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51. Artemether-lumefantrine dosing for malaria treatment in young children and pregnant women: A pharmacokinetic-pharmacodynamic meta-analysis

Author

Beeson, JG, Kloprogge, F, Workman, L, Borrmann, S, Tekete, M, Lefevre, G, Hamed, K, Piola, P, Ursing, J, Kofoed, PE, Martensson, A, Ngasala, B, Bjorkman, A, Ashton, M, Hietala, SF, Aweeka, F, Parikh, S, Mwai, L, Davis, TME, Karunajeewa, H, Salman, S, Checchi, F, Fogg, C, Newton, PN, Mayxay, M, Deloron, P, Faucher, JF, Nosten, F, Ashley, EA, McGready, R, van Vugt, M, Proux, S, Price, RN, Karbwang, J, Ezzet, F, Bakshi, R, Stepniewska, K, White, NJ, Guerin, PJ, Barnes, K, Tarning, J, Beeson, JG, Kloprogge, F, Workman, L, Borrmann, S, Tekete, M, Lefevre, G, Hamed, K, Piola, P, Ursing, J, Kofoed, PE, Martensson, A, Ngasala, B, Bjorkman, A, Ashton, M, Hietala, SF, Aweeka, F, Parikh, S, Mwai, L, Davis, TME, Karunajeewa, H, Salman, S, Checchi, F, Fogg, C, Newton, PN, Mayxay, M, Deloron, P, Faucher, JF, Nosten, F, Ashley, EA, McGready, R, van Vugt, M, Proux, S, Price, RN, Karbwang, J, Ezzet, F, Bakshi, R, Stepniewska, K, White, NJ, Guerin, PJ, Barnes, K, and Tarning, J

Abstract

BACKGROUND: The fixed dose combination of artemether-lumefantrine (AL) is the most widely used treatment for uncomplicated Plasmodium falciparum malaria. Relatively lower cure rates and lumefantrine levels have been reported in young children and in pregnant women during their second and third trimester. The aim of this study was to investigate the pharmacokinetic and pharmacodynamic properties of lumefantrine and the pharmacokinetic properties of its metabolite, desbutyl-lumefantrine, in order to inform optimal dosing regimens in all patient populations. METHODS AND FINDINGS: A search in PubMed, Embase, ClinicalTrials.gov, Google Scholar, conference proceedings, and the WorldWide Antimalarial Resistance Network (WWARN) pharmacology database identified 31 relevant clinical studies published between 1 January 1990 and 31 December 2012, with 4,546 patients in whom lumefantrine concentrations were measured. Under the auspices of WWARN, relevant individual concentration-time data, clinical covariates, and outcome data from 4,122 patients were made available and pooled for the meta-analysis. The developed lumefantrine population pharmacokinetic model was used for dose optimisation through in silico simulations. Venous plasma lumefantrine concentrations 7 days after starting standard AL treatment were 24.2% and 13.4% lower in children weighing <15 kg and 15-25 kg, respectively, and 20.2% lower in pregnant women compared with non-pregnant adults. Lumefantrine exposure decreased with increasing pre-treatment parasitaemia, and the dose limitation on absorption of lumefantrine was substantial. Simulations using the lumefantrine pharmacokinetic model suggest that, in young children and pregnant women beyond the first trimester, lengthening the dose regimen (twice daily for 5 days) and, to a lesser extent, intensifying the frequency of dosing (3 times daily for 3 days) would be more efficacious than using higher individual doses in the current standard treatment regimen (twice

Published
2018

52. Antibiotics and activity spaces: protocol of an exploratory study of behaviour, marginalisation and knowledge diffusion

Author

Haenssgen, M, Charoenboon, N, Zanello, G, Mayxay, M, Reed-Tsochas, F, Jones, C, Kosaikanont, R, Praphattong, P, Manohan, P, Lubell, Y, Newton, P, Keomany, S, Wertheim, H, Lienert, J, Xayavong, T, Warapikuptanun, P, Khine Zaw, Y, U-Thong, P, Benjaroon, P, Sangkham, N, Wibunjak, K, Chai-In, P, Chailert, S, Thavethanutthanawin, P, Promsutt, K, Thepkhamkong, A, Sithongdeng, N, Keovilayvanh, M, Khamsoukthavong, N, Phanthasomchit, P, Phanthavong, C, Boualaiseng, S, Vongsavang, S, Greer, R, Althaus, T, Nedsuwan, S, Intralawan, D, Wangrangsimakul, T, Limmathurotsakul, D, and Ariana, P

Subjects
lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Lao PDR, treatment-seeking behaviour, marginalisation, activity space, Protocol, survey, antimicrobial resistance, Thailand, qualitative research, QR, social research
Abstract

Contains fulltext : 193552.pdf (Publisher’s version ) (Open Access) Background: Antimicrobial resistance (AMR) is a global health priority. Leading UK and global strategy papers to fight AMR recognise its social and behavioural dimensions, but current policy responses to improve the popular use of antimicrobials (eg, antibiotics) are limited to education and awareness-raising campaigns. In response to conceptual, methodological and empirical weaknesses of this approach, we study people's antibiotic-related health behaviour through three research questions.RQ1: What are the manifestations and determinants of problematic antibiotic use in patients' healthcare-seeking pathways?RQ2: Will people's exposure to antibiotic awareness activities entail changed behaviours that diffuse or dissipate within a network of competing healthcare practices?RQ3: Which proxy indicators facilitate the detection of problematic antibiotic behaviours across and within communities? Methods: We apply an interdisciplinary analytical framework that draws on the public health, medical anthropology, sociology and development economics literature. Our research involves social surveys of treatment-seeking behaviour among rural dwellers in northern Thailand (Chiang Rai) and southern Lao PDR (Salavan). We sample approximately 4800 adults to produce district-level representative and social network data. Additional 60 cognitive interviews facilitate survey instrument development and data interpretation. Our survey data analysis techniques include event sequence analysis (RQ1), multilevel regression (RQ1-3), social network analysis (RQ2) and latent class analysis (RQ3). Discussion: Social research in AMR is nascent, but our unprecedentedly detailed data on microlevel treatment-seeking behaviour can contribute an understanding of behaviour beyond awareness and free choice, highlighting, for example, decision-making constraints, problems of marginalisation and lacking access to healthcare and competing ideas about desirable behaviour. Trial registration number: NCT03241316; Pre-results.

Published
2017

54. Host immunity and the assessment of emerging artemisinin resistance in a multinational cohort

Author

Ataide, R, Ashley, EA, Powell, R, Chan, J-A, Malloy, M, O'Flaherty, K, Takashima, E, Langer, C, Tsuboi, T, Dondorp, AM, Day, NP, Dhorda, M, Fairhurst, RM, Lim, P, Amaratunga, C, Pukrittayakamee, S, Hien, TT, Htut, Y, Mayxay, M, Faiz, MA, Beeson, JG, Nosten, F, Simpson, JA, White, N, and Fowkes, FJI

Subjects
parasitic diseases
Abstract

38 Artemisinin-resistant falciparum malaria, defined by a slow-clearance phenotype and the presence of kelch13 mutants, has emerged in the Greater Mekong Subregion. Naturally-acquired immunity to malaria clears parasites independently of antimalarial drugs. We hypothesise that between- and within-population variations in host immunity influence parasite clearance after artemisinin treatment and the interpretation of emerging artemisinin resistance. Antibodies specific to 12 P. falciparum sporozoite and blood-stage antigens were determined in 959 patients (from 11 sites in Southeast Asia) participating in a multinational cohort study assessing parasite clearance half-life (PCt½) after artesunate treatment and kelch13 mutations. Linear mixed-effects modelling of pooled individual patient data assessed the association between antibody responses and PCt½. P. falciparum antibodies were lowest in areas where the prevalence of kelch13 mutations and slow PCt½ were highest (Spearman ρ = -0·90 (95% CI: -0·97, -0·65) and -0·94 (-0·98, -0·77) respectively). P. falciparum antibodies were associated with faster PCt½ (mean difference in PCt½ according to seropositivity -0·16 to -0·65 hours depending on antigen); antibodies have a greater impact on the clearance of kelch13 mutant compared to wild-type parasites (mean difference in PCt½ according to seropositivity -0·22 to -0·61 hours faster in kelch13 mutants compared to wild-type parasites). Naturally-acquired immunity accelerates the clearance of artemisinin-resistant parasites in patients with falciparum malaria, and may confound the current working definition of artemisinin resistance. Immunity may also play an important role in the emergence and transmission potential of artemisinin-resistant parasites.

Published
2017

55. Acute respiratory infections in hospitalized children in Vientiane, Lao PDR - the importance of Respiratory Syncytial Virus

Author

Van, HN, Dubot-Peres, A, Russell, FM, Dance, DAB, Vilivong, K, Phommachan, S, Syladeth, C, Lai, J, Lim, R, Morpeth, M, Mayxay, M, Newton, PN, Richet, H, De lamballerie, X, Van, HN, Dubot-Peres, A, Russell, FM, Dance, DAB, Vilivong, K, Phommachan, S, Syladeth, C, Lai, J, Lim, R, Morpeth, M, Mayxay, M, Newton, PN, Richet, H, and De lamballerie, X

Abstract

The Human respiratory syncytial virus (RSV) is one of the most important viral pathogens, causing epidemics of acute respiratory infection (ARI), especially bronchiolitis and pneumonia, in children worldwide. To investigate the RSV burden in Laos, we conducted a one-year study in children <5 years old admitted to Mahosot Hospital, Vientiane Capital, to describe clinical and epidemiological characteristics and predictive factors for severity of RSV-associated ARI. Pooled nasal and throat swabs were tested using multiplex real-time PCR for 33 respiratory pathogens (FTD® kit). A total of 383 patients were included, 277 (72.3%) of whom presented with pneumonia. 377 (98.4%) patients were positive for at least one microorganism, of which RSV was the most common virus (41.0%), with a peak observed between June and September, corresponding to the rainy season. Most RSV inpatients had pneumonia (84.1%), of whom 35% had severe pneumonia. Children <3-months old were a high-risk group for severe pneumonia, independently of RSV infection. Our study suggests that RSV infection is frequent in Laos and commonly associated with pneumonia in hospitalized young children. Further investigations are required to provide a better overall view of the Lao nationwide epidemiology and public health burden of RSV infection over time.

Published
2017

56. Adverse drug reaction-related hospitalizations of adults in the Lao People's Democratic Republic: health risks of unknown medicines

Author

Caillet, C., Sichanh, C., Assemat, G., Malet-Martino, M., Sommet, A., Bagheri, H., Mayxay, M., Syhakhang, L., Maryse Lapeyre-Mestre, Newton, P. N., and Roussin, A.

Abstract

Although important to take preventive measures towards drug-related morbidity reduction, drug safety research is impaired by the lack of knowledge of medicines used by patients. The danger of medicines of unknown identity (MUIs) (not sold in their original packaging and without written identity) has been suspected in previous studies in low- and middle-income countries of South-East Asia. Using visual and analytical tools to identify MUIs, we designed a cross-sectional study to evaluate the incidence of and factors associated to adverse drug reaction (ADR)-related hospitalizations in adults in a Laotian central hospital in Vientiane Capital.

Published
2016

58. Causes of community-acquired bacteremia and patterns of antimicrobial resistance in Vientiane, Laos

Author

Phetsouvanh, R, Phongmany, S, Soukaloun, D, Rasachak, B, Soukhaseum, V, Soukhaseum, S, Frichithavong, K, Khounnorath, S, Pengdee, B, Phiasakha, K, Chu, V, Luangxay, K, Rattanavong, S, Sisouk, K, Keolouangkot, V, Mayxay, M, Ramsay, A, Blacksell, S, Campbell, J, Martinez-Aussel, B, Heuanvongsy, M, Bounxouei, B, Thammavong, C, Syhavong, B, and Strobel, M

Abstract

There is no published information on the causes of bacteremia in the Lao PDR (Laos). Between 2000 and 2004, 4512 blood culture pairs were taken from patients admitted to Mahosot Hospital, Vientiane, Laos, with suspected community-acquired bacteremia; 483 (10.7%) cultures grew a clinically significant community-acquired organism, most commonly Salmonella enterica serovar typhi (50.9%), Staphylococcus aureus (19.0%), and Escherichia coli (12.4%). S. aureus bacteremia was common among infants (69.2%), while children 1-5 years had a high frequency of typhoid (44%). Multi-drug-resistant S. Typhi was rare (6%). On multiple logistic regression analysis, typhoid was associated with younger age, longer illness, diarrhea, higher admission temperature, and lower peripheral white blood cell count than non-typhoidal bacteremia. Empirical parenteral ampicillin and gentamicin would have some activity against approximately 88% of clinically significant isolates at a cost of US $1.4/day, an important exception being B. pseudomallei. Bacteremic infants in this setting require an anti-staphylococcal antibiotic.

Published
2016

61. Drug resistance. Population transcriptomics of human malaria parasites reveals the mechanism of artemisinin resistance

Author

Mok, S, Ashley, E, Ferreira, P, Zhu, L, Lin, Z, Yeo, T, Chotivanich, K, Imwong, M, Pukrittayakamee, S, Dhorda, M, Nguon, C, Lim, P, Amaratunga, C, Suon, S, Hien, T, Htut, Y, Faiz, M, Onyamboko, M, Mayxay, M, Newton, P, Tripura, R, Woodrow, C, Miotto, O, Kwiatkowski, D, and Nosten, F

Abstract

Artemisinin resistance in Plasmodium falciparum threatens global efforts to control and eliminate malaria. Polymorphisms in the kelch domain-carrying protein K13 are associated with artemisinin resistance, but the underlying molecular mechanisms are unknown. We analyzed the in vivo transcriptomes of 1043 P. falciparum isolates from patients with acute malaria and found that artemisinin resistance is associated with increased expression of unfolded protein response (UPR) pathways involving the major PROSC and TRiC chaperone complexes. Artemisinin-resistant parasites also exhibit decelerated progression through the first part of the asexual intraerythrocytic development cycle. These findings suggest that artemisinin-resistant parasites remain in a state of decelerated development at the young ring stage, whereas their up-regulated UPR pathways mitigate protein damage caused by artemisinin. The expression profiles of UPR-related genes also associate with the geographical origin of parasite isolates, further suggesting their role in emerging artemisinin resistance in the Greater Mekong Subregion.

Published
2016

63. Adjunctive Dexamethasone in HIV-Associated Cryptococcal Meningitis

Author

Beardsley, J., Wolbers, M., Kibengo, F.M., Ggayi, A.B., Kamali, A., Cuc, N.T., Binh, T.Q., Chau, N.V., Farrar, J., Merson, L., Phuong, L., Thwaites, G., Kinh, N. Van, Thuy, P.T., Chierakul, W., Siriboon, S., Thiansukhon, E., Onsanit, S., Supphamongkholchaikul, W., Chan, A.K., Heyderman, R., Mwinjiwa, E., Oosterhout, J.J. van, Imran, D., Basri, H., Mayxay, M., Dance, D., Phimmasone, P., Rattanavong, S., Lalloo, D.G., Day, J.N., and Wertheim, H.F.L.

Subjects
0301 basic medicine, medicine.medical_specialty, business.industry, 030106 microbiology, Hazard ratio, General Medicine, Odds ratio, medicine.disease, Placebo, Tuberculous meningitis, Article, Surgery, 03 medical and health sciences, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Internal medicine, medicine, Cerebrospinal fluid pressure, business, Adverse effect, Meningitis, Dexamethasone, medicine.drug
Abstract

Cryptococcal meningitis associated with human immunodeficiency virus (HIV) infection causes more than 600,000 deaths each year worldwide. Treatment has changed little in 20 years, and there are no imminent new anticryptococcal agents. The use of adjuvant glucocorticoids reduces mortality among patients with other forms of meningitis in some populations, but their use is untested in patients with cryptococcal meningitis.In this double-blind, randomized, placebo-controlled trial, we recruited adult patients with HIV-associated cryptococcal meningitis in Vietnam, Thailand, Indonesia, Laos, Uganda, and Malawi. All the patients received either dexamethasone or placebo for 6 weeks, along with combination antifungal therapy with amphotericin B and fluconazole.The trial was stopped for safety reasons after the enrollment of 451 patients. Mortality was 47% in the dexamethasone group and 41% in the placebo group by 10 weeks (hazard ratio in the dexamethasone group, 1.11; 95% confidence interval [CI], 0.84 to 1.47; P=0.45) and 57% and 49%, respectively, by 6 months (hazard ratio, 1.18; 95% CI, 0.91 to 1.53; P=0.20). The percentage of patients with disability at 10 weeks was higher in the dexamethasone group than in the placebo group, with 13% versus 25% having a prespecified good outcome (odds ratio, 0.42; 95% CI, 0.25 to 0.69; P

Published
2016

64. Drug resistance. Population transcriptomics of human malaria parasites reveals the mechanism of artemisinin resistance

Author

Mok, S, Ashley, EA, Ferreira, PE, Zhu, L, Lin, Z, Yeo, T, Chotivanich, K, Imwong, M, Pukrittayakamee, S, Dhorda, M, Nguon, C, Lim, P, Amaratunga, C, Suon, S, Hien, TT, Htut, Y, Faiz, MA, Onyamboko, MA, Mayxay, M, Newton, PN, Tripura, R, Woodrow, CJ, Miotto, O, Kwiatkowski, DP, Nosten, F, Day, NP, Preiser, PR, White, NJ, Dondorp, AM, Fairhurst, RM, and Bozdech, Z

Subjects
parasitic diseases
Abstract

Artemisinin resistance in Plasmodium falciparum threatens global efforts to control and eliminate malaria. Polymorphisms in the kelch domain-carrying protein K13 are associated with artemisinin resistance, but the underlying molecular mechanisms are unknown. We analyzed the in vivo transcriptomes of 1043 P. falciparum isolates from patients with acute malaria and found that artemisinin resistance is associated with increased expression of unfolded protein response (UPR) pathways involving the major PROSC and TRiC chaperone complexes. Artemisinin-resistant parasites also exhibit decelerated progression through the first part of the asexual intraerythrocytic development cycle. These findings suggest that artemisinin-resistant parasites remain in a state of decelerated development at the young ring stage, whereas their up-regulated UPR pathways mitigate protein damage caused by artemisinin. The expression profiles of UPR-related genes also associate with the geographical origin of parasite isolates, further suggesting their role in emerging artemisinin resistance in the Greater Mekong Subregion.

Published
2015

65. The effect of dose on the antimalarial efficacy of artemether-lumefantrine: a systematic review and pooled analysis of individual patient data

Author

Anstey, NM, Price, RN, Davis, TME, Karunajeewa, HA, Mueller, I, D'Alessandro, U, Massougbodji, A, Nikiema, F, Ouedraogo, JB, Tinto, H, Zongo, I, Same-Ekobo, A, Kone, M, Menan, H, Toure, AO, Yavo, W, Kofoed, PE, Alemayehu, BH, Jima, D, Baudin, E, Espie, E, Nabasumba, C, Pinoges, L, Schramm, B, Cot, M, Deloron, P, Faucher, JF, Guthmann, JP, Lell, B, Borrmann, S, Adjei, GO, Ursing, J, Tjitra, E, Marsh, K, Peshu, J, Juma, E, Ogutu, BR, Omar, SA, Sawa, P, Talisuna, AO, Khanthavong, M, Mayxay, M, Newton, PN, Piola, P, Djimde, AA, Doumbo, OK, Fofana, B, Sagara, I, Bassat, Q, Gonzalez, R, Menendez, C, Smithuis, F, Bousema, T, Kager, PA, Mens, PF, Schallig, HDFH, van Den Broek, I, van Vugt, M, Ibrahim, ML, Falade, CO, Meremikwu, M, Gil, JP, Karema, C, Ba, MS, Faye, B, Faye, O, Gaye, O, Ndiaye, JL, Pene, M, Sow, D, Sylla, K, Tine, RCK, Penali, LK, Barnes, KI, Workman, LJ, Lima, A, Adam, I, Gadalla, NB, Malik, EFM, Bjorkman, A, Martensson, A, Ngasala, BE, Rombo, L, Aliu, P, Duparc, S, Filler, S, Genton, B, Hodel, EM, Olliaro, P, Abdulla, S, Kamugisha, E, Premji, Z, Shekalaghe, SA, Ashley, EA, Carrara, VI, McGready, R, Nosten, F, Faiz, AM, Lee, SJ, White, NJ, Dondorp, AM, Smith, JJ, Tarning, J, Achan, J, Bukirwa, H, Yeka, A, Arinaitwe, E, Staedke, SG, Kamya, MR, Kironde, F, Drakeley, CJ, Oguike, M, Sutherland, CJ, Checchi, F, Dahal, P, Flegg, JA, Guerin, PJ, Moreira, C, Nsanzabana, C, Sibley, CH, Stepniewska, K, Gething, PW, Hay, SI, Greenwood, B, Ward, SA, Winstanley, PA, Dorsey, G, Greenhouse, B, Rosenthal, PJ, Grivoyannis, A, Hamed, K, Hwang, J, Kachur, PS, and Nambozi, M

Published
2015

66. Genomic epidemiology of artemisinin resistant malaria

Author

Amato, R., Miotto, O., Woodrow, C.J., Almagro-Garcia, J., Sinha, I., Campino, S., Mead, D., Drury, E., Kekre, M., Sanders, M., Amambua-Ngwa, A., Amaratunga, C., Amenga-Etego, L., Andrianaranjaka, V., Apinjoh, T., Ashley, E., Auburn, S., Awandare, G.A., Baraka, V., Barry, Alyssa, Boni, M.F., Borrmann, S., Bousema, T., Branch, O., Bull, P.C., Chotivanich, K., Conway, D.J., Craig, A., Day, N.P., Djimdé, A., Dolecek, C., Dondorp, A.M., Drakeley, C., Duffy, P., Echeverry, D.F., Egwang, T.G., Fairhurst, R.M., Faiz, A., Fanello, C.I., Hien, T.T., Hodgson, A., Imwong, M., Ishengoma, D., Lim, P., Lon, C., Marfurt, J., Marsh, K., Mayxay, M., Michon, P., Mobegi, V., Mokuolu, O.A., Montgomery, J., Mueller, I., Kyaw, M.P., Newton, P.N., Nosten, F., Noviyanti, R., Nzila, A., Ocholla, H., Oduro, A., Onyamboko, M., Ouedraogo, J.B., Phyo, A.P.P., Plowe, C., Price, R.N., Pukrittayakamee, S., Randrianarivelojosia, M., Ringwald, P., Ruiz, L., Saunders, D., Shayo, A., Siba, P., Takala-Harrison, S., Thanh, T.N.N., Thathy, V., Verra, F., Wendler, J., White, N.J., Ye, H., Cornelius, V.J., Giacomantonio, R., Muddyman, D., Henrichs, C., Malangone, C., Jyothi, D., Pearson, R.D., Rayner, J.C., McVean, G., Rockett, K.A., Miles, A., Vauterin, P., Jeffery, B., Manske, M., Stalker, J., Macinnis, B., Kwiatkowski, D.P., Amato, R., Miotto, O., Woodrow, C.J., Almagro-Garcia, J., Sinha, I., Campino, S., Mead, D., Drury, E., Kekre, M., Sanders, M., Amambua-Ngwa, A., Amaratunga, C., Amenga-Etego, L., Andrianaranjaka, V., Apinjoh, T., Ashley, E., Auburn, S., Awandare, G.A., Baraka, V., Barry, Alyssa, Boni, M.F., Borrmann, S., Bousema, T., Branch, O., Bull, P.C., Chotivanich, K., Conway, D.J., Craig, A., Day, N.P., Djimdé, A., Dolecek, C., Dondorp, A.M., Drakeley, C., Duffy, P., Echeverry, D.F., Egwang, T.G., Fairhurst, R.M., Faiz, A., Fanello, C.I., Hien, T.T., Hodgson, A., Imwong, M., Ishengoma, D., Lim, P., Lon, C., Marfurt, J., Marsh, K., Mayxay, M., Michon, P., Mobegi, V., Mokuolu, O.A., Montgomery, J., Mueller, I., Kyaw, M.P., Newton, P.N., Nosten, F., Noviyanti, R., Nzila, A., Ocholla, H., Oduro, A., Onyamboko, M., Ouedraogo, J.B., Phyo, A.P.P., Plowe, C., Price, R.N., Pukrittayakamee, S., Randrianarivelojosia, M., Ringwald, P., Ruiz, L., Saunders, D., Shayo, A., Siba, P., Takala-Harrison, S., Thanh, T.N.N., Thathy, V., Verra, F., Wendler, J., White, N.J., Ye, H., Cornelius, V.J., Giacomantonio, R., Muddyman, D., Henrichs, C., Malangone, C., Jyothi, D., Pearson, R.D., Rayner, J.C., McVean, G., Rockett, K.A., Miles, A., Vauterin, P., Jeffery, B., Manske, M., Stalker, J., Macinnis, B., and Kwiatkowski, D.P.

Published
2016

67. Genomic epidemiology of artemisinin resistant malaria

Author

Amato, R, Miotto, O, Woodrow, CJ, Almagro-Garcia, J, Sinha, I, Campino, S, Mead, D, Drury, E, Kekre, M, Sanders, M, Amambua-Ngwa, A, Amaratunga, C, Amenga-Etego, L, Andrianaranjaka, V, Apinjoh, T, Ashley, E, Auburn, S, Awandare, GA, Baraka, V, Barry, A, Boni, MF, Borrmann, S, Bousema, T, Branch, O, Bull, PC, Chotivanich, K, Conway, DJ, Craig, A, Day, NP, Djimde, A, Dolecek, C, Dondorp, AM, Drakeley, C, Duffy, P, Echeverry, DF, Egwang, TG, Fairhurst, RM, Faiz, MA, Fanello, CI, Tran, TH, Hodgson, A, Imwong, M, Ishengoma, D, Lim, P, Lon, C, Marfurt, J, Marsh, K, Mayxay, M, Michon, P, Mobegi, V, Mokuolu, OA, Montgomery, J, Mueller, I, Kyaw, MP, Newton, PN, Nosten, F, Noviyanti, R, Nzila, A, Ocholla, H, Oduro, A, Onyamboko, M, Ouedraogo, J-B, Phyo, APP, Plowe, C, Price, RN, Pukrittayakamee, S, Randrianarivelojosia, M, Ringwald, P, Ruiz, L, Saunders, D, Shayo, A, Siba, P, Takala-Harrison, S, Thanh, T-NN, Thathy, V, Verra, F, Wendler, J, White, NJ, Ye, H, Cornelius, VJ, Giacomantonio, R, Muddyman, D, Henrichs, C, Malangone, C, Jyothi, D, Pearson, RD, Rayner, JC, McVean, G, Rockett, KA, Miles, A, Vauterin, P, Jeffery, B, Manske, M, Stalker, J, Maclnnis, B, Kwiatkowski, DP, Amato, R, Miotto, O, Woodrow, CJ, Almagro-Garcia, J, Sinha, I, Campino, S, Mead, D, Drury, E, Kekre, M, Sanders, M, Amambua-Ngwa, A, Amaratunga, C, Amenga-Etego, L, Andrianaranjaka, V, Apinjoh, T, Ashley, E, Auburn, S, Awandare, GA, Baraka, V, Barry, A, Boni, MF, Borrmann, S, Bousema, T, Branch, O, Bull, PC, Chotivanich, K, Conway, DJ, Craig, A, Day, NP, Djimde, A, Dolecek, C, Dondorp, AM, Drakeley, C, Duffy, P, Echeverry, DF, Egwang, TG, Fairhurst, RM, Faiz, MA, Fanello, CI, Tran, TH, Hodgson, A, Imwong, M, Ishengoma, D, Lim, P, Lon, C, Marfurt, J, Marsh, K, Mayxay, M, Michon, P, Mobegi, V, Mokuolu, OA, Montgomery, J, Mueller, I, Kyaw, MP, Newton, PN, Nosten, F, Noviyanti, R, Nzila, A, Ocholla, H, Oduro, A, Onyamboko, M, Ouedraogo, J-B, Phyo, APP, Plowe, C, Price, RN, Pukrittayakamee, S, Randrianarivelojosia, M, Ringwald, P, Ruiz, L, Saunders, D, Shayo, A, Siba, P, Takala-Harrison, S, Thanh, T-NN, Thathy, V, Verra, F, Wendler, J, White, NJ, Ye, H, Cornelius, VJ, Giacomantonio, R, Muddyman, D, Henrichs, C, Malangone, C, Jyothi, D, Pearson, RD, Rayner, JC, McVean, G, Rockett, KA, Miles, A, Vauterin, P, Jeffery, B, Manske, M, Stalker, J, Maclnnis, B, and Kwiatkowski, DP

Abstract

The current epidemic of artemisinin resistant Plasmodium falciparum in Southeast Asia is the result of a soft selective sweep involving at least 20 independent kelch13 mutations. In a large global survey, we find that kelch13 mutations which cause resistance in Southeast Asia are present at low frequency in Africa. We show that African kelch13 mutations have originated locally, and that kelch13 shows a normal variation pattern relative to other genes in Africa, whereas in Southeast Asia there is a great excess of non-synonymous mutations, many of which cause radical amino-acid changes. Thus, kelch13 is not currently undergoing strong selection in Africa, despite a deep reservoir of variations that could potentially allow resistance to emerge rapidly. The practical implications are that public health surveillance for artemisinin resistance should not rely on kelch13 data alone, and interventions to prevent resistance must account for local evolutionary conditions, shown by genomic epidemiology to differ greatly between geographical regions.

Published
2016

68. Optimal health and disease management using spatial uncertainty: a geographic characterization of emergent artemisinin-resistant Plasmodium falciparum distributions in Southeast Asia

Author

Grist, EPM, Flegg, JA, Humphreys, G, Mas, IS, Anderson, TJC, Ashley, EA, Day, NPJ, Dhorda, M, Dondorp, AM, Abul Faiz, M, Gething, PW, Hien, TT, Hlaing, TM, Imwong, M, Kindermans, J-M, Maude, RJ, Mayxay, M, McDew-White, M, Menard, D, Nair, S, Nosten, F, Newton, PN, Price, RN, Pukrittayakamee, S, Takala-Harrison, S, Smithuis, F, Nguyen, NT, Tun, KM, White, NJ, Witkowski, B, Woodrow, CJ, Fairhurst, RM, Sibley, CH, Guerin, PJ, Grist, EPM, Flegg, JA, Humphreys, G, Mas, IS, Anderson, TJC, Ashley, EA, Day, NPJ, Dhorda, M, Dondorp, AM, Abul Faiz, M, Gething, PW, Hien, TT, Hlaing, TM, Imwong, M, Kindermans, J-M, Maude, RJ, Mayxay, M, McDew-White, M, Menard, D, Nair, S, Nosten, F, Newton, PN, Price, RN, Pukrittayakamee, S, Takala-Harrison, S, Smithuis, F, Nguyen, NT, Tun, KM, White, NJ, Witkowski, B, Woodrow, CJ, Fairhurst, RM, Sibley, CH, and Guerin, PJ

Abstract

BACKGROUND: Artemisinin-resistant Plasmodium falciparum malaria parasites are now present across much of mainland Southeast Asia, where ongoing surveys are measuring and mapping their spatial distribution. These efforts require substantial resources. Here we propose a generic 'smart surveillance' methodology to identify optimal candidate sites for future sampling and thus map the distribution of artemisinin resistance most efficiently. METHODS: The approach uses the 'uncertainty' map generated iteratively by a geostatistical model to determine optimal locations for subsequent sampling. RESULTS: The methodology is illustrated using recent data on the prevalence of the K13-propeller polymorphism (a genetic marker of artemisinin resistance) in the Greater Mekong Subregion. CONCLUSION: This methodology, which has broader application to geostatistical mapping in general, could improve the quality and efficiency of drug resistance mapping and thereby guide practical operations to eliminate malaria in affected areas.

Published
2016

71. Assessment of therapeutic responses to gametocytocidal drugs in Plasmodium falciparum malaria.

Author

White, N.J., Ashley, E.A., Recht, J., Delves, M.J., Ruecker, A., Smithuis, F.M., Eziefula, A.C., Bousema, T., Drakeley, C., Chotivanich, K., Imwong, M., Pukrittayakamee, S., Prachumsri, J., Chu, C., Andolina, C., Bancone, G., Hien, T.T., Mayxay, M., Taylor, W.R., Seidlein, L. von, Price, R.N., Barnes, K.I., Djimdé, A., Kuile, F. ter, Gosling, R., Chen, I., Dhorda, M.J., Stepniewska, K., Guérin, P., Woodrow, C.J., Dondorp, A.M., Day, N.P., Nosten, F.H., White, N.J., Ashley, E.A., Recht, J., Delves, M.J., Ruecker, A., Smithuis, F.M., Eziefula, A.C., Bousema, T., Drakeley, C., Chotivanich, K., Imwong, M., Pukrittayakamee, S., Prachumsri, J., Chu, C., Andolina, C., Bancone, G., Hien, T.T., Mayxay, M., Taylor, W.R., Seidlein, L. von, Price, R.N., Barnes, K.I., Djimdé, A., Kuile, F. ter, Gosling, R., Chen, I., Dhorda, M.J., Stepniewska, K., Guérin, P., Woodrow, C.J., Dondorp, A.M., Day, N.P., and Nosten, F.H.

Abstract

Contains fulltext : 154582.pdf (publisher's version ) (Open Access)

Published
2015

72. Baseline data of parasite clearance in patients with falciparum malaria treated with an artemisinin derivative: an individual patient data meta-analysis

Author

Abdulla, S, Ashley, EA, Bassat, Q, Bethell, D, Bjorkman, A, Borrmann, S, D'Alessandro, U, Dahal, P, Day, NP, Diakite, M, Djimde, AA, Dondorp, AM, Duong, S, Edstein, MD, Fairhurst, RM, Faiz, MA, Falade, C, Flegg, JA, Fogg, C, Gonzalez, R, Greenwood, B, Guerin, PJ, Guthmann, J-P, Hamed, K, Tran, TH, Htut, Y, Juma, E, Lim, P, Martensson, A, Mayxay, M, Mokuolu, OA, Moreira, C, Newton, P, Noedl, H, Nosten, F, Ogutu, BR, Onyamboko, MA, Owusu-Agyei, S, Phyo, AP, Premji, Z, Price, RN, Pukrittayakamee, S, Ramharter, M, Sagara, I, Se, Y, Suon, S, Stepniewska, K, Ward, SA, White, NJ, Winstanley, PA, Abdulla, S, Ashley, EA, Bassat, Q, Bethell, D, Bjorkman, A, Borrmann, S, D'Alessandro, U, Dahal, P, Day, NP, Diakite, M, Djimde, AA, Dondorp, AM, Duong, S, Edstein, MD, Fairhurst, RM, Faiz, MA, Falade, C, Flegg, JA, Fogg, C, Gonzalez, R, Greenwood, B, Guerin, PJ, Guthmann, J-P, Hamed, K, Tran, TH, Htut, Y, Juma, E, Lim, P, Martensson, A, Mayxay, M, Mokuolu, OA, Moreira, C, Newton, P, Noedl, H, Nosten, F, Ogutu, BR, Onyamboko, MA, Owusu-Agyei, S, Phyo, AP, Premji, Z, Price, RN, Pukrittayakamee, S, Ramharter, M, Sagara, I, Se, Y, Suon, S, Stepniewska, K, Ward, SA, White, NJ, and Winstanley, PA

Abstract

BACKGROUND: Artemisinin resistance in Plasmodium falciparum manifests as slow parasite clearance but this measure is also influenced by host immunity, initial parasite biomass and partner drug efficacy. This study collated data from clinical trials of artemisinin derivatives in falciparum malaria with frequent parasite counts to provide reference parasite clearance estimates stratified by location, treatment and time, to examine host factors affecting parasite clearance, and to assess the relationships between parasite clearance and risk of recrudescence during follow-up. METHODS: Data from 24 studies, conducted from 1996 to 2013, with frequent parasite counts were pooled. Parasite clearance half-life (PC1/2) was estimated using the WWARN Parasite Clearance Estimator. Random effects regression models accounting for study and site heterogeneity were used to explore factors affecting PC1/2 and risk of recrudescence within areas with reported delayed parasite clearance (western Cambodia, western Thailand after 2000, southern Vietnam, southern Myanmar) and in all other areas where parasite populations are artemisinin sensitive. RESULTS: PC1/2 was estimated in 6975 patients, 3288 of whom also had treatment outcomes evaluate d during 28-63 days follow-up, with 93 (2.8 %) PCR-confirmed recrudescences. In areas with artemisinin-sensitive parasites, the median PC1/2 following three-day artesunate treatment (4 mg/kg/day) ranged from 1.8 to 3.0 h and the proportion of patients with PC1/2 >5 h from 0 to 10 %. Artesunate doses of 4 mg/kg/day decreased PC1/2 by 8.1 % (95 % CI 3.2-12.6) compared to 2 mg/kg/day, except in populations with delayed parasite clearance. PC1/2 was longer in children and in patients with fever or anaemia at enrolment. Long PC1/2 (HR = 2.91, 95 % CI 1.95-4.34 for twofold increase, p < 0.001) and high initial parasitaemia (HR = 2.23, 95 % CI 1.44-3.45 for tenfold increase, p < 0.001) were associated independently with an increased risk of recrudescence. In

Published
2015

74. An Open-Label, Randomised Study of Dihydroartemisinin-Piperaquine Versus Artesunate-Mefloquine for Falciparum Malaria in Asia

Author

Valecha N, Ap, Phyo, Mayxay M, Pn, Newton, Krudsood S, Keomany S, Khanthavong M, Pongvongsa T, Ruangveerayuth R, Uthaisil C, Ubben D, Duparc S, Bacchieri A, Corsi M, Bhk, Rao, Pc, Bhattacharya, Dubhashi N, Sk, Ghosh, Dev V, Kumar A, and Pukrittayakamee S

Subjects
Multidisciplinary, Science, lcsh:R, Medicine, Correction, lcsh:Medicine, lcsh:Q, lcsh:Science
Published
2010

77. Diagnosis and management of malaria by rural community health providers in the Lao People's Democratic Republic (Laos)

Author

Mayxay, M, Pongvongsa, T, Phompida, S, Phetsouvanh, R, White, N, and Newton, P

Subjects
parasitic diseases
Abstract

We assessed the knowledge of malaria diagnosis and management by community health providers in rural Vientiane and Savannakhet Provinces, Lao PDR. Sixty health providers (17 pharmacy owners/drug sellers and 43 village health volunteers) were interviewed. All diagnosed malaria using symptoms and signs only; 14% were aware of >2 criteria for the diagnosis of severe malaria. Although chloroquine and quinine, the then recommended Lao national policy for uncomplicated malaria treatment, were the most common antimalarials prescribed - 65% gave incorrect doses and 70% did not know the side effects. Although not recommended by the then national policy, 27% of the health providers used combinations of antimalarials as they considered monotherapy ineffective. This study strongly suggests that further training of Lao rural health providers in malaria diagnosis and management is needed to improve the quality of health services in areas remote from district hospitals.

Published
2007

79. The Effect of Dosing Regimens on the Antimalarial Efficacy of Dihydroartemisinin-Piperaquine: A Pooled Analysis of Individual Patient Data

Author

Garner, P, Achan, J, Adam, I, Arinaitwe, E, Ashley, EA, Awab, GR, Ba, MS, Barnes, KI, Bassat, Q, Borrmann, S, Bousema, T, Dahal, P, D'Alessandro, U, Davis, TME, Dondorp, AM, Dorsey, G, Drakeley, CJ, Fanello, CI, Faye, B, Flegg, JA, Gaye, O, Gething, PW, Gonzalez, R, Guerin, PJ, Hay, SI, Hien, TT, Janssens, B, Kamya, MR, Karema, C, Karunajeewa, HA, Kone, M, Lell, B, Marsh, K, Mayxay, M, Menendez, C, Mens, PF, Meremikwu, M, Moreira, C, Mueller, I, Nabasumba, C, Nambozi, M, Ndiaye, J-L, Newton, PN, Thuy-Nhien, N, Nosten, F, Nsanzabana, C, Omar, SA, Ouedraogo, J-B, Penali, LK, Pene, M, Phyo, AP, Piola, P, Price, RN, Sasithon, P, Rosenthal, PJ, Same-Ekobo, A, Sawa, P, Schallig, HDFH, Shekalaghe, SA, Sibley, CH, Smith, J, Smithuis, F, Some, AF, Stepniewska, K, Talisuna, AO, Tarning, J, Tjitra, E, Tine, RCK, Tinto, H, Valecha, N, Van Herp, M, Van Vugt, M, White, NJ, Woodrow, CJ, Yavo, W, Yeka, A, Zongo, I, Garner, P, Achan, J, Adam, I, Arinaitwe, E, Ashley, EA, Awab, GR, Ba, MS, Barnes, KI, Bassat, Q, Borrmann, S, Bousema, T, Dahal, P, D'Alessandro, U, Davis, TME, Dondorp, AM, Dorsey, G, Drakeley, CJ, Fanello, CI, Faye, B, Flegg, JA, Gaye, O, Gething, PW, Gonzalez, R, Guerin, PJ, Hay, SI, Hien, TT, Janssens, B, Kamya, MR, Karema, C, Karunajeewa, HA, Kone, M, Lell, B, Marsh, K, Mayxay, M, Menendez, C, Mens, PF, Meremikwu, M, Moreira, C, Mueller, I, Nabasumba, C, Nambozi, M, Ndiaye, J-L, Newton, PN, Thuy-Nhien, N, Nosten, F, Nsanzabana, C, Omar, SA, Ouedraogo, J-B, Penali, LK, Pene, M, Phyo, AP, Piola, P, Price, RN, Sasithon, P, Rosenthal, PJ, Same-Ekobo, A, Sawa, P, Schallig, HDFH, Shekalaghe, SA, Sibley, CH, Smith, J, Smithuis, F, Some, AF, Stepniewska, K, Talisuna, AO, Tarning, J, Tjitra, E, Tine, RCK, Tinto, H, Valecha, N, Van Herp, M, Van Vugt, M, White, NJ, Woodrow, CJ, Yavo, W, Yeka, A, and Zongo, I

Abstract

BACKGROUND: Dihydroartemisinin-piperaquine (DP) is increasingly recommended for antimalarial treatment in many endemic countries; however, concerns have been raised over its potential under dosing in young children. We investigated the influence of different dosing schedules on DP's clinical efficacy. METHODS AND FINDINGS: A systematic search of the literature was conducted to identify all studies published between 1960 and February 2013, in which patients were enrolled and treated with DP. Principal investigators were approached and invited to share individual patient data with the WorldWide Antimalarial Resistance Network (WWARN). Data were pooled using a standardised methodology. Univariable and multivariable risk factors for parasite recrudescence were identified using a Cox's regression model with shared frailty across the study sites. Twenty-four published and two unpublished studies (n = 7,072 patients) were included in the analysis. After correcting for reinfection by parasite genotyping, Kaplan-Meier survival estimates were 97.7% (95% CI 97.3%-98.1%) at day 42 and 97.2% (95% CI 96.7%-97.7%) at day 63. Overall 28.6% (979/3,429) of children aged 1 to 5 years received a total dose of piperaquine below 48 mg/kg (the lower limit recommended by WHO); this risk was 2.3-2.9-fold greater compared to that in the other age groups and was associated with reduced efficacy at day 63 (94.4% [95% CI 92.6%-96.2%], p<0.001). After adjusting for confounding factors, the mg/kg dose of piperaquine was found to be a significant predictor for recrudescence, the risk increasing by 13% (95% CI 5.0%-21%) for every 5 mg/kg decrease in dose; p = 0.002. In a multivariable model increasing the target minimum total dose of piperaquine in children aged 1 to 5 years old from 48 mg/kg to 59 mg/kg would halve the risk of treatment failure and cure at least 95% of patients; such an increment was not associated with gastrointestinal toxicity in the ten studies in which this could be assessed.

Published
2013

80. Optimal sampling designs for estimation of Plasmodium falciparum clearance rates in patients treated with artemisinin derivatives

Author

Flegg, JA, Guerin, PJ, Nosten, F, Ashley, EA, Phyo, AP, Dondorp, AM, Fairhurst, RM, Socheat, D, Borrmann, S, Bjorkman, A, Martensson, A, Mayxay, M, Newton, PN, Bethell, D, Se, Y, Noedl, H, Diakite, M, Djimde, AA, Hien, TT, White, NJ, Stepniewska, K, Flegg, JA, Guerin, PJ, Nosten, F, Ashley, EA, Phyo, AP, Dondorp, AM, Fairhurst, RM, Socheat, D, Borrmann, S, Bjorkman, A, Martensson, A, Mayxay, M, Newton, PN, Bethell, D, Se, Y, Noedl, H, Diakite, M, Djimde, AA, Hien, TT, White, NJ, and Stepniewska, K

Abstract

BACKGROUND: The emergence of Plasmodium falciparum resistance to artemisinins in Southeast Asia threatens the control of malaria worldwide. The pharmacodynamic hallmark of artemisinin derivatives is rapid parasite clearance (a short parasite half-life), therefore, the in vivo phenotype of slow clearance defines the reduced susceptibility to the drug. Measurement of parasite counts every six hours during the first three days after treatment have been recommended to measure the parasite clearance half-life, but it remains unclear whether simpler sampling intervals and frequencies might also be sufficient to reliably estimate this parameter. METHODS: A total of 2,746 parasite density-time profiles were selected from 13 clinical trials in Thailand, Cambodia, Mali, Vietnam, and Kenya. In these studies, parasite densities were measured every six hours until negative after treatment with an artemisinin derivative (alone or in combination with a partner drug). The WWARN Parasite Clearance Estimator (PCE) tool was used to estimate "reference" half-lives from these six-hourly measurements. The effect of four alternative sampling schedules on half-life estimation was investigated, and compared to the reference half-life (time zero, 6, 12, 24 (A1); zero, 6, 18, 24 (A2); zero, 12, 18, 24 (A3) or zero, 12, 24 (A4) hours and then every 12 hours). Statistical bootstrap methods were used to estimate the sampling distribution of half-lives for parasite populations with different geometric mean half-lives. A simulation study was performed to investigate a suite of 16 potential alternative schedules and half-life estimates generated by each of the schedules were compared to the "true" half-life. The candidate schedules in the simulation study included (among others) six-hourly sampling, schedule A1, schedule A4, and a convenience sampling schedule at six, seven, 24, 25, 48 and 49 hours. RESULTS: The median (range) parasite half-life for all clinical studies combined was 3.1 (0.7-12.9)

Published
2013

81. Dengue in peri-urban Pak-Ngum district, Vientiane capital of Laos: a community survey on knowledge, attitudes and practices

Author

Mayxay, M, Cui, W, Thammavong, S, Khensakhou, K, Vongxay, V, Inthasoum, L, Sychareun, V, Armstrong, G, Mayxay, M, Cui, W, Thammavong, S, Khensakhou, K, Vongxay, V, Inthasoum, L, Sychareun, V, and Armstrong, G

Abstract

BACKGROUND: Dengue remains an important cause of morbidity in Laos. Good knowledge, attitudes and practices (KAP) among the public regarding dengue prevention are required for the success of disease control. Very little is known about dengue KAP among the Lao general population. METHODS: This was a KAP household survey on dengue conducted in a peri-urban Pak-Ngum district of Vientiane capital, Laos. A two-stage cluster sampling method was used to select a sample of participants to represent the general community. Participants from 231 households were surveyed using an interviewer-administered questionnaire. RESULTS: Although 97% of the participants heard of dengue, there was a lack of depth of knowledge on dengue: 33% of them did not know that malaria and dengue were different diseases, 32% incorrectly believed that Aedes mosquito transmits malaria, 36% could not correctly report that Aedes mosquitoes bite most frequently at sunrise and sunset; and < 10% of them recognized that indoor water containers could be Aedes mosquito breeding sites. Attitude levels were moderately good with a high proportion (96%) of participants recognizing that dengue was a severe yet preventable disease. Self reported prevention methods were quite high yet observation of the participants' yards showed use of prevention methods to be only moderate. The majority (93%) of the interviewees did not believe that they had enough information on dengue. There was an association between good knowledge and better practices, but good knowledge was associated with worse attitudes. CONCLUSIONS: There is a lack of depth of knowledge regarding dengue in Pak-Ngum community and observation methods revealed that more needs to be done by community members themselves to prevent the spread of Aedes mosquitoes.

Published
2013

82. In Vivo Assessment of Drug Efficacy against Plasmodium falciparum Malaria: Duration of Follow-Up

Author

Stepniewska, K, Taylor, WRJ, Mayxay, M, Price, Ric N., Smithuis, F., Guthmann, J. P., Barnes, Karen I., Myint, HY, Adjuik, M, Olliaro, P, Pukrittayakamee, S, Looareesuwan, S, Hien, TT, Farrar, J, Nosten, F, Day, NPJ, White, N, Stepniewska, K, Taylor, WRJ, Mayxay, M, Price, Ric N., Smithuis, F., Guthmann, J. P., Barnes, Karen I., Myint, HY, Adjuik, M, Olliaro, P, Pukrittayakamee, S, Looareesuwan, S, Hien, TT, Farrar, J, Nosten, F, Day, NPJ, and White, N

Abstract

To determine the optimum duration of follow-up for the assessment of drug efficacy against Plasmodium falciparum malaria, 96 trial arms from randomized controlled trials (RCTs) with follow-up of 28 days or longer that were conducted between 1990 and 2003 were analyzed. These trials enrolled 13,772 patients, and participating patients comprised 23% of all patients enrolled in RCTs over the past 40 years; 61 (64%) trial arms were conducted in areas where the rate of malaria transmission was low, and 58 (50%) trial arms were supported by parasite genotyping to distinguish true recrudescences from reinfections. The median overall failure rate reported was 10% (range, 0 to 47%). The widely used day 14 assessment had a sensitivity of between 0 and 37% in identifying treatment failures and had no predictive value. Assessment at day 28 had a sensitivity of 66% overall (28 to 100% in individual trials) but could be used to predict the true failure rate if either parasite genotyping was performed (r2 = 0.94) or if the entomological inoculation rate was known. In the assessment of drug efficacy against falciparum malaria, 28 days should be the minimum period of follow-up.

Published
2004

83. Randomized Comparison of Chloroquine plus Sulfadoxine-Pyrimethamine versus Artesunate plus Mefloquine versus Artemether-Lumefantrine in the Treatment of Uncomplicated Falciparum Malaria in the Lao People's Democratic Republic

Author

Mayxay, M., primary, Khanthavong, M., additional, Lindegardh, N., additional, Keola, S., additional, Barends, M., additional, Pongvongsa, T., additional, Yapom, R., additional, Annerberg, A., additional, Phompida, S., additional, Phetsouvanh, R., additional, White, N. J., additional, and Newton, P. N., additional

Published
2004
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88. Automating the Generation of Antimicrobial Resistance Surveillance Reports: Proof-of-Concept Study Involving Seven Hospitals in Seven Countries

Author

Lim, Cherry, Miliya, Thyl, Chansamouth, Vilada, Aung, Myint Thazin, Karkey, Abhilasha, Teparrukkul, Prapit, Rahul, Batra, Lan, Nguyen Phu Huong, Stelling, John, Turner, Paul, Ashley, Elizabeth, van Doorn, H Rogier, Lin, Htet Naing, Ling, Clare, Hinjoy, Soawapak, Iamsirithaworn, Sopon, Dunachie, Susanna, Wangrangsimakul, Tri, Hantrakun, Viriya, Schilling, William, Yen, Lam Minh, Tan, Le Van, Hlaing, Htay Htay, Mayxay, Mayfong, Vongsouvath, Manivanh, Basnyat, Buddha, Edgeworth, Jonathan, Peacock, Sharon J, Thwaites, Guy, Day, Nicholas PJ, Cooper, Ben S, and Limmathurotsakul, Direk

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Public aspects of medicine, RA1-1270
Abstract

BackgroundReporting cumulative antimicrobial susceptibility testing data on a regular basis is crucial to inform antimicrobial resistance (AMR) action plans at local, national, and global levels. However, analyzing data and generating a report are time consuming and often require trained personnel. ObjectiveThis study aimed to develop and test an application that can support a local hospital to analyze routinely collected electronic data independently and generate AMR surveillance reports rapidly. MethodsAn offline application to generate standardized AMR surveillance reports from routinely available microbiology and hospital data files was written in the R programming language (R Project for Statistical Computing). The application can be run by double clicking on the application file without any further user input. The data analysis procedure and report content were developed based on the recommendations of the World Health Organization Global Antimicrobial Resistance Surveillance System (WHO GLASS). The application was tested on Microsoft Windows 10 and 7 using open access example data sets. We then independently tested the application in seven hospitals in Cambodia, Lao People’s Democratic Republic, Myanmar, Nepal, Thailand, the United Kingdom, and Vietnam. ResultsWe developed the AutoMated tool for Antimicrobial resistance Surveillance System (AMASS), which can support clinical microbiology laboratories to analyze their microbiology and hospital data files (in CSV or Excel format) onsite and promptly generate AMR surveillance reports (in PDF and CSV formats). The data files could be those exported from WHONET or other laboratory information systems. The automatically generated reports contain only summary data without patient identifiers. The AMASS application is downloadable from https://www.amass.website/. The participating hospitals tested the application and deposited their AMR surveillance reports in an open access data repository. ConclusionsThe AMASS is a useful tool to support the generation and sharing of AMR surveillance reports.

Published
2020
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89. Persistence of Plasmodium falciparum HRP-2 in successfully treated acute falciparum malaria.

Author

Mayxay, M, Pukrittayakamee, S, Chotivanich, K, Looareesuwan, S, and White, N J

Abstract

The potential for Plasmodium falciparum histidine-rich protein-2 (PfHRP-2) dipstick tests to predict antimalarial treatment failure was investigated in a prospective study in Thailand of 38 patients admitted with severe malaria and 54 hospitalized with uncomplicated P. falciparum infections. Of these, 40 had subsequent recrudescence of their infections. Overall, 89% of patients with severe malaria and 61% of patients with uncomplicated malaria had positive PfHRP-2 dipstick tests for > 2 weeks following the start of treatment. Persistence was correlated positively with admission parasite counts, PfHRP-2 intensity scores and disease severity. PfHRP-2 tests which remained positive for > 2 weeks and PfHRP-2 reactive intensity scores on admission, at day 7 and day 14 did not predict treatment failure independent of admission parasitaemia. Freezing and thawing the blood samples did not significantly affect PfHRP-2 results tested by the dipstick technique. The PfHRP-2 dipstick test provides a useful indicator of recent severe malaria, but does not predict the therapeutic response.

Published
2001
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90. Combined molecular and clinical assessment of Plasmodium falciparum antimalarial drug resistance in the Lao People's Democratic Republic (Laos)

Author

Mayxay, M., Nair, S., Sudimack, D., Imwong, M., Tanomsing, N., Pongvongsa, T., Phompida, S., Phetsouvanh, R., Nicholas White, Anderson, T. J. C., and Newton, P. N.

Subjects
parasitic diseases
Abstract

Molecular markers provide a rapid and relatively inexpensive approach for assessing antimalarial drug susceptibility. We collected 884 Plasmodium falciparum-infected blood samples from 17 Lao provinces. Each sample was genotyped for 11 codons in the chloroquine resistance transporter (pfcrt), dihydrofolate reductase (pfdhfr), and dihydropteroate synthase (pfdhps) genes. The samples included 227 collected from patients recruited to clinical trials. The pfcrt K76T mutation was an excellent predictor of treatment failure for both chloroquine and chloroquine plus sulfadoxine-pyrimethamine, and mutations in both pfdhfr and pfdhps were predictive of sulfadoxine-pyrimethamine treatment failure. In multivariate analysis, the presence of the pfdhfr triple mutation (51 + 59 + 108) was strongly and independently correlated with sulfadoxine-pyrimethamine failure (odds ratio = 9.1, 95% confidence interval = 1.4-60.2, P = 0.017). Considerable geographic heterogeneity in allele frequencies occurred at all three loci with lower frequencies of mutant alleles in southern than in northern Laos. These findings suggest that chloroquine and sulfadoxine-pyrimethamine are no longer viable therapy in this country.

93. Haematological consequences of acute uncomplicated falciparum malaria: a WorldWide Antimalarial Resistance Network pooled analysis of individual patient data

Author

Mansoor, Rashid, Commons, Robert J, Douglas, Nicholas M, Abuaku, Benjamin, Achan, Jane, Adam, Ishag, Adjei, George O, Adjuik, Martin, Alemayehu, Bereket H, Allan, Richard, Allen, Elizabeth N, Anvikar, Anupkumar R, Arinaitwe, Emmanuel, Ashley, Elizabeth A, Ashurst, Hazel, Asih, Puji BS, Bakyaita, Nathan, Barennes, Hubert, Barnes, Karen I, Basco, Leonardo, Bassat, Quique, Baudin, Elisabeth, Bell, David J, Bethell, Delia, Bjorkman, Anders, Boulton, Caroline, Bousema, Teun, Brasseur, Philippe, Bukirwa, Hasifa, Burrow, Rebekah, Carrara, Verena I, Cot, Michel, D'Alessandro, Umberto, Das, Debashish, Das, Sabyasachi, Davis, Timothy ME, Desai, Meghna, Djimde, Abdoulaye A, Dondorp, Arjen M, Dorsey, Grant, Drakeley, Chris J, Duparc, Stephan, Espie, Emmanuelle, Etard, Jean-Francois, Falade, Catherine, Faucher, Jean Francois, Filler, Scott, Fogg, Carole, Fukuda, Mark, Gaye, Oumar, Genton, Blaise, Rahim, Awab Ghulam, Gilayeneh, Julius, Gonzalez, Raquel, Grais, Rebecca F, Grandesso, Francesco, Greenwood, Brian, Grivoyannis, Anastasia, Hatz, Christoph, Hodel, Eva Maria, Humphreys, Georgina S, Hwang, Jimee, Ishengoma, Deus, Juma, Elizabeth, Kachur, S Patrick, Kager, Piet A, Kamugisha, Erasmus, Kamya, Moses R, Karema, Corine, Kayentao, Kassoum, Kazienga, Adama, Kiechel, Jean-Rene, Kofoed, Poul-Erik, Koram, Kwadwo, Kremsner, Peter G, Lalloo, David G, Laman, Moses, Lee, Sue J, Lell, Bertrand, Maiga, Amelia W, Martensson, Andreas, Mayxay, Mayfong, Mbacham, Wilfred, McGready, Rose, Menan, Herve, Menard, Didier, Mockenhaupt, Frank, Moore, Brioni R, Muller, Olaf, Nahum, Alain, Ndiaye, Jean-Louis, Newton, Paul N, Ngasala, Billy E, Nikiema, Frederic, Nji, Akindeh M, Noedl, Harald, Nosten, Francois, Ogutu, Bernhards R, Ojurongbe, Olusola, Osorio, Lyda, Ouedraogo, Jean-Bosco, Owusu-Agyei, Seth, Pareek, Anil, Penali, Louis K, Piola, Patrice, Plucinski, Mateusz, Premji, Zul, Ramharter, Michael, Richmond, Caitlin L, Rombo, Lars, Rosenthal, Philip J, Salman, Sam, Same-Ekobo, Albert, Sibley, Carol, Sirima, Sodiomon B, Smithuis, Frank M, Some, Fabrice A, Staedke, Sarah G, Starzengruber, Peter, Strub-Wourgaft, Nathalie, Sutanto, Inge, Swarthout, Todd D, Syafruddin, Din, Talisuna, Ambrose O, Taylor, Walter R, Temu, Emmanuel A, Thwing, Julie I, Tinto, Halidou, Tjitra, Emiliana, Toure, Offianan A, Tran, T Hien, Ursing, Johan, Valea, Innocent, Valentini, Giovanni, van Vugt, Michele, von Seidlein, Lorenz, Ward, Stephen A, Were, Vincent, White, Nicholas J, Woodrow, Charles J, Yavo, William, Yeka, Adoke, Zongo, Issaka, Simpson, Julie A, Guerin, Philippe J, Stepniewska, Kasia, Price, Ric N, Roper, Cally, Resistance, WorldWide Antimalarial, WorldWide Antimalarial Resistance Network Falciparum Haematology Study Group, Vecteurs - Infections tropicales et méditerranéennes (VITROME), Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Institut de Recherche Biomédicale des Armées [Brétigny-sur-Orge] (IRBA), Epidémiologie des Maladies Chroniques en zone tropicale (EpiMaCT), CHU Limoges-Institut d'Epidémiologie Neurologique et de Neurologie Tropicale-Institut National de la Santé et de la Recherche Médicale (INSERM)-OmégaHealth (ΩHealth), Université de Limoges (UNILIM)-Université de Limoges (UNILIM), Group, WorldWide Antimalarial Resistance Network Falciparum Haematology Study, Mansoor, R, Ashley, EA, Ashurst, H, Burrow, R, Carrara, VI, Das, D, Dondorp, AM, Humphreys, GS, Lee, SJ, Mayxay, M, McGready, R, Newton, PN, Nosten, F, Richmond, CL, Sibley, C, Smithuis, FM, Taylor, WR, Tran, TH, von Seidlein, L, White, NJ, Woodrow, CJ, Guerin, PJ, Stepniewska, K, Price, RN, AII - Infectious diseases, Intensive Care Medicine, Infectious diseases, APH - Global Health, and APH - Quality of Care

Subjects
Infectious Medicine, Plasmodium falciparum, wh_120, Infektionsmedicin, Severe anaemia, Parasitemia, wa_530, Antimalarials, Non-artemisinin-based therapy, [SDV.MHEP.CSC]Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system, [SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases, parasitic diseases, qv_256, Humans, [SDV.MP.PAR]Life Sciences [q-bio]/Microbiology and Parasitology/Parasitology, Malaria, Falciparum, Child, [SDV.MHEP.ME]Life Sciences [q-bio]/Human health and pathology/Emerging diseases, Pooled analysis of individual patient data, Anemia, Public Health, Global Health, Social Medicine and Epidemiology, General Medicine, Artemisinin-based therapy, [SDV.MP.BAC]Life Sciences [q-bio]/Microbiology and Parasitology/Bacteriology, Malaria, wc_750, Folkhälsovetenskap, global hälsa, socialmedicin och epidemiologi, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Haemoglobin
Abstract

Background Plasmodium falciparum malaria is associated with anaemia-related morbidity, attributable to host, parasite and drug factors. We quantified the haematological response following treatment of uncomplicated P. falciparum malaria to identify the factors associated with malarial anaemia. Methods Individual patient data from eligible antimalarial efficacy studies of uncomplicated P. falciparum malaria, available through the WorldWide Antimalarial Resistance Network data repository prior to August 2015, were pooled using standardised methodology. The haematological response over time was quantified using a multivariable linear mixed effects model with nonlinear terms for time, and the model was then used to estimate the mean haemoglobin at day of nadir and day 7. Multivariable logistic regression quantified risk factors for moderately severe anaemia (haemoglobin < 7 g/dL) at day 0, day 3 and day 7 as well as a fractional fall ≥ 25% at day 3 and day 7. Results A total of 70,226 patients, recruited into 200 studies between 1991 and 2013, were included in the analysis: 50,859 (72.4%) enrolled in Africa, 18,451 (26.3%) in Asia and 916 (1.3%) in South America. The median haemoglobin concentration at presentation was 9.9 g/dL (range 5.0–19.7 g/dL) in Africa, 11.6 g/dL (range 5.0–20.0 g/dL) in Asia and 12.3 g/dL (range 6.9–17.9 g/dL) in South America. Moderately severe anaemia (Hb < 7g/dl) was present in 8.4% (4284/50,859) of patients from Africa, 3.3% (606/18,451) from Asia and 0.1% (1/916) from South America. The nadir haemoglobin occurred on day 2 post treatment with a mean fall from baseline of 0.57 g/dL in Africa and 1.13 g/dL in Asia. Independent risk factors for moderately severe anaemia on day 7, in both Africa and Asia, included moderately severe anaemia at baseline (adjusted odds ratio (AOR) = 16.10 and AOR = 23.00, respectively), young age (age < 1 compared to ≥ 12 years AOR = 12.81 and AOR = 6.79, respectively), high parasitaemia (AOR = 1.78 and AOR = 1.58, respectively) and delayed parasite clearance (AOR = 2.44 and AOR = 2.59, respectively). In Asia, patients treated with an artemisinin-based regimen were at significantly greater risk of moderately severe anaemia on day 7 compared to those treated with a non-artemisinin-based regimen (AOR = 2.06 [95%CI 1.39–3.05], p < 0.001). Conclusions In patients with uncomplicated P. falciparum malaria, the nadir haemoglobin occurs 2 days after starting treatment. Although artemisinin-based treatments increase the rate of parasite clearance, in Asia they are associated with a greater risk of anaemia during recovery.

Published
2022

94. Studies to provide recommendations on the pre-elimination of Plasmodium vivax in Lao PDR

Author

Phommasone, K., van Leth, Frank C. M., Dondorp, Arjen M., Mayxay, M., Cobelens, Franciscus G. J., AII - Infectious diseases, Graduate School, Global Health, APH - Methodology, APH - Global Health, van Leth, F.C.M., Dondorp, A.M., Cobelens, F.G.J., and Faculteit der Geneeskunde

Subjects
parasitic diseases
Abstract

Malaria remains a major public health problem in malaria endemic countries despite a global reduction in the burden of the disease over the last two decades. The malaria control program has been threatened with the emergence and spread of multidrug resistant P. falciparum across the Greater Mekong Subregion (GMS). To achieve the goal of malaria elimination by 2030, mass drug administration with three monthly rounds of 3 day course of dihydroartemisinin-piperaquine plus single dose of primaquine was assessed in the four countries of GMS including Lao PDR. This thesis shows that asymptomatic malaria infections are prevalent in Lao PDR. Mass drug administration with the aim to eliminate P. falciparum was safe, feasible and acceptable by community in the Lao context with a significant reduction of P. falciparum for at least one year follow-up. However, it had a transient impact on P. vivax infections with the rebound in prevalence by month 6. A single low dose of primaquine used in MDA is to clear P. falciparum gametocytes but has no effect on the hypnozoites of P. vivax. MDA to eliminate all malarias should include both schizontocaidal and hypnozoitocidal drugs. A subset study to assess the efficacy of 14 day primaquine following three rounds of MDA in the prevention of recurrent of P. vivax infections showed that the strategy was safe and effective in the prevention of recurrence of asymptomatic P. vivax infections.

Published
2020

96. Community engagement for targeted malaria elimination in Lao PDR (Laos)

Author

Adhikari, B, Parker, M, Hardon, A, Cheah, P, Pell, C, Mayxay, M, and Day, N

Subjects
Community Engagement for Malaria Elimination
Abstract

The emergence of artemisinin-resistant malaria in Southeast Asia has prompted malaria control programs to expedite efforts to eliminate malaria. One suggested approach is the mass administration of antimalarials (MDA) to entire target population regardless of malaria infection. MDA is one of the central components of Targeted Malaria Elimination (TME), an approach recently piloted in Laos. For MDA to be successful (leading to interruption of local malaria transmission), a high population coverage is critical. Among myriad factors, community engagement has been recognized as critical to promoting high coverage. The main aim of this study was to design, execute and assess a locally suitable community engagement strategy that can promote the uptake of and adherence to MDA. This study utilized a longitudinal mixed method approach. In addition to the local social and cultural factors, five main elements of community engagement that contributed to high population coverage were identified: 1. Stakeholder and authority engagement: a stepwise approach from central to the local level; 2. Local human resources: recruitment and training of local community members to execute TME; 3. Formative research: an exploration of the local social and cultural context to guide the community engagement; 4. Responsiveness: flexible and adaptable approach based on the demands and needs of the community and 5. Sharing control/leadership with the community: joint decision making with the community members. Various factors contributed to the high population coverage recorded in the Lao TME study (above 85%): community engagement to promote the concept of asymptomatic malaria and the rationale for MDA, baseline understanding of malaria as a health concern, perceptions that TME was worthwhile, provision of free primary health care, partnering of the research with local volunteers and authorities, building social relationship with community members and the cohesive nature of the communities that boosted the trust and participation in MDA.

Published
2019

98. Artemether-lumefantrine treatment of uncomplicated Plasmodium falciparum malaria: a systematic review and meta-analysis of day 7 lumefantrine concentrations and therapeutic response using individual patient data

Author

Nicholas J. White, Jullien, Andreas Mårtensson, Carol Hopkins Sibley, Steffen Borrmann, Gilbert Lefèvre, Michèle van Vugt, Karen I. Barnes, François Nosten, Christian Nsanzabana, Lars Rombo, Rose McGready, Kamal Hamed, Blaise Genton, Harin Karunajeewa, Francesca T. Aweeka, Philippe J Guerin, Liusheng Huang, Birgit Schramm, Pascal Ringwald, Tme Davis, Johan Ursing, Sunil Parikh, Eva Maria Hodel, Mey Bouth Denis, Prabin Dahal, C Moreira, Mayfong Mayxay, Ric N. Price, Kiechel, Kasia Stepniewska, Paul N. Newton, Lesley Workman, Quique Bassat, Poul-Erik Kofoed, Billy Ngasala, Philippe Deloron, Elizabeth A. Ashley, Niklas Lindegardh, Jean-François Faucher, Kevin Marsh, Abdoulaye Djimde, WorldWide Antimalarial Resistance Network (WWARN) Lumefantrine PK/PD Study Group, Ashley, E.A., Aweeka, F., Barnes, K.I., Bassat, Q., Borrmann, S., Dahal, P., Davis, T.M., Deloron, P., Denis, M.B., Djimde, A.A., Faucher, J.F., Genton, B., Guérin, P.J., Hamed, K., Hodel, E.M., Huang, L., Jullien, V., Karunajeewa, H.A., Kiechel, J.R., Kofoed, P.E., Lefèvre, G., Lindegardh, N., Marsh, K., Mårtensson, A., Mayxay, M., McGready, R., Moreira, C., Newton, P.N., Ngasala, B.E., Nosten, F., Nsanzabana, C., Parikh, S., Piola, P., Price, R.N., Ringwald, P., Rombo, L., Schramm, B., Sibley, C.H., Stepniewska, K., Tarning, J., Ursing, J., Van Vugt, M., White, N.J., and Workman, L.J.

Subjects
Artemether/lumefantrine, Baseline parasitemia, Drug resistance, Parasitemia, Pharmacology, Artemisinins/therapeutic use, chemistry.chemical_compound, 0302 clinical medicine, Recurrence, 030212 general & internal medicine, Treatment Failure, Malaria, Falciparum, Artemether-lumefantrine, Medicine(all), 0303 health sciences, biology, Malaria, Falciparum/drug therapy, Fluorenes/therapeutic use, Antimalarials/administration & dosage, Antimalarials/therapeutic use, Dose-Response Relationship, Drug, Drug Therapy, Combination, Ethanolamines/therapeutic use, Humans, General Medicine, Artemisinins, 3. Good health, Medicaments antipalúdics, Ethanolamines, Meta-analysis, Uncomplicated Plasmodium falciparum malaria, Artemether, Erratum, Early parasitological response, medicine.drug, Research Article, medicine.medical_specialty, Plasmodium falciparum, Pharmacokinetic, Malària, Lumefantrine, Online bibliographic searching, 03 medical and health sciences, Antimalarials, Internal medicine, medicine, Dosing, Cerca documental en línia, 030304 developmental biology, Fluorenes, Pharmacodynamic, business.industry, Malnutrition, medicine.disease, biology.organism_classification, Day 7 lumefantrine concentration, Malaria, chemistry, business
Abstract

BACKGROUND: Achieving adequate antimalarial drug exposure is essential for curing malaria. Day 7 blood or plasma lumefantrine concentrations provide a simple measure of drug exposure that correlates well with artemether-lumefantrine efficacy. However, the 'therapeutic' day 7 lumefantrine concentration threshold needs to be defined better, particularly for important patient and parasite sub-populations. METHODS: The WorldWide Antimalarial Resistance Network (WWARN) conducted a large pooled analysis of individual pharmacokinetic-pharmacodynamic data from patients treated with artemether-lumefantrine for uncomplicated Plasmodium falciparum malaria, to define therapeutic day 7 lumefantrine concentrations and identify patient factors that substantially alter these concentrations. A systematic review of PubMed, Embase, Google Scholar, ClinicalTrials.gov and conference proceedings identified all relevant studies. Risk of bias in individual studies was evaluated based on study design, methodology and missing data. RESULTS: Of 31 studies identified through a systematic review, 26 studies were shared with WWARN and 21 studies with 2,787 patients were included. Recrudescence was associated with low day 7 lumefantrine concentrations (HR 1.59 (95% CI 1.36 to 1.85) per halving of day 7 concentrations) and high baseline parasitemia (HR 1.87 (95% CI 1.22 to 2.87) per 10-fold increase). Adjusted for mg/kg dose, day 7 concentrations were lowest in very young children (/=200 ng/ml were associated with >98% cure rates (if parasitemia /=200 ng/ml and high cure rates in most uncomplicated malaria patients. Three groups are at increased risk of treatment failure: very young children (particularly those underweight-for-age); patients with high parasitemias; and patients in very low transmission intensity areas with emerging parasite resistance. In these groups, adherence and treatment response should be monitored closely. Higher, more frequent, or prolonged dosage regimens should now be evaluated in very young children, particularly if malnourished, and in patients with hyperparasitemia.

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99. Understanding hospital antimicrobial prescribing decisions and determinants of uptake of new local antimicrobial prescribing guidelines in Laos.

Author

Chansamouth V, Douangnouvong A, Thammavongsa P, Sombandith X, Keomany S, Rattana S, Newton PN, Day NP, Turner P, Mayxay M, van Doorn HR, and Ashley EA

Abstract

Background: Antimicrobial use in Laos is among the highest in Southeast Asia. The first Lao comprehensive antimicrobial prescribing guidelines have been available since 2021. This study explored the determinants of antibiotic prescribing decisions and how the new prescribing guidelines were being used., Methods: In August 2022, in-depth interviews were conducted with 16 Lao prescribers from two hospitals. Participants were questioned about their prescribing behaviours, attitudes to guidelines, how they learned about the guidelines and factors influencing their uptake. The interviews were audio-recorded, transcribed, and translated into English. Thematic analysis of the transcripts was conducted., Results: Lao prescribers considered multiple factors before deciding to prescribe antibiotics to their patients. The most common factor was based on the clinical judgement of the prescribers. Lack of certain antibiotics and turnaround times of laboratory results were the main challenges to prescribing antibiotics appropriately. The majority of participants were satisfied with the guidelines, regarding them as comprehensive, simple and convenient. However, most participants admitted that they did not access the guidelines very often. The main reason was that they could remember the treatment recommendations because they treat similar diseases on a daily basis. Improving antibiotic knowledge was the most common recommendation in order to improve the appropriate use of antibiotics. Raising awareness of the guidelines and promoting their use should also be considered. In addition, heads of the wards, and policy and implementation leaders, should support, monitor and feedback their use to encourage all prescribers to follow the guidelines., Conclusions: Several factors contribute to enhancing appropriate antibiotic prescription. Key factors for improving antibiotic prescription include enhancing prescribers' clinical knowledge, ensuring access to essential antibiotics, and updating guidelines regularly. Health leaders must get involved to promote their use., Competing Interests: No competing interests were disclosed., (Copyright: © 2024 Chansamouth V et al.)

Published
2024
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100. Bayesian spatio-temporal analysis of dengue transmission in Lao PDR.

Author

Soukavong M, Thinkhamrop K, Pratumchart K, Soulaphy C, Xangsayarath P, Mayxay M, Phommachanh S, Kelly M, Wangdi K, Clements ACA, and Suwannatrai AT

Subjects
Laos epidemiology, Humans, Incidence, Animals, Mosquito Vectors virology, Seasons, Climate, Dengue epidemiology, Dengue transmission, Bayes Theorem, Spatio-Temporal Analysis, Aedes virology
Abstract

Dengue, a zoonotic viral disease transmitted by Aedes mosquitoes, poses a significant public health concern throughout the Lao People's Democratic Republic (Lao PDR). This study aimed to describe spatial-temporal patterns and quantify the effects of environmental and climate variables on dengue transmission at the district level. The dengue data from 2015 to 2020 across 148 districts of Lao PDR were obtained from the Lao PDR National Center for Laboratory and Epidemiology (NCLE). The association between monthly dengue occurrences and environmental and climate variations was investigated using a multivariable Zero-inflated Poisson regression model developed in a Bayesian framework. The study analyzed a total of 72,471 dengue cases with an incidence rate of 174 per 100,000 population. Each year, incidence peaked from June to September and a large spike was observed in 2019. The Bayesian spatio-temporal model revealed a 9.1% decrease (95% credible interval [CrI] 8.9%, 9.2%) in dengue incidence for a 0.1 unit increase in monthly normalized difference vegetation index at a 1-month lag and a 5.7% decrease (95% CrI 5.3%, 6.2%) for a 1 cm increase in monthly precipitation at a 6-month lag. Conversely, dengue incidence increased by 43% (95% CrI 41%, 45%) for a 1 °C increase in monthly mean temperature at a 3-month lag. After accounting for covariates, the most significant high-risk spatial clusters were detected in the southern regions of Lao PDR. Probability analysis highlighted elevated trends in 45 districts, emphasizing the importance of targeted control strategies in high-risk areas. This research underscores the impact of climate and environmental factors on dengue transmission, emphasizing the need for proactive public health interventions tailored to specific contexts in Lao PDR., (© 2024. The Author(s).)

Published
2024
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