110 results on '"Robert D. Newman"'
Search Results
2. Rage and Beauty
- Author
-
Robert D. Newman
- Subjects
Aesthetics ,media_common.quotation_subject ,Beauty ,Art ,Rage (emotion) ,Democracy ,media_common - Published
- 2019
- Full Text
- View/download PDF
3. Gavi’s Transition Policy: Moving From Development Assistance To Domestic Financing Of Immunization Programs
- Author
-
Helen Saxenian, Robert D. Newman, Judith Kallenberg, Wilson Mok, Theresa Ryckman, Aurélia Nguyen, and Paul Wilson
- Subjects
Economic growth ,International Cooperation ,Developing country ,Global Health ,03 medical and health sciences ,0302 clinical medicine ,Global health ,Economics ,Financial Support ,Humans ,030212 general & internal medicine ,Cooperative Behavior ,Developing Countries ,Health policy ,Finance ,Vaccines ,Immunization Programs ,business.industry ,030503 health policy & services ,Health Policy ,Immunization (finance) ,Gross national income ,Sustainability ,Immunization ,Cooperative behavior ,0305 other medical science ,business - Abstract
Gavi, the Vaccine Alliance, was created in 2000 to accelerate the introduction of new and underused vaccines in lower-income countries. The period 2000-15 was marked by the rapid uptake of new vaccines in more than seventy countries eligible for Gavi support. To stay focused on the poorest countries, Gavi's support phases out after countries' gross national income per capita surpasses a set threshold, which requires governments to assume responsibility for the continued financing of vaccines introduced with Gavi support. Gavi's funding will end in the period 2016-20 for nineteen countries that have exceeded the eligibility threshold. To avoid disrupting lifesaving immunization programs and to ensure the long-term sustainable impact of Gavi's investments, it is vital that governments succeed in transitioning from development assistance to domestic financing of immunization programs. This article discusses some of the challenges facing countries currently transitioning out of Gavi support, how Gavi's policies have evolved to help manage the risks involved in this process, and the lessons learned from this experience.
- Published
- 2016
- Full Text
- View/download PDF
4. Notes from the Field: Public Health Response to a Human Immunodeficiency Virus Outbreak Associated with Unsafe Injection Practices - Roka Commune, Cambodia, 2016
- Author
-
Sok Srun, Bakary Drammeh, Anindya K. De, Selenic Dejana, Vanthy Ly, Hoy Vannara, Renuka Gadde, Naomi Bock, Ugonna C Ijeoma, Sou Sanith, Ahmed Saadani Hassani, Sin Sansam, Tek Sopheap, Johnita Byrd, and Robert D. Newman
- Subjects
0301 basic medicine ,medicine.medical_specialty ,Health (social science) ,Epidemiology ,Health, Toxicology and Mutagenesis ,MEDLINE ,Human immunodeficiency virus (HIV) ,HIV Infections ,medicine.disease_cause ,Disease Outbreaks ,Injections ,03 medical and health sciences ,0302 clinical medicine ,Health Information Management ,Environmental health ,Medicine ,Humans ,030212 general & internal medicine ,business.industry ,Field (Bourdieu) ,Public health ,Outbreak ,General Medicine ,030112 virology ,Public Health Practice ,business ,Cambodia ,Notes from the Field - Published
- 2018
5. The Role of Micro Algae in Removal of Selenate from Subsurface Tile Drainage
- Author
-
David F. Von Hippel, F. Bailey Green, Yakup Nurdogan, Christine S. Tarn, William J. Oswald, Robert D. Newman, Matthew B. Gerhardt, Leslie Shown, and Paris Honglay Chen
- Subjects
chemistry.chemical_compound ,chemistry ,Algae ,biology ,Tile drainage ,Environmental chemistry ,Environmental science ,biology.organism_classification ,Selenate - Published
- 2018
- Full Text
- View/download PDF
6. A research agenda for malaria eradication: drugs
- Author
-
R Chandra, Quique Bassat, Janice Culpepper, François Nosten, J Nájera, Dyann F. Wirth, J Pottage, Christopher V. Plowe, Ramanan Laxminarayan, Pascal Ringwald, C Marzetta, Steve A. Ward, Pedro L. Alonso, Peter G. Kremsner, MacArthur, Mark M. Fukuda, R. Sinden, Theonest K. Mutabingwa, Ivo Mueller, Alan J. Magill, Y Yuthavong, Jessica Milman, Nicholas J. White, Thomas E. Wellems, Regina Rabinovich, Abdoulaye Djimde, Rhoel R. Dinglasan, C Ohrt, Dennis Shanks, Ric N. Price, Stephan Duparc, Fred Binka, K Duncan, Marcel Tanner, H Vial, Robert D. Newman, Solomon Nwaka, Shunmay Yeung, A. Serazin, Thomas G. Brewer, Timothy N. C. Wells, and Myaing M. Nyunt
- Subjects
Insecticides ,Plasmodium ,Mosquito Control ,Plasmodium vivax ,Drug Resistance ,lcsh:Medicine ,Review ,Parasitemia ,Lactones ,Pregnancy ,Recurrence ,Mass treatment ,Pregnancy Complications, Infectious ,Child ,health care economics and organizations ,media_common ,Travel ,biology ,Transmission (medicine) ,General Medicine ,humanities ,Artemisinins ,Aminoquinolines ,Female ,Drug ,Adult ,medicine.medical_specialty ,Asia ,media_common.quotation_subject ,macromolecular substances ,Antimalarials ,Malaria transmission ,Species Specificity ,Malaria elimination ,Anopheles ,Malaria Vaccines ,parasitic diseases ,medicine ,Animals ,Humans ,Intensive care medicine ,Contraindications ,Research ,lcsh:R ,Plasmodium falciparum ,social sciences ,biology.organism_classification ,medicine.disease ,Insect Vectors ,Malaria ,Glucosephosphate Dehydrogenase Deficiency ,Infectious Diseases/Neglected Tropical Diseases ,Immunology ,Africa ,Program Evaluation - Abstract
The Malaria Eradication Research Agenda (malERA) Consultative Group on Drugs present a research and development agenda to ensure that appropriate drugs are available for use in malaria eradication., Antimalarial drugs will be essential tools at all stages of malaria elimination along the path towards eradication, including the early control or “attack” phase to drive down transmission and the later stages of maintaining interruption of transmission, preventing reintroduction of malaria, and eliminating the last residual foci of infection. Drugs will continue to be used to treat acute malaria illness and prevent complications in vulnerable groups, but better drugs are needed for elimination-specific indications such as mass treatment, curing asymptomatic infections, curing relapsing liver stages, and preventing transmission. The ideal malaria eradication drug is a coformulated drug combination suitable for mass administration that can be administered in a single encounter at infrequent intervals and that results in radical cure of all life cycle stages of all five malaria species infecting humans. Short of this optimal goal, highly desirable drugs might have limitations such as targeting only one or two parasite species, the priorities being Plasmodium falciparum and Plasmodium vivax. The malaria research agenda for eradication should include research aimed at developing such drugs and research to develop situation-specific strategies for using both current and future drugs to interrupt malaria transmission.
- Published
- 2016
7. Associations between Peripheral Plasmodium falciparum Malaria Parasitemia, Human Immunodeficiency Virus, and Concurrent Helminthic Infection among Pregnant Women in Malawi
- Author
-
Peter N. Kazembe, Carl H. Campbell, Monica E. Parise, Allan Macheso, Richard W. Steketee, Scott J Filler, Robert D. Newman, Michael C. Thigpen, and Mary J. Hamel
- Subjects
Malawi ,medicine.medical_specialty ,Adolescent ,Anti-HIV Agents ,Plasmodium falciparum ,Helminthiasis ,HIV Infections ,Schistosomiasis ,Parasitemia ,Antimalarials ,Young Adult ,Acquired immunodeficiency syndrome (AIDS) ,Pregnancy ,Risk Factors ,Virology ,parasitic diseases ,Odds Ratio ,medicine ,Animals ,Humans ,Malaria, Falciparum ,Schistosoma ,Anthelmintics ,biology ,Articles ,medicine.disease ,biology.organism_classification ,Infectious Diseases ,Tropical medicine ,Immunology ,Female ,Parasitology ,Malaria - Abstract
Approximately 2 billion persons worldwide are infected with schistosomiasis and soil-transmitted helminthes (STH), many in areas where endemic malaria transmission coexists. Few data exist on associations between these infec- tions. Nested within a larger clinical trial, primigravid and secundigravid women provided blood samples for human immu- nodeficiency virus (HIV) testing and peripheral malaria films and stool and urine for evaluation of STH and Schistosoma spp. during their initial antenatal clinic visit. The most common parasitic infections were malaria (37.6%), S. haematobium (32.3%), and hookworm (14.4%); 14.2% of women were HIV-infected. S. haematobium infection was associated with lower malarial parasite densities (344 versus 557 parasites/μL blood; P < 0.05). In multivariate analysis, HIV and hook- worm infection were independently associated with malaria infection (adjusted odds ratio = 1.9 and 95% confidence interval = 1.2-3.0 for HIV; adjusted odds ratio = 1.9 and 95% confidence interval = 1.03-3.5 for hookworm). Concurrent helminthic infection had both positive and negative effects on malaria parasitemia among pregnant women in Malawi.
- Published
- 2011
- Full Text
- View/download PDF
8. Adenocarcinoma of the small intestine arising in crohn's disease: Demonstration of a tumor-associated antigen in invasive and intraepithelial components
- Author
-
Robert D. Newman, Sidney J. Bennett, and Robert R. Pascal
- Subjects
Cancer Research ,Oncology - Published
- 2010
- Full Text
- View/download PDF
9. Interview: WHO Global Malaria Program: the road ahead
- Author
-
Robert D Newman
- Subjects
International research ,Gerontology ,medicine.medical_specialty ,business.industry ,Epidemic Intelligence Service ,General Medicine ,medicine.disease ,Disease control ,Officer ,Family medicine ,parasitic diseases ,Medicine ,Pharmacology (medical) ,business ,health care economics and organizations ,Malaria - Abstract
Robert D Newman became Head of the WHO Global Malaria Programme in 2009. Previously, Dr Newman was Deputy Chief for Science and Chief of the Program Implementation Unit in the Malaria Branch at the Centers for Disease Control and Prevention (CDC). Dr Newman also served as the CDC Team Lead for the President’s Malaria Initiative. Dr Newman originally joined CDC as an Epidemic Intelligence Service Officer in 2000. During his 9 years at CDC, Dr Newman was dedicated to advancing the science of preventing malaria during pregnancy and infancy in sub-Saharan Africa, and served as the principal investigator for numerous epidemiological studies and clinical trials. Dr Newman has served as a founding member of two large international research consortia, and has published more than 50 peer-reviewed articles on malaria and other infectious diseases.
- Published
- 2010
- Full Text
- View/download PDF
10. In-vivoefficacy of amodiaquine-artesunate in children with uncomplicatedPlasmodium falciparummalaria in western Kenya
- Author
-
Laurence Slutsker, John M. Vulule, Rosalynn Ord, J. I. Thwing, Meredith McMorrow, Meghna Desai, Cally Roper, Kephas Otieno, Robert D. Newman, Simon Kariuki, Mary J. Hamel, Frank Odhiambo, and Chris Odero
- Subjects
medicine.medical_specialty ,Artemether/lumefantrine ,biology ,business.industry ,Public Health, Environmental and Occupational Health ,Plasmodium falciparum ,Amodiaquine ,medicine.disease ,biology.organism_classification ,Lumefantrine ,chemistry.chemical_compound ,Infectious Diseases ,chemistry ,Artesunate ,Chloroquine ,Internal medicine ,parasitic diseases ,Immunology ,medicine ,Parasitology ,Artemether ,business ,Malaria ,medicine.drug - Abstract
Summary objectives To assess the efficacy of amodiaquine-artesunate in an area with high chloroquine resistance in western Kenya. methods Twenty-eight day in-vivo efficacy trial of amodiaquine-artesunate in 103 children aged 6‐59 months in western Kenya with smear-confirmed uncomplicated Plasmodium falciparum malaria. results The 28-day uncorrected adequate clinical and parasitological response (ACPR) was 69.0%, with 15.5% Late Clinical Failure and 15.5% Late Parasitologic Failure rates. The PCR-corrected 28-day ACPR was 90.2%. Clinical risk factors for recurrent infection (recrudescences and reinfections) were lower axillary temperature at enrolment and low weight-for-age Z-score. The presence of single nucleotide polymorphisms pfcrt 76T and pfmdr1 86Y at baseline was associated with increased risk of recurrent infections, both reinfections and recrudescences. conclusion Although artemether-lumefantrine (Coartem � ) is the first line ACT in Kenya, amodiaquine-artesunate is registered as an option for treatment of uncomplicated P. falciparum and remains an
- Published
- 2009
- Full Text
- View/download PDF
11. Pre-departure and Post-arrival Management of P. falciparum Malaria in Refugees Relocating from Sub-Saharan Africa to the United States
- Author
-
Mary J. Hamel, Michelle Weinberg, Robert D. Newman, Martin S. Cetron, William M. Stauffer, Laurence Slutsker, and Louise M. Causer
- Subjects
medicine.medical_specialty ,education.field_of_study ,business.industry ,Refugee ,Public health ,fungi ,Population ,food and beverages ,medicine.disease ,Infectious Diseases ,Environmental protection ,Virology ,Environmental health ,parasitic diseases ,Health care ,medicine ,Parasitology ,education ,business ,Developed country ,Malaria ,Health policy ,Social policy - Abstract
Plasmodium infection, often sub-clinical, is common in migrating sub-Saharan refugee populations. Refugees who subsequently develop clinical malaria suffer illness and exact a cost on state and local health care facilities. Untreated infection is also of public health concern because of the potential for local transmission. In response to increasing numbers of refugees originating in sub-Saharan Africa guidelines for the management of malaria in refugees migrating to the United States have been broadened and updated. The guidelines are based on available evidence-based literature and recent public health experience. These guidelines were critically reviewed, assessed, and approved by multiple National and State entities as well as outside experts. These consensus guidelines recommend that sub-Saharan African refugees relocating to the United States receive presumptive treatment of P. falciparum malaria before departure or during the domestic refugee medical screening after arrival. Presumptive therapy is not currently recommended for either non-falciparum malaria or for refugees relocating from areas outside sub-Saharan Africa.
- Published
- 2008
- Full Text
- View/download PDF
12. Intermittent preventive therapy for malaria: progress and future directions
- Author
-
Andrea Egan, Roly Gosling, Martin P. Grobusch, and Robert D. Newman
- Subjects
Microbiology (medical) ,medicine.medical_specialty ,Intermittent preventive therapy ,business.industry ,Alternative medicine ,MEDLINE ,medicine.disease ,Drug Administration Schedule ,Surgery ,Antimalarials ,Infectious Diseases ,parasitic diseases ,medicine ,Humans ,Malaria, Falciparum ,Intensive care medicine ,business ,Malaria - Abstract
PURPOSE OF REVIEW: This review summarizes recent evidence regarding the efficacy of intermittent preventive treatment with focus on infancy (IPTi) and the rationale behind such a control strategy. RECENT FINDINGS: Pooled safety and efficacy analyses of all six trials of IPTi with sulfadoxine-pyrimethamine conducted between 1999 and 2007 have demonstrated a 30% protective efficacy against clinical malaria, a 24% protective efficacy against all-cause hospital admissions, a 37% protective efficacy against malaria-related hospital admissions, and a 15% protective efficacy against anemia, all in the first year of life. Rebound in malaria following discontinuation of the intervention has not been noted in pooled analyses of the IPTi trials. SUMMARY: Given the efficacy, excellent safety and tolerability of the intervention and the fact that it is inexpensive and easily deliverable if linked to the Expanded Programme on Immunization, IPTi-sulfadoxine-pyrimethamine appears to add a valuable tool to the malaria-control armamentarium in endemic areas of Africa. Routine monitoring of sulfadoxine-pyrimethamine efficacy will be required to guide future IPTi programme implementation. Variations of IPTi that target older children may be required for areas of Africa with highly seasonal malaria transmission
- Published
- 2007
- Full Text
- View/download PDF
13. Safety and Toxicity of Sulfadoxine/Pyrimethamine
- Author
-
Michael C Thigpen, Philip J. Peters, Robert D. Newman, and Monica E. Parise
- Subjects
Pediatrics ,medicine.medical_specialty ,Sulfadoxine ,medicine.medical_treatment ,Plasmodium falciparum ,Population ,Drug Resistance ,Pharmacology ,Toxicology ,Drug Administration Schedule ,Antimalarials ,Pregnancy ,parasitic diseases ,Animals ,Humans ,Medicine ,Pharmacology (medical) ,Malaria, Falciparum ,education ,Kernicterus ,Antibacterial agent ,education.field_of_study ,business.industry ,Infant, Newborn ,Abnormalities, Drug-Induced ,medicine.disease ,Sulfadoxine/pyrimethamine ,Drug Combinations ,Pyrimethamine ,Pregnancy Complications, Parasitic ,Africa ,Female ,business ,Drugs in pregnancy ,Malaria ,medicine.drug - Abstract
Plasmodium falciparum infection during pregnancy is strongly associated with maternal anaemia and low birth weight, contributing to substantial morbidity and mortality in sub-Saharan Africa. Intermittent preventive treatment in pregnancy with sulfadoxine/pyrimethamine (IPTp-SP) has been one of the most effective approaches to reduce the burden of malaria during pregnancy in Africa. IPTp-SP is based on administeringor=2 treatment doses of sulfadoxine/pyrimethamine to pregnant women at predefined intervals after quickening (around 18-20 weeks). Randomised, controlled trials have demonstrated decreased rates of maternal anaemia and low birth weight with this approach. The WHO currently recommends IPTp-SP in malaria-endemic areas of sub-Saharan Africa. However, implementation has been suboptimal in part because of concerns of potential drug toxicities. This review evaluates the toxicity data of sulfadoxine/pyrimethamine, including severe cutaneous adverse reactions, teratogenicity and alterations in bilirubin metabolism. Weekly sulfadoxine/pyrimethamine prophylaxis is associated with rare but potentially fatal cutaneous reactions. Fortunately, sulfadoxine/pyrimethamine use in IPTp programmes in Africa, with 2-4 treatment doses over 6 months, has been well tolerated in multiple IPTp trials. However, sulfadoxine/pyrimethamine should not be administered concurrently with cotrimoxazole given their redundant mechanisms of action and synergistic worsening of adverse drug reactions. Therefore, HIV-infected pregnant women in malaria endemic areas who are already receiving cotrimoxazole prophylaxis should not also receive IPTp-SP. Although folate antagonist use in the first trimester is associated with neural tube defects, large case-control studies have demonstrated that sulfadoxine/pyrimethamine administered as IPTp (exclusively in the second and third trimesters and after organogenesis) does not result in an increased risk of teratogenesis. Folic acid supplementation is recommended for all pregnant women to reduce the rate of congenital anomalies but high doses of folic acid (5 mg/day) may interfere with the antimalarial efficacy of sulfadoxine/pyrimethamine. However, the recommended standard dose of folic acid supplementation (0.4 mg/day) does not affect antimalarial efficacy and may provide the optimal balance to prevent neural tube defects and maintain the effectiveness of IPTp-SP. No clinical association between sulfadoxine/pyrimethamine use and kernicterus has been reported despite the extensive use of sulfadoxine/pyrimethamine and related compounds to treat maternal malaria and congenital toxoplasmosis in near-term pregnant women and newborns. Although few drugs in pregnancy can be considered completely safe, sulfadoxine/pyrimethamine - when delivered as IPTp - has a favourable safety profile. Improved pharmacovigilance programmes throughout Africa are now needed to confirm its safety as access to IPTp-SP increases. Given the documented benefits of IPTp-SP in malaria endemic areas of Africa, access to this treatment for pregnant women should continue to expand.
- Published
- 2007
- Full Text
- View/download PDF
14. Randomized Trial of 2‐Dose versus Monthly Sulfadoxine‐Pyrimethamine Intermittent Preventive Treatment for Malaria in HIV‐Positive and HIV‐Negative Pregnant Women in Malawi
- Author
-
Michael C. Thigpen, Richard W. Steketee, Alan Macheso, Scott J Filler, Peter N. Kazembe, Mary J. Hamel, Monica E. Parise, and Robert D. Newman
- Subjects
Adult ,Malawi ,medicine.medical_specialty ,Adolescent ,Sulfadoxine ,medicine.medical_treatment ,Population ,HIV Infections ,Parasitemia ,Drug Administration Schedule ,Antimalarials ,Acquired immunodeficiency syndrome (AIDS) ,Pregnancy ,Trimethoprim, Sulfamethoxazole Drug Combination ,parasitic diseases ,medicine ,Humans ,Immunology and Allergy ,Malaria, Falciparum ,Pregnancy Complications, Infectious ,education ,education.field_of_study ,Intermittent preventive therapy ,Obstetrics ,business.industry ,Infant, Newborn ,medicine.disease ,Sulfadoxine/pyrimethamine ,Drug Combinations ,Regimen ,Pyrimethamine ,Infectious Diseases ,Pregnancy Complications, Parasitic ,Immunology ,Female ,business ,Malaria ,medicine.drug - Abstract
Intermittent preventive treatment during pregnancy (IPTp) with sulfadoxine-pyrimethamine (SP) decreases placental malaria parasitemia and associated maternal anemia, premature delivery, and low birth weight. However, the optimal regimen in the setting of a high prevalence of human immunodeficiency virus (HIV) infection remains unclear.In Malawi, where the efficacy of SP for the treatment of malaria in children is decreasing, we conducted a randomized, nonblinded study to compare the efficacy of monthly SP IPTp with a 2-dose regimen for the prevention of placental parasitemia in HIV-positive and -negative primigravid and secundigravid women.Of HIV-positive women, 7.8% who received monthly SP had placental malaria, compared with 21.5% of those who received 2-dose SP (relative risk [RR], 0.36 [95% confidence interval {CI}, 0.17-0.79]). Of HIV-negative women, 2.3% who received monthly SP and 6.3% who received 2-dose SP had placental malaria (RR, 0.37 [95% CI, 0.11-1.19]). Less than 1% of women reported adverse drug reactions, with no increase in HIV-positive women or those who received monthly SP.In HIV-positive pregnant women, monthly SP IPTp is more efficacious than a 2-dose regimen in preventing placental malaria. The study also demonstrates the continued efficacy of SP for the prevention of placental malaria, even in the face of its decreasing efficacy for the treatment of malaria in children. In areas with intense transmission of falciparum malaria and a high prevalence of HIV infection, monthly SP IPTp should be adopted.
- Published
- 2006
- Full Text
- View/download PDF
15. SEVERE CUTANEOUS REACTIONS TO SULFADOXINE-PYRIMETHAMINE AND TRIMETHOPRIM-SULFAMETHOXAZOLE IN BLANTYRE DISTRICT, MALAWI
- Author
-
Michael H. Kramer, Nyson Chizani, Carl H. Campbell, Robert S. Stern, Maurice M’Bang’Ombe, John R. MacArthur, John E. Gimnig, Richard W. Steketee, Robert D. Newman, and Chris Mkandala
- Subjects
medicine.medical_specialty ,Sulfadoxine ,business.industry ,medicine.medical_treatment ,Sulfamethoxazole ,medicine.disease ,Trimethoprim ,Toxic epidermal necrolysis ,Sulfadoxine/pyrimethamine ,Infectious Diseases ,Pyrimethamine ,Virology ,Internal medicine ,Immunology ,medicine ,Parasitology ,business ,Malaria ,medicine.drug ,Antibacterial agent - Abstract
We estimated the frequency of clinically diagnosed Stevens-Johnson syndrome and toxic epidermal necrolysis associated with sulfadoxine-pyrimethamine (SP) and trimethoprim-sulfamethoxazole (CTX) in Blantyre District, Malawi. Cases were detected by passive surveillance at 22 health centers from March 2001 through September 2002. Denominators were estimated from the Malawi national census for Blantyre District and the frequency of SP and CTX use reported in five household surveys. Crude rates of adverse reactions were estimated to be 1.2 per 100,000 exposures for SP and 1.5 per 100,000 exposures for CTX. Rates were higher in adults (1.7 cases per 100,000 SP exposures and 2.6 cases per 100,000 CTX exposures) and in persons positive for human immunodeficiency virus (4.9 cases per 100,000 SP exposures and 8.4 cases per 100,000 CTX exposures). Infrequent treatment doses with SP are associated with a low risk of an adverse cutaneous reaction, and SP can be recommended for treatment of malaria in areas where P. falciparum is susceptible.
- Published
- 2006
- Full Text
- View/download PDF
16. Prevention of malaria during pregnancy in West Africa: policy change and the power of subregional action
- Author
-
Ogobara K. Doumbo, Elizabeth Benga-De, Richard W. Steketee, Youssoufa Lo, Mathias Yameogo, Ousmane Faye, Allisyn C. Moran, Oumar Gaye, Monica E. Parise, Kassoum Kayentao, Robert D. Newman, and Philippe Marc Moreira
- Subjects
Economic growth ,education.field_of_study ,medicine.medical_specialty ,Evidence-based practice ,business.industry ,Public health ,Population ,Public Health, Environmental and Occupational Health ,Psychological intervention ,Developing country ,medicine.disease ,Technical support ,Infectious Diseases ,Environmental protection ,parasitic diseases ,Medicine ,Parasitology ,education ,business ,Health policy ,Malaria - Abstract
Despite a broadening consensus about the effectiveness of intermittent preventive treatment (IPTp) in preventing the adverse outcomes of malaria during pregnancy policy change to IPTp was initially limited to East Africa. In West Africa where the policy change process for the prevention of malaria during pregnancy started much later IPTp has been taken up swiftly. The objective was to describe the factors that contributed to the rapid adoption of policies to prevent malaria during pregnancy in West Africa. Several factors appear to have accelerated the process: (1) recognition of the extent of the problem of malaria during pregnancy and its adverse consequences; (2) a clear evidence based program strategy strongly articulated by an important multilateral organization (World Health Organization); (3) subregionally generated evidence to support the proposed strategy; (4) a subregional forum for dissemination of data and discussion regarding the proposed policy changes; (5) widespread availability of the proposed intervention drug (sulfadoxine-pyrimethamine); (6) technical support from reputable and respected institutions in drafting new policies and planning for implementation; (7) donor support for pilot experiences in integrating proposed policy change into a package of preventive services; and (8) financial support for scaling up the proposed interventions. (authors)
- Published
- 2006
- Full Text
- View/download PDF
17. Comparison of Intermittent Preventive Treatment with Chemoprophylaxis for the Prevention of Malaria during Pregnancy in Mali
- Author
-
Didier Doumtabe, Mamoudou Kodio, Hamma Maiga, Bouboucar Maiga, Abdoul S. Keita, Robert D. Newman, Kassoum Kayentao, Drissa Coulibaly, Aissata Ongoiba, Monica E. Parise, Mary Mungai, and Ogobara K. Doumbo
- Subjects
Adult ,Pediatrics ,medicine.medical_specialty ,Placenta Diseases ,Adolescent ,Anemia ,medicine.medical_treatment ,Population ,Mali ,Parasitemia ,Chemoprevention ,Drug Administration Schedule ,Pregnancy ,Chloroquine ,Sulfadoxine ,parasitic diseases ,medicine ,Birth Weight ,Humans ,Immunology and Allergy ,education ,Gynecology ,education.field_of_study ,business.industry ,Infant, Newborn ,Pregnancy Outcome ,Infant ,medicine.disease ,Malaria ,Abortion, Spontaneous ,Drug Combinations ,Low birth weight ,Pyrimethamine ,Infectious Diseases ,Pregnancy Complications, Parasitic ,Multivariate Analysis ,Chemoprophylaxis ,Interpersonal psychotherapy ,Female ,medicine.symptom ,business ,medicine.drug - Abstract
Background. Malaria during pregnancy contributes to maternal anemia and low birth weight. In East Africa, several studies have demonstrated that intermittent preventive treatment (IPT) with sulfadoxine-pyrimethamine (SP) is more efficacious than weekly chloroquine (CQ) chemoprophylaxis in preventing these adverse consequences. To our knowledge, there are no published trials evaluating IPT in West Africa. Methods. We undertook a randomized controlled trial of weekly CQ chemoprophylaxis, 2-dose IPT with CQ, and 2-dose IPT with SP; 1163 women were enrolled. Results. In multivariate analyses, when compared with weekly CQ, IPT/SP was associated with a reduction in third-trimester anemia (adjusted odds ratio [AOR], 0.49; ), placental parasitemia (AOR, 0.69; P ! .001 P p ), and low birth weight (!2500 g) (AOR, 0.69; ). The prevalence of placental infection remained .04 P p .04 unexpectedly high, even in the IPT/SP group (24.5%), possibly because of the intensity of seasonal transmission. There were no significant differences in stillbirths, spontaneous abortions, or neonatal deaths among the 3 groups. Conclusions. In Mali, IPT with SP appears more efficacious than weekly chloroquine chemoprophylaxis in preventing malaria during pregnancy. These data support World Health Organization recommendations to administer at least 2 doses of IPT during pregnancy. In intensely seasonal transmission settings in Mali, 12 doses may be required to prevent placental reinfection prior to delivery.
- Published
- 2005
- Full Text
- View/download PDF
18. Assessment of the RTS,S/AS01 malaria vaccine
- Author
-
Vasee S. Moorthy, Jean-Marie Okwo-Bele, Pete Smith, Robert D Newman, and Philippe Duclos
- Subjects
Male ,Malaria vaccine ,business.industry ,Plasmodium falciparum ,RTS,S ,Articles ,Virology ,Infectious Diseases ,Adjuvants, Immunologic ,Malaria Vaccines ,Humans ,Medicine ,Female ,Malaria, Falciparum ,business - Abstract
Summary Background The efficacy of RTS,S/AS01 as a vaccine for malaria is being tested in a phase 3 clinical trial. Early results show significant, albeit partial, protection against clinical malaria and severe malaria. To ascertain variations in vaccine efficacy according to covariates such as transmission intensity, choice of adjuvant, age at vaccination, and bednet use, we did an individual-participant pooled analysis of phase 2 clinical data. Methods We analysed data from 11 different sites in Africa, including 4453 participants. We measured heterogeneity in vaccine efficacy by estimating the interactions between covariates and vaccination in pooled multivariable Cox regression and Poisson regression analyses. Endpoints for measurement of vaccine efficacy were infection, clinical malaria, severe malaria, and death. We defined transmission intensity levels according to the estimated local parasite prevalence in children aged 2–10 years (PrP2–10), ranging from 5% to 80%. Choice of adjuvant was either AS01 or AS02. Findings Vaccine efficacy against all episodes of clinical malaria varied by transmission intensity (p=0·001). At low transmission (PrP2–10 10%) vaccine efficacy was 60% (95% CI 54 to 67), at moderate transmission (PrP2–10 20%) it was 41% (21 to 57), and at high transmission (PrP2–10 70%) the efficacy was 4% (−10 to 22). Vaccine efficacy also varied by adjuvant choice (p
- Published
- 2013
- Full Text
- View/download PDF
19. Evaluation of Reported Malaria Chemoprophylactic Failure among Travelers in a US University Exchange Program, 2002
- Author
-
Stephen Papagiotas, Louise M. Causer, Robert D. Newman, Marianna Wilson, and Scott G. Filler
- Subjects
Microbiology (medical) ,medicine.medical_specialty ,business.industry ,Public health ,Drug resistance ,Disease cluster ,medicine.disease ,Surgery ,Diagnosis of malaria ,Infectious Diseases ,Family medicine ,parasitic diseases ,Chemoprophylaxis ,Medicine ,Travel medicine ,Risk factor ,business ,Malaria - Abstract
Background. Travelers to malarious areas are at risk of acquiring malaria; however, with chemoprophylaxis and prompt, effective therapy, serious complications of infection are generally preventable. In June 2002, we investigated a report of a cluster of malaria cases among US university staff and students who visited Ghana and were reportedly adherent to appropriate malaria chemoprophylaxis. Methods. We administered a questionnaire to all participants and collected blood specimens for malaria serological examinations from those reporting malaria infection diagnosed by blood smear in Ghana. Results. Of the 33 participants, 25 completed the questionnaire. Twenty-four took a Centers for Disease Control and Prevention-recommended chemoprophylactic drug; 14 (56%) of 25 reported complete adherence to therapy. Twenty (80%) of 25 subjects reported symptoms consistent with possible malaria. Six of these persons reported a microscopic diagnosis of malaria and were treated in Ghana. Serological examination for malaria was performed using blood samples obtained from 5 of these participants; the results for all were negative, suggesting that incorrect diagnoses of malaria were made. Conclusions. Misdiagnosis of malaria made while a person is abroad may not only lead to erroneous reports of drug resistance, but it could also result in unnecessary administration of antimalarial treatment. Health care providers and public health authorities must critically evaluate reports of chemoprophylactic failures and disseminate accurate information to travelers.
- Published
- 2004
- Full Text
- View/download PDF
20. THE BURDEN OF CO-INFECTION WITH HUMAN IMMUNODEFICIENCY VIRUS TYPE 1 AND MALARIA IN PREGNANT WOMEN IN SUB-SAHARAN AFRICA
- Author
-
Francine H. Verhoeff, Richard W. Steketee, Anne M. Van Eijk, Robert D. Newman, Venkatachalam Udhayakumar, Feiko O. ter Kuile, Monica E. Parise, and Stephen J. Rogerson
- Subjects
education.field_of_study ,Pregnancy ,medicine.medical_specialty ,Obstetrics ,business.industry ,Transmission (medicine) ,Population ,Parasitemia ,Prenatal care ,medicine.disease ,Women in development ,Infectious Diseases ,Acquired immunodeficiency syndrome (AIDS) ,Virology ,parasitic diseases ,Immunology ,medicine ,Parasitology ,education ,business ,Malaria - Abstract
In sub-Saharan Africa, human immunodeficiency virus (HIV) and malaria are among the leading causes of morbidity during pregnancy. We reviewed available information collected since the first report 15 years ago that HIV impaired the ability of pregnant women to control malaria parasitemia. Results from 11 studies showed that HIV-infected women experienced consistently more peripheral and placental malaria (summary relative risk = 1.58 and 1.66, respectively), higher parasite densities, and more febrile illnesses, severe anemia, and adverse birth outcomes than HIV-uninfected women, particularly in multigravidae. Thus, HIV alters the typical gravidity-specific pattern of malaria risk by shifting the burden from primarily primigravidae and secundigravidae to all pregnant women. The proportional increase of malaria during pregnancy attributable to HIV was estimated to be 5.5% and 18.8% for populations with HIV prevalences of 10% and 40%, respectively. Maternal malaria was associated with a two-fold higher HIV-1 viral concentrations. Three studies investigating whether placental malaria increased mother-to-child HIV-1 transmission showed conflicting results, possibly reflecting a complex balance between placental malarial immune responses and stimulation of HIV-1 viral replication. Further investigations of interactions between antiretroviral drugs, prophylaxis with cotrimoxazole, and antimalarial drugs in pregnant women are urgently needed. Although much has been learned in the past 15 years about the interaction between malaria and HIV-1 during pregnancy, many issues still require further information to improve our understanding. There is a clear need to strengthen the deployment of existing malaria and HIV prevention and intervention measures for pregnant women.
- Published
- 2004
- Full Text
- View/download PDF
21. EVALUATION OF A MALARIA RAPID DIAGNOSTIC TEST FOR ASSESSING THE BURDEN OF MALARIA DURING PREGNANCY
- Author
-
Sodiomon B. Sirima, Robert D. Newman, Mathias Yameogo, Lauren M. Singer, Gail Stennies, Allisyn C. Moran, Romial Sawadogo, Amidou Diarra, John W. Barnwell, Curtis S. Huber, Amadou T. Konaté, and Monica E. Parise
- Subjects
Rapid diagnostic test ,education.field_of_study ,Pregnancy ,business.industry ,Population ,Parasitemia ,Dipstick ,Gold standard (test) ,medicine.disease ,Infectious Diseases ,Virology ,parasitic diseases ,Immunology ,Gestation ,Medicine ,Parasitology ,business ,education ,Malaria - Abstract
Plasmodium falciparum infection during pregnancy may cause placental malaria and subsequently low birth weight, primarily through the placental sequestration of infected red blood cells. Measuring the burden of malaria during pregnancy usually involves determining the prevalence of placental malaria infection through microscopic ex- amination of placental blood films, a difficult and error-prone process. A number of rapid diagnostic tests (RDTs) for malaria have been developed, most of them immunochromatographic dipstick assays. However, none have been tested for the direct determination of malaria antigen in placental blood. We undertook an evaluation of the Malaria Rapid Test (MAKROmed ®) in determining placental malaria infection. The prevalence of placental parasitemia was 22.6% by microscopy, 51.0% by a polymerase chain reaction (PCR), and 43.1% by RDT. When the PCR was used as the gold standard, RDTs had a sensitivity of 89% and a specificity of 76%. The MAKROmed RDT was highly sensitive in the detection of placental malaria, but had lower than expected specificity.
- Published
- 2004
- Full Text
- View/download PDF
22. Maternal Malaria and Perinatal HIV Transmission, Western Kenya1,2
- Author
-
Robert D. Newman, Margarette S. Kolczak, John G. Ayisi, Juliana A. Otieno, Chunfu Yang, Richard W. Steketee, Ya Ping Shi, Feiko O. ter Kuile, Ambrose O. Misore, Anna Maria van Eijk, Renu B. Lal, Piet A. Kager, and Bernard L. Nahlen
- Subjects
Microbiology (medical) ,Episiotomy ,medicine.medical_specialty ,placenta ,Epidemiology ,medicine.medical_treatment ,malaria ,HIV Infections ,Perinatal hiv ,Immune system ,Pregnancy ,Risk Factors ,parasitic diseases ,Perineal tear ,medicine ,Humans ,vertical disease transmission ,Obstetrics ,Transmission (medicine) ,business.industry ,Research ,Infant, Newborn ,HIV ,virus diseases ,medicine.disease ,Kenya ,Infectious Disease Transmission, Vertical ,Infectious Diseases ,Pregnancy Complications, Parasitic ,Africa ,Multivariate Analysis ,Female ,business ,Viral load ,Malaria - Abstract
To determine whether maternal placental malaria is associated with an increased risk for perinatal mother-to-child HIV transmission (MTCT), we studied HIV-positive women in western Kenya. We enrolled 512 mother-infant pairs; 128 (25.0%) women had placental malaria, and 102 (19.9%) infants acquired HIV perinatally. Log10 HIV viral load and episiotomy or perineal tear were associated with increased perinatal HIV transmission, whereas low-density placental malaria (10,000 parasites/mL) was associated with reduced risk (adjusted relative risk [ARR] 0.4). Among women dually infected with malaria and HIV, high-density placental malaria (10,000 parasites/mL) was associated with increased risk for perinatal MTCT (ARR 2.0), compared to low-density malaria. The interaction between placental malaria and MTCT appears to be variable and complex: placental malaria that is controlled at low density may cause an increase in broad-based immune responses that protect against MTCT; uncontrolled, high-density malaria may simultaneously disrupt placental architecture and generate substantial antigen stimulus to HIV replication and increase risk for MTCT.
- Published
- 2004
- Full Text
- View/download PDF
23. Genetic diversity of HIV-1 in western Kenya
- Author
-
Chunfu Yang, Ming Li, Robert D Newman, Ya-Ping Shi, John Ayisi, Anna M van Eijk, Juliana Otieno, Ambrose O Misore, Richard W Steketee, Bernard L Nahlen, and Renu B Lal
- Subjects
Infectious Diseases ,Immunology ,Immunology and Allergy - Published
- 2003
- Full Text
- View/download PDF
24. China–Africa Cooperation Initiatives in Malaria Control and Elimination
- Author
-
Jia-wen Yao, Andrea Bosman, Ru-Bo Wang, Tambo Ernest, Salim Abdulla, Qi Zheng, Zhi-Gui Xia, Mike O'Leary, Duoquan Wang, Ning Xiao, Ying-Jun Qian, Yayi Guan, Chang-Sheng Deng, Wei Ding, Robert D. Newman, and Jun Feng
- Subjects
medicine.medical_specialty ,Economic growth ,business.industry ,Public health ,Environmental resource management ,Control (management) ,Primary health care ,Developing country ,medicine.disease ,Investment (macroeconomics) ,parasitic diseases ,medicine ,business ,Malaria control ,China ,Malaria - Abstract
Malaria has affected human health globally with a significant burden of disease, and also has impeded social and economic development in the areas where it is present. In Africa, many countries have faced serious challenges in controlling malaria, in part due to major limitations in public health systems and primary health care infrastructure. Although China is a developing country, a set of control strategies and measures in different local settings have been implemented successfully by the National Malaria Control Programme over the last 60 years, with a low cost of investment. It is expected that Chinese experience may benefit malaria control in Africa. This review will address the importance and possibility of China-Africa collaboration in control of malaria in targeted African countries, as well as how to proceed toward the goal of elimination where this is technically feasible.
- Published
- 2014
- Full Text
- View/download PDF
25. A longitudinal study of Giardia lamblia infection in north-east Brazilian children
- Author
-
James P. Nataro, Sean R. Moore, Richard L. Guerrant, Robert D. Newman, Cynthia L. Sears, and Aldo A. M. Lima
- Subjects
Diarrhea ,Giardiasis ,medicine.medical_specialty ,Pediatrics ,Longitudinal study ,Urban Population ,medicine.disease_cause ,Asymptomatic ,Feces ,fluids and secretions ,parasitic diseases ,Epidemiology ,medicine ,Animals ,Humans ,Giardia lamblia ,Longitudinal Studies ,Poverty ,biology ,Public Health, Environmental and Occupational Health ,Infant ,Giardia ,biology.organism_classification ,medicine.disease ,Malnutrition ,Infectious Diseases ,El Niño ,Immunology ,Parasitology ,medicine.symptom ,Brazil ,Cohort study - Abstract
OBJECTIVE To evaluate the epidemiology of Giardia lamblia infection, investigate factors which might be associated with clinical manifestations and recurrence, and examine the role of copathogens in disease course. METHODS Prospective 4-year cohort study of children born in an urban slum in north-eastern Brazil. RESULTS Of 157 children followed for ≥ 3 months, 43 (27.4%) were infected with Giardia. The organism was identified in 8.8% of all stool specimens, and although found with similar frequency in non-diarrhoeal (7.4%) and diarrhoeal stools (9.7%), was more common in children with persistent (20.6%) than acute diarrhoea (7.6%, P=0.002). Recurrent or relapsing infections were common (46%). Children with symptomatic infections had significantly lower weight-for-age and height-for-age than asymptomatic children. Copathogens were not associated with disease course. CONCLUSION With its protean clinical manifestations, Giardia may be associated with substantial morbidity amongst children in Brazil.
- Published
- 2001
- Full Text
- View/download PDF
26. The Use of Carbon Marking after Stereotactic Large-Core-Needle Breast Biopsy
- Author
-
John C. Wilsey, Robert D. Newman, Patricia M. Perrone, David Mullen, and Richard N. Eisen
- Subjects
Breast biopsy ,medicine.medical_specialty ,Needle localization ,medicine.diagnostic_test ,business.industry ,Needle breast biopsy ,Biopsy, Needle ,Breast Neoplasms ,Equipment Design ,Biopsy Site ,Charcoal ,Needle biopsy ,Biopsy ,medicine ,Large core ,Humans ,Mammography ,Female ,Radiology, Nuclear Medicine and imaging ,Breast ,Radiology ,business ,Follow-Up Studies - Abstract
PURPOSE: To investigate the use of activated charcoal to mark the biopsy site and needle track after large-core-needle breast biopsy. MATERIALS AND METHODS: Three hundred seventy-six consecutive patients (with 383 lesions) were referred for stereotactic breast biopsy. Two hundred forty-seven lesions were carbon marked when the need for surgery was likely. Patients who underwent marking were followed up for the results of surgery or mammography performed at our institution. Specimen sizes obtained by using the carbon mark were compared with sizes of consecutive biopsy specimens obtained after hook-wire localization. RESULTS: Carbon marking was well tolerated in all cases. All 132 surgeries performed at the authors' institution were successful in removing the marked target. Specimen sizes compared favorably with sizes of comparison hook-wire localization specimens. All 68 lesions followed mammographically revealed no changes that were attributable to the use of carbon. Two minor complications were observed. Two small cancers were completely removed at needle biopsy. CONCLUSION: Carbon marking is safe and effective for marking the biopsy site and needle track created by stereotactic large-core-needle biopsy of the breast. Marking eliminates the need for postprocedural needle localization. It remains effective when small lesions have been completely removed. This technique should be considered in properly selected cases by those performing large-core-needle biopsy of the breast.
- Published
- 2001
- Full Text
- View/download PDF
27. Persistent Diarrhea Signals a Critical Period of Increased Diarrhea Burdens and Nutritional Shortfalls: A Prospective Cohort Study among Children in Northeastern Brazil
- Author
-
Aldo A. M. Lima, Richard L. Guerrant, Robert D. Newman, Cynthia L. Sears, John B. Schorling, Alberto M. Soares, M. A. Schleupner, Tadesse Wuhib, D. P. Fedorko, M. S. Barboza, James P. Nataro, and Sean R. Moore
- Subjects
Diarrhea ,Pediatrics ,medicine.medical_specialty ,Nutritional Status ,medicine.disease_cause ,Cohort Studies ,Risk Factors ,Enterotoxigenic Escherichia coli ,Epidemiology ,Parasitic Diseases ,Prevalence ,medicine ,Humans ,Immunology and Allergy ,Longitudinal Studies ,Prospective Studies ,Prospective cohort study ,Poverty ,biology ,business.industry ,Incidence ,Incidence (epidemiology) ,Infant, Newborn ,Cryptosporidium ,Bacterial Infections ,biology.organism_classification ,Breast Feeding ,Infectious Diseases ,Socioeconomic Factors ,Virus Diseases ,Female ,medicine.symptom ,business ,Breast feeding ,Brazil ,Cohort study - Abstract
Persistent diarrhea (PD; duration >/=14 days) is a growing part of the global burden of diarrheal diseases. A 45-month prospective cohort study (with illness, nutritional, and microbiologic surveillance) was conducted in a shantytown in northeastern Brazil, to elucidate the epidemiology, nutritional impact, and causes of PD in early childhood (0-3 years of age). A nested case-control design was used to examine children's diarrhea burden and nutritional status before and after a first PD illness. PD illnesses accounted for 8% of episodes and 34% of days of diarrhea. First PD illnesses were preceded by a doubling of acute diarrhea burdens, were followed by further 2.6-3.5-fold increased diarrhea burdens for 18 months, and were associated with acute weight shortfalls. Exclusively breast-fed children had 8-fold lower diarrhea rates than did weaned children. PD-associated etiologic agents included Cryptosporidium, Giardia, enteric adenoviruses, and enterotoxigenic Escherichia coli. PD signals growth shortfalls and increased diarrhea burdens; children with PD merit extended support, and the illness warrants further study to elucidate its prevention, treatment, and impact.
- Published
- 2000
- Full Text
- View/download PDF
28. Malaria scale-up progress: is the glass half-empty or half-full?
- Author
-
Robert D. Newman and Laurence Slutsker
- Subjects
Bed nets ,medicine.medical_specialty ,education.field_of_study ,business.industry ,Public health ,Population ,Psychological intervention ,Developing country ,General Medicine ,medicine.disease ,Mosquito control ,Environmental health ,parasitic diseases ,medicine ,business ,Malaria control ,education ,health care economics and organizations ,Malaria - Abstract
This letter makes the case as to why the glass is half-full in terms of malaria in African countries. It describes several reasons for that stance including: some success has been achieved with seven African countries projecting use of insecticide-treated bednets of more than 40% international funding for malaria control has increased three-fold from 2004 to 2007 and leadership is more effective at global and national levels resulting in improved coordination and more effective advocacy.
- Published
- 2009
- Full Text
- View/download PDF
29. Satisfaction With Outpatient Health Care Services in Manica Province, Mozambique
- Author
-
Jorine Muiser, Stephen Gloyd, Julio M Nyangezi, Francisco Machobo, and Robert D. Newman
- Subjects
Adult ,Male ,Program evaluation ,medicine.medical_specialty ,Adolescent ,MEDLINE ,Health Services Accessibility ,Catchment Area, Health ,Health care ,Ambulatory Care ,medicine ,Humans ,Child ,Mozambique ,Health policy ,Aged ,business.industry ,Health Policy ,Training level ,Middle Aged ,Patient Satisfaction ,Health Care Surveys ,Family medicine ,Ambulatory ,Female ,Customer satisfaction ,Rural Health Services ,Rural area ,business ,Public Health Administration ,Program Evaluation - Abstract
The objective of the study was to describe ambulatory health care services, determine the level of client satisfaction, and identify obstacles to care in a rural area of Mozambique. Exit surveys at 34 health clinics in Manica Province were completed on a sample of 879 adults representing between 1% and 2% of the average monthly visit totals at each clinic. Eighty-three per cent of interviewees were women. Just over half of the visits were for paediatric patients. Men were more likely to be at the clinic for their own health care needs than women (81% vs. 40%, p < 0.001). Of patients seen for acute illness, 45% were examined, 22% received preventive education, and 23% received prognostic information. Overall, 55% of interviewees believed that the service they received was good or very good, 32% rated it as fair, and 13% as poor. Satisfaction was positively associated with increased training level of the provider (p < 0.005), and shorter waiting times (p < 0.001). The most common complaints about the clinic visits were lack of adequate transportation, long waiting times, lack of physical examinations, and failure to receive prescribed medications. These findings suggest that the majority of Mozambicans interviewed are moderately satisfied with the available outpatient services in Manica. Provider training, provider availability and distribution of medicines were areas identified by respondents as needing improvement.
- Published
- 1998
- Full Text
- View/download PDF
30. Mosquito Larval Source Management: Evaluating Evidence in the Context of Practice and Policy
- Author
-
Abraham Mnzava, Zsofia Szilagyi, and Robert D. Newman
- Subjects
Insecticides ,Larva ,Mosquito Control ,Knowledge management ,business.industry ,MEDLINE ,Context (language use) ,medicine.disease ,Malaria ,Mosquito control ,Culicidae ,Meta-Analysis as Topic ,Africa ,medicine ,Animals ,business - Published
- 2013
- Full Text
- View/download PDF
31. WHO and the future of disease control programmes
- Author
-
Robert D. Newman, Lorenzo Savioli, Winnie Mpanju-Shumbusho, Hiroki Nakatani, Mario C. Raviglione, Gottfried Hirnschall, Christopher Dye, and Thierry Mertens
- Subjects
Economic growth ,Tuberculosis ,Communicable disease ,business.industry ,International Cooperation ,Environmental resource management ,International health ,Neglected Diseases ,HIV Infections ,General Medicine ,medicine.disease ,World Health Organization ,Malaria ,Acquired immunodeficiency syndrome (AIDS) ,Tropical Medicine ,Communicable Disease Control ,Global health ,medicine ,Neglected tropical diseases ,Parasitic Diseases ,Normative ,Humans ,business - Abstract
Summary Huge increases in funding for international health over the past two decades have led to a proliferation of donors, partnerships, and health organisations. Over the same period, the global burden of non-communicable diseases has increased absolutely and relative to communicable diseases. In this changing landscape, national programmes for the control of HIV/AIDS, tuberculosis, malaria, and neglected tropical diseases must be reinforced and adapted for three reasons: the global burden of these communicable diseases remains enormous, disease control programmes have an integral and supporting role in developing health systems, and the health benefits of these control programmes go beyond the containment of specific infections. WHO's traditional role in promoting communicable disease control programmes must also adapt to new circumstances. Among a multiplicity of actors, WHO's task is to enhance its normative role as convenor, coordinator, monitor, and standard-setter, fostering greater coherence in global health.
- Published
- 2013
32. Progress towards malaria control targets in relation to national malaria programme funding
- Author
-
Eline L. Korenromp, Mehran Hosseini, Robert D. Newman, Richard E Cibulskis, and Public Health
- Subjects
medicine.medical_specialty ,National Health Programs ,Millennium Development Goals ,World Health Organization ,Malaria/mortality ,Capital Financing ,SDG 3 - Good Health and Well-being ,Environmental protection ,parasitic diseases ,medicine ,Humans ,Resource-poor countries ,Investments ,Socioeconomics ,Malaria/prevention and control ,Programme impact ,Africa South of the Sahara ,health care economics and organizations ,Child health ,Research ,Incidence ,Mortality rate ,Public health ,Health services research ,Health resources ,medicine.disease ,Survival Analysis ,Malaria ,Infectious Diseases ,Communicable Disease Control ,Tropical medicine ,Mosquito net ,Parasitology ,Health Services Research ,Business ,Financing - Abstract
Background Malaria control has been dramatically scaled up the past decade, mainly thanks to increasing international donor financing since 2003. This study assessed progress up to 2010 towards global malaria impact targets, in relation to Global Fund, other donor and domestic malaria programme financing over 2003 to 2009. Methods Assessments used domestic malaria financing reported by national programmes, and Global Fund/OECD data on donor financing for 90 endemic low- and middle-income countries, WHO estimates of households owning one or more insecticide-treated mosquito net (ITN) for countries in sub-Saharan Africa, and WHO-estimated malaria case incidence and deaths in countries outside sub-Saharan Africa. Results Global Fund and other donor funding is concentrated in a subset of the highest endemic African countries. Outside Africa, donor funding is concentrated in those countries with highest malaria mortality and case incidence rates over the years 2000 to 2003. ITN coverage in 2010 in Africa, and declines in case and death rates per person at risk over 2004 to 2010 outside Africa, were greatest in countries with highest donor funding per person at risk, and smallest in countries with lowest donor malaria funding per person at risk. Outside Africa, all-source malaria programme funding over 2003 to 2009 per case averted ($56-5,749) or per death averted ($58,000-3,900,000) over 2004 to 2010 tended to be lower (more favourable) in countries with higher donor malaria funding per person at risk. Conclusions Increases in malaria programme funding are associated with accelerated progress towards malaria control targets. Associations between programme funding per person at risk and ITN coverage increases and declines in case and death rates suggest opportunities to maximize the impact of donor funding, by strategic re-allocation to countries with highest continued need.
- Published
- 2013
33. Artemisinin-resistant malaria in the Asia-Pacific region
- Author
-
Jim Tulloch, Sylvia Meek, Robert D. Newman, and Benedict David
- Subjects
Asia ,Australia ,Drug Resistance ,General Medicine ,medicine.disease ,Asia pacific region ,Artemisinins ,Antimalarials ,Geography ,medicine ,Humans ,Artemisinin ,Malaria, Falciparum ,Socioeconomics ,Malaria ,medicine.drug - Published
- 2012
34. New global estimates of malaria deaths
- Author
-
Steven S. Yoon, Eline L. Korenromp, Michael Lynch, Robert D. Newman, John R. MacArthur, Thom Eisele, Bernard Nahlen, Richard E Cibulskis, Holly Newby, Richard W. Steketee, S. Patrick Kachur, and Achuyt Bhattarai
- Subjects
Male ,biology ,Endemic area ,General Medicine ,medicine.disease ,biology.organism_classification ,Malaria ,Geography ,Tanzania ,Dar es salaam ,Cerebral Malaria ,Environmental health ,medicine ,Humans ,Female - Abstract
www.thelancet.com Vol 380 August 11, 2012 559 Submissions should be made via our electronic submission system at http://ees.elsevier.com/ thelancet/ 4 Kahama-Maro J, D’Acremont V, Mtasiwa D, Genton B, Lengeler C. Low quality of routine microscopy for malaria at diff erent levels of the health system in Dar es Salaam. Malaria J 2011; 10: 332. 5 Makani J, Matuja W, Liyombo E, Snow RW, Marsh K, Warrell DA. Admission diagnosis of cerebral malaria in adults in an endemic area of Tanzania: implications and clinical description. QJM 2003; 96: 355–62. New global estimates of malaria deaths
- Published
- 2012
35. Relegating malaria resurgences to history
- Author
-
Robert D. Newman
- Subjects
Economic growth ,medicine.medical_specialty ,lcsh:Arctic medicine. Tropical medicine ,lcsh:RC955-962 ,Universal design ,Communicable Diseases, Emerging ,World health ,lcsh:Infectious and parasitic diseases ,Acquired immunodeficiency syndrome (AIDS) ,parasitic diseases ,Humans ,Medicine ,lcsh:RC109-216 ,health care economics and organizations ,business.industry ,Research ,Public health ,medicine.disease ,Investment (macroeconomics) ,Quarter (United States coin) ,Malaria ,Infectious Diseases ,Work (electrical) ,Communicable Disease Control ,Parasitology ,Resurgence ,Financing ,business - Abstract
Progress in malaria control over the past decade has been striking, with malaria mortality rates falling by approximately one quarter globally and more than a third in the World Health Organization African Region. In the accompanying paper, Cohen et al. demonstrate the potential fragility of these gains, comprehensively describing malaria resurgences that have occurred over the past 80 or so years. They found that the vast majority of resurgences were due, at least in part, to the weakening of malaria control programmes; resource constraints were the most commonly identified factor. Their findings are timely and compelling, demonstrating that global efforts will be wasted if the required resources are not secured to achieve and maintain universal access to life-saving malaria prevention and control tools. The greatest threats to current malaria control efforts are not biological, but financial. The increases in funding for malaria over the past decade, while impressive, still fall far short of the nearly $6 billion dollars required annually. Domestic spending by endemic country governments on malaria specifically, and health more generally, could go a long way towards filling the projected funding gap. However, external funding is also essential, and the global community needs to work together to ensure full funding of the Global Fund to Fight AIDS, Tuberculosis, and Malaria, which has been the single largest source of malaria funding over the past decade. This year, on April 25th, World Malaria Day will be celebrated with the theme Sustain Gains, Save Lives: Invest in Malaria. The review by Cohen et al. suggests one possible future if such investment is not made. However, with sufficient support, malaria resurgences can be relegated to history.
- Published
- 2012
- Full Text
- View/download PDF
36. Cryptosporidial and Microsporidial Infections in Human Immunodeficiency Virus-Infected Patients in Northeastern Brazil
- Author
-
Telma Régia Bezerra Sales de Queiroz, Cynthia L. Sears, Lynne S. Garcia, Tadesse Wuhib, Maria Lúcia Duarte Pereira, Ralph T. Bryan, S P Wahlquist, Anastacio de Queiroz Sousa, Terezinha M. J. Silva, Cristina de Souza Chaves, Richard L. Guerrant, and Robert D. Newman
- Subjects
Adult ,Diarrhea ,Male ,Adolescent ,Rain ,Population ,AIDS-related complex ,Cryptosporidiosis ,Feces ,Acquired immunodeficiency syndrome (AIDS) ,Risk Factors ,Microsporidiosis ,parasitic diseases ,medicine ,Animals ,Humans ,Immunology and Allergy ,Child ,education ,Aged ,Retrospective Studies ,Cryptosporidium parvum ,Observer Variation ,education.field_of_study ,AIDS-Related Opportunistic Infections ,biology ,Transmission (medicine) ,Incidence (epidemiology) ,Infant ,virus diseases ,Middle Aged ,biology.organism_classification ,medicine.disease ,Virology ,Infectious Diseases ,Child, Preschool ,Microsporidia ,Female ,Seasons ,medicine.symptom ,Brazil - Abstract
To determine the frequency of the parasitic pathogens in human immunodeficiency virus (HIV)-infected patients in a developing world setting 295 stool specimens were examined from 166 HIV-positive patients (49% with AIDS) at Sao Jose Hospital Fortaleza Brazil from September 1990 to March 1992. Significantly more patients with diarrhea (85%) than without (66%) had AIDS or AIDS-related complex (ARC) (p < 0.005). Of the potential parasitic causes of diarrhea only Cryptosporidium parvum and microsporidia were significantly associated with diarrheal disease. Infections with C. parvum but not microsporidia were associated with the rainy season (p < 0.005). Thus C. parvum and microsporidia are the most common intestinal parasites associated with diarrhea in an HIV-infected population in Brazil and are associated with advanced HIV disease. The association of C. parvum infections with the rainy season suggests that contaminated water may be important in its transmission; however the source of human microsporidia requires further investigation. (authors)
- Published
- 1994
- Full Text
- View/download PDF
37. Environmental Sources of Cryptosporidium in an Urban Slum in Northeastern Brazil
- Author
-
Cynthia L. Sears, Tadesse Wuhib, A. A. M. Lima, Robert D. Newman, and R. L. Guerrant
- Subjects
Wet season ,Pathology ,medicine.medical_specialty ,Veterinary medicine ,Swine ,Rain ,Water source ,Cryptosporidiosis ,Cryptosporidium ,Feces ,Dogs ,Poverty Areas ,Virology ,parasitic diseases ,Dry season ,medicine ,Animals ,Humans ,Toilet Facilities ,Child ,Perissodactyla ,Disease Reservoirs ,biology ,Goats ,Urban Health ,Infant ,Water ,biology.organism_classification ,Diarrhea ,Infectious Diseases ,Child, Preschool ,Parasitology ,Urban slum ,High incidence ,medicine.symptom ,Diarrheal disease ,Brazil - Abstract
Cryptosporidium is an important cause of diarrheal disease in children worldwide. To elucidate the environmental sources of this parasite, we selected an urban slum in Fortaleza, Brazil, a community with a known high incidence of cryptosporidiosis, and examined both stool smears from household animals (n = 127) and filtrates from local water sources (n = 18) for Cryptosporidium oocysts. Because previous work in this community has demonstrated the seasonal nature of human infection with Cryptosporidium, collections were made separately for the dry and rainy seasons. Of the 64 stools collected during the dry season (September-December 1990), four (6.3%) were positive by acid-fast staining for Cryptosporidium. Of the 63 rainy season samples (March-May 1991), nine (14.3%) were positive. Overall, oocysts were detected in 13 (10.2%) of 127 animal stool samples. Freshwater samples were obtained from a variety of sources including open and closed wells, and running city water and then processed. Four of 18 samples (22.2%), including a sample from city water were positive by at least one of two staining techniques (acid-fast and immunofluorescence). In summary, animals may serve as a reservoir of Cryptosporidium, with potential for the contamination of immediate household water sources. These findings may help to explain the high incidence of cryptosporidiosis among infants in this impoverished community.
- Published
- 1993
- Full Text
- View/download PDF
38. The Galvano-Cautery Sound, and its Application Especially in Hypertrophied Prostate; with Report of Cases
- Author
-
Robert D. Newman
- Subjects
World Wide Web ,geography ,Information retrieval ,geography.geographical_feature_category ,Computer science ,General Engineering ,General Earth and Planetary Sciences ,General Medicine ,Articles ,Sound (geography) ,General Environmental Science - Published
- 2010
39. Malaria control beyond 2010
- Author
-
Robert D. Newman
- Subjects
Economic growth ,medicine.medical_specialty ,Mosquito Control ,Point-of-Care Systems ,Drug Resistance ,Insecticide Resistance ,Antimalarials ,Lactones ,medicine ,Humans ,Community Health Services ,Insecticide-Treated Bednets ,Protozoal disease ,Health policy ,General Environmental Science ,business.industry ,Public health ,General Engineering ,General Medicine ,Investment (macroeconomics) ,medicine.disease ,Disease control ,Artemisinins ,Malaria ,Insecticide resistance ,Immunology ,Africa ,General Earth and Planetary Sciences ,Malaria control ,business - Abstract
Although substantial progress has been made in controlling malaria, Robert Newman says wider investment will be essential for success
- Published
- 2010
40. The Cost-Effectiveness of Intermittent Preventive Treatment for Malaria in Infants in Sub-Saharan Africa
- Author
-
Martin P. Grobusch, John J. Aponte, Laurence Slutsker, Robert D. Newman, David Schellenberg, Paul M Masika, Eusebio Macete, Guy Hutton, Fatuma Manzi, Elisa Sicuri, Fabrizio Tediosi, Marcel Tanner, Clara Menéndez, Frank Odhiambo, Roly Gosling, Prosper Biao, Peter Otieno, Fred Matovu, Daniel Chandramohan, Lesong Conteh, Peter G. Kremsner, Andrea Egan, Pedro L. Alonso, Benson Obonyo, Mary J. Hamel, AII - Amsterdam institute for Infection and Immunity, APH - Amsterdam Public Health, and Infectious diseases
- Subjects
Veterinary medicine ,Sulfadoxine ,Cost effectiveness ,General Science & Technology ,Science ,medicine.medical_treatment ,Cost-Benefit Analysis ,Pediatrics and Child Health ,cost-effectiveness analysis ,malaria prevention ,preventive care ,Amodiaquine ,Public Health and Epidemiology/Health Policy ,chemistry.chemical_compound ,Antimalarials ,Evidence-Based Healthcare/Health Services Research and Economics ,Public Health and Epidemiology/Health Services Research and Economics ,Environmental health ,parasitic diseases ,MD Multidisciplinary ,medicine ,Humans ,health care economics and organizations ,Africa South of the Sahara ,Multidisciplinary ,business.industry ,Mefloquine ,Infant ,Cost-effectiveness analysis ,medicine.disease ,Sulfadoxine/pyrimethamine ,Malaria ,Drug Combinations ,Pyrimethamine ,chemistry ,Artesunate ,Medicine ,business ,Research Article ,medicine.drug - Abstract
BackgroundIntermittent preventive treatment in infants (IPTi) has been shown to decrease clinical malaria by approximately 30% in the first year of life and is a promising malaria control strategy for Sub-Saharan Africa which can be delivered alongside the Expanded Programme on Immunisation (EPI). To date, there have been limited data on the cost-effectiveness of this strategy using sulfadoxine pyrimethamine (SP) and no published data on cost-effectiveness using other antimalarials.MethodsWe analysed data from 5 countries in sub-Saharan Africa using a total of 5 different IPTi drug regimens; SP, mefloquine (MQ), 3 days of chlorproguanil-dapsone (CD), SP plus 3 days of artesunate (SP-AS3) and 3 days of amodiaquine-artesunate (AQ3-AS3).The cost per malaria episode averted and cost per Disability-Adjusted Life-Year (DALY) averted were modeled using both trial specific protective efficacy (PE) for all IPTi drugs and a pooled PE for IPTi with SP, malaria incidence, an estimated malaria case fatality rate of 1.57%, IPTi delivery costs and country specific provider and household malaria treatment costs.FindingsIn sites where IPTi had a significant effect on reducing malaria, the cost per episode averted for IPTi-SP was very low, USD 1.36-4.03 based on trial specific data and USD 0.68-2.27 based on the pooled analysis. For IPTi using alternative antimalarials, the lowest cost per case averted was for AQ3-AS3 in western Kenya (USD 4.62) and the highest was for MQ in Korowge, Tanzania (USD 18.56). Where efficacious, based only on intervention costs, IPTi was shown to be cost effective in all the sites and highly cost-effective in all but one of the sites, ranging from USD 2.90 (Ifakara, Tanzania with SP) to USD 39.63 (Korogwe, Tanzania with MQ) per DALY averted. In addition, IPTi reduced health system costs and showed significant savings to households from malaria cases averted. A threshold analysis showed that there is room for the IPTi-efficacy to fall and still remain highly cost effective in all sites where IPTi had a statistically significant effect on clinical malaria.ConclusionsIPTi delivered alongside the EPI is a highly cost effective intervention against clinical malaria with a range of drugs in a range of malaria transmission settings. Where IPTi did not have a statistically significant impact on malaria, generally in low transmission sites, it was not cost effective.
- Published
- 2010
41. How much malaria occurs in urban Luanda, Angola? A health facility-based assessment
- Author
-
Julie Thwing, Robert D. Newman, Alexandra Pataca Fernandes, Alexandre Macedo de Oliveira, Francisco Saute, Jules Mihigo, Carolina Miguel Ferreira, and Filomeno Fortes
- Subjects
Adult ,Male ,medicine.medical_specialty ,Veterinary medicine ,Insecticides ,Mosquito Control ,Adolescent ,Urban Population ,Prevalence ,Health facility ,Malaria transmission ,Virology ,Epidemiology ,Medicine ,Humans ,Child ,Demography ,business.industry ,Bedding and Linens ,medicine.disease ,Malaria ,Blood film ,Infectious Diseases ,Angola ,Child, Preschool ,Tropical medicine ,Parasitology ,Female ,Health Facilities ,Rural area ,business - Abstract
We conducted a health facility-based survey of patients with fever during malaria transmission season to determine the proportion with laboratory-confirmed malaria in Luanda, Angola. We enrolled 864 patients at 30 facilities; each underwent a blood film for malaria and a questionnaire. Only 3.6% had a positive blood film. When stratified by distance of the facility to city center (< 15 km and ³ 15 km), the proportions were 1.5% (9/615) and 8.8% (22/249), respec- tively ( P < 0.0001). Of patients traveling outside Luanda in the preceding 3 months, 6.8% (6/88) had malaria, compared with 3.2% (26/776) not traveling ( P = 0.13). Children < 5 years of age were less likely to have malaria (2.4%; 12/510) than children ages 5-14 (8.7%; 9/104) and adults (4.0%; 10/250) ( P = 0.03). The prevalence of laboratory-confirmed malaria in febrile patients in Luanda is very low, but increases with distance from the urban center. Prevention and treatment should be focused in surrounding rural areas.
- Published
- 2009
42. Pre-departure and post-arrival management of P. falciparum malaria in refugees relocating from sub-Saharan Africa to the United States
- Author
-
William M, Stauffer, Michelle, Weinberg, Robert D, Newman, Louise M, Causer, Mary J, Hamel, Laurence, Slutsker, and Martin S, Cetron
- Subjects
Adult ,Refugees ,Travel ,Time Factors ,Health Policy ,Plasmodium falciparum ,Emigrants and Immigrants ,United States ,Antimalarials ,Pregnancy ,Animals ,Humans ,Female ,Malaria, Falciparum ,Child ,Africa South of the Sahara - Abstract
Plasmodium infection, often sub-clinical, is common in migrating sub-Saharan refugee populations. Refugees who subsequently develop clinical malaria suffer illness and exact a cost on state and local health care facilities. Untreated infection is also of public health concern because of the potential for local transmission. In response to increasing numbers of refugees originating in sub-Saharan Africa guidelines for the management of malaria in refugees migrating to the United States have been broadened and updated. The guidelines are based on available evidence-based literature and recent public health experience. These guidelines were critically reviewed, assessed, and approved by multiple National and State entities as well as outside experts. These consensus guidelines recommend that sub-Saharan African refugees relocating to the United States receive presumptive treatment of P. falciparum malaria before departure or during the domestic refugee medical screening after arrival. Presumptive therapy is not currently recommended for either non-falciparum malaria or for refugees relocating from areas outside sub-Saharan Africa.
- Published
- 2008
43. Insecticide-treated net ownership and usage in Niger after a nationwide integrated campaign
- Author
-
Julie, Thwing, Natasha, Hochberg, Jodi, Vanden Eng, Sanouna, Issifi, M James, Eliades, Etienne, Minkoulou, Adam, Wolkon, Habi, Gado, Ousmane, Ibrahim, Robert D, Newman, and Marcel, Lama
- Subjects
Health Knowledge, Attitudes, Practice ,Insecticides ,Mosquito Control ,Ownership ,Vaccination ,Infant, Newborn ,Bedding and Linens ,Infant ,Health Promotion ,Malaria ,Poliovirus Vaccines ,Cross-Sectional Studies ,Pregnancy ,Child, Preschool ,Humans ,Female ,Seasons - Abstract
In December 2005 and March 2006, Niger conducted nationwide integrated campaigns to distribute polio vaccine and long lasting insecticide-treated nets (LLINs) to children5 years of age. We evaluated the campaign effectiveness, net retention, insecticide-treated net (ITN) ownership, and usage.Two nationwide cross-sectional surveys in January 2006 (dry season) and September 2006 (rainy season), using a stratified two-stage cluster sampling design. We mapped selected communities, selected households by simple random sampling, and administered questionnaires by interviewers using personal digital assistants.The first survey showed that ITN ownership in all households was 6.3% prior to the campaign, increasing to 65.1% after the campaign in the second survey. The second survey also showed that 73.4% of households with children5 received an LLIN and that 97.7% of households that receivedor = one LLIN retained it. The wealth equity ratio for ITN ownership in households with children5 increased from 0.17 prior to the campaign to 0.79 afterward. During the dry season, 15.4% of all children5 and 11.3% of pregnant women slept under an ITN, while during rainy season, 55.5% of children5 and 48.2% of pregnant women slept under an ITN.Free distribution during the integrated campaign rapidly increased ITN ownership and decreased inequities between those in the highest and lowest wealth quintiles. Retention of ITNs was very high, and usage was high during malaria transmission season. However, ITN ownership and usage by vulnerable groups continues to fall short of RBM targets, and additional strategies are needed to increase ownership and usage.
- Published
- 2008
44. Giardia duodenalis assemblage, clinical presentation and markers of intestinal inflammation in Brazilian children
- Author
-
Richard L. Guerrant, Cynthia L. Sears, Relana Pinkerton, Oluma Y. Bushen, Robert D. Newman, Anita Kohli, Aldo A. M. Lima, and Eric R. Houpt
- Subjects
Diarrhea ,Giardiasis ,Male ,medicine.medical_specialty ,Genotype ,Population ,Antigens, Protozoan ,medicine.disease_cause ,Gastroenterology ,Polymerase Chain Reaction ,Sensitivity and Specificity ,Article ,Host-Parasite Interactions ,Feces ,Internal medicine ,Poverty Areas ,medicine ,Escherichia coli ,Giardia lamblia ,Animals ,Humans ,Cyst ,Longitudinal Studies ,education ,education.field_of_study ,biology ,Incidence (epidemiology) ,Giardia ,Public Health, Environmental and Occupational Health ,Infant ,General Medicine ,Sequence Analysis, DNA ,DNA, Protozoan ,medicine.disease ,biology.organism_classification ,Infectious Diseases ,Child, Preschool ,Immunology ,Coinfection ,Parasitology ,Female ,medicine.symptom ,Brazil ,Polymorphism, Restriction Fragment Length - Abstract
Data on the relationship between the two genotypes of Giardia duodenalis that infect humans, assemblages A and B, their clinical presentation and intestinal inflammation are limited. We analyzed 108 stool samples previously collected for a diarrhoeal study among Brazilian children, representing 71 infections in 47 children. Assemblage B was most prevalent, accounting for 43/58 (74.1%) infections, while assemblage A accounted for 9/58 (15.5%) infections and 6/58 (10.3%) infections were mixed (contained both assemblage A and B). There was no significant difference in diarrhoeal symptoms experienced during assemblage A, B or mixed infections. Children with assemblage B demonstrated greater variability in G. duodenalis cyst shedding but at an overall greater level (n=43, mean 3.6 x 10(5), range 5.3 x 10(2)-2.5 x 10(6)cysts/ml) than children infected with assemblage A (n=9, mean 1.4 x 10(5), range 1.5 x 10(4)-4.6 x 10(5)cysts/ml; P=0.009). Children with mixed infections shed more cysts (mean 8.3 x 10(5), range 3.1 x 10(4)-2.8 x 10(6)cysts/ml) than children with assemblage A or B alone (P=0.069 and P=0.046 respectively). This higher rate of cyst shedding in children with assemblage B may promote its spread, accounting for its increased incidence. Additionally, second and third infections had decreasing faecal lactoferrin, suggesting some protection against severity, albeit not against infection, by prior infection.
- Published
- 2007
45. Malaria surveillance - United States, 2005
- Author
-
Julie, Thwing, Jacek, Skarbinski, Robert D, Newman, Ann M, Barber, Sonja, Mali, Jacquelin M, Roberts, Laurence, Slutsker, and Paul M, Arguin
- Subjects
Adult ,Male ,Blood Specimen Collection ,Plasmodium ,Travel ,Adolescent ,Infant, Newborn ,Infant ,Middle Aged ,United States ,Malaria ,Fatal Outcome ,Pregnancy ,Child, Preschool ,Population Surveillance ,Animals ,Humans ,Female ,Pregnancy Complications, Infectious ,Child - Abstract
Malaria in humans is caused by any of four species of intraerythrocytic protozoa of the genus Plasmodium (i.e., P. falciparum, P. vivax, P. ovale, or P. malariae). These parasites are transmitted by the bite of an infective female Anopheles sp. mosquito. The majority of malaria infections in the United States occur among persons who have traveled to or from areas with ongoing malaria transmission. In the United States, cases can occur through exposure to infected blood products, congenital transmission, or local mosquitoborne transmission. Malaria surveillance is conducted to identify episodes of local transmission and to guide prevention recommendations for travelers.This report summarizes cases in persons with onset of illness in 2005 and summarizes trends during previous years.Malaria cases confirmed by blood film or polymerase chain reaction (PCR) are mandated to be reported to local and state health departments by health-care providers or laboratory staff. Case investigations are conducted by local and state health departments, and reports are transmitted to CDC through the National Malaria Surveillance System (NMSS). Data from NMSS serve as the basis for this report.CDC received reports of 1,528 cases of malaria, including seven fatal cases, with an onset of symptoms in 2005 among persons in the United States or one of its territories. This number represents an increase of 15.4% from the 1,324 cases reported for 2004. P. falciparum, P. vivax, P. malariae, and P. ovale were identified in 48.6%, 22.1%, 3.5%, and 2.5% of cases, respectively. Twelve patients (0.8% of total) were infected by two or more species. The infecting species was unreported or undetermined in 22.6% of cases. Compared with 2004, the largest increases in cases came from the Americas (23.1%; n = 213) and Asia and the Middle East (18.6%; n = 204). On the basis of estimated volume of travel, the highest estimated case rates of malaria among travelers occurred among those returning from West Africa. Of 870 U.S. civilians who acquired malaria abroad, only 160 (18.4%) reported that they had followed a chemoprophylactic drug regimen recommended by CDC for the area to which they had traveled. Two patients became infected in the United States, both attributed to congenital transmission; both were infected with P. vivax. Seven deaths were attributed to malaria, all caused by infection with P. falciparum.The 15.4% increase in malaria cases in 2005, compared with 2004, resulted primarily from increases in the number of cases reported from Asia and the Middle East and from the Americas. This increase might in part reflect more complete reporting and in part increased travel to malarious areas. No change was noted in proportions of cases from other areas of the world, or in species responsible for the infection. In the majority of reported cases, U.S. civilians who acquired infection abroad had not adhered to a chemoprophylaxis regimen that was appropriate for the country in which they acquired malaria. U.S. civilians who traveled to West Africa had the highest estimated relative case rate.Additional investigations were conducted for the seven fatal cases and two infections acquired in the United States. Persons traveling to a malarious area should take one of the recommended chemoprophylaxis regimens appropriate for the region of travel and use personal protection measures to prevent mosquito bites. Any person who has been to a malarious area and who subsequently has a fever or influenza-like symptoms should seek medical care immediately and report their travel history to the clinician; investigation should include at least one blood-film test for malaria. Malaria infections can be fatal if not diagnosed and treated promptly. Recommendations concerning malaria prevention can be obtained from CDC at http://www.cdc.gov/travel or by calling the Malaria Hotline (telephone 770-488-7788). Recommendations for malaria treatment can be obtained at http://www.cdc.gov/malaria/diagnosis_treatment/treatment.htm or by calling the Malaria Hotline.
- Published
- 2007
46. Malaria prevention during pregnancy: assessing the disease burden one year after implementing a program of intermittent preventive treatment in Koupela District, Burkina Faso
- Author
-
Sodiomon B, Sirima, Annett H, Cotte, Amadou, Konaté, Allisyn C, Moran, Kwame, Asamoa, Edith C, Bougouma, Amidou, Diarra, Alphonse, Ouédraogo, Monica E, Parise, and Robert D, Newman
- Subjects
Adult ,Insecticides ,Adolescent ,National Health Programs ,Placenta ,Infant, Newborn ,Bedding and Linens ,Infant, Low Birth Weight ,Middle Aged ,Parasitemia ,Malaria ,Antimalarials ,Drug Combinations ,Pyrimethamine ,Pregnancy ,Pregnancy Complications, Parasitic ,Burkina Faso ,Sulfadoxine ,Humans ,Female - Abstract
The World Health Organization recommends that pregnant women in malaria-endemic areas receiveor= 2 doses of intermittent preventive treatment with sulfadoxine-pyrimethamine (IPTp/SP) in the second and third trimesters of pregnancy to prevent maternal anemia, placental parasitemia, and low birth weight (LBW). In 2001, a program evaluation in Koupéla District, Burkina Faso demonstrated that despite widespread use of chloroquine chemoprophylaxis, the burden of malaria during pregnancy remained high. In 2003, the Burkina Faso Ministry of Health piloted a program of IPTp/SP (three doses) and accelerated distribution of insecticide-treated nets (ITN) to pregnant women in Koupéla District. In 2004, a follow-up program evaluation was conducted. Coverage withor= 1 doses of IPTp/SP was high among women attending antenatal clinics (ANCs) (96.2%) and delivery units (DUs) (93.5%); ITN ownership was moderately high (ANC = 53.9%, DU = 61.6%). In multivariate analysis,or= 1 dose of IPTp/SP was associated with a significant reduction in the prevalence of peripheral parasitemia at ANCs (risk ratio [RR] = 0.49, P = 0.008),or= 2 doses of IPTp/SP were associated with a reduction in the prevalence of placental parasitemia (RR = 0.56, P = 0.02), and three doses of IPTp/SP were associated with a reduced risk of LBW (RR = 0.51, P = 0.04). The proportions of women at ANCs with peripheral parasitemia and anemia were significantly lower in 2004 than in 2001 (RR = 0.53, P = 0.001 and RR = 0.78, P = 0.003, respectively). The proportions of women at DUs with peripheral and placental parasitemia were also significantly lower in 2004 than in 2001 (RR = 0.66, P0.0001 and RR = 0.71, P = 0.0002, respectively). These data suggest that a package of IPTp/SP and ITNs is effective in reducing the burden of malaria during pregnancy in Burkina Faso.
- Published
- 2006
47. Malaria surveillance--United States, 2004
- Author
-
Jacek, Skarbinski, Eliades M, James, Louise M, Causer, Ann M, Barber, Sonja, Mali, Phuc, Nguyen-Dinh, Jacquelin M, Roberts, Monica E, Parise, Laurence, Slutsker, and Robert D, Newman
- Subjects
Adult ,Male ,Blood Specimen Collection ,Plasmodium ,Travel ,Adolescent ,Infant, Newborn ,Infant ,Middle Aged ,United States ,Malaria ,Pregnancy ,Child, Preschool ,Population Surveillance ,Animals ,Humans ,Female ,Pregnancy Complications, Infectious ,Child ,Aged - Abstract
Malaria in humans is caused by any of four species of intraerythrocytic protozoa of the genus Plasmodium (i.e., P. falciparum, P. vivax, P. ovale, or P. malariae). These parasites are transmitted by the bite of an infective female Anopheles sp. mosquito. The majority of malaria infections in the United States occur among persons who have traveled to areas with ongoing malaria transmission. In the United States, cases can occur through exposure to infected blood products, congenital transmission, or local mosquitoborne transmission. Malaria surveillance is conducted to identify episodes of local transmission and to guide prevention recommendations for travelers.This report summarizes cases in persons with onset of illness in 2004 and summarizes trends during previous years.Malaria cases confirmed by blood film are mandated to be reported to local and state health departments by health-care providers or laboratory staff. Case investigations are conducted by local and state health departments, and reports are transmitted to CDC through the National Malaria Surveillance System (NMSS). Data from NMSS serve as the basis for this report.CDC received reports of 1,324 cases of malaria, including four fatal cases, with an onset of symptoms in 2004 among persons in the United States or one of its territories. This number represents an increase of 3.6% from the 1,278 cases reported for 2003. P. falciparum, P. vivax, P. malariae, and P. ovale were identified in 49.6%, 23.8%, 3.6%, and 2.0% of cases, respectively. Seventeen patients (1.3% of total) were infected by two or more species. The infecting species was unreported or undetermined in 262 (19.8%) cases. Compared with 2003, the number of reported malaria cases acquired in the Americas (n = 173) increased 17.7%, whereas the number of cases acquired in Asia (n = 172) and Africa (n = 809) decreased 2.8% and 3.7%, respectively. Of 775 U.S. civilians who acquired malaria abroad, only 160 (20.6%) reported that they had followed a chemoprophylactic drug regimen recommended by CDC for the area to which they had traveled. Four patients became infected in the United States; three cases were attributed to congenital transmission and one to laboratory-related mosquitoborne transmission. Four deaths were attributed to malaria, including two caused by P. falciparum, one by P. vivax, and one by a mixed infection with P. falciparum and P. malariae.The 3.6% increase in malaria cases in 2004, compared with 2003, resulted primarily from an increase in the number of cases acquired in the Americas but was offset by a decrease in the number of cases acquired in Africa and Asia. This limited increase might reflect local changes in disease transmission, increased travel to regions in which malaria is endemic, or fluctuations in reporting to state and local health departments. These changes likely reflect expected variation in annual reporting and should not be interpreted as indicating a longer-term trend. In the majority of reported cases, U.S. civilians who acquired infection abroad had not adhered to a chemoprophylaxis regimen that was appropriate for the country in which they acquired malaria.Additional investigations were conducted for the four fatal cases and four infections acquired in the United States. Persons traveling to a malarious area should take one of the recommended chemoprophylaxis regimens appropriate for the region of travel and use personal protection measures to prevent mosquito bites. Any person who has been to a malarious area and who subsequently has a fever or influenza-like symptoms should seek medical care immediately and report their travel history to the clinician; investigation should include a blood-film test for malaria. Malaria infections can be fatal if not diagnosed and treated promptly. Recommendations concerning malaria prevention can be obtained from CDC at http://www.cdc.gov/travel or by calling the Malaria Hotline at telephone 770-488-7788. Recommendations concerning malaria treatment can be obtained at http://www.cdc.gov/malaria/diagnosis_treatment/treatment.htm or by calling the Malaria Hotline.
- Published
- 2006
48. Severe cutaneous reactions to sulfadoxine-pyrimethamine and trimethoprim-sulfamethoxazole in Blantyre District, Malawi
- Author
-
John E, Gimnig, John R, MacArthur, Maurice, M'bang'ombe, Michael H, Kramer, Nyson, Chizani, Robert S, Stern, Chris, Mkandala, Robert D, Newman, Richard W, Steketee, and Carl H, Campbell
- Subjects
Adult ,Male ,Malawi ,Adolescent ,Infant, Newborn ,Infant ,Middle Aged ,Severity of Illness Index ,Malaria ,Antimalarials ,Drug Combinations ,Pyrimethamine ,Pregnancy ,Child, Preschool ,Pregnancy Complications, Parasitic ,Sulfadoxine ,Trimethoprim, Sulfamethoxazole Drug Combination ,Adverse Drug Reaction Reporting Systems ,Humans ,Female ,Drug Eruptions ,Child ,Aged - Abstract
We estimated the frequency of clinically diagnosed Stevens-Johnson syndrome and toxic epidermal necrolysis associated with sulfadoxine-pyrimethamine (SP) and trimethoprim-sulfamethoxazole (CTX) in Blantyre District, Malawi. Cases were detected by passive surveillance at 22 health centers from March 2001 through September 2002. Denominators were estimated from the Malawi national census for Blantyre District and the frequency of SP and CTX use reported in five household surveys. Crude rates of adverse reactions were estimated to be 1.2 per 100,000 exposures for SP and 1.5 per 100,000 exposures for CTX. Rates were higher in adults (1.7 cases per 100,000 SP exposures and 2.6 cases per 100,000 CTX exposures) and in persons positive for human immunodeficiency virus (4.9 cases per 100,000 SP exposures and 8.4 cases per 100,000 CTX exposures). Infrequent treatment doses with SP are associated with a low risk of an adverse cutaneous reaction, and SP can be recommended for treatment of malaria in areas where P. falciparum is susceptible.
- Published
- 2006
49. Heavy cryptosporidial infections in children in northeast Brazil: comparison of Cryptosporidium hominis and Cryptosporidium parvum
- Author
-
Anita Kohli, Kate Dupnik, Ronald Fayer, Cynthia L. Sears, Robert D. Newman, Aldo A. M. Lima, Oluma Y. Bushen, Richard L. Guerrant, and Relana Pinkerton
- Subjects
Veterinary medicine ,animal diseases ,Population ,Cryptosporidiosis ,Cryptosporidium ,Nutritional Status ,Asymptomatic ,Polymerase Chain Reaction ,Host-Parasite Interactions ,Feces ,Species Specificity ,Protozoan infection ,parasitic diseases ,medicine ,Animals ,Humans ,Prospective Studies ,education ,Cryptosporidium parvum ,education.field_of_study ,biology ,Anthropometry ,Public Health, Environmental and Occupational Health ,Urban Health ,Infant ,General Medicine ,biology.organism_classification ,medicine.disease ,Diarrhea ,Lactoferrin ,Infectious Diseases ,Child, Preschool ,Immunology ,Diarrhea, Infantile ,Parasitology ,medicine.symptom ,Cryptosporidium hominis ,Polymorphism, Restriction Fragment Length - Abstract
Cryptosporidium is an important cause of infectious diarrhoea worldwide, but little is known about the course of illness when infected with different species. Over a period of 5 years, Cryptosporidium was identified in the stools of 58 of 157 children prospectively followed from birth in an urban slum (favela) in northeast Brazil. Forty isolates were available for quantification and 42 for speciation (24 Cryptosporidium hominis and 18 C. parvum). Children with C. hominis shed significantly more oocysts/ml of stool (3.5 x 10(6) vs. 1.7 x 10(6)perml; P=0.001), and oocyst counts were higher among symptomatic children (P=0.002). Heavier C. parvum shedding was significantly associated with symptoms (P=0.004), and symptomatic C. parvum-infected children were significantly more likely than asymptomatic children to be lactoferrin-positive (P=0.004). Height-for-age (HAZ) Z-scores showed significant declines within 3 months of infection for children infected with either C. hominis (P=0.028) or C. parvum (P=0.001). However, in the 3-6 month period following infection, only C. hominis-infected children continued to demonstrate declining HAZ score and asymptomatic children showed even greater decline (P=0.01). Cryptosporidium hominis is more common than C. parvum in favela children and is associated with heavier infections and greater growth shortfalls, even in the absence of symptoms.
- Published
- 2006
50. Prevention of malaria during pregnancy in West Africa: policy change and the power of subregional action
- Author
-
Robert D, Newman, Allisyn C, Moran, Kassoum, Kayentao, Elizabeth, Benga-De, Mathias, Yameogo, Oumar, Gaye, Ousmane, Faye, Youssoufa, Lo, Philippe Marc, Moreira, Ogobara, Doumbo, Monica E, Parise, and Richard W, Steketee
- Subjects
Evidence-Based Medicine ,Health Policy ,International Cooperation ,Interprofessional Relations ,Communication Barriers ,Financing, Organized ,Drug Resistance ,Chloroquine ,Africa, Western ,Antimalarials ,Drug Combinations ,Pyrimethamine ,Pregnancy ,Pregnancy Complications, Parasitic ,Sulfadoxine ,Humans ,Female ,Malaria, Falciparum ,Health Education - Abstract
Despite a broadening consensus about the effectiveness of intermittent preventive treatment (IPTp) in preventing the adverse outcomes of malaria during pregnancy, policy change to IPTp was initially limited to East Africa. In West Africa, where the policy change process for the prevention of malaria during pregnancy started much later, IPTp has been taken up swiftly.To describe the factors that contributed to the rapid adoption of policies to prevent malaria during pregnancy in West Africa.Several factors appear to have accelerated the process: (1) recognition of the extent of the problem of malaria during pregnancy and its adverse consequences; (2) a clear, evidence-based program strategy strongly articulated by an important multilateral organization (World Health Organization); (3) subregionally generated evidence to support the proposed strategy; (4) a subregional forum for dissemination of data and discussion regarding the proposed policy changes; (5) widespread availability of the proposed intervention drug (sulfadoxine-pyrimethamine); (6) technical support from reputable and respected institutions in drafting new policies and planning for implementation; (7) donor support for pilot experiences in integrating proposed policy change into a package of preventive services; and (8) financial support for scaling up the proposed interventions.
- Published
- 2006
Catalog
Discovery Service for Jio Institute Digital Library
For full access to our library's resources, please sign in.