meningococcal vaccine ,Serogroup ,Meningococcal disease ,Islam ,Young Adult ,03 medical and health sciences ,Environmental health ,Humans ,Aged ,business.industry ,Public Health, Environmental and Occupational Health ,Outbreak ,Patient Acceptance of Health Care ,medicine.disease ,Meningococcal Infections ,Cross-Sectional Studies ,Carriage ,Meningococcal carriage ,pharyngeal carriage ,Parasitology ,business ,Original Research Papers - Abstract
Objective The Saudi government requires that all pilgrims receive a quadrivalent meningococcal vaccine at least 10 days before the Hajj. We conducted a study to determine the uptake of meningococcal vaccine and antibiotic use. We also investigated risk factors of meningococcal carriage and carriage of Neisseria meningitidis pathogenic serogroups A, C, W and Y. Methods A cross‐sectional oropharyngeal carriage survey was conducted in 2973 Hajj pilgrims in September 2017. A real‐time polymerase chain reaction (rt‐PCR) assay was used to identify N. meningitidis from the oropharyngeal swabs. A questionnaire investigated potential risk factors for carriage of N. meningitidis. Results Two thousand two hundred forty nine oropharyngeal swabs were obtained. The overall prevalence of carriage of N. meningitidis was 4.6% (95% CI: 3.4%–6%). Carriage of pathogenic serogroups was not associated significantly with any of the meningococcal risk factors evaluated. 77% of pilgrims were vaccinated but 22.58 % said they were carrying unofficial vaccination cards. Conclusion Carriage of serogroups A, C, W and Y was not significantly associated with any of the risk factors investigated. Almost a quarter of pilgrims were unlikely to have been vaccinated, highlighting a need to strengthen compliance with the current policy of vaccination to prevent meningococcal disease outbreaks during and after the Hajj.
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- 2021
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6. Integration of prevention and control measures for female genital schistosomiasis, HIV and cervical cancer
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Makia Christine Masong, Camilla Ducker, Dirk Engels, Wendy Harrison, Kreeneshni Govender, William Evan Secor, Rachael Thomson, Pamela Sabina Mbabazi, Sally Theobald, Mwelecele N. Malecela, Patrick J. Lammie, Peter J. Hotez, Amaya L. Bustinduy, Margaret Gyapong, and Victoria Gamba
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Health Knowledge, Attitudes, Practice ,medicine.medical_specialty ,030231 tropical medicine ,Sexual and reproductive health and rights ,Human Papilloma Virus Vaccine ,Uterine Cervical Neoplasms ,HIV Infections ,Schistosomiasis ,Disease ,Global Health ,Praziquantel ,Schistosomiasis haematobia ,03 medical and health sciences ,0302 clinical medicine ,Global health ,medicine ,Humans ,Papillomavirus Vaccines ,Africa South of the Sahara ,Anthelmintics ,Cervical cancer ,Schistosoma haematobium ,biology ,business.industry ,Public health ,Public Health, Environmental and Occupational Health ,Awareness ,medicine.disease ,biology.organism_classification ,Anti-Retroviral Agents ,Family medicine ,Women's Health ,Female ,Pre-Exposure Prophylaxis ,Reproductive Health Services ,business ,Genital Diseases, Female - Abstract
Female genital schistosomiasis as a result of chronic infection withLa schistosomiase génitale féminine, résultant d'une infection chronique àLos responsables de formular las políticas sanitarias nacionales y globales siguen ignorando en gran medida la esquistosomiasis genital femenina como consecuencia de la infección crónica porإن داء البلهارسيا التناسلية الأنثوية كنتيجة للإصابة المزمنة بالبلهارسيا الدموية (المعروفة باسم البلهارسيا)، يستمر في تعرضه للتجاهل إلى حد كبير من جانب واضعي السياسات الصحية الوطنية والعالمية. يركز الاهتمام الدولي للعمل على نطاق واسع ضد المرض على ما إذا كان عامل خطر لانتقال فيروس نقص المناعة البشرية (HIV). إلا إن داء البلهارسيا التناسلية الأنثوية نفسه يرتبط بالألم والنزيف والعقم أو عدم الخصوبة، أو يؤدي إلى الوصم الاجتماعي، وهو مشكلة شائعة بالنسبة للنساء في المناطق الموبوءة بالبلهارسيا في الدول الأفريقية جنوب الصحراء الكبرى. وعلى ذلك يجب الاعتراف بالمرض كمكون آخر من مكونات جدول أعمال الصحة الشاملة وحقوق الإنسان للنساء والفتيات في أفريقيا، إلى جانب فيروس نقص المناعة البشرية ((HIV وسرطان عنق الرحم. كل من هذه الأمراض الثلاثة لها تدخل وقائي مستهدف ومثبت: وهو العلاج بمضادات الفيروسات القهقرية، والوقاية قبل التعرض لفيروس نقص المناعة البشرية/الإيدز؛ لقاح فيروس الورم الحليمي البشري لسرطان عنق الرحم؛ وعلاج البرازيكوانتيل لمرض البلهارسيا التناسلية الأنثوية. نحن نناقش كيف يمكن دمج السيطرة على داء البلهارسيا التناسلية الأنثوية، مع رعاية نقص المناعة البشرية المكتسبة/ الإيدز، وسرطان عنق الرحم. سيكون هذا البرنامج جزءاً من إطار عمل أوسع للصحة والحقوق الجنسية والإنجابية، وتمكين المرأة والعدالة الاجتماعية في أفريقيا. إن النهج المتكاملة التي تشمل العديد من برامج الصحة العامة، لديها القدرة على توسيع أو خلق فرص للوصول إلى المزيد من الفتيات والنساء طوال فترات حياتهن. نحن نوجز جدول أعمال بحثي تشغيلي عملي، لديه إمكانية تحسين التنفيذ المشترك لحزمة من التدابير التي تستجيب للاحتياجات المحددة للفتيات والنساء.由于感染慢性埃及裂体吸虫(俗称血吸虫)而导致的女性生殖器血吸虫病,在很大程度上仍然被国家和全球卫生政策制定者所忽视。国际社会针对该疾病采取的大规模行动的关注焦点在于其是否为人体免疫缺陷病毒 (HIV) 传播的危险因素。然而,女性生殖器血吸虫病本身与伤痛、出血和生育能力低下或不孕症有关,进而导致患者蒙受社会耻辱,而且在撒哈拉以南非洲血吸虫病流行地区,这种疾病已成为常见问题。因此,应将该疾病与 HIV 和宫颈癌一起,认定为非洲妇女和女童全面健康和人权议程的另一个组成部分。这三种疾病中的每一种都有针对性和经过验证的预防性干预措施:针对 HIV 的抗逆转录病毒治疗和暴露前的预防措施;针对宫颈癌的人乳头瘤病毒疫苗;以及针对女性生殖器血吸虫病的吡喹酮治疗。我们讨论如何将女性生殖器血吸虫病的控制与 HIV和宫颈癌护理结合起来。此类方案将成为非洲性健康和生殖健康与权利、赋予妇女权力和社会正义这一宽泛框架的一部分。结合多种公共卫生方案的综合方法有可能扩大或创造机会,帮助更多女童和妇女终生受益。我们拟定了一项针对实际运作研究的议程,该议程有可能优化联合实施一揽子措施,以满足女童和妇女的特定需要。.Генитальный шистосомоз у женщин в результате хронической инфекции, вызванной паразитом
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- 2020
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7. An update on female and male genital schistosomiasis and a call to integrate efforts to escalate diagnosis, treatment and awareness in endemic and non-endemic settings: The time is now
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Amaya L, Bustinduy, Bodo, Randriansolo, Amy S, Sturt, Seke A, Kayuni, Peter D C, Leustcher, Bonnie L, Webster, Lisette, Van Lieshout, J Russell, Stothard, Hermann, Feldmeier, and Margaret, Gyapong
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Male ,Schistosomiasis haematobia ,Schistosoma haematobium ,Animals ,Humans ,Female ,Genitalia, Female ,Genitalia, Male ,Praziquantel - Abstract
The last decades have brought important insight and updates in the diagnosis, management and immunopathology of female genital schistosomiasis (FGS) and male genital schistosomiasis (MGS). Despite sharing a common parasitic aetiological agent, FGS and MGS have typically been studied separately. Infection with Schistosoma haematobium manifests with gender-specific clinical manifestations and consequences of infection, albeit having a similar pathogenesis within the human genital tract. Schistosoma haematobium is a known urinary bladder carcinogen, but its potential causative role in other types of neoplasia, such as cervical cancer, is not fully understood. Furthermore, the impact of praziquantel treatment on clinical outcomes remains largely underexplored, as is the interplay of FGS/MGS with relevant reproductive tract infections such as HIV and Human Papillomavirus. In non-endemic settings, travel and immigrant health clinics need better guidance to correctly identify and treat FGS and MGS. Our review outlines the latest advances and remaining knowledge gaps in FGS and MGS research. We aim to pave a way forward to formulate more effective control measures and discuss elimination targets. With a growing community awareness in health practitioners, scientists and epidemiologists, alongside the sufferers from these diseases, we aspire to witness a new generation of young women and men free from the downstream disabling manifestations of disease.
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- 2022
8. An update on female and male genital schistosomiasis and a call to integrate efforts to escalate diagnosis, treatment and awareness in endemic and non-endemic settings: The time is now
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Amaya L. Bustinduy, Bodo Randriansolo, Amy S. Sturt, Sekeleghe A. Kayuni, Peter D.C. Leutscher, Bonnie L. Webster, Lisette Van Lieshout, J. Russell Stothard, Hermann Feldmeier, Margaret Gyapong, Rollinson, David, and Stothard, Russell
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HPV ,Urogenital Schistosomiasis ,MGS ,Cervical cancer ,HIV ,S. mansoni ,FGS ,Schistosoma Haematobium ,Praziquantel - Abstract
The last decades have brought important insight and updates in the diagnosis, management and immunopathology of female genital schistosomiasis (FGS) and male genital schistosomiasis (MGS). Despite sharing a common parasitic aetiological agent, FGS and MGS have typically been studied separately. Infection with Schistosoma haematobium manifests with gender-specific clinical manifestations and consequences of infection, albeit having a similar pathogenesis within the human genital tract. Schistosoma haematobium is a known urinary bladder carcinogen, but its potential causative role in other types of neoplasia, such as cervical cancer, is not fully understood. Furthermore, the impact of praziquantel treatment on clinical outcomes remains largely underexplored, as is the interplay of FGS/MGS with relevant reproductive tract infections such as HIV and Human Papillomavirus. In non-endemic settings, travel and immigrant health clinics need better guidance to correctly identify and treat FGS and MGS. Our review outlines the latest advances and remaining knowledge gaps in FGS and MGS research. We aim to pave a way forward to formulate more effective control measures and discuss elimination targets. With a growing community awareness in health practitioners, scientists and epidemiologists, alongside the sufferers from these diseases, we aspire to witness a new generation of young women and men free from the downstream disabling manifestations of disease.
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- 2022
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9. The praziquantel in preschoolers (PIP) trial: study protocol for a phase II PK/PD-driven randomised controlled trial of praziquantel in children under 4 years of age
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Andrew Edielu, Edridah M. Tukahebwa, William W. Hope, Emily L. Webb, Moses Adriko, Amaya L. Bustinduy, Alison M. Elliott, Narcis B. Kabatereine, Hannah W Wu, Alfred Mubangizi, Patrice A. Mawa, and Jennifer F. Friedman
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Medicine (General) ,medicine.medical_specialty ,Medicine (miscellaneous) ,Schistosomiasis ,Placebo ,Praziquantel ,Schistosoma japonicum ,law.invention ,Efficacy ,Study Protocol ,R5-920 ,Clinical Trials, Phase II as Topic ,Randomized controlled trial ,Intestinal schistosomiasis ,law ,Internal medicine ,parasitic diseases ,medicine ,Animals ,Humans ,Pharmacology (medical) ,Child ,Preschool ,Adverse effect ,Children ,PK/PD models ,Randomized Controlled Trials as Topic ,Anthelmintics ,business.industry ,Schistosoma mansoni ,medicine.disease ,Schistosomiasis mansoni ,Treatment Outcome ,Child, Preschool ,Pharmacodynamics ,business ,medicine.drug - Abstract
Background Over 200 million individuals worldwide are infected with Schistosoma species, with over half of infections occurring in children. Many children experience first infections early in life and this impacts their growth and development; however praziquantel (PZQ), the drug used worldwide for the treatment of schistosomiasis, only has regulatory approval among adults and children over the age of four, although it is frequently used “off label” in endemic settings. Furthermore, pharmacokinetic/pharmacodynamics (PK/PD) evidence suggests the standard PZQ dose of 40 mg/kg is insufficient in preschool-aged children (PSAC). Our goal is to understand the best approaches to optimising the treatment of PSAC with intestinal schistosomiasis. Methods We will conduct a randomised, controlled phase II trial in a Schistosoma mansoni endemic region of Uganda and a Schistosoma japonicum endemic region of the Philippines. Six hundred children, 300 in each setting, aged 12–47 months with Schistosoma infection will be randomised in a 1:1:1:1 ratio to receive either (1) 40 mg/kg PZQ at baseline and placebo at 6 months, (2) 40 mg/kg PZQ at baseline and 40 mg/kg PZQ at 6 months, (3) 80 mg/kg PZQ at baseline and placebo at 6 months, or (4) 80 mg/kg PZQ at baseline and 80 mg/kg PZQ at 6 months. Following baseline treatment, children will be followed up for 12 months. The co-primary outcomes will be cure rate and egg reduction rate at 4 weeks. Secondary outcomes include drug efficacy assessed by novel antigenic endpoints at 4 weeks, actively collected adverse events and toxicity for 12 h post-treatment, morbidity and nutritional outcomes at 6 and 12 months, biomarkers of inflammation and environmental enteropathy and PZQ PK/PD parameters. Discussion The trial will provide valuable information on the safety and efficacy of the 80 mg/kg PZQ dose in PSAC, and on the impact of six-monthly versus annual treatment, in this vulnerable age group. Trial registration ClinicalTrials.gov NCT03640377. Registered on 21 Aug 2018.
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- 2021
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10. Schistosoma mansoni Infection as a Predictor of Low Aerobic Capacity in Ugandan Children
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Amaya L. Bustinduy, Aaron Atuhaire, Michelle C. Stanton, Edridah M. Tukahebwa, Moses Arinaitwe, J. Russell Stothard, Georgia McLachlan, Courtney Smith, E. James LaCourse, Hajri Al Shehri, and Moses Adriko
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medicine.medical_specialty ,Anemia ,030231 tropical medicine ,Schistosomiasis ,Gastroenterology ,03 medical and health sciences ,0302 clinical medicine ,Interquartile range ,Virology ,Internal medicine ,parasitic diseases ,medicine ,Wasting ,Aerobic capacity ,biology ,business.industry ,Articles ,medicine.disease ,biology.organism_classification ,Infectious Diseases ,Cohort ,Parasitology ,Schistosoma mansoni ,medicine.symptom ,business ,Malaria - Abstract
Using the 20-meter shuttle run test (20mSRT) as a morbidity metric, we assessed whether Schistosoma mansoni infection was associated with decreased aerobic capacity in Ugandan children across a range of altitudes, either at low (∼600 m) or high (∼1,000 m) altitudes. A total of 305 children were recruited from six schools within the Buliisa District, Lake Albert, Uganda. A subset (n = 96) of these had been previously assessed and treated for schistosomiasis ± malaria 2 weeks prior. Fitness scores on the 20mSRT were translated into VO2max using a standardized equation. Unadjusted and multivariable-adjusted analyses were performed using VO2max as the primary outcome. Analysis of fitness scores from 304 children, inclusive of the subset follow-up cohort, revealed a median VO2max of 45.4 mL kg(−1) min(−1) (interquartile range: 42.9–48.0 mL kg(−1) min(−1)). Children residing at high altitudes demonstrated increased aerobic capacities (46.3 versus 44.8 mL kg(−1) min(−1), P = 0.031). The prevalence of stunting, wasting, S. mansoni egg patent infection, malaria, giardiasis, anemia, and fecal occult blood were 36.7%, 16.1%, 44.3%, 65.2%, 21.4%, 50.6%, and 41.2%, respectively. Median VO2max was elevated in those previously treated, compared with those newly recruited (46.3 versus 44 mL kg(−1) min(−1), P < 0.001). Multivariable-adjusted analysis revealed a strong negative association between S. mansoni egg patent infection and VO2max at low altitude (beta coefficient: −3.96, 95% CI: −6.56 to −137, P = 0.004). This is the first study to document a negative association between S. mansoni infection and aerobic capacity at low altitudes using the 20mSRT.
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- 2019
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11. Impact of a Novel, Low-Cost and Sustainable Health Education Program on the Knowledge, Attitudes, and Practices Related to Intestinal Schistosomiasis in School Children in a Hard-to-Reach District of Madagascar
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Stephen A. Spencer, Emmanuel H. Andriamasy, Cortland Linder, James M. StJ. Penney, Jemima Henstridge-Blows, Hannah J. Russell, Kate Hyde, Caitlin Sheehy, Isla L. Young, Benedicte Sjoflot, Daniel A. L. Rakotomampianina, Anjara M. Nandimbiniaina, Gina U. Raderalazasoa, Tahiry N. Ranaivoson, Antsa Andrianiaina, Rasolofomanana S. M. Michèle, Zafera A. Rohe, Amaya L. Bustinduy, J. Russell Stothard, Sheena M. Cruickshank, Glenn T. Edosoa, and Alain M. Rahetilahy
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Male ,wa_30 ,Health Knowledge, Attitudes, Practice ,Adolescent ,Child Health ,Community Participation ,wa_590 ,wc_810 ,26bc6fb8 ,Infectious Diseases ,Cross-Sectional Studies ,Virology ,Child, Preschool ,Madagascar ,Humans ,Schistosomiasis ,Parasitology ,Female ,Child ,f0e481db ,Health Education ,Follow-Up Studies ,Program Evaluation - Abstract
Schistosomiasis control requires multisectoral approaches including praziquantel treatment, access to safe water, sanitation and hygiene, and health education. Community input can help ensure health education programs are culturally appropriate to effectively direct protective behavior change. This study reports on the three-stage development of an education program for Malagasy children, with an impact evaluation on their knowledge, attitudes, and practices (KAP) related to intestinal schistosomiasis. A cross-sectional study took place in 2017 with follow-up in 2018 in the hard-to-reach Marolambo district, Madagascar. A novel schistosomiasis education program (SEP) was designed in collaboration with researchers, stakeholders, and local community and included cartoon books, games, songs, puzzles, and blackboard lessons, costing $10 USD per school. KAP questionnaires were completed by 286 children pre-SEP and 273 children post-SEP in 2017, and by 385 and 337 children pre-SEP and post-SEP, respectively, in 2018. Improvements were observed in responses to all questions between pre- and post-education answers in 2017 (53–77%, P < 0.0001) and 2018 (72–98%, P < 0.0001) and in the pre-education answers between years (53–72%, P < 0.0001). Praziquantel mass drug administration attendance improved, rising from 64% to 91% (P < 0.0001), alongside improved latrine use, from 89% to 96% (P = 0.005). This community-consulted and -engaged SEP resulted in substantial improvements in children’s understanding of schistosomiasis, with improvements in praziquantel uptake and latrine use. Socioculturally tailored education programs can help gain schistosomiasis control. Continued investment in SEP will help promote the future well-being of children through increased participation in control and treatment activities.
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- 2021
12. Use of face masks and other personal preventive measures by Hajj pilgrims and their impact on health problems during the Hajj
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Phil Edwards, Abrar K Alasmari, Ron H Behrens, Abdullah M. Assiri, and Amaya L. Bustinduy
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Infection Control ,Hand washing ,Traveler's diarrhea ,business.industry ,media_common.quotation_subject ,Masks ,Saudi Arabia ,General Medicine ,Odds ratio ,Infections ,medicine.disease ,Islam ,International airport ,Open data ,Cross-Sectional Studies ,Hygiene ,Environmental health ,medicine ,Humans ,Hajj ,Electronic data ,Travel-Related Illness ,business ,Personal Protective Equipment ,media_common - Abstract
Background The Hajj is one of the world’s largest pilgrimage and gathers millions of Muslims from different nationalities every year. Communicable diseases have been reported frequently, during and following the Hajj, and these have been linked to individual behavioural measures. This study aimed to measure the effect of personal preventive measures, such as face mask use, hand hygiene and others, adopted by pilgrims in reducing the acquisition of infectious diseases. Methods We conducted a cross-sectional study at the Hajj terminal in King Abdulaziz International Airport in Jeddah, Saudi Arabia. Pilgrims were approached in the airport lounges after the 2017 Hajj season and prior to the departure of their flights from Jeddah to their home countries. An electronic data collection tool (‘Open Data Kit’) was used to gather survey data in regards to health problems and preventive measures during the Hajj. Results A total of 2973 Hajj pilgrims were surveyed. In all, 38.7% reported symptoms of upper respiratory tract infections (URTIs) and 5.4% reported symptoms of travel diarrhoea. Compliance with face mask use was 50.2%. Changing a face mask every 4 h was found to be significantly associated with lower prevalence of URTIs [adjusted odds ratio 0.56 (95% confidence interval 0.34–0.92), P = 0.02]. There was no statistical difference between overall face mask use and URTI acquisition. The main sources of food, eating raw vegetables/food, frequency of hand washing or use of hand sanitizers were not found to be significantly associated with reported travellers’ diarrhoea. Unlicensed barbers were used by 12% of pilgrims and 9.2% of pilgrims reported using blades that were reused by other pilgrims. Conclusion Preventive measures are the most effective way to prevent infections. Pilgrims can benefit from face masks by changing them frequently. There is still limited information on the effect of the use of face mask in decreasing the risk of URTI in mass gatherings.
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- 2020
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13. Acceptability and feasibility of genital self-sampling for the diagnosis of female genital schistosomiasis: a cross-sectional study in Zambia
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Emily L. Webb, Amaya L. Bustinduy, Kwame Shanaube, Richard J. Hayes, Comfort R Phiri, Amy S. Sturt, Bilhiv study team, Namakau Chola, Helen Ayles, and Isaiah Hansingo
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Female circumcision ,medicine.medical_specialty ,Cross-sectional study ,030231 tropical medicine ,Medicine (miscellaneous) ,Schistosomiasis ,vaginal self-sampling ,Disease ,General Biochemistry, Genetics and Molecular Biology ,03 medical and health sciences ,0302 clinical medicine ,cervical self-sampling ,acceptability ,female genital schistosomiasis ,Medicine ,Sex organ ,Sampling (medicine) ,030212 general & internal medicine ,Schistosoma haematobium ,biology ,business.industry ,Genitourinary system ,Obstetrics ,self-sampling ,Articles ,biology.organism_classification ,medicine.disease ,self-collection ,3. Good health ,genital self-sampling ,business ,Research Article ,feasibility - Abstract
Background: Female genital schistosomiasis (FGS) is a neglected and disabling gynaecological disorder that is difficult to diagnose and is part of the wider spectrum of urogenital disease caused by the waterborne parasite Schistosoma haematobium. Over 90% of human schistosomiasis cases are found in sub-Saharan Africa with 3.8 million people infected with schistosomes in Zambia. Reported FGS prevalence ranges from 33-75% of those with urinary schistosomiasis in endemic areas, suggesting a potentially high FGS burden in Zambia alone. The Bilharzia and HIV (BILHIV) study evaluated home self-sampling genital collection methods for the diagnosis of FGS. Methods: Eligible participants included non-pregnant, sexually active women aged 18-31 who were previously recruited for the HPTN 071 (PopART) trial in Livingstone, Zambia. Household demographic and symptom questionnaires were administered by community workers. Participants were offered vaginal and cervical self-swabs and a urine cup. Cervicovaginal lavage (CVL) was performed in clinic by midwives. Information was collected from participants on the acceptability and feasibility of genital self-sampling. Results: From January-August 2018, 603 women were enrolled, and 87.3% (527/603) completed clinic follow up. A high proportion of participants indicated that self-collection of specimens was “easy” or “very easy” on a 5-point Likert scale. A high proportion of women would be willing to self-collect all three specimens again in future: vaginal swab 96.7% (583/603), cervical swab 96.5% (582/603), and urine 96.2% (580/603). Overall, 90.0% (543/603) preferred to self-collect samples at home, compared with sampling in the clinic Home-based self-sampling was preferred over provider-based sampling in the clinic due to greater privacy 65.0% (353/543), convenience 51.4% (279/543) and lack of needed transportation 17.7% (96/543). Conclusions: Home based genital self-sampling for FGS diagnosis is highly acceptable. This scalable method may inform future efforts for community-based diagnosis of FGS
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- 2020
14. Promoting gender, equity, human rights and ethnic equality in neglected tropical disease programmes
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W Prasetyanti, Amaya L. Bustinduy, Julie Jacobson, M Seunik, Camilla Ducker, Laura Dean, Pamela Sabina Mbabazi, S Del Pino, H Broekkamp, Mwelecele N. Malecela, and Alison Krentel
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0301 basic medicine ,Economic growth ,wc_680 ,Human Rights ,Service delivery framework ,media_common.quotation_subject ,030231 tropical medicine ,Ethnic group ,Vulnerability ,wa_395 ,wa_20_5 ,equity ,03 medical and health sciences ,0302 clinical medicine ,inequalities ,Tropical Medicine ,Political science ,gender ,Ethnicity ,medicine ,Humans ,AcademicSubjects/MED00860 ,neglected tropical diseases ,media_common ,Equity (economics) ,Human rights ,Public Health, Environmental and Occupational Health ,Neglected Diseases ,Tropical disease ,General Medicine ,ethinic ,medicine.disease ,AcademicSubjects/MED00290 ,030104 developmental biology ,Infectious Diseases ,Commentary ,Neglected tropical diseases ,Parasitology ,wa_309 ,Intersectoral Collaboration - Abstract
Limited attention to tackling neglected tropical diseases (NTDs) through the lenses of gender, equity, ethnicity and human rights inadvertently undermines progress due to the exclusion of subgroups in populations living in conditions of vulnerability. Supporting national NTD programmes to make equity analysis part of their routine activities and revitalising intersectoral collaboration will be essential to achieve effective, sustainable service delivery with a person-centred approach. Gender, equity, human rights and ethnic equality for NTD programmes should therefore be incorporated in multisectoral engagements.
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- 2021
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15. Paediatric and maternal schistosomiasis: shifting the paradigms
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Jennifer F. Friedman, Amaya L. Bustinduy, and J. Russell Stothard
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Female circumcision ,medicine.medical_specialty ,Pediatrics ,030231 tropical medicine ,Schistosomiasis ,Praziquantel ,03 medical and health sciences ,0302 clinical medicine ,Communicable Diseases, Imported ,Pregnancy ,parasitic diseases ,Humans ,Medicine ,030212 general & internal medicine ,Dosing ,Subclinical disease ,Child ,Mass drug administration ,Anthelmintics ,Invited Review ,business.industry ,General Medicine ,medicine.disease ,Surgery ,Pregnancy Complications, Parasitic ,Expanded access ,Female ,business ,medicine.drug - Abstract
Background: In endemic areas, schistosomiasis causes both overt and subclinical disease in young children and their mothers, as well as in returned travellers. Sources of data: Key recently published literature. Areas of agreement: An action plan for paediatric schistosomiasis and female genital schistosomiasis (FGS) is needed with expanded access to praziquantel (PZQ) treatment required. Areas of controversy: Schistosomiasis-related morbidity is underappreciated. Present and future demand for PZQ treatment is bottlenecked, imbalanced and inequitable. Current dosing, treatment algorithms and access plans are suboptimal with treatment stalled during pregnancy. Growing points: Raised dosing of PZQ (>40 mg/kg) is being explored in young children. Surveillance of female genital schistosomiasis FGS is increasing. Use of PZQ in pregnancy is safe and preventive chemotherapy guidelines are being revised in morbidity- and transmission-control settings. Areas timely for developing research: Shifting focus of population-level control to individual-case management. Detection and prevention of FGS within general health services and integration of PZQ treatment for women and children in antenatal clinics. Feasibility studies assessing alternative and expanded access to PZQ treatment to at-risk children and mothers and pregnant women.
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- 2017
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16. Application of a recombinase polymerase amplification (RPA) assay and pilot field testing for Giardia duodenalis at Lake Albert, Uganda
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Bonnie L. Webster, Stephen Allen, J. Russell Stothard, Michael A. Miles, Amaya L. Bustinduy, Kate Poulton, Tapan Bhattacharyya, Sandra Molina-Gonzalez, Hajri Al-Shehri, Edridah M. Tukahebwa, and Moses Arianitwe
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0301 basic medicine ,Giardiasis ,Epidemiology ,Protozoan Proteins ,Recombinase Polymerase Amplification ,Pilot Projects ,wc_700 ,medicine.disease_cause ,Feces ,0302 clinical medicine ,Uganda ,Child ,Schools ,Giardia ,Cryptosporidium ,Amplicon ,Giardia intestinalis ,Infectious Diseases ,qx_20 ,Health Resources ,Nucleic Acid Amplification Techniques ,wc_680 ,Genotype ,Recombinase polymerase amplification ,030231 tropical medicine ,Loop-mediated isothermal amplification ,wa_395 ,Biology ,lcsh:Infectious and parasitic diseases ,Recombinases ,03 medical and health sciences ,parasitic diseases ,medicine ,Giardia lamblia ,Humans ,lcsh:RC109-216 ,Assemblage typing ,Research ,Ribosomal RNA ,DNA, Protozoan ,biology.organism_classification ,Virology ,Cytoskeletal Proteins ,Lakes ,030104 developmental biology ,Parasitology ,Point-of-care ,Giardia duodenalis - Abstract
Background Giardia duodenalis is a gastrointestinal protozoan causing 184 million cases of giardiasis worldwide annually. Detection is by microscopy or coproantigen assays, although sensitivity is often compromised by intermittent shedding of cysts or trophozoites, or operator expertise. Therefore, for enhanced surveillance field-applicable, point-of-care (POC), molecular assays are needed. Our aims were to: (i) optimise the recombinase polymerase amplification (RPA) assay for the isothermal amplification of the G. duodenalis β-giardin gene from trophozoites and cysts, using published primer and probes; and (ii) perform a pilot field validation of RPA at a field station in a resource-poor setting, on DNA extracted from stool samples from schoolchildren in villages around Lake Albert, Uganda. Results were compared to an established laboratory small subunit ribosomal RNA (SSU rDNA) qPCR assay with additional testing using a qPCR targeting the triose phosphate isomerase (tpi) DNA regions that can distinguish G. duodenalis of two different assemblages (A and B), which are human-specific. Results Initial optimisation resulted in the successful amplification of predicted RPA products from G. duodenalis-purified gDNA, producing a double-labelled amplicon detected using lateral flow strips. In the field setting, of 129 stool samples, 49 (37.9%) were positive using the Giardia/Cryptosporidium QuikChek coproantigen test; however, the RPA assay when conducted in the field was positive for a single stool sample. Subsequent molecular screening in the laboratory on a subset (n = 73) of the samples demonstrated better results with 21 (28.8%) RPA positive. The SSU rDNA qPCR assay resulted in 30/129 (23.3%) positive samples; 18 out of 73 (24.7%) were assemblage typed (9 assemblage A; 5 assemblage B; and 4 mixed A+B). Compared with the SSU rDNA qPCR, QuikChek was more sensitive than RPA (85.7 vs 61.9%), but with similar specificities (80.8 vs 84.6%). In comparison to QuikChek, RPA had 46.4% sensitivity and 82.2% specificity. Conclusions To the best of our knowledge, this is the first in-field and comparative laboratory validation of RPA for giardiasis in low resource settings. Further refinement and technology transfer, specifically in relation to stool sample preparation, will be needed to implement this assay in the field, which could assist better detection of asymptomatic Giardia infections.
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- 2020
17. Focused Assessment with Sonography for Urinary Schistosomiasis (FASUS)—pilot evaluation of a simple point-of-care ultrasound protocol and short training program for detecting urinary tract morbidity in highly endemic settings
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A Verheyden, Tom Heller, R Obiang, Martin P. Grobusch, Michael Ramharter, Jonathan Remppis, Amaya L. Bustinduy, Sabine Bélard, A.A. Adegnika, N García-Tardón, Gédéon Prince Manouana, Elizabeth Joekes, Infectious diseases, AII - Infectious diseases, APH - Aging & Later Life, and APH - Global Health
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Adult ,medicine.medical_specialty ,wj_151 ,diagnostic imaging ,Point-of-Care Systems ,Urinary system ,Point-of-care testing ,Pilot Projects ,wa_395 ,Schistosomiasis ,Schistosomiasis haematobia ,Ureter ,hydronephrosis ,wn_20 ,medicine ,Animals ,Humans ,Gabon ,Child ,Hydronephrosis ,Ultrasonography ,Schistosoma haematobium ,Urinary bladder ,biology ,business.industry ,Ultrasound ,Public Health, Environmental and Occupational Health ,wc_810 ,General Medicine ,medicine.disease ,biology.organism_classification ,point-of-care testing ,Infectious Diseases ,medicine.anatomical_structure ,tropical medicine ,Parasitology ,Radiology ,Morbidity ,business - Abstract
Background Urogenital schistosomiasis (UGS) causes inflammation and fibrosis of the urinary tract. In resource-limited settings, affordable tools for morbidity assessment in clinical care are needed. Point-of-care ultrasound has not yet been validated for UGS-related pathology. Methods We developed a protocol for Focused Assessment with Sonography for Urinary Schistosomiasis (FASUS), assessing pathology of the bladder wall, ureters and kidneys. Following standardized training, two clinicians performed FASUS on children and adults with hematuria in Lambaréné, Gabon. Recorded ultrasound clips were remotely reviewed by two ultrasound experts as a diagnostic reference. Results In 2015 and 2016, scans were performed in 118 patients. The image quality was sufficient in 90% of bladder views and more than 97% of kidney views. UGS-compatible pathology was detected in 51/118 (43%) by the operator and in 46/107 (43%) by the experts among baseline scans of sufficient quality. Inter-rater agreement between operators and experts was very good (κ > 0.8) for hydronephrosis and good (κ > 0.6) for bladder wall thickening. Conclusions FASUS is a promising clinical, point-of-care tool for detecting UGS-related urinary tract morbidity in symptomatic patients. Based on larger validation studies, appropriate diagnostic and therapeutic algorithms for the use of FASUS should be established.
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- 2019
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18. Beyond the barrier: Female Genital Schistosomiasis as a potential risk factor for HIV-1 acquisition
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Amy S. Sturt, Suzanna C. Francis, Amaya L. Bustinduy, Emily L. Webb, and Richard J. Hayes
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0301 basic medicine ,Female circumcision ,Veterinary (miscellaneous) ,030231 tropical medicine ,Human immunodeficiency virus (HIV) ,Physiology ,Urogenital schistosomiasis, Vaginal or cervicovaginal microbiota ,Schistosomiasis ,HIV Infections ,medicine.disease_cause ,Article ,03 medical and health sciences ,Schistosomiasis haematobia ,0302 clinical medicine ,Pathognomonic ,parasitic diseases ,Prevalence ,Medicine ,Humans ,Schistosoma ,Schistosoma haematobium ,Sexually transmitted infection ,biology ,business.industry ,Potential risk ,Transmission (medicine) ,virus diseases ,Genitalia, Female ,030108 mycology & parasitology ,biology.organism_classification ,medicine.disease ,Infectious Diseases ,Cross-Sectional Studies ,Insect Science ,Vaginal or cervicovaginal inflammation ,HIV-1 ,Parasitology ,Female ,business ,Genital Diseases, Female - Abstract
Highlights • FGS is associated with prevalent HIV-1 infection. • Characteristic FGS lesions may allow HIV-1 access to sub-epithelial target cells • Cervical egg granulomas bring together the target cells needed for HIV-1 infection • S. haematobium has been associated with altered systemic/genital cytokine levels • HIV-1 RNA concentrations may be altered in HIV-1 and schistosomiasis coinfection, Female genital schistosomiasis (FGS) results from egg-deposition in the female reproductive tract primarily by the waterborne parasite Schistosoma (S.) haematobium, and less commonly by Schistosoma (S.) mansoni. FGS affects an estimated 20-56 million women worldwide, mostly in sub-Saharan Africa. There is cross-sectional evidence of increased HIV-1 prevalence in schistosomiasis-infected women, but a causal relationship between FGS and either HIV-1 acquisition or transmission has not been fully established. Beyond the pathognomonic breach in the cervicovaginal barrier caused by FGS, this narrative review explores potential mechanisms for a synergistic relationship between S. haematobium infection, FGS, and HIV-1 acquisition through vaginal inflammation and target cell recruitment., Graphical abstract Female Genital Schistosomiasis and HIV-1 acquisition may be associated through vaginal inflammation, barrier dysfunction, and target cell recruitment. Image, graphical abstract
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- 2019
19. A cross-sectional study of periportal fibrosis and Schistosoma mansoni infection among school-aged children in a hard-to-reach area of Madagascar
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Amaya L. Bustinduy, Lalarizo R Mahary, Alain M. Rahetilahy, Emmanuel H Andriamasy, J. Russell Stothard, Elodie P Ranjanoro, Cortland Linder, Elizabeth Joekes, James M StJ Penney, Daniel A L Rakotomampianina, Stephen A. Spencer, and Hannah J Russell
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0301 basic medicine ,Liver Cirrhosis ,medicine.medical_specialty ,Cross-sectional study ,030231 tropical medicine ,Schistosomiasis ,03 medical and health sciences ,Feces ,0302 clinical medicine ,Stool microscopy ,Fibrosis ,Internal medicine ,medicine ,Madagascar ,Prevalence ,Animals ,Humans ,Child ,School age child ,Schools ,biology ,business.industry ,Public Health, Environmental and Occupational Health ,General Medicine ,Schistosoma mansoni ,030108 mycology & parasitology ,biology.organism_classification ,medicine.disease ,Schistosomiasis mansoni ,Young age ,Infectious Diseases ,Cross-Sectional Studies ,Periportal fibrosis ,Antigens, Helminth ,Parasitology ,business - Abstract
Background A cross-sectional survey was performed to estimate the prevalence of periportal fibrosis in children based on ultrasound examination in the Marolambo district of the Atsinanana region of Madagascar. This is a remote area known to have a high prevalence of intestinal schistosomiasis. Methods School-aged children (5–14 y) were selected from six villages for parasitological and sonographic examination. Circulating cathodic antigen (CCA) tests and Kato Katz (KK) stool microscopy were performed. Video-clips of liver views were recorded with a SonoSite iViz and interpreted in the UK by comparison with standardised images (WHO protocol). Results The prevalence of schistosomiasis according to CCA testing was 97.8% (269/275) and 73.8% (203/275) by KK. Sonographic evidence of periportal fibrosis was observed in 11.3% (31/275). The youngest children with fibrosis were aged 6 y. Fibrosis was more common in older children (p=0.03) but was not associated with either infection intensity category (p=0.07) or gender (p=0.67). Conclusions Findings of periportal fibrosis among children in these hard-to-reach villages suggests chronic Schistosoma mansoni infection from a very young age. This may reflect other similarly remote schistosomiasis-endemic areas and reinforces the need to investigate morbidity in neglected communities to understand the true extent of disease burden in endemic countries.
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- 2019
20. Schistosomiasis-associated pulmonary arterial hypertension: a systematic review
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Marc Humbert, Daniela Knafl, Christian Gerges, Charles H. King, and Amaya L. Bustinduy
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Pulmonary and Respiratory Medicine ,medicine.medical_specialty ,Cardiac output ,Cardiac index ,Hemodynamics ,030204 cardiovascular system & hematology ,Pulmonary Artery ,Risk Assessment ,03 medical and health sciences ,0302 clinical medicine ,Risk Factors ,Internal medicine ,medicine.artery ,polycyclic compounds ,medicine ,Animals ,Humans ,Schistosomiasis ,Arterial Pressure ,Familial Primary Pulmonary Hypertension ,Associated Pulmonary Arterial Hypertension ,lcsh:RC705-779 ,Pulmonary Arterial Hypertension ,business.industry ,lcsh:Diseases of the respiratory system ,Prognosis ,Blood pressure ,medicine.anatomical_structure ,030228 respiratory system ,Pulmonary artery ,Cardiology ,Vascular resistance ,Complication ,business - Abstract
Schistosomiasis-associated pulmonary arterial hypertension (Sch-PAH) is a life-threatening complication of chronic hepatosplenic schistosomiasis. It is suggested to be the leading cause of pulmonary arterial hypertension (PAH) worldwide. However, pathophysiological data on Sch-PAH are scarce. We examined the hypothesis that there are pronounced similarities in pathophysiology, haemodynamics, and survival of Sch-PAH and idiopathic PAH (iPAH).This systematic review and meta-analysis was registered in the PROSPERO database (identifier CRD42018104066). A systematic search and review of the literature was performed according to PRISMA guidelines for studies published between 01 January 1990 and 29 June 2018.For Sch-PAH, 18 studies evaluating pathophysiological mechanisms, eight studies on haemodynamics (n=277), and three studies on survival (n=191) were identified. 16 clinical registries reporting data on haemodynamics and survival including a total of 5792 patients with iPAH were included for comparison. Proinflammatory molecular pathways are involved in both Sch-PAH and iPAH. The transforming growth factor (TGF)-β signalling pathway is upregulated in Sch-PAH and iPAH. While there was no difference in mean pulmonary artery pressure (54±17 mmHg versus 55±15 mmHg, p=0.29), cardiac output (4.4±1.3 L·min−1versus 4.1±1.4 L·min−1, p=0.046), and cardiac index (2.6±0.7 L·min−1·m−2versus 2.3±0.8 L·min−1·m−2, pversus 13±7 Woods units, pSch-PAH and iPAH share common pathophysiological mechanisms related to inflammation and the TGF-β signalling pathway. Patients with Sch-PAH show a significantly better haemodynamic profile and survival than patients with iPAH.
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- 2019
21. Schistosomiasis in Africa : improving strategies for long-term and sustainable morbidity control
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Louis Albert Tchuem Tchuenté, Jutta Reinhard-Rupp, Nana Kwadwo Biritwum, Jürg Utzinger, Michael D. French, Yaobi Zhang, Narcis B. Kabatereine, Anouk N. Gouvras, W. Evan Secor, Simon Brooker, David Rollinson, Fiona M. Fleming, Maria Rebollo Polo, Charles H. King, Johannes Waltz, Darin S. Evans, and Amaya L. Bustinduy
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Schistosoma Mansoni ,Global Health ,Geographical Locations ,0302 clinical medicine ,Global health ,Medicine and Health Sciences ,Schistosomiasis ,Public and Occupational Health ,030212 general & internal medicine ,Schistosoma haematobium ,biology ,lcsh:Public aspects of medicine ,Neglected Diseases ,Eukaryota ,11 Medical And Health Sciences ,Viewpoints ,Infectious Diseases ,Helminth Infections ,Schistosoma ,Schistosoma mansoni ,Anatomy ,Neglected Tropical Diseases ,lcsh:Arctic medicine. Tropical medicine ,lcsh:RC955-962 ,030231 tropical medicine ,MEDLINE ,03 medical and health sciences ,Age groups ,Tropical Medicine ,Environmental health ,Helminths ,medicine ,Parasitic Diseases ,Animals ,Humans ,business.industry ,Public Health, Environmental and Occupational Health ,Organisms ,Biology and Life Sciences ,lcsh:RA1-1270 ,06 Biological Sciences ,medicine.disease ,biology.organism_classification ,Tropical Diseases ,Invertebrates ,Schistosoma Haematobium ,Term (time) ,Health Care ,Gastrointestinal Tract ,Age Groups ,Africa ,People and Places ,Population Groupings ,Morbidity ,Health Statistics ,business ,Digestive System - Abstract
Schistosomiasis affects over 200 million people worldwide [1] and accounts for an estimated 1.9 million disability-adjusted life years (DALYs) annually [2], with 90% of the burden currently concentrated in Africa. The last decade has witnessed an extraordinary surge of advocacy and funding for neglected tropical diseases (NTDs), including schistosomiasis. Large-scale schistosomiasis control is now implemented in 30 countries in Africa [1], funded primarily through support from the United States Agency for International Development (USAID) and the Department for International Development (DFID), private philanthropic funds from the END Fund and through GiveWell recommendations, and leveraging praziquantel donations from Merck KGaA. However, the number of people still requiring treatment remains daunting [1]. The aim of current public health strategies for schistosomiasis is to decrease morbidity through preventive chemotherapy (PC) (Fig 1) [3]. Periodic large-scale administration of the drug praziquantel focusing on the school-aged population and high-risk adults aims to reduce the prevalence and intensity of infection [4].
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- 2018
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22. One hundred years of neglect in paediatric schistosomiasis
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Amaya L. Bustinduy, Stephen Wright, Charles H. King, Jutta Reinhard-Rupp, Elizabeth Joekes, Narcis B. Kabatereine, and J. Russell Stothard
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0301 basic medicine ,medicine.medical_specialty ,wz_64 ,media_common.quotation_subject ,030231 tropical medicine ,wa_395 ,Schistosomiasis ,Colonialism ,Neglect ,03 medical and health sciences ,0302 clinical medicine ,Schistosomiasis control ,Tropical Medicine ,medicine ,wz_80 ,Urogenital Schistosomiasis ,Humans ,wz_40 ,Mass drug administration ,Child ,Schistosoma ,media_common ,biology ,business.industry ,Public health ,Imperial unit system ,wc_810 ,History, 20th Century ,biology.organism_classification ,medicine.disease ,United Kingdom ,wa_320 ,Surgery ,ws_200 ,030104 developmental biology ,Infectious Diseases ,Family medicine ,Child, Preschool ,Animal Science and Zoology ,Parasitology ,Public Health ,business ,ws_100 - Abstract
SUMMARYEarly in the history of schistosomiasis research, children under 5 years of age were known to be infected. Although this problem was recognized over 100 years ago, insufficient action has been taken to address this issue. Under current policy, such infected children only receive their first antiparasitic treatment (praziquantel – PZQ) upon entry into primary school as current mass drug administration programmes typically target school-aged children. For many infected children, they will wait up to 6 years before receiving their first medication and significant schistosomiasis-related morbidity may have already established. This inequity would not be accepted for other diseases. To unveil some of the reasons behind this neglect, it is paramount to understand the intricate historical relationship between schistosomiasis and British Imperial medicine, to underline its lasting influence on today's public health priorities. This review presents a perspective on the historical neglect of paediatric schistosomiasis, focusing on important gaps that persist from the early days after discovery of this parasite. Looking to end this inequity, we address several issues that need to be overcome to move forward towards the lasting success of schistosomiasis control and elimination efforts.
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- 2017
23. Human schistosomiasis
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Daniel G Colley, Amaya L Bustinduy, W Evan Secor, and Charles H King
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Adult ,Male ,Immunity, Cellular ,Life Cycle Stages ,Adolescent ,Infant ,General Medicine ,Middle Aged ,Global Health ,Article ,Schistosomicides ,Young Adult ,Age Distribution ,Cost of Illness ,Child, Preschool ,Communicable Disease Control ,Animals ,Humans ,Schistosoma ,Schistosomiasis ,Female ,Child ,Parasite Egg Count ,Aged - Abstract
Human schistosomiasis-or bilharzia-is a parasitic disease caused by trematode fl ukes of the genus Schistosoma. By conservative estimates, at least 230 million people worldwide are infected with Schistosoma spp. Adult schistosome worms colonise human blood vessels for years, successfully evading the immune system while excreting hundreds to thousands of eggs daily, which must either leave the body in excreta or become trapped in nearby tissues. Trapped eggs induce a distinct immune-mediated granulomatous response that causes local and systemic pathological eff ects ranging from anaemia, growth stunting, impaired cognition, and decreased physical fi tness, to organ-specifi c eff ects such as severe hepatosplenism, periportal fi brosis with portal hypertension, and urogenital infl ammation and scarring. At present, preventive public health measures in endemic regions consist of treatment once every 1 or 2 years with the isoquinolinone drug, praziquantel, to suppress morbidity. In some locations, elimination of transmission is now the goal; however, more sensitive diagnostics are needed in both the fi eld and clinics, and integrated environmental and health-care management will be needed to ensure elimination. © Chataway et al. Open Access article distributed under the terms of CC BY.
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- 2014
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24. Preventive chemotherapy for schistosomiasis and soil-transmitted helminthiasis by cotreatment with praziquantel and albendazole
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Amaya L. Bustinduy, Antonio Montresor, and J. Russell Stothard
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Pediatrics ,medicine.medical_specialty ,Trichuriasis ,business.industry ,Helminthiasis ,Schistosomiasis ,Soil-transmitted helminthiasis ,General Medicine ,medicine.disease ,Albendazole ,Praziquantel ,Deworming ,Ascariasis ,Immunology ,medicine ,business ,medicine.drug - Abstract
In disease-endemic areas, preventive chemotherapy with two orally administered anthelminthic drugs, praziquantel and albendazole, forms the foundation of control of schistosomiasis and soil-transmitted helminthiasis. Where diseases overlap, these two drugs are typically co-administered simultaneously, although albendazole is often interchangeable with mebendazole. With a supportive pharmaceutical industry that donates drugs and a strong international partnership that mobilizes donor funds for drug delivery, scale-up of treatment in school-aged children has expanded significantly in line with the WHO 2012–2020 strategic plan. Other high-risk groups, such as pre-school-aged children, are now benefiting from deworming campaigns conducted alongside other childhood interventions, such as vaccination, less so, however, for schistosomiasis as infections in this age class are not being treated. Looking to the future, maintaining an effective drug distribution and reporting system that regularly checks anthelminth...
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- 2014
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25. A call to strengthen the global strategy against schistosomiasis and soil-transmitted helminthiasis: the time is now
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Charles H. King, David G. Addiss, Amaya L. Bustinduy, Jason R. Andrews, Jürg Utzinger, Isaac I. Bogoch, Lorenzo Savioli, Alan Fenwick, Peter J. Hotez, J. Russell Stothard, Giovanna Raso, Eran Bendavid, Daniel G. Colley, Darin S. Evans, Jean T. Coulibaly, William Lin, Nathan Lo, and David H. Molyneux
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Veterinary medicine ,030231 tropical medicine ,Population ,Helminthiasis ,Schistosomiasis ,Guidelines as Topic ,Global Health ,Article ,03 medical and health sciences ,Soil ,0302 clinical medicine ,Environmental health ,Global health ,Medicine ,Humans ,030212 general & internal medicine ,education ,Disease burden ,Africa South of the Sahara ,Anthelmintics ,education.field_of_study ,business.industry ,Global strategy ,Soil-transmitted helminthiasis ,medicine.disease ,Quality-adjusted life year ,Infectious Diseases ,Quality-Adjusted Life Years ,Morbidity ,business - Abstract
In 2001, the World Health Assembly (WHA) passed the landmark WHA 54.19 resolution for global scale-up of mass administration of anthelmintic drugs for morbidity control of schistosomiasis and soil-transmitted helminthiasis, which affect more than 1·5 billion of the world's poorest people. Since then, more than a decade of research and experience has yielded crucial knowledge on the control and elimination of these helminthiases. However, the global strategy has remained largely unchanged since the original 2001 WHA resolution and associated WHO guidelines on preventive chemotherapy. In this Personal View, we highlight recent advances that, taken together, support a call to revise the global strategy and guidelines for preventive chemotherapy and complementary interventions against schistosomiasis and soil-transmitted helminthiasis. These advances include the development of guidance that is specific to goals of morbidity control and elimination of transmission. We quantify the result of forgoing this opportunity by computing the yearly disease burden, mortality, and lost economic productivity associated with maintaining the status quo. Without change, we estimate that the population of sub-Saharan Africa will probably lose 2·3 million disability-adjusted life-years and US$3·5 billion of economic productivity every year, which is comparable to recent acute epidemics, including the 2014 Ebola and 2015 Zika epidemics. We propose that the time is now to strengthen the global strategy to address the substantial disease burden of schistosomiasis and soil-transmitted helminthiasis.
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- 2016
26. Impact of Drought on the Spatial Pattern of Transmission of Schistosoma haematobium in Coastal Kenya
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Amaya L. Bustinduy, Eric M. Muchiri, Uriel Kitron, Peter Mungai, Francis M. Mutuku, and Charles H. King
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Adolescent ,Rain ,Severity of Illness Index ,law.invention ,Disasters ,Schistosomiasis haematobia ,Young Adult ,Extreme weather ,Age groups ,law ,Virology ,parasitic diseases ,Prevalence ,Animals ,Humans ,Bulinus ,Child ,Schistosoma haematobium ,biology ,Ecology ,fungi ,Age Factors ,Articles ,biology.organism_classification ,Kenya ,Droughts ,Infectious Diseases ,Transmission (mechanics) ,Schistosoma haematobium infection ,Child, Preschool ,Spatial ecology ,Common spatial pattern ,Parasitology - Abstract
We analyzed temporal changes in spatial patterns of active Schistosoma haematobium infection in different age groups and associated them with ponds infested with Bulinus snails. A major drought between 2001 and 2009 resulted in drying of ponds that were known sources of infection, and we detected very few or no snails in ponds that were infested in the past. The household-level spatial pattern of infection for children of various age groups in 2009 was contrasted with historical data from 2000. The significant local clustering of high- and low-infection levels among school-aged children that occurred in 2000 was absent in 2009. We attribute the disappearance of significant clustering around historical transmission hot spots to a decade-long drought in our study area. The implications of extreme weather and climate conditions on risk and transmission of S. haematobium and their relevance to control strategies are discussed. Copyright © 2011 by The American Society of Tropical Medicine and Hygiene.
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- 2011
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27. Endomyocardial Fibrosis (EMF) in a Ugandan Child with Advanced Hepatosplenic Schistosomiasis: Coincidence or Connection?
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Neil Stone, J. Russell Stothard, Kenneth Luzinda, Amaya L. Bustinduy, Stephen Wright, Philip Gothard, and Simon Mpoya
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Male ,Pathology ,medicine.medical_specialty ,animal structures ,Vasodilator Agents ,Endomyocardial fibrosis ,Biology ,Praziquantel ,Feces ,Virology ,parasitic diseases ,medicine ,Animals ,Humans ,Uganda ,Child ,Splenic Diseases ,Anthelmintics ,Liver Diseases ,Hepatosplenic schistosomiasis ,Schistosoma mansoni ,Articles ,Endomyocardial Fibrosis ,biology.organism_classification ,Propranolol ,Schistosomiasis mansoni ,Infectious Diseases ,Periportal fibrosis ,Vasodilator agents ,Parasitology - Abstract
An association between late-stage hepatosplenic schistosomiasis and endomyocardial fibrosis (EMF) has been suggested but not proven. We present the case of a 12-year-old Ugandan boy with striking comorbidities, including advanced periportal fibrosis caused by Schistosoma mansoni infection and right ventricular EMF, and discuss the possible correlation between both diseases.
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- 2014
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28. Soil-transmitted Helminth Infection, Loss of Education and Cognitive Impairment in School-Aged Children: A Systematic Review and Meta-Analysis
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Amaya L. Bustinduy, Amara E. Ezeamama, Leonardo Martinez, Michael J. Boivin, Noel Pabalan, Charles H. King, and Allan Nkwata
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Psychometrics ,Intelligence ,Social Sciences ,Pediatrics ,Praziquantel ,Families ,Cognition ,Learning and Memory ,0302 clinical medicine ,Sociology ,Innate intelligence ,Medicine and Health Sciences ,Schistosomiasis ,Psychology ,Medicine ,030212 general & internal medicine ,Child ,Children ,Anthelmintics ,Cognitive Impairment ,Schistosoma haematobium ,Schools ,biology ,Learning Disabilities ,Cognitive Neurology ,lcsh:Public aspects of medicine ,Attendance ,Eukaryota ,Infectious Diseases ,Neurology ,Child, Preschool ,Meta-analysis ,Schistosoma ,Pediatric Infections ,Research Article ,Clinical psychology ,lcsh:Arctic medicine. Tropical medicine ,Adolescent ,lcsh:RC955-962 ,Cognitive Neuroscience ,030231 tropical medicine ,Memory and Learning Tests ,Education ,03 medical and health sciences ,Memory ,Helminths ,Reaction Time ,Animals ,Humans ,Learning ,Cognitive Dysfunction ,Memory Disorders ,business.industry ,Organisms ,Cognitive Psychology ,Public Health, Environmental and Occupational Health ,Biology and Life Sciences ,lcsh:RA1-1270 ,biology.organism_classification ,Invertebrates ,Schistosoma Haematobium ,Confidence interval ,Age Groups ,People and Places ,Cognitive Science ,Population Groupings ,Observational study ,business ,Neuroscience - Abstract
Background By means of meta-analysis of information from all relevant epidemiologic studies, we examined the hypothesis that Schistosoma infection in school-aged children (SAC) is associated with educational loss and cognitive deficits. Methodology/Principal findings This review was prospectively registered in the PROSPERO database (CRD42016040052). Medline, Biosis, and Web of Science were searched for studies published before August 2016 that evaluated associations between Schistosoma infection and cognitive or educational outcomes. Cognitive function was defined in four domains—learning, memory, reaction time, and innate intelligence. Educational outcome measures were defined as attendance and scholastic achievement. Risk of bias (ROB) was evaluated using the Newcastle-Ottawa quality assessment scale. Standardized mean differences (SMD) and 95% confidence intervals (CI) were calculated to compare cognitive and educational measures for Schistosoma infected /not dewormed vs. uninfected/dewormed children. Sensitivity analyses by study design, ROB, and sequential exclusion of individual studies were implemented. Thirty studies from 14 countries, including 38,992 SAC between 5–19 years old, were identified. Compared to uninfected children and children dewormed with praziquantel, the presence of Schistosoma infection and/or non-dewormed status was associated with deficits in school attendance (SMD = -0.36, 95%CI: -0.60, -0.12), scholastic achievement (SMD = -0.58, 95%CI: -0.96, -0.20), learning (SMD = -0.39, 95%CI: -0.70, -0.09) and memory (SMD = -0.28, 95%CI: -0.52, -0.04) tests. By contrast, Schistosoma-infected/non-dewormed and uninfected/dewormed children were similar with respect to performance in tests of reaction time (SMD = -0.06, 95%CI: -0.42, 0.30) and intelligence (SMD = -0.25, 95%CI: -0.57, 0.06). Schistosoma infection-associated deficits in educational measures were robust among observational studies, but not among interventional studies. The significance of infection-associated deficits in scholastic achievement was sensitive to ROB. Schistosoma infection-related deficits in learning and memory tests were invariant by ROB and study design. Conclusion/Significance Schistosoma infection/non-treatment was significantly associated with educational, learning, and memory deficits in SAC. Early treatment of children in Schistosoma-endemic regions could potentially mitigate these deficits. Trial registration ClinicalTrials.gov CRD42016040052, Author summary Empirical evidence for cognitive or educational benefits of anti-Schistosoma treatment is currently uncertain, despite the recommended practice of wide-scale deworming with praziquantel. We addressed this knowledge gap by synthesizing information from 30 relevant epidemiologic studies reporting on 38,992 children between 5–19 years old from 14 countries. In those studies, Schistosoma infection or non-dewormed status was associated with educational loss and cognitive deficits. Specifically, there were small to moderate deficits in both school attendance and scholastic achievement. Similarly, Schistosoma infection or non-dewormed status was associated with deficits in learning and memory domains of psychometrically tested cognitive function. However, there was no evidence of Schistosoma infection- or non-deworming-associated deficits on tests of innate intelligence or reaction-time. Overall, compared to Schistosoma-uninfected or to dewormed children, the presence of Schistosoma infection or non-dewormed status was associated with educational, learning, and memory deficits in school-aged children. The combined evidence suggests that early treatment of children in Schistosoma-endemic regions could mitigate these deficits.
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- 2018
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29. Diagnostics for schistosomiasis in Africa and Arabia: a review of present options in control and future needs for elimination
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Amaya L. Bustinduy, Michelle C. Stanton, David Rollinson, Fiona Allan, David Waterhouse, Ziad A. Memish, José Carlos Sousa-Figueiredo, J. Russell Stothard, Amir Hassan, Mohammad A. Al-Helal, Steve A. Ward, Martha Betson, and Govert J. van Dam
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Male ,Time Factors ,Intestinal schistosomiasis ,Kingdom of Saudi Arabia ,Control (management) ,Saudi Arabia ,morbidity markers ,Schistosomiasis ,Context (language use) ,Disease ,rapid diagnostic test ,World health ,Praziquantel ,Medicine ,Animals ,Humans ,Disease Eradication ,intestinal schistosomiasis ,Anthelmintics ,Rapid diagnostic test ,business.industry ,Diagnostic Tests, Routine ,urogenital schistosomiasis ,medicine.disease ,Infectious Diseases ,Risk analysis (engineering) ,Immunology ,Africa ,Schistosoma ,Animal Science and Zoology ,Parasitology ,point-of-contact ,Female ,business ,Strengths and weaknesses - Abstract
SUMMARYWithin the World Health Organization 2012–2020 roadmap for control and elimination of schistosomiasis, the scale-up of mass drug administration with praziquantel is set to change the epidemiological landscape across Africa and Arabia. Central in measuring progress is renewed emphasis upon diagnostics which operate at individual, community and environmental levels by assessing reductions in disease, infections and parasite transmission. However, a fundamental tension is revealed between levels for present diagnostic tools, and methods applied in control settings are not necessarily adequate for application in elimination scenarios. Indeed navigating the transition from control to elimination needs careful consideration and planning. In the present context of control, we review current options for diagnosis of schistosomiasis at different levels, highlighting several strengths and weaknesses therein. Future challenges in elimination are raised and we propose that more cost-effective diagnostics and clinical staging algorithms are needed. Using the Kingdom of Saudi Arabia as a contemporary example, embedding new diagnostic methods within the primary care health system is discussed with reference to both urogenital and intestinal schistosomiasis.
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- 2014
30. Parasitic Helminths
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Amaya L. Bustinduy and Charles H. King
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- 2014
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31. HIV and schistosomiasis co-infection in African children
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Amaya L. Bustinduy, Sarah C Appleton, José Carlos Sousa-Figueiredo, Janet T Scott, J. Russell Stothard, Charles H. King, and Martha Betson
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medicine.medical_specialty ,business.industry ,Coinfection ,Psychological intervention ,Human immunodeficiency virus (HIV) ,Schistosomiasis ,HIV Infections ,medicine.disease ,medicine.disease_cause ,Infectious Diseases ,Acquired immunodeficiency syndrome (AIDS) ,Risk Factors ,Environmental health ,Epidemiology ,Immunology ,Africa ,Medicine ,Humans ,business ,Hiv transmission ,Child ,Disease burden ,Co infection - Abstract
HIV/AIDS and schistosomiasis both cause a substantial disease burden in sub-Saharan Africa and the two diseases often overlap in their epidemiological characteristics. Although disease-specific control interventions are continuing, potential synergies in the control efforts for these two diseases have not been investigated. With a focus on children with schistosomiasis, we assess the risk for increased HIV transmission, HIV progression, and impaired response to drugs when given alongside HIV interventions. A new research agenda tailored to children is needed to better understand the interactions of these two diseases and the potential for combined responses.
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- 2014
32. Schistosomiasis
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Amaya L. Bustinduy and Charles H. King
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- 2014
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33. Fecal occult blood and fecal calprotectin as point-of-care markers of intestinal morbidity in Ugandan children with Schistosoma mansoni infection
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Martha Betson, Narcis B. Kabatereine, Alan Fenwick, José Carlos Sousa-Figueiredo, J. Russell Stothard, Moses Adriko, and Amaya L. Bustinduy
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Male ,medicine.medical_specialty ,lcsh:Arctic medicine. Tropical medicine ,Anemia ,lcsh:RC955-962 ,030231 tropical medicine ,Schistosomiasis ,Inflammatory bowel disease ,Gastroenterology ,03 medical and health sciences ,Feces ,0302 clinical medicine ,Internal medicine ,parasitic diseases ,medicine ,Animals ,Humans ,030212 general & internal medicine ,Child ,qy_160 ,biology ,lcsh:Public aspects of medicine ,Fecal occult blood ,Public Health, Environmental and Occupational Health ,ws_20 ,lcsh:RA1-1270 ,wc_810 ,Schistosoma mansoni ,medicine.disease ,biology.organism_classification ,Schistosomiasis mansoni ,3. Good health ,Praziquantel ,Intestines ,Infectious Diseases ,qx_355 ,Child, Preschool ,Occult Blood ,Immunology ,Female ,Calprotectin ,Leukocyte L1 Antigen Complex ,medicine.drug ,Research Article - Abstract
Background Calprotectin is a calcium-binding cytoplasmic protein found in neutrophils and increasingly used as a marker of bowel inflammation. Fecal occult blood (FOB) is also a dependable indicator of bowel morbidity. The objective of our study was to determine the applicability of these tests as surrogate markers of Schistosoma mansoni intestinal morbidity before and after treatment with praziquantel (PZQ). Methods 216 children (ages 3–9 years old) from Buliisa District in Lake Albert, Uganda were examined and treated with PZQ at baseline in October 2012 with 211 of them re-examined 24 days later for S. mansoni and other soil transmitted helminths (STH). POC calprotectin and FOB assays were performed at both time points on a subset of children. Associations between the test results and infection were analysed by logistic regression. Results Fecal calprotectin concentrations of 150–300 µg/g were associated with S. mansoni egg patent infection both at baseline and follow up (OR: 12.5 P = 0.05; OR: 6.8 P = 0.02). FOB had a very strong association with baseline anemia (OR: 9.2 P = 0.03) and medium and high egg intensity schistosomiasis at follow up (OR: 6.6 P = 0.03; OR: 51.3 P = 0.003). Both tests were strongly associated with heavy intensity S. mansoni infections. There was a significant decrease in FOB and calprotectin test positivity after PZQ treatment in those children who had egg patent schistosomiasis at baseline. Conclusions Both FOB and calprotectin rapid assays were found to correlate positively and strongly with egg patent S. mansoni infection with a positive ameloriation response after PZQ treatment indicative of short term reversion of morbidity. Both tests were appropriate for use in the field with excellent operational performance and reliability. Due to its lower-cost which makes its scale-up of use affordable, FOB could be immediately adopted as a monitoring tool for PC campaigns for efficacy evaluation before and after treatment., Author Summary The severity of intestinal schistosomiasis, a disease caused by Schistosoma mansoni infection, is likely under-reported in part due to the scarcity of field-appropriate morbidity markers. Downstream potential complications of this disease include anemia, failure to thrive, and chronic multi-organ damage. Point-of-care (POC) tools to monitor intestinal schistosomiasis in low resource settings are urgently needed to better quantify the burden of disease in endemic countries and to gauge the clinical impact of scale-up of preventive PC. For the present study in rural Uganda, fecal occult blood and fecal calprotectin were identified as potential surrogate markers of intestinal morbidity. We tested both POC tests and found that they were both associated with active schistosomiasis as detected by eggs in stool with significant decrease in test positivity after PZQ treatment demonstrating short term morbidity reversion. Calprotectin was a strong indicator of intestinal inflammation, however, owing to its high per-test price makes it difficult to scale-up accordingly. Conversely, fecal occult blood was technically feasible, low-cost and had optimal performance as a morbidity marker, hence we strongly advocate for its immediate inclusion as a monitoring tool for PC programs.
- Published
- 2013
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