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1. Microbiota from human infants consuming secretors or non-secretors mothers’ milk impacts the gut and immune system in mice

Author

Manoj Gurung, Brent Thomas Schlegel, Dhivyaa Rajasundaram, Renee Fox, Lars Bode, Tianming Yao, Stephen R. Lindemann, Tanya LeRoith, Quentin D. Read, Christy Simecka, Laura Carroll, Aline Andres, and Laxmi Yeruva

Subjects
human milk oligosaccharides, HMO, immunity, gastrointestinal tract, neonatal, microbiome, Microbiology, QR1-502
Abstract

ABSTRACTMaternal secretor status is one of the determinants of human milk oligosaccharides (HMOs) composition, which, in turn, influences the gut microbiota composition of infants. To understand if this change in gut microbiota impacts immune cell composition, intestinal morphology, and gene expression, 21-day-old germ-free C57BL/6 mice were transplanted with fecal microbiota from infants whose mothers were either secretors (SMM) or non-secretors (NSM) or from infants consuming dairy-based formula (MFM). For each group, one set of mice was supplemented with HMOs. HMO supplementation did not significantly impact the microbiota diversity; however, SMM mice had a higher abundance of genus Bacteroides, Bifidobacterium, and Blautia, whereas, in the NSM group, there was a higher abundance of Akkermansia, Enterocloster, and Klebsiella. In MFM, gut microbiota was represented mainly by Parabacteroides, Ruminococcaceae_unclassified, and Clostrodium_sensu_stricto. In mesenteric lymph node, Foxp3+ T cells and innate lymphoid cells type 2 were increased in MFM mice supplemented with HMOs, while in the spleen, they were increased in SMM + HMOs mice. Similarly, serum immunoglobulin A was also elevated in MFM + HMOs group. Distinct global gene expression of the gut was observed in each microbiota group, which was enhanced with HMOs supplementation. Overall, our data show that distinct infant gut microbiota due to maternal secretor status or consumption of dairy-based formula and HMO supplementation impacts immune cell composition, antibody response, and intestinal gene expression in a mouse model.IMPORTANCEEarly life factors like neonatal diet modulate gut microbiota, which is important for the optimal gut and immune function. One such factor, human milk oligosaccharides (HMOs), the composition of which is determined by maternal secretor status, has a profound effect on infant gut microbiota. However, how the infant gut microbiota composition determined by maternal secretor status or consumption of infant formula devoid of HMOs impacts infant intestinal ammorphology, gene expression, and immune signature is not well explored. This study provides insights into the differential establishment of infant microbiota derived from infants fed by secretor or non-secretor mothers milk or those consuming infant formula and demonstrates that the secretor status of mothers promotes Bifidobacteria and Bacteroides sps. establishment. This study also shows that supplementation of pooled HMOs in mice changed immune cell composition in the spleen and mesenteric lymph nodes and immunoglobulins in circulation. Hence, this study highlights that maternal secretor status has a role in infant gut microbiota composition, and this, in turn, can impact host gut and immune system.

Published
2024
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2. Elimination of lymphatic filariasis as a public health problem in Malawi.

Author

John Chiphwanya, Square Mkwanda, Storn Kabuluzi, Themba Mzilahowa, Bagrey Ngwira, Dorothy E Matipula, Limbikani Chaponda, Paul Ndhlova, Prince Katchika, Chawananga Mahebere Chirambo, Philemon Moses, Justin Kumala, Martin Chiumia, Carrie Barrett, Hannah Betts, Joan Fahy, Maria Rebollo Polo, Lisa Reimer, Michelle C Stanton, Brent Thomas, Sian Freer, David H Molyneux, Moses J Bockarie, Charles D Mackenzie, Mark J Taylor, Sarah Martindale, and Louise A Kelly-Hope

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

BackgroundLymphatic filariasis (LF) is a parasitic disease transmitted by mosquitoes, causing severe pain, disfiguring, and disabling clinical conditions such as lymphoedema and hydrocoele. LF is a global public health problem affecting 72 countries, primarily in Africa and Asia. Since 2000, the World Health Organization (WHO) has led the Global Programme to Eliminate Lymphatic Filariasis (GPELF) to support all endemic regions. This paper focuses on the achievements of the Malawi LF Elimination Programme between 2000 and 2020 to eliminate LF as a public health problem, making it the second sub-Saharan country to receive validation from the WHO.Methodology/principal findingsThe Malawi LF Programme addressed the widespread prevalence of LF infection and disease across the country, using the recommended WHO GPELF strategies and operational research initiatives in collaboration with key national and international partners. First, to stop the spread of infection (i.e., interrupt transmission) and reduce the circulating filarial antigen prevalence from as high as 74.4% to below the critical threshold of 1-2% prevalence, mass drug administration (MDA) using a two-drug regime was implemented at high coverage rates (>65%) of the total population, with supplementary interventions from other programmes (e.g., malaria vector control). The decline in prevalence was monitored and confirmed over time using several impact assessment and post-treatment surveillance tools including the standard sentinel site, spot check, and transmission assessment surveys and alternative integrated, hotspot, and easy-access group surveys. Second, to alleviate suffering of the affected populations (i.e., control morbidity) the morbidity management and disability prevention (MMDP) package of care was implemented. Specifically, clinical case estimates were obtained via house-to-house patient searching activities; health personnel and patients were trained in self-care protocols for lymphoedema and/or referrals to hospitals for hydrocoele surgery; and the readiness and quality of treatment and services were assessed with new survey tools.ConclusionsMalawi's elimination of LF will ensure that future generations are not infected and suffer from the disfiguring and disabling disease. However, it will be critical that the Malawi LF Elimination programme remains vigilant, focussing on post-elimination surveillance and MMDP implementation and integration into routine health systems to support long-term sustainability and ongoing success.SummaryLymphatic filariasis, also known as elephantiasis, is a disabling, disfiguring, and painful disease caused by a parasite that infected mosquitoes transmit to millions of people worldwide. Since 2000, the Global Programme to Eliminate Lymphatic Filariasis (GPELF) has supported endemic countries such as Malawi in south-eastern Africa, to eliminate the disease as a public health problem. The Malawi National LF Elimination Programme has worked tirelessly over the past two decades to implement the GPELF recommended strategies to interrupt the transmission with a two-drug regime, and to alleviate suffering in patients with lymphoedema and/or hydrocoele through morbidity management and disability prevention. Additionally, the LF Programme has collaborated with national and international stakeholders to implement a range of supplementary operational research projects to address outstanding knowledge gaps and programmatic barriers. In 2020, the World Health Organisation validated that Malawi had successfully eliminated LF as a public health problem, making it the second country in sub-Saharan Africa to achieve this, which is remarkable given that Malawi previously had very high infection rates. The LF Programme now remains vigilant, putting its efforts towards post-elimination surveillance and the continued implementation of care for patients with chronic conditions. Malawi's elimination of LF will ensure that future generations are not affected by this devastating disease.

Published
2024
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3. Stakeholder perspectives from 15 countries in Africa on barriers in snakebite envenoming research and the potential role of research hubs.

Author

Ymkje Stienstra, Leslie Mawuli Aglanu, Janna M Schurer, Rhona Mijumbi, Jean Bosco Mbonigaba, Abdulrazaq G Habib, Brent Thomas, Jonathan Steinhorst, Rachael Thomson, Sara Padidar, John H Amuasi, George O Oluoch, and David G Lalloo

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

Snakebite envenoming is a debilitating neglected tropical disease disproportionately affecting the rural poor in low and middle-income countries in the tropics and sub-tropics. Critical questions and gaps in public health and policy need to be addressed if major progress is to be made towards reducing the negative impact of snakebite, particularly in the World Health Organisation (WHO) Africa region. We engaged key stakeholders to identify barriers to evidence-based snakebite decision making and to explore how development of research and policy hubs could help to overcome these barriers. We conducted an electronic survey among 73 stakeholders from ministries of health, health facilities, academia and non-governmental organizations from 15 countries in the WHO Africa region. The primary barriers to snakebite research and subsequent policy translation were limited funds, lack of relevant data, and lack of interest from policy makers. Adequate funding commitment, strong political will, building expert networks and a demand for scientific evidence were all considered potential factors that could facilitate snakebite research. Participants rated availability of antivenoms, research skills training and disease surveillance as key research priorities. All participants indicated interest in the development of research and policy hubs and 78% indicated their organization would be willing to actively participate. In conclusion, our survey affirms that relevant stakeholders in the field of snakebite perceive research and policy hubs as a promising development, which could help overcome the barriers to pursuing the WHO goals and targets for reducing the burden of snakebite.

Published
2023
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4. Snakebite epidemiology, outcomes and multi-cluster risk modelling in Eswatini.

Author

Sara Padidar, Ara Monadjem, Thea Litschka-Koen, Brent Thomas, Nondusimo Shongwe, Clare Baker, Lindelwa Mmema, Trevor Sithole, James Murray, Nicholas R Casewell, Jonathan Pons, David G Lalloo, Robert A Harrison, Ymkje Stienstra, and Wisdom M Dlamini

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

BackgroundHalving snakebite morbidity and mortality by 2030 requires countries to develop both prevention and treatment strategies. The paucity of data on the global incidence and severity of snakebite envenoming causes challenges in prioritizing and mobilising resources for snakebite prevention and treatment. In line with the World Health Organisation's 2019 Snakebite Strategy, this study sought to investigate Eswatini's snakebite epidemiology and outcomes, and identify the socio-geographical factors associated with snakebite risk.MethodologyProgrammatic data from the Ministry of Health, Government of Eswatini 2019-2021, was used to assess the epidemiology and outcomes of snakebite in Eswatini. We developed a snake species richness map from the occurrence data of all venomous snakes of medical importance in Eswatini that was subjected to niche modelling. We formulated four risk indices using snake species richness, various geospatial datasets and reported snakebites. A multivariate cluster modelling approach using these indices was developed to estimate risk of snakebite and the outcomes of snakebite in Eswatini.Principal findingsAn average of 466 snakebites was recorded annually in Eswatini. Bites were recorded across the entire country and peaked in the evening during summer months. Two cluster risk maps indicated areas of the country with a high probability of snakebite and a high probability of poor snakebite outcomes. The areas with the highest rate of snakebite risk were primarily in the rural and agricultural regions of the country.SignificanceThese models can be used to inform better snakebite prevention and treatment measures to enable Eswatini to meet the global goal of reducing snakebite morbidity and mortality by 50% by 2030. The supply chain challenges of antivenom affecting southern Africa and the high rates of snakebite identified in our study highlight the need for improved snakebite prevention and treatment tools that can be employed by health care workers stationed at rural, community clinics.

Published
2023
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5. Two snakebite antivenoms have potential to reduce Eswatini's dependency upon a single, increasingly unavailable product: Results of preclinical efficacy testing.

Author

Stefanie K Menzies, Thea Litschka-Koen, Rebecca J Edge, Jaffer Alsolaiss, Edouard Crittenden, Steven R Hall, Adam Westhorpe, Brent Thomas, James Murray, Nondusimo Shongwe, Sara Padidar, David G Lalloo, Nicholas R Casewell, Jonathan Pons, and Robert A Harrison

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

BackgroundSnakebite is a major public health concern in Eswatini, where treatment relies upon one antivenom-SAIMR Polyvalent. Although effective in treating snakebite, SAIMR Polyvalent is difficult to source outside its manufacturing country (South Africa) and is dauntingly expensive. We compared the preclinical venom-neutralising efficacy of two alternative antivenoms with that of SAIMR Polyvalent against the lethal and tissue-destructive effects of venoms from five species of medically important snakes using in vivo murine assays. The test antivenoms were 'Panafrican' manufactured by Instituto Clodomiro Picado and 'PANAF' manufactured by Premium Serums & Vaccines.Principal findingsIn vivo murine preclinical studies identified both test antivenoms were equally or more effective than SAIMR Polyvalent at neutralising lethal and tissue-destructive effects of Naja mossambica venom. Both test antivenoms were less effective than SAIMR Polyvalent at neutralising the lethal effects of Bitis arietans, Dendroaspis polylepis, Hemachatus haemachatus and Naja annulifera venoms, but similarly effective at neutralising tissue damage induced by B. arietans and H. haemachatus venoms. In vitro immunological assays identified that the titres and toxin-specificities of immunoglobulins (iGs) in the test antivenoms were comparable to that of SAIMR Polyvalent. Plasma clotting disturbances by H. haemachatus and N. mossambica were neutralised by the test antivenoms, whereas SAIMR Polyvalent failed to neutralise this bioactivity of N. mossambica venom. B. arietans SVMP activity was equally reduced by all three antivenoms, and H. haemachatus and N. mossambica PLA2 activities were neutralised by all three antivenoms.ConclusionsWhile both Panafrican and PANAF antivenoms exhibited promising preclinical efficacies, both were less poly-specifically effective than SAIMR Polyvalent in these murine assays. The efficacy of these antivenoms against the lethal and tissue-destructive effects of N. mossambica venom, the most common biting species in Eswatini, identify that Panafrican and PANAF antivenoms offer effective alternatives to SAIMR Polyvalent for the treatment of snakebite in Eswatini, and potentially for neighbouring countries.

Published
2022
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6. Temporal and spatial trends in insecticide resistance in Anopheles arabiensis in Sudan: outcomes from an evaluation of implications of insecticide resistance for malaria vector control

Author

Bashir Adam Ismail, Hmooda Toto Kafy, Jihad Eltaher Sulieman, Krishanthi Subramaniam, Brent Thomas, Abraham Mnzava, Nur Faeza Abu Kassim, Abu Hassan Ahmad, Tessa B. Knox, Immo Kleinschmidt, and Martin J. Donnelly

Subjects
Anopheles arabiensis, Deltamethrin, Bendiocarb, Susceptibility bioassay, Combination, Resistance management, Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Long-lasting insecticidal nets (LLINs) (with pyrethroids) and indoor residual spraying (IRS) are the cornerstones of the Sudanese malaria control program. Insecticide resistance to the principal insecticides in LLINs and IRS is a major concern. This study was designed to monitor insecticide resistance in Anopheles arabiensis from 140 clusters in four malaria-endemic areas of Sudan from 2011 to 2014. All clusters received LLINs, while half (n = 70), distributed across the four regions, had additional IRS campaigns. Methods Anopheles gambiae (s.l.) mosquitoes were identified to species level using PCR techniques. Standard WHO insecticide susceptibility bioassays were carried out to detect resistance to deltamethrin (0.05%), DDT (4%) and bendiocarb (0.1%). TaqMan assays were performed on random samples of deltamethrin-resistant phenotyped and pyrethrum spray collected individuals to determine Vgsc-1014 knockdown resistance mutations. Results Anopheles arabiensis accounted for 99.9% of any anopheline species collected across all sites. Bioassay screening indicated that mosquitoes remained susceptible to bendiocarb but were resistance to deltamethrin and DDT in all areas. There were significant increases in deltamethrin resistance over the four years, with overall mean percent mortality to deltamethrin declining from 81.0% (95% CI: 77.6–84.3%) in 2011 to 47.7% (95% CI: 43.5–51.8%) in 2014. The rate of increase in phenotypic deltamethrin-resistance was significantly slower in the LLIN + IRS arm than in the LLIN-only arm (Odds ratio 1.34; 95% CI: 1.02–1.77). The frequency of Vgsc-1014F mutation varied spatiotemporally with highest frequencies in Galabat (range 0.375–0.616) and New Halfa (range 0.241–0.447). Deltamethrin phenotypic-resistance correlated with Vgsc-1014F frequency. Conclusion Combining LLIN and IRS, with different classes of insecticide, may delay pyrethroid resistance development, but the speed at which resistance develops may be area-specific. Continued monitoring is vital to ensure optimal management and control.

Published
2018
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7. Loa loa vectors Chrysops spp.: perspectives on research, distribution, bionomics, and implications for elimination of lymphatic filariasis and onchocerciasis

Author

Louise Kelly-Hope, Rossely Paulo, Brent Thomas, Miguel Brito, Thomas R. Unnasch, and David Molyneux

Subjects
Loa loa, Loiasis, Tropical eye worm, Chrysops, Vector control, Lymphatic filariasis, Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Loiasis is a filarial disease caused Loa loa. The main vectors are Chrysops silacea and C. dimidiata which are confined to the tropical rainforests of Central and West Africa. Loiasis is a mild disease, but individuals with high microfilaria loads may suffer from severe adverse events if treated with ivermectin during mass drug administration campaigns for the elimination of lymphatic filariasis and onchocerciasis. This poses significant challenges for elimination programmes and alternative interventions are required in L. loa co-endemic areas. The control of Chrysops has not been considered as a viable cost-effective intervention; we reviewed the current knowledge of Chrysops vectors to assess the potential for control as well as identified areas for future research. Results We identified 89 primary published documents on the two main L. loa vectors C. silacea and C dimidiata. These were collated into a database summarising the publication, field and laboratory procedures, species distributions, ecology, habitats and methods of vector control. The majority of articles were from the 1950–1960s. Field studies conducted in Cameroon, Democratic Republic of Congo, Equatorial Guinea, Nigeria and Sudan highlighted that C. silacea is the most important and widespread vector. This species breeds in muddy streams or swampy areas of forests or plantations, descends from forest canopies to feed on humans during the day, is more readily adapted to human dwellings and attracted to wood fires. Main vector targeted measures proposed to impact on L. loa transmission included personal repellents, household screening, indoor residual spraying, community-based environmental management, adulticiding and larviciding. Conclusions This is the first comprehensive review of the major L. loa vectors for several decades. It highlights key vector transmission characteristics that may be targeted for vector control providing insights into the potential for integrated vector management, with multiple diseases being targeted simultaneously, with shared human and financial resources and multiple impact. Integrated vector management programmes for filarial infections, especially in low transmission areas of onchocerciasis, require innovative approaches and alternative strategies if the elimination targets established by the World Health Organization are to be achieved.

Published
2017
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8. Optimising cluster survey design for planning schistosomiasis preventive chemotherapy.

Author

Sarah C L Knowles, Hugh J W Sturrock, Hugo Turner, Jane M Whitton, Charlotte M Gower, Samuel Jemu, Anna E Phillips, Aboulaye Meite, Brent Thomas, Karsor Kollie, Catherine Thomas, Maria P Rebollo, Ben Styles, Michelle Clements, Alan Fenwick, Wendy E Harrison, and Fiona M Fleming

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

The cornerstone of current schistosomiasis control programmes is delivery of praziquantel to at-risk populations. Such preventive chemotherapy requires accurate information on the geographic distribution of infection, yet the performance of alternative survey designs for estimating prevalence and converting this into treatment decisions has not been thoroughly evaluated.We used baseline schistosomiasis mapping surveys from three countries (Malawi, Côte d'Ivoire and Liberia) to generate spatially realistic gold standard datasets, against which we tested alternative two-stage cluster survey designs. We assessed how sampling different numbers of schools per district (2-20) and children per school (10-50) influences the accuracy of prevalence estimates and treatment class assignment, and we compared survey cost-efficiency using data from Malawi. Due to the focal nature of schistosomiasis, up to 53% simulated surveys involving 2-5 schools per district failed to detect schistosomiasis in low endemicity areas (1-10% prevalence). Increasing the number of schools surveyed per district improved treatment class assignment far more than increasing the number of children sampled per school. For Malawi, surveys of 15 schools per district and 20-30 children per school reliably detected endemic schistosomiasis and maximised cost-efficiency. In sensitivity analyses where treatment costs and the country considered were varied, optimal survey size was remarkably consistent, with cost-efficiency maximised at 15-20 schools per district.Among two-stage cluster surveys for schistosomiasis, our simulations indicated that surveying 15-20 schools per district and 20-30 children per school optimised cost-efficiency and minimised the risk of under-treatment, with surveys involving more schools of greater cost-efficiency as treatment costs rose.

Published
2017
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9. Elimination of lymphatic filariasis in the Gambia.

Author

Maria P Rebollo, Sana Malang Sambou, Brent Thomas, Nana-Kwadwo Biritwum, Momodou C Jaye, Louise Kelly-Hope, Alba Gonzalez Escalada, David H Molyneux, and Moses J Bockarie

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

BACKGROUND:The prevalence of Wuchereria bancrofti, which causes lymphatic filariasis (LF) in The Gambia was among the highest in Africa in the 1950s. However, surveys conducted in 1975 and 1976 revealed a dramatic decline in LF endemicity in the absence of mass drug administration (MDA). The decline in prevalence was partly attributed to a significant reduction in mosquito density through the widespread use of insecticidal nets. Based on findings elsewhere that vector control alone can interrupt LF, we asked the question in 2013 whether the rapid scale up in the use of insecticidal nets in The Gambia had interrupted LF transmission. METHODOLOGY/PRINCIPAL FINDING:We present here the results of three independently designed filariasis surveys conducted over a period of 17 years (1997-2013), and involving over 6000 subjects in 21 districts across all administrative divisions in The Gambia. An immunochromatographic (ICT) test was used to detect W. bancrofti antigen during all three surveys. In 2001, tests performed on stored samples collected between 1997 and 2000, in three divisions, failed to show positive individuals from two divisions that were previously highly endemic for LF, suggesting a decline towards extinction in some areas. Results of the second survey conducted in 2003 showed that LF was no longer endemic in 16 of 21 districts surveyed. The 2013 survey used a WHO recommended LF transmission verification tool involving 3180 6-7 year-olds attending 60 schools across the country. We demonstrated that transmission of W. bancrofti has been interrupted in all 21 districts. CONCLUSIONS:We conclude that LF transmission may have been interrupted in The Gambia through the extensive use of insecticidal nets for malaria control for decades. The growing evidence for the impact of malaria vector control activities on parasite transmission has been endorsed by WHO through a position statement in 2011 on integrated vector management to control malaria and LF.

Published
2015
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10. Cessation of mass drug administration for lymphatic filariasis in Zanzibar in 2006: was transmission interrupted?

Author

Maria P Rebollo, Khalfan A Mohammed, Brent Thomas, Shaali Ame, Said Mohammed Ali, Jorge Cano, Alba Gonzalez Escalada, and Moses J Bockarie

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

BACKGROUND:Lymphatic filariasis (LF) is targeted for elimination through annual mass drug administration (MDA) for 4-6 years. In 2006, Zanzibar stopped MDA against LF after five rounds of MDA revealed no microfilaraemic individuals during surveys at selected sentinel sites. We asked the question if LF transmission was truly interrupted in 2006 when MDA was stopped. METHODOLOGY/PRINCIPAL FINDINGS:In line with ongoing efforts to shrink the LF map, we performed the WHO recommended transmission assessment surveys (TAS) in January 2012 to verify the absence of LF transmission on the main Zanzibar islands of Unguja and Pemba. Altogether, 3275 children were tested on both islands and 89 were found to be CFA positive; 70 in Pemba and 19 in Unguja. The distribution of schools with positive children was heterogeneous with pronounced spatial variation on both islands. Based on the calculated TAS cut-offs of 18 and 20 CFA positive children for Pemba and Unguja respectively, we demonstrated that transmission was still ongoing in Pemba where the cut-off was exceeded. CONCLUSIONS:Our findings indicated ongoing transmission of LF on Pemba in 2012. Moreover, we presented evidence from previous studies that LF transmission was also active on Unguja shortly after stopping MDA in 2006. Based on these observations the government of Zanzibar decided to resume MDA against LF on both islands in 2013.

Published
2015
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14. Stratigraphy and structure of the Drake Point Anticline, Sabine Peninsula, Canadian Arctic Islands

Author

Dewing, Keith, Brake, Virginia, Duchesne, Mathieu J., Brent, Thomas A., and Joyce, Nancy

Subjects
Arctic Archipelago -- Natural history, Anticlines -- Natural history, Geology, Stratigraphic -- Research, Grabens (Geology) -- Research, Petroleum -- Natural history, Earth sciences
Abstract

Abstract: Modern processing methods were applied to 3400 line-kilometres of legacy seismic data from Sabine Peninsula of Melville Island in the Canadian Arctic Islands. Post-stack reprocessing improved the imaging, allowing [...]

Published
2016

15. The Use of Conversational Laughter by an Individual with Dementia

Author

Wilson, Brent Thomas, Muller, Nicole, and Damico, Jack S.

Abstract

While laughter has been shown to play a significant role in any social interaction; its conversational usage by a person with dementia has rarely been investigated. This paper will investigate the functional aspects of laughter during conversation in an individual with dementia. Conversation analysis is used in order to investigate laughter as a social phenomenon and to be able to investigate laughter in an empirical and authentic manner. The conversational strategies employed through laughter will be detailed and implications will be discussed. [Includes appendix of symbols used in transcription.]

Published
2007
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18. A Comparison of Transportation Systems for Human Missions to Mars

Author

Brand Griffin, Brent Thomas, Diane Vaughan, Bret Drake, Les Johnson, and Gordon Woodcock

Subjects
Air Transportation And Safety
Abstract

There are many ways to send humans to Mars. Credible technical reports can be traced to the 1950's. More recently, NASA has funded major studies that depict a broad variety of trajectories, technologies, stay times, and costs. Much of this data is still valid with direct application to today's exploration planning. This paper presents results comparing these studies with particular emphasis on the in-space transportation aspects of the mission. Specifically, comparisons are made on propulsion systems used for getting the crew and mission equipment from Earth orbit to Mars orbit, descending and ascending from the surface, and returning to Earth orbit. Areas of comparison for each of these phases include crew size, mission mass, propellant mass, delta v, specific impulse, transit time, surface stay time, aero-braking, and others. Data is analyzed to demonstrate either strong trends toward particular technologies or diverging solutions.

Published
2004
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20. Temporal and spatial trends in insecticide resistance in Anopheles arabiensis in Sudan: outcomes from an evaluation of implications of insecticide resistance for malaria vector control

Author

Tessa B. Knox, Bashir Adam Ismail, Krishanthi Subramaniam, Nur Faeza Abu Kassim, Brent Thomas, Jihad Eltaher Sulieman, Abraham Mnzava, Hmooda Toto Kafy, Immo Kleinschmidt, Abu Hassan Ahmad, and Martin J. Donnelly

Subjects
0301 basic medicine, Veterinary medicine, Insecticides, Mosquito Control, Resistance management, Bendiocarb, Anopheles gambiae, Pyrethrum, 030231 tropical medicine, Indoor residual spraying, Mosquito Vectors, lcsh:Infectious and parasitic diseases, Insecticide Resistance, Sudan, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Anopheles, Nitriles, Pyrethrins, parasitic diseases, qx_600, Anopheles arabiensis, Animals, Susceptibility bioassay, lcsh:RC109-216, Insecticide-Treated Bednets, biology, Research, wa_240, Knockdown resistance, biology.organism_classification, Malaria, 030104 developmental biology, Infectious Diseases, Deltamethrin, chemistry, Parasitology, qx_650, qx_510, Combination, Biological Assay, Female, qx_515
Abstract

Background Long-lasting insecticidal nets (LLINs) (with pyrethroids) and indoor residual spraying (IRS) are the cornerstones of the Sudanese malaria control program. Insecticide resistance to the principal insecticides in LLINs and IRS is a major concern. This study was designed to monitor insecticide resistance in Anopheles arabiensis from 140 clusters in four malaria-endemic areas of Sudan from 2011 to 2014. All clusters received LLINs, while half (n = 70), distributed across the four regions, had additional IRS campaigns. Methods Anopheles gambiae (s.l.) mosquitoes were identified to species level using PCR techniques. Standard WHO insecticide susceptibility bioassays were carried out to detect resistance to deltamethrin (0.05%), DDT (4%) and bendiocarb (0.1%). TaqMan assays were performed on random samples of deltamethrin-resistant phenotyped and pyrethrum spray collected individuals to determine Vgsc-1014 knockdown resistance mutations. Results Anopheles arabiensis accounted for 99.9% of any anopheline species collected across all sites. Bioassay screening indicated that mosquitoes remained susceptible to bendiocarb but were resistance to deltamethrin and DDT in all areas. There were significant increases in deltamethrin resistance over the four years, with overall mean percent mortality to deltamethrin declining from 81.0% (95% CI: 77.6–84.3%) in 2011 to 47.7% (95% CI: 43.5–51.8%) in 2014. The rate of increase in phenotypic deltamethrin-resistance was significantly slower in the LLIN + IRS arm than in the LLIN-only arm (Odds ratio 1.34; 95% CI: 1.02–1.77). The frequency of Vgsc-1014F mutation varied spatiotemporally with highest frequencies in Galabat (range 0.375–0.616) and New Halfa (range 0.241–0.447). Deltamethrin phenotypic-resistance correlated with Vgsc-1014F frequency. Conclusion Combining LLIN and IRS, with different classes of insecticide, may delay pyrethroid resistance development, but the speed at which resistance develops may be area-specific. Continued monitoring is vital to ensure optimal management and control. Electronic supplementary material The online version of this article (10.1186/s13071-018-2732-9) contains supplementary material, which is available to authorized users.

Published
2018

22. Loa loa vectors Chrysops spp.: perspectives on research, distribution, bionomics, and implications for elimination of lymphatic filariasis and onchocerciasis

Author

Rossely Paulo, Thomas R. Unnasch, David H. Molyneux, Louise A. Kelly-Hope, Brent Thomas, and Miguel Brito

Subjects
Indoor residual spraying, Review, Onchocerciasis, Loa, 0302 clinical medicine, Ivermectin, Insect vectors, 030212 general & internal medicine, Socioeconomics, Lymphatic filariasis, Neglected tropical diseases, wa_30, biology, Ecology, Loa loa, Infectious Diseases, Tropical eye worm, medicine.drug, wc_880, 030231 tropical medicine, Bionomics, NTDs, wc_885, Microfilaria, wa_110, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Loiasis, parasitic diseases, qx_600, medicine, Animals, Humans, lcsh:RC109-216, Disease Eradication, Disease eradication, Diptera, Animal distribution, biology.organism_classification, medicine.disease, Vector control, Insect Vectors, qx_650, Vector (epidemiology), Africa, Parasitology, Chrysops, Integrated vector management, Animal Distribution
Abstract

Background Loiasis is a filarial disease caused Loa loa. The main vectors are Chrysops silacea and C. dimidiata which are confined to the tropical rainforests of Central and West Africa. Loiasis is a mild disease, but individuals with high microfilaria loads may suffer from severe adverse events if treated with ivermectin during mass drug administration campaigns for the elimination of lymphatic filariasis and onchocerciasis. This poses significant challenges for elimination programmes and alternative interventions are required in L. loa co-endemic areas. The control of Chrysops has not been considered as a viable cost-effective intervention; we reviewed the current knowledge of Chrysops vectors to assess the potential for control as well as identified areas for future research. Results We identified 89 primary published documents on the two main L. loa vectors C. silacea and C dimidiata. These were collated into a database summarising the publication, field and laboratory procedures, species distributions, ecology, habitats and methods of vector control. The majority of articles were from the 1950–1960s. Field studies conducted in Cameroon, Democratic Republic of Congo, Equatorial Guinea, Nigeria and Sudan highlighted that C. silacea is the most important and widespread vector. This species breeds in muddy streams or swampy areas of forests or plantations, descends from forest canopies to feed on humans during the day, is more readily adapted to human dwellings and attracted to wood fires. Main vector targeted measures proposed to impact on L. loa transmission included personal repellents, household screening, indoor residual spraying, community-based environmental management, adulticiding and larviciding. Conclusions This is the first comprehensive review of the major L. loa vectors for several decades. It highlights key vector transmission characteristics that may be targeted for vector control providing insights into the potential for integrated vector management, with multiple diseases being targeted simultaneously, with shared human and financial resources and multiple impact. Integrated vector management programmes for filarial infections, especially in low transmission areas of onchocerciasis, require innovative approaches and alternative strategies if the elimination targets established by the World Health Organization are to be achieved. Electronic supplementary material The online version of this article (doi:10.1186/s13071-017-2103-y) contains supplementary material, which is available to authorized users.

Published
2017

23. Elimination of lymphatic filariasis in the Gambia

Author

Brent Thomas, Sana Sambou, Alba Gonzalez Escalada, Momodou C. Jaye, David H. Molyneux, Nana-Kwadwo Biritwum, Louise A. Kelly-Hope, Maria P. Rebollo, and Moses J. Bockarie

Subjects
Adult, Male, Veterinary medicine, Insecticides, wc_880, lcsh:Arctic medicine. Tropical medicine, Mosquito Control, lcsh:RC955-962, wa_395, medicine.disease_cause, law.invention, Filariasis, Elephantiasis, Filarial, law, qx_301, Environmental health, Surveys and Questionnaires, parasitic diseases, qx_600, medicine, Prevalence, Animals, Humans, Wuchereria bancrofti, Disease Eradication, Insecticide-Treated Bednets, Mass drug administration, Lymphatic filariasis, business.industry, lcsh:Public aspects of medicine, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, medicine.disease, Insect Vectors, Mosquito control, Infectious Diseases, Transmission (mechanics), Neglected tropical diseases, Gambia, business, Malaria, Research Article
Abstract

Background The prevalence of Wuchereria bancrofti, which causes lymphatic filariasis (LF) in The Gambia was among the highest in Africa in the 1950s. However, surveys conducted in 1975 and 1976 revealed a dramatic decline in LF endemicity in the absence of mass drug administration (MDA). The decline in prevalence was partly attributed to a significant reduction in mosquito density through the widespread use of insecticidal nets. Based on findings elsewhere that vector control alone can interrupt LF, we asked the question in 2013 whether the rapid scale up in the use of insecticidal nets in The Gambia had interrupted LF transmission. Methodology/Principal Finding We present here the results of three independently designed filariasis surveys conducted over a period of 17 years (1997–2013), and involving over 6000 subjects in 21 districts across all administrative divisions in The Gambia. An immunochromatographic (ICT) test was used to detect W. bancrofti antigen during all three surveys. In 2001, tests performed on stored samples collected between 1997 and 2000, in three divisions, failed to show positive individuals from two divisions that were previously highly endemic for LF, suggesting a decline towards extinction in some areas. Results of the second survey conducted in 2003 showed that LF was no longer endemic in 16 of 21 districts surveyed. The 2013 survey used a WHO recommended LF transmission verification tool involving 3180 6–7 year-olds attending 60 schools across the country. We demonstrated that transmission of W. bancrofti has been interrupted in all 21 districts. Conclusions We conclude that LF transmission may have been interrupted in The Gambia through the extensive use of insecticidal nets for malaria control for decades. The growing evidence for the impact of malaria vector control activities on parasite transmission has been endorsed by WHO through a position statement in 2011 on integrated vector management to control malaria and LF., Author Summary The prevalence of lymphatic filariasis (LF), in The Gambia was among the highest in Africa in the 1950s when about 50% of the adult population was positive for microfilaraemia. However, surveys conducted in 1975 and 1976 revealed a dramatic decline in LF endemicity in the absence of systematic treatment with anti-filaria medicines. This decline in LF prevalence in all villages was partly attributed to a significant drop in human-mosquito contact through a sustained reduction in rainfall in the 1960s and 1970s and the widespread use of insecticidal nets to protect against malaria. We asked the question in 2013 whether the rapid scale up in the use of insecticidal nets for malaria control in Gambia had resulted in the interruption of LF transmission. In this paper we present the results of three independently designed filariasis surveys conducted over a period of 17 years (1997–2013), and involving over 6000 subjects in 21 districts across all administrative divisions in the country. In 2001, tests performed to detect circulating filarial antigens (CFA) in serum samples collected between 1997 and 2000, in three divisions, failed to show positive individuals from two that were previously highly endemic for the LF. Results of the second survey conducted in 2003 indicated that five of the 21 districts were slightly endemic for LF with CFA rates of 1% or 2% but MDA was never implemented in The Gambia. The results of our final survey conducted in 2013 were unequivocal in confirming the absence of transmission of LF in all 21 districts surveyed using WHO recommended statistically robust and validated tool known as transmission assessment survey (TAS). The Gambia achieving a non-endemic status for LF represents a significant step in the efforts to shrink the filariasis endemicity map and demonstrates the value of cross sector approaches in disease control.

Published
2015

24. Readers Report.

Author

Bird, Ronald, Mandel, Michael, Willson, Steven, Brent, Thomas, Welsh, Frank, Gourley, Janet M., Leonard, Jeremy, Fanning, Thomas H., Maraviglia, Frank L., Purcell, Howard, Patton, Sam, Haas, Mark R., Daniels, Bret, Bohdan, Tim, and Leone, Joseph T.

Subjects
LETTERS to the editor, BRAINSTORMING, WINES, SAVINGS, FINANCE
Abstract

The article presents letters to the editor in response to articles in previous issues, including "What's really propping up the economy," in the September 25, 2006 issue, "The truth about brainstorming," in the September 25, 2006 issue, and "Jack of two grapes, master of both," by Robert Parker in the September 4, 2006 issue.

Published
2006

25. Effects of the frequency and satisfaction with leisure profile on dementia caregivers distress.

Author

Romero-Moreno, Rosa, Losada, Andrés, Márquez-González, María, and Mausbach, Brent Thomas

Subjects
TREATMENT of dementia, PSYCHOLOGY of caregivers, PATIENT satisfaction, PSYCHOLOGICAL distress, PSYCHOLOGICAL adaptation, MENTAL depression
Abstract

Copyright of Anales de Psicología is the property of Servicio de Publicaciones de la Universidad de Murcia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2014
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27. Acoustic impedance inversion and seismic reflection continuity analysis for delineating gas hydrate resources near the Mallik research sites, Mackenzie Delta, Northwest Territories, Canada.

Author

Riedel, Michael, Bellefleur, Gilles, Mair, Stephanie, Brent, Thomas A., and Dallimore, Scott R.

Subjects
ACOUSTIC impedance, SEISMIC reflection method, GAS hydrates
Abstract

We combine acoustic impedance inversion of 3D seismic data, log-to-seismic correlation, and seismic attribute analyses to delineate gas-hydrate zones at the Mallik site, Mackenzie Delta, Northwest Territories, Canada. Well-log data define three distinct hydrate zones over a depth range of 890-1100 ml Synthetic seismic modeling indicates the base of the two deeper hydrate zones are prominent reflectors. The uppermost gas-hydrate zone correlates to seismic data with a lower degree of confidence. The extent and geometry of the two lower hydrate zones suggest that local geology plays a significant role in the lateral and vertical distribution of gas hydrate at Mallik. The reliability of the hydrate concentrations calculated from the inverted impedances is qualified by the match between original and synthetic seismic data to produce confidence maps for the two lower gas-hydrate-bearing intervals. A total in-place volume estimate of solid gas hydrate for an area of 1.44 km² around well 5L-38 yields a value of approximately 45 x 106 m³ (equivalently, 6.6 x 109 m³ of gas). We further qualify our mapping of gas hydrates by some amount of continuous resource, defined as lateral continuity measured by seismic attribute similarity and sand-dominated rock. Using these attributes, the continuous amount of hydrate at Mallik is about half the in-place volume (i.e., 25 x 106 m²). Elsewhere within the 3D seismic cube, the seismic impedance inversion yields evidence of potential gas-hydrate deposits near wells A-06 and P-59 at levels near the predicted base of the hydrate stability zone. [ABSTRACT FROM AUTHOR]

Published
2009
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30. DNA Replication in Methotrexate-Treated Human Lymphoblasts.

Author

Fridland, Arnold and Brent, Thomas P.

Subjects
*METHOTREXATE, *HETEROCYCLIC compounds, *FOLIC acid antagonists, *IMMUNOSUPPRESSIVE agents, *ANTINEOPLASTIC agents, *GENES
Abstract

The rate of DNA synthesis in cultures of human lymphoblasts decreased more than 80% within 30 min after the cells were exposed to methotrexate, a potent inhibitor of dihydrofolate reductase. Despite this rapid initial inhibition, DNA continued to be synthesized for at least an additional 6 h. The mode of this subsequent replication appeared to be semiconservative, as indicated by the buoyant density of 5-bromodeoxyuridine-substituted DNA in alkaline CsCl gradients. The growth rates of DNA chains in cells exposed to methotrexate were determined by sedimentation rate analysis in alkaline sucrose gradients. DNA synthesized during 2-min or 10-min pulses with labeled deoxycitidine in the presence of methotrexate had about the same sedimentation coefficient, 35 S, as controls. When methotrexate-treated cultures were pulse-labeled for 10 min and then chased for various times, DNA fragments of about 80 S accumulated. DNA synthesized in the presence of methotrexate was stable and elongated to bulk-size DNA after methotrexate inhibition of growth was removed by addition of thymidine and deoxycytidine. The data suggest that methotrexate reduces the rate of DNA replication by inhibiting chain initiation independently of chain elongation. [ABSTRACT FROM AUTHOR]

Published
1975
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35. Effect of DNA Polymerase on the Nuclei from Different Phases of Cell Cycle.

Author

Bernard, Ora, Momparler, Richard L., and Brent, Thomas P.

Subjects
DNA replication, DNA polymerases, HELA cells, CELL nuclei, CELL cycle, CYTOPLASM
Abstract

DNA replication was investigated in isolated HeLa cell nuclei from different phases of the cell cycle. The addition of S-phase cytoplasm to S-phase nuclei restored the ability of these nuclei to synthesize DNA. The S-phase cytoplasm requirement could be replaced by partially purified calfthymus DNA polymerases A and B. The activity of both the S-phase cytoplasm and purified DNA polymerases in the nuclear system was ATP-dependent. Using nuclei prelabelied with bromodeoxyuridine and CsCl equilibrium centrifugation, the DNA synthesis in vitro was shown to be of the replicative, not repair type when supported by either S-phase cytoplasm or DNA polymerase A. DNA polymerase B, but not DNA polymerase A, was capable of using G1 nuclei to synthesize DNA; however, this synthesis was not ATP-dependent. Gel-filtration chromatography of HeLa cell-free extracts have shown that DNA polymerases B and C are present in S-phase and missing in G1-phase cells. [ABSTRACT FROM AUTHOR]

Published
1974
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39. Changes in O6-methylguanine-DNA methyltransferase expression during immortalization of cloned human fibroblasts.

Author

Harris, Linda C., von Wronski, Mathew A., Venable, Carol C., Remack, Joanna S., Howell, Sherie R., and Brent, Thomas P.

Abstract

Suppressed expression of the DNA repair enzyme O6-methylguanine-DNA methyltransferase (MGMT), characterized as the Mer− phenotype, occurs only in malignant or transformed cell lines. To investigate the relationship between the transformation process and loss of MGMT expression, we derived 20 cloned lines of IMR90 normal fibroblasts transfected with the plasmid pSV3neo expressing the SV40 large-T antigen. Of the five lines that were grown until crisis phase, four emerged as continuously proliferating immortal lines. Of these, only one retained MGMT, the other three having become Mer−. In every case the loss of MGMT coincided with the final phase of immortalization following crisis. Because these were cloned cell lines it is clear that the phenotypic change to Mer− is not merely due to selection of a Mer− cell from the initial population, but must involve a cellular change in MGMT regulation, but must involve a cellular change in MGMT regulation. It is not clear if increased mutation rate associated with loss of MGMT results in increased frequency of an immortalization event or if an immortalization event, such as telomere disruption, results in MGMT suppression. In addition, we have shown that, consistent with previous observations, both hypermethylation in promoter sequences and hypomethylation of downstream sequences in the body of the gene were closely associated with loss of MGMT expression. These studies also illustrate the utility of these new cloned cell lines for characterizing molecular events associated with transformation and immortalization. [ABSTRACT FROM PUBLISHER]

Published
1996
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40. Localization of methylation sites in the human O-methylguanine-DNA methyltransferase promoter: correlation with gene suppression.

Author

Qian, Xilin, von Wronski, Mathew A., and Brent, Thomas P.

Abstract

Adducts of -alkylguanine in DNA that are induced by cytotoxic, carcinogenic or mutagenic alkylating agents can be removed by the DNA repair enzyme -methylguanine-DNA methyltransferase (MGMT). Human tumor cell lines that do not express this enzyme (Mer) are hypersensitive to the effects of such alkylating agents, although the molecular basis of MGMT gene suppression is not yet understood. Previous studies suggested that Mer cells deficient in this enzyme lack neither the gene nor the -acting factors necessary for normal transcription. Methylation of CpG dinucleotides is an attractive mechanism to account for suppression of the MGMT gene; however, there have been reports of both direct and inverse correlations between methylation and MGMT expression. We previously demonstrated an inverse correlation between methylation at a single l site in the human MGMT promoter and gene expression. To substantiate this observation, we examined additional CpGs in the promoters of three Mer and three Mer cell lines, using rare methyl-ation-sensitive restriction sites, and then sought to identify the region where methylation correlated with gene expression. Six CpGs in the region from -245 bp to +225 bp (relative to the transcription start site) were completely unmethylated in all Mer cells, whereas in Mer cells were at least partially methylated. The methylation status of CpGs further upstream did not correlate with MGMT expression. We conclude, therefore, that the association between CpG methylation and suppressed MGMT gene activity extends to sites other than Smal but is limited to a core region of the promoter. [ABSTRACT FROM PUBLISHER]

Published
1995

41. Effect of 5-azacytidine on expression of the human DNA repair enzyme O-methylguanine-DNA methyltransferase.

Author

von Wronski, Mathew A. and Brent, Thomas P.

Abstract

The role of methylatlon of CpG dinucleotides in the regulation of O-methylguanine-DNA methyltransferase (MGMT) gene expression has been investigated. A previous observation, that cell lines deficient in MGMT (Men are methylated in a I site in the MGMT gene promoter whereas MGMT expressing cells (Mer) are unmethylated in the same site, has been extended to a total of 30 cell lines, tumors and normal tissues. To examine further the association between methylation in the MGMT promoter and the Mer phenotype we have treated Mer and Mer cell lines with 5-azacytidine to inhibit DNA methylation. Reduced methylation in the I site coincided with induction of MGMT expression for one of three Mer cell lines. MGMT increased several-fold further upon continued culture of the induced cells in the absence of 5-azacytidlne, coincident with an abrupt increase in methylation in the body of the MGMT gene even though the I site remained demethylated. These results, and those of other previous studies, suggest that methylation of sequences within the MGMT gene promoter and methylation within the body of the gene have opposite effects. [ABSTRACT FROM PUBLISHER]

Published
1994

42. Expression of O-methylguanine-DNA methyltransferase in malignant human glioma cell lines.

Author

Ostrowski, Lawrence E., von Wronski, Mathew A., Bigner, Sandra H., Rasheed, Ahmed, Schold, S.Clifford, Brent, Thomas P., Mitra, Sankar, and Bigner, Darell D.

Abstract

When animals are treated with carcinogenic agents that alkylate -guanine residues, the incidence of tumors in specific tissues often relates inversely to the level of the DNA repair enzyme methylguanine-DNA methyhransferase (MGMT) present in the tissue. Similarly, the hypersensitivity to anticancer chloroethylnitrosoureas of some human tumor cell lines is believed to result from their deficiency in MGMT. We have undertaken a comprehensive investigation of MGMT expression in a panel of nine characterized human glioma cell lines. Methyltransferase activity determined by incubating protein extracts of these glioma lines with [H]methylated DNA ranged from undetectable in six lines (the phenotype) to >0.8 pmol/mg in two lines (U-373 MG and D-392 MG). MGMT protein was undetectable in Western blots of the cell extracts probed with specific antiMGMT monoclonal antibodies. Consistent with these results, steady-state levels of MGMT mRNA, determined by Northern blot analysis, were detectable only in the three glioma lines (U-373 MG, D-392 MG, D-263 MG). Southern analysis of RI-digested DNA probed with MGMT cDNA revealed no amplification, rearrangement or deletions of the MGMT gene in any of the glioma cell lines. This is the first report that examines MGMT expression at the biochemical, molecular and genetic levels in a particular tumor type. These studies suggest that transcriptional regulation is the basis of the phenotype in these malignant human glioma cell lines, since no gross structural or quantitative abnormalities of the MGMT gene were seen in the phenotypically lines. [ABSTRACT FROM PUBLISHER]

Published
1991

44. Lymphatic filariasis in the Democratic Republic of Congo; micro-stratification overlap mapping (MOM) as a prerequisite for control and surveillance

Author

Brent Thomas, Moses J. Bockarie, Louise A. Kelly-Hope, and David H. Molyneux

Subjects
Veterinary medicine, wc_880, Mosquito Control, medicine.disease_cause, wa_110, lcsh:Infectious and parasitic diseases, Ivermectin, qx_200, Elephantiasis, Filarial, Drug Therapy, Environmental health, qx_600, parasitic diseases, medicine, Animals, Humans, lcsh:RC109-216, Wuchereria bancrofti, Mass drug administration, Lymphatic filariasis, Anthelmintics, biology, Geography, Research, biology.organism_classification, medicine.disease, Mosquito control, Infectious Diseases, Democratic Republic of the Congo, Parasitology, Loa loa, Onchocerciasis, Malaria, medicine.drug
Abstract

Background The Democratic Republic of Congo (DRC) has a significant burden of lymphatic filariasis (LF) caused by the parasite Wuchereria bancrofti. A major impediment to the expansion of the LF elimination programme is the risk of serious adverse events (SAEs) associated with the use of ivermectin in areas co-endemic for onchocerciasis and loiasis. It is important to analyse these and other factors, such as soil transmitted helminths (STH) and malaria co-endemicity, which will impact on LF elimination. Results We analysed maps of onchocerciasis community-directed treatment with ivermectin (CDTi) from the African Programme for Onchocerciasis Control (APOC); maps of predicted prevalence of Loa loa; planned STH control maps of albendazole (and mebendazole) from the Global Atlas of Helminth Infections (GAHI); and bed nets and insecticide treated nets (ITNs) distribution from Demographic and Health Surveys (DHS) as well as published historic data which were incorporated into overlay maps. We developed an approach we designate as micro-stratification overlap mapping (MOM) to identify areas that will assist the implementation of LF elimination in the DRC. The historic data on LF was found through an extensive review of the literature as no recently published information was available. Conclusions This paper identifies an approach that takes account of the various factors that will influence not only country strategies, but suggests that country plans will require a finer resolution mapping than usual, before implementation of LF activities can be efficiently deployed. This is because 1) distribution of ivermectin through APOC projects will already have had an impact of LF intensity and prevalence 2) DRC has been up scaling bed net distribution which will impact over time on transmission of W. bancrofti and 3) recently available predictive maps of L. loa allow higher risk areas to be identified, which allow LF implementation to be initiated with reduced risk where L. loa is considered non-endemic. We believe that using the proposed MOM approach is essential for planning the expanded distribution of drugs for LF programmes in countries co-endemic for filarial infections.

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46. Microbiota from human infants consuming secretors or non-secretors mothers' milk impacts the gut and immune system in mice.

Author

Gurung M, Schlegel BT, Rajasundaram D, Fox R, Bode L, Yao T, Lindemann SR, LeRoith T, Read QD, Simecka C, Carroll L, Andres A, and Yeruva L

Subjects
Infant, Female, Humans, Animals, Mice, Mice, Inbred C57BL, Lymphocytes metabolism, Milk, Human chemistry, Immune System metabolism, Oligosaccharides analysis, Bifidobacterium genetics, Immunity, Innate, Microbiota
Abstract

Maternal secretor status is one of the determinants of human milk oligosaccharides (HMOs) composition, which, in turn, influences the gut microbiota composition of infants. To understand if this change in gut microbiota impacts immune cell composition, intestinal morphology, and gene expression, 21-day-old germ-free C57BL/6 mice were transplanted with fecal microbiota from infants whose mothers were either secretors (SMM) or non-secretors (NSM) or from infants consuming dairy-based formula (MFM). For each group, one set of mice was supplemented with HMOs. HMO supplementation did not significantly impact the microbiota diversity; however, SMM mice had a higher abundance of genus Bacteroides , Bifidobacterium , and Blautia , whereas, in the NSM group, there was a higher abundance of Akkermansia , Enterocloster , and Klebsiella . In MFM, gut microbiota was represented mainly by Parabacteroides , Ruminococcaceae_unclassified , and Clostrodium_sensu_stricto . In mesenteric lymph node, Foxp3+ T cells and innate lymphoid cells type 2 were increased in MFM mice supplemented with HMOs, while in the spleen, they were increased in SMM + HMOs mice. Similarly, serum immunoglobulin A was also elevated in MFM + HMOs group. Distinct global gene expression of the gut was observed in each microbiota group, which was enhanced with HMOs supplementation. Overall, our data show that distinct infant gut microbiota due to maternal secretor status or consumption of dairy-based formula and HMO supplementation impacts immune cell composition, antibody response, and intestinal gene expression in a mouse model., Importance: Early life factors like neonatal diet modulate gut microbiota, which is important for the optimal gut and immune function. One such factor, human milk oligosaccharides (HMOs), the composition of which is determined by maternal secretor status, has a profound effect on infant gut microbiota. However, how the infant gut microbiota composition determined by maternal secretor status or consumption of infant formula devoid of HMOs impacts infant intestinal ammorphology, gene expression, and immune signature is not well explored. This study provides insights into the differential establishment of infant microbiota derived from infants fed by secretor or non-secretor mothers milk or those consuming infant formula and demonstrates that the secretor status of mothers promotes Bifidobacteria and Bacteroides sps. establishment. This study also shows that supplementation of pooled HMOs in mice changed immune cell composition in the spleen and mesenteric lymph nodes and immunoglobulins in circulation. Hence, this study highlights that maternal secretor status has a role in infant gut microbiota composition, and this, in turn, can impact host gut and immune system., Competing Interests: The authors declare no conflict of interest.

Published
2024
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47. Epigenetic regulation of O6-methylguanine-DNA methyltransferase gene expression by histone acetylation and methyl-CpG binding proteins.

Author

Danam RP, Howell SR, Brent TP, and Harris LC

Subjects
Acetylation, Azacitidine toxicity, Cell Line, Transformed, Cell Line, Tumor, DNA Methylation, Female, HeLa Cells, Humans, Hydroxamic Acids toxicity, Promoter Regions, Genetic drug effects, Protein Synthesis Inhibitors toxicity, Reverse Transcriptase Polymerase Chain Reaction, Transcription, Genetic, Uterine Cervical Neoplasms, DNA-Binding Proteins metabolism, Gene Expression Regulation, Enzymologic drug effects, Gene Silencing, Histones metabolism, O(6)-Methylguanine-DNA Methyltransferase genetics
Abstract

Transcriptional silencing of the DNA repair gene, O6-methylguanine-DNA methyltransferase (MGMT) in a proportion of transformed cell lines is associated with methylated CpG hotspots in the MGMT 5' flank. The goal of the study was to evaluate the mechanism by which CpG methylation of theMGMT promoter region influenced silencing of the gene. Analysis of histone acetylation status in two regions of the promoter using chromatin immunoprecipitation assay showed that a higher level of histone acetylation was associated with expression in three MGMT-expressing cell lines (HeLa CCL2, HT29, and Raji) compared with three MGMT-silenced cell lines (HeLa S3, BE, and TK6). To determine how the modulation of CpG methylation and histone acetylation influenced MGMT expression, we exposed the cells to 5-aza-2'deoxycytidine (5-Aza-dC), inhibitor of DNA methylation, which strongly up-regulated MGMT expression in three MGMT-silenced cell lines whereas trichostatin A, inhibitor of histone deacetylase, weakly induced MGMT. However, combined treatment with 5-Aza-dC and trichostatin A significantly up-regulated MGMT RNA expression to a greater extent than in cells treated with either agent alone suggesting that histone deacetylation plays a role in MGMT silencing but that CpG methylation has a dominant effect. Consistent with enhanced MGMT expression, 5-Aza-dC increased the association of acetylated histone H3 and H4 bound to the MGMT promoter. Chromatin immunoprecipitation analysis of methyl-CpG binding domain containing proteins detected a greater amount of MeCP2, MBD1, and CAF-1 bound to the MGMT promoter in MGMT-silenced cells. Our findings implicate specific MBD proteins in methylation-mediated transcriptional silencing of MGMT.

Published
2005

48. O6-methylguanine-DNA methyltransferase gene: epigenetic silencing and prognostic value in head and neck squamous cell carcinoma.

Author

Zuo C, Ai L, Ratliff P, Suen JY, Hanna E, Brent TP, and Fan CY

Subjects
Adult, Aged, Aged, 80 and over, Carcinoma, Squamous Cell enzymology, DNA Adducts, DNA Methylation, Guanine metabolism, Head and Neck Neoplasms enzymology, Humans, Male, Middle Aged, Polymerase Chain Reaction, Prognosis, Promoter Regions, Genetic, Proto-Oncogene Mas, Risk Factors, Survival Analysis, Carcinoma, Squamous Cell genetics, DNA Repair Enzymes genetics, Gene Silencing, Head and Neck Neoplasms genetics, O(6)-Methylguanine-DNA Methyltransferase genetics
Abstract

Background: Alkylating N-nitroso compounds can interact directly with DNA, forming O(6)-alkylguanine, a DNA adduct proved to be mutagenic and carcinogenic if not sufficiently repaired. A specific DNA repair enzyme, O(6)-methylguanine-DNA methyltransferase (MGMT), can remove the alkyl group from the O(6)-position of the guanine, thereby preventing its mutagenic and carcinogenic effects. Inactivation of the MGMT gene in association with promoter hypermethylation results in persistence of O(6)-alkylguanine in DNA, leading to G:C to A:T transition mutation and these G:C to A:T transition mutations can inactivate p53 tumor suppressor gene or activate ras proto-oncogene., Methods: We analyzed MGMT promoter hypermethylation and protein expression patterns in 94 cases of primary head and neck squamous cell carcinoma (HNSCC) by methylation-specific PCR (MSP) and immunohistochemical staining. The results were then correlated with clinical follow-up data., Results: MGMT promoter hypermethylation was present in 17 of 94 patients (18.1%) and apparent loss of protein expression was seen in 19 of 93 HNSCC patients (20.4%). The presence of MGMT promoter hypermethylation was significantly correlated with loss of MGMT protein expression in HNSCC. Both MGMT promoter hypermethylation and loss of protein expression were significantly correlated to increased tumor recurrences and decreased patient survival, independent of other risk factors, such as tumor site, tumor size, nodal status, age, and chemoradiation therapy., Conclusions: MGMT promoter hypermethylation and apparent loss of protein expression are reliable and independent prognostic factors in HNSCC. The above study may also provide guideline or basis for applying alkylating antitumor agents to patients with HNSCC that display MGMT promoter hypermethylation and/or loss of MGMT protein expression.

Published
2004

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