Your search keyword '"Htoo GN"' showing total 5 results

1. Transmission-blocking activities of artesunate, chloroquine, and methylene blue on Plasmodium vivax gametocytes.

Author

Odom John, A, Chaumeau, V, Wasisakun, P, Watson, JA, Oo, T, Aryalamloed, S, Sue, MP, Htoo, GN, Tha, NM, Archusuksan, L, Sawasdichai, S, Gornsawun, G, Mehra, S, White, NJ, Nosten, FH, Odom John, A, Chaumeau, V, Wasisakun, P, Watson, JA, Oo, T, Aryalamloed, S, Sue, MP, Htoo, GN, Tha, NM, Archusuksan, L, Sawasdichai, S, Gornsawun, G, Mehra, S, White, NJ, and Nosten, FH

Abstract

Plasmodium vivax is now the main cause of malaria outside Africa. The gametocytocidal effects of antimalarial drugs are important to reduce malaria transmissibility, particularly in low-transmission settings, but they are not well characterized for P. vivax. The transmission-blocking effects of chloroquine, artesunate, and methylene blue on P. vivax gametocytes were assessed. Blood specimens were collected from patients presenting with vivax malaria, incubated with or without the tested drugs, and then fed to mosquitos from a laboratory-adapted colony of Anopheles dirus (a major malaria vector in Southeast Asia). The effects on oocyst and sporozoite development were analyzed under a multi-level Bayesian model accounting for assay variability and the heterogeneity of mosquito Plasmodium infection. Artesunate and methylene blue, but not chloroquine, exhibited potent transmission-blocking effects. Gametocyte exposures to artesunate and methylene blue reduced the mean oocyst count 469-fold (95% CI: 345 to 650) and 1,438-fold (95% CI: 970 to 2,064), respectively. The corresponding estimates for the sporozoite stage were a 148-fold reduction (95% CI: 61 to 470) and a 536-fold reduction (95% CI: 246 to 1,311) in the mean counts, respectively. In contrast, high chloroquine exposures reduced the mean oocyst count only 1.40-fold (95% CI: 1.20 to 1.64) and the mean sporozoite count 1.34-fold (95% CI: 1.12 to 1.66). This suggests that patients with vivax malaria often remain infectious to anopheline mosquitos after treatment with chloroquine. Use of artemisinin combination therapies or immediate initiation of primaquine radical cure should reduce the transmissibility of P. vivax infections.

Published

2024

2. Effect of generalised access to early diagnosis and treatment and targeted mass drug administration on Plasmodium falciparum malaria in Eastern Myanmar : an observational study of a regional elimination programme

Author

Jordi Landier, Daniel M Parker, Aung Myint Thu, Khin Maung Lwin, Gilles Delmas, François H Nosten, Chiara Andolina, Ricardo Aguas, Saw Moe Ang, Ei Phyo Aung, Naw Baw Baw, Saw Aye Be, Saw B'Let, Hay Bluh, Craig A. Bonnington, Victor Chaumeau, Miasa Chirakiratinant, Win Cho Cho, Peter Christensen, Vincent Corbel, Nicholas PJ Day, Saw Hsa Dah, Mehul Dhorda, Arjen M Dondorp, Jean Gaudart, Gornpan Gornsawun, Warat Haohankhunnatham, Saw Kyaw Hla, Saw Nay Hsel, Gay Nay Htoo, Saw Nay Htoo, Mallika Imwong, Saw John, Ladda Kajeechiwa, Lily Kereecharoen, Praphan Kittiphanakun, Keerati Kittitawee, Kamonchanok Konghahong, Saw Diamond Khin, Saw Win Kyaw, Clare Ling, Khine Shwe War Lwin, Naw K' Yin Ma, Alexandra Marie, Cynthia Maung, Ed Marta, Myo Chit Minh, Olivo Miotto, Paw Khu Moo, Ku Ler Moo, Merry Moo, Naw Na Na, Mar Nay, François H. Nosten, Suphak Nosten, Slight Naw Nyo, Eh Kalu Shwe Oh, Phu Thit Oo, Tun Pyit Oo, Daniel M. Parker, Eh Shee Paw, Choochai Phumiya, Aung Pyae Phyo, Kasiha Pilaseng, Stéphane Proux, Santisuk Rakthinthong, Wannee Ritwongsakul, Kloloi Salathibuphha, Armon Santirad, Sunisa Sawasdichai, Lorenz von Seidlein, Paw Wah Shee, Paw Bway Shee, Decha Tangseefa, May Myo Thwin, Saw Win Tun, Chode Wanachaloemlep, Lisa J White, Nicholas J White, Jacher Wiladphaingern, Saw Nyunt Win, Nan Lin Yee, Daraporn Yuwapan, Shoklo Malaria Research Unit [Mae Sot, Thailand] (SMRU), Mahidol Oxford Tropical Medicine Research Unit (MORU), Wellcome Trust-Mahidol University [Bangkok]-University of Oxford [Oxford]-Wellcome Trust-Mahidol University [Bangkok]-University of Oxford [Oxford], Sciences Economiques et Sociales de la Santé & Traitement de l'Information Médicale (SESSTIM - U1252 INSERM - Aix Marseille Univ - UMR 259 IRD), Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Department of Population Health and Disease Prevention [Irvine, CA, USA], University of California [Irvine] (UCI), University of California-University of California, Centre for Tropical Medicine and Global Health [Oxford, UK], Nuffield Department of Medicine [Oxford, UK] (Big Data Institute), University of Oxford [Oxford]-University of Oxford [Oxford], This work was supported by the Wellcome Trust (041843), the Bill & Melinda Gates Foundation (OPP1117507), and the Regional Artemisinin Initiative (Global Fund against AIDS, Tuberculosis and Malaria)., Malaria Elimination Task Force Group : Andolina C, Aguas R, Ang SM, Aung EP, Baw NB, Be SA, B'Let S, Bluh H, Bonnington CA, Chaumeau V, Chirakiratinant M, Cho WC, Christensen P, Corbel V, Day NP, Dah SH, Delmas G, Dhorda M, Dondorp AM, Gaudart J, Gornsawun G, Haohankhunnatham W, Hla SK, Hsel SN, Htoo GN, Htoo SN, Imwong M, John S, Kajeechiwa L, Kereecharoen L, Kittiphanakun P, Kittitawee K, Konghahong K, Khin SD, Kyaw SW, Landier J, Ling C, Lwin KM, Lwin KSW, Ma NKY, Marie A, Maung C, Marta E, Minh MC, Miotto O, Moo PK, Moo KL, Moo M, Na NN, Nay M, Nosten FH, Nosten S, Nyo SN, Oh EKS, Oo PT, Oo TP, Parker DM, Paw ES, Phumiya C, Phyo AP, Pilaseng K, Proux S, Rakthinthong S, Ritwongsakul W, Salathibuphha K, Santirad A, Sawasdichai S, von Seidlein L, Shee PW, Shee PB, Tangseefa D, Thu AM, Thwin MM, Tun SW, Wanachaloemlep C, White LJ, White NJ, Wiladphaingern J, Win SN, Yee NL, Yuwapan D., Dupuis, Christine, University of Oxford-Mahidol University [Bangkok]-Wellcome Trust-University of Oxford-Mahidol University [Bangkok]-Wellcome Trust, University of California [Irvine] (UC Irvine), University of California (UC)-University of California (UC), and University of Oxford-University of Oxford

Subjects

Male, Rural Population, Primaquine, Drug Resistance, Myanmar, Drug resistance, Rate ratio, Health Services Accessibility, State Medicine, 0302 clinical medicine, [SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Prevalence, 030212 general & internal medicine, Artemether, Malaria, Falciparum, Artemisinin, 2. Zero hunger, biology, Incidence, 1. No poverty, General Medicine, Artemisinins, 3. Good health, Drug Combinations, Treatment Outcome, Ethanolamines, [SDV.MHEP.MI] Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Mass Drug Administration, Female, medicine.drug, 030231 tropical medicine, Article, Antimalarials, 03 medical and health sciences, parasitic diseases, medicine, Humans, Mass drug administration, Fluorenes, business.industry, Artemether, Lumefantrine Drug Combination, Plasmodium falciparum, medicine.disease, biology.organism_classification, Malaria, Early Diagnosis, [SDV.SPEE] Life Sciences [q-bio]/Santé publique et épidémiologie, [SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie, business, Demography

Abstract

Summary Background Potentially untreatable Plasmodium falciparum malaria threatens the Greater Mekong subregion. A previous series of pilot projects in Myanmar, Laos, Cambodia, and Vietnam suggested that mass drug administration was safe, and when added to provision of early diagnosis and treatment, could reduce the reservoir of P falciparum and interrupts transmission. We examined the effects of a scaled-up programme of this strategy in four townships of eastern Myanmar on the incidence of P falciparum malaria. Methods The programme was implemented in the four townships of Myawaddy, Kawkareik, Hlaingbwe, and Hpapun in Kayin state, Myanmar. Increased access to early diagnosis and treatment of malaria was provided to all villages through community-based malaria posts equipped with rapid diagnostic tests, and treatment with artemether–lumefantrine plus single low-dose primaquine. Villages were identified as malarial hotspots (operationally defined as >40% malaria, of which 20% was P falciparum ) with surveys using ultrasensitive quantitative PCR either randomly or targeted at villages where the incidence of clinical cases of P falciparum malaria remained high (ie, >100 cases per 1000 individuals per year) despite a functioning malaria post. During each survey, a 2 mL sample of venous blood was obtained from randomly selected adults. Hotspots received targeted mass drug administration with dihydroartemisinin–piperaquine plus single-dose primaquine once per month for 3 consecutive months in addition to the malaria posts. The main outcome was the change in village incidence of clinical P falciparum malaria, quantified using a multivariate, generalised, additive multilevel model. Malaria prevalence was measured in the hotspots 12 months after mass drug administration. Findings Between May 1, 2014, and April 30, 2017, 1222 malarial posts were opened, providing early diagnosis and treatment to an estimated 365 000 individuals. Incidence of P falciparum malaria decreased by 60 to 98% in the four townships. 272 prevalence surveys were undertaken and 69 hotspot villages were identified. By April 2017, 50 hotspots were treated with mass drug administration. Hotspot villages had a three times higher incidence of P falciparum at malarial posts than neighbouring villages (adjusted incidence rate ratio [IRR] 2·7, 95% CI 1·8–4·4). Early diagnosis and treatment was associated with a significant decrease in P falciparum incidence in hotspots (IRR 0·82, 95% CI 0·76–0·88 per quarter) and in other villages (0·75, 0·73–0·78 per quarter). Mass drug administration was associated with a five-times decrease in P falciparum incidence within hotspot villages (IRR 0·19, 95% CI 0·13–0·26). By April, 2017, 965 villages (79%) of 1222 corresponding to 104 village tracts were free from P falciparum malaria for at least 6 months. The prevalence of wild-type genotype for K13 molecular markers of artemisinin resistance was stable over the three years (39%; 249/631). Interpretation Providing early diagnosis and effective treatment substantially decreased village-level incidence of artemisinin-resistant P falciparum malaria in hard-to-reach, politically sensitive regions of eastern Myanmar. Targeted mass drug administration significantly reduced malaria incidence in hotspots. If these activities could proceed in all contiguous endemic areas in addition to standard control programmes already implemented, there is a possibility of subnational elimination of P falciparum . Funding The Bill & Melinda Gates Foundation, the Regional Artemisinin Initiative (Global Fund against AIDS, Tuberculosis and Malaria), and the Wellcome Trust.

Published

2018

3. Transmission-blocking activities of artesunate, chloroquine, and methylene blue on Plasmodium vivax gametocytes.

Author

Chaumeau V, Wasisakun P, Watson JA, Oo T, Aryalamloed S, Sue MP, Htoo GN, Tha NM, Archusuksan L, Sawasdichai S, Gornsawun G, Mehra S, White NJ, and Nosten FH

Subjects

Animals, Humans, Sporozoites drug effects, Artemisinins pharmacology, Artemisinins therapeutic use, Oocysts drug effects, Methylene Blue pharmacology, Methylene Blue therapeutic use, Artesunate pharmacology, Artesunate therapeutic use, Chloroquine pharmacology, Chloroquine therapeutic use, Plasmodium vivax drug effects, Antimalarials pharmacology, Antimalarials therapeutic use, Malaria, Vivax drug therapy, Malaria, Vivax parasitology, Malaria, Vivax transmission, Anopheles parasitology, Anopheles drug effects

Abstract

Plasmodium vivax is now the main cause of malaria outside Africa. The gametocytocidal effects of antimalarial drugs are important to reduce malaria transmissibility, particularly in low-transmission settings, but they are not well characterized for P. vivax . The transmission-blocking effects of chloroquine, artesunate, and methylene blue on P. vivax gametocytes were assessed. Blood specimens were collected from patients presenting with vivax malaria, incubated with or without the tested drugs, and then fed to mosquitos from a laboratory-adapted colony of Anopheles dirus (a major malaria vector in Southeast Asia). The effects on oocyst and sporozoite development were analyzed under a multi-level Bayesian model accounting for assay variability and the heterogeneity of mosquito Plasmodium infection. Artesunate and methylene blue, but not chloroquine, exhibited potent transmission-blocking effects. Gametocyte exposures to artesunate and methylene blue reduced the mean oocyst count 469-fold (95% CI: 345 to 650) and 1,438-fold (95% CI: 970 to 2,064), respectively. The corresponding estimates for the sporozoite stage were a 148-fold reduction (95% CI: 61 to 470) and a 536-fold reduction (95% CI: 246 to 1,311) in the mean counts, respectively. In contrast, high chloroquine exposures reduced the mean oocyst count only 1.40-fold (95% CI: 1.20 to 1.64) and the mean sporozoite count 1.34-fold (95% CI: 1.12 to 1.66). This suggests that patients with vivax malaria often remain infectious to anopheline mosquitos after treatment with chloroquine. Use of artemisinin combination therapies or immediate initiation of primaquine radical cure should reduce the transmissibility of P. vivax infections., Competing Interests: The authors declare no conflict of interest.

Published

2024

4. Human movement patterns of farmers and forest workers from the Thailand-Myanmar border.

Author

Tun STT, Min MC, Aguas R, Fornace K, Htoo GN, White LJ, and Parker DM

Abstract

Background : Human travel patterns play an important role in infectious disease epidemiology and ecology. Movement into geographic spaces with high transmission can lead to increased risk of acquiring infections. Pathogens can also be distributed across the landscape via human travel. Most fine scale studies of human travel patterns have been done in urban settings in wealthy nations. Research into human travel patterns in rural areas of low- and middle-income nations are useful for understanding the human components of epidemiological systems for malaria or other diseases of the rural poor. The goal of this research was to assess the feasibility of using GPS loggers to empirically measure human travel patterns in this setting, as well as to quantify differing travel patterns by age, gender, and seasonality among study participants. Methods : In this pilot study we recruited 50 rural villagers from along the Myanmar-Thailand border to carry GPS loggers for the duration of a year. The GPS loggers were programmed to take a time-stamped reading every 30 minutes. We calculated daily movement ranges and multi-day trips by age and gender. We incorporated remote sensing data to assess patterns of days and nights spent in forested or farm areas, also by age and gender. Results : Our study showed that it is feasible to use GPS devices to measure travel patterns, though we had difficulty recruiting women and management of the project was relatively intensive. We found that older adults traveled farther distances than younger adults and adult males spent more nights in farms or forests. Conclusion : The results of this study suggest that further work along these lines would be feasible in this region. Furthermore, the results from this study are useful for individual-based models of disease transmission and land use., Competing Interests: No competing interests were disclosed., (Copyright: © 2023 Tun STT et al.)

Published

2023

5. Longevity of the insecticidal effect of three pyrethroid formulations applied to outdoor vegetation on a laboratory-adapted colony of the Southeast Asian malaria vector Anopheles dirus.

Author

Chaumeau V, Wisisakun P, Sawasdichai S, Kankew P, Htoo GN, Saithanmettajit S, Aryalamloed S, Lee NY, Delmas G, and Nosten F

Subjects

Animals, Anopheles growth & development, Insect Vectors growth & development, Insecticides chemistry, Myanmar, Nitriles chemistry, Pyrethrins chemistry, Thailand, Anopheles drug effects, Insect Vectors drug effects, Insecticide Resistance, Insecticides pharmacology, Mosquito Control methods, Nitriles pharmacology, Pyrethrins pharmacology

Abstract

Outdoor residual spraying is proposed for the control of exophilic mosquitoes. However, the residual effect of insecticide mists applied to outdoor resting habitats of mosquitoes is not well characterized. The objective of this study was to assess the longevity of the residual insecticidal effect of three pyrethroid formulations applied to outdoor vegetation against the Southeast Asian malaria vector Anopheles dirus. Lambda-cyhalothrin capsule suspension, deltamethrin emulsifiable concentrate and bifenthrin wettable powder were sprayed on dense bamboo bushes on the Thailand-Myanmar border during the dry season 2018. The duration and magnitude of the residual insecticidal effect were assessed weekly with a standard cone assay, using freshly collected insecticide-treated bamboo leaves and a laboratory-adapted colony of Anopheles dirus sensu stricto susceptible to pyrethroids. The experiment was repeated during the rainy season to assess the persistence of the lambda-cyhalothrin formulation after natural rains and artificial washings. During the dry season (cumulative rainfall = 28 mm in 111 days), mortality and knockdown (KD) rates were >80% for 60 days with bifenthrin and 90 days with lambda-cyhalothrin and deltamethrin. The 50% knockdown time (TKD50) was <15 min with lambda-cyhalothrin and deltamethrin, and <30 min with bifenthrin. During the rainy season (cumulative rainfall = 465 mm in 51 days), mortality and KD rates were >80% for 42 days and TKD50 was <15 min with lambda-cyhalothrin. Additional artificial washing of the testing material with 10L of tap water before performing the cone tests had no significant effect on the residual insecticidal effect of this formulation. Long-lasting residual insecticidal effect can be obtained when spraying pyrethroid insecticides on the outdoor resting habitats of malaria vectors., Competing Interests: The authors have declared that no competing interests exist.

Published

2020