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Vector competence of Glossina austeni and Glossina brevipalpis for Trypanosoma congolense in KwaZulu-Natal, South Africa
2012
Makhosazana Motloang | Justin Masumu | Barend Mans | Peter van den Bossche | Abdalla Latif
Tsetse-transmitted trypanosomosis (nagana) has been the cause of stock losses in the recent past and still presents a major problem to livestock owners in certain areas of KwaZulu- Natal, South Africa. Over 10 000 cattle mortalities were reported in the 1990 nagana outbreak. Although information on the distribution and abundance of the tsetse flies Glossina brevipalpis and Glossina austeni in KwaZulu-Natal exists, data on their vector competence are lacking. This study aimed to determine the rate of natural Trypanosoma congolense infection by field-collected as well as colony-reared flies of these species. A total of 442 field-collected G. brevipalpis and 40 G. austeni flies were dissected immediately after collection to determine their infection rates, whilst 699 G. brevipalpis and 49 G. austeni flies were fed on susceptible animals in 10 and four batches, respectively, for use in xenodiagnosis experiments. Teneral colony flies were fed on infected animals and dissected 21 days post infection to confirm their infectivity testing. Glossina austeni harboured 8% immature and mature infections. In G. brevipalpis, the infection with the immature stages was lower (1%) and no mature infections were observed. Although all four batches of G. austeni transmitted T. congolense to four susceptible animals, no transmission resulted from 10 batches of G. brevipalpis fed on susceptible cattle. Colony-derived G. austeni (534) and G. brevipalpis (882) were fed on four bovines infected with different T. congolense isolates. Both G. austeni and G. brevipalpis acquired trypanosome infection from the bovines, with immature infection ranges of 20% – 33% and 1% – 4%, respectively. Parasites, however, only matured in G. austeni (average = 4%). Glossina austeni plays a larger role in the epidemiology of animal trypanosomosis in KwaZulu-Natal than G. brevipalpis and therefore more focus should be aimed at the former when control measures are implemented.
Afficher plus [+] Moins [-]Ascofuranone antibiotic is a promising trypanocidal drug for nagana
2024
Keisuke Suganuma | Kennedy M. Mochabo | Judith K. Chemuliti | Kita Kiyoshi | Inoue Noboru | Shin-ichiro Kawazu
Trypanosomosis is a disease complex which affects both humans and animals in sub-Saharan Africa, transmitted by the tsetse fly and distributed within the tsetse belt of Africa. But some trypanosome species, for example, Trypanosoma brucei evansi, T. vivax, T. theileri and T. b. equiperdum are endemic outside the tsetse belt of Africa transmitted by biting flies, for example, Tabanus and Stomoxys, or venereal transmission, respectively. Trypanocidal drugs remain the principal method of animal trypanosomosis control in most African countries. However, there is a growing concern that their effectiveness may be severely curtailed by widespread drug resistance. A minimum number of six male cattle calves were recruited for the study. They were randomly grouped into two (T. vivax and T. congolense groups) of three calves each. One calf per group served as a control while two calves were treatment group. They were inoculated with 105 cells/mL parasites in phosphate buffered solution (PBS) in 2 mL. When parasitaemia reached 1 × 107.8 cells/mL trypanosomes per mL in calves, treatment was instituted with 20 mL (25 mg/kg in 100 kg calf) ascofuranone (AF) for treatment calves, while the control ones were administered a placebo (20 mL PBS) intramuscularly. This study revealed that T. vivax was successfully cleared by AF but the T. congolense group was not cleared effectively. Contribution: There is an urgent need to develop new drugs which this study sought to address. It is suggested that the AF compound can be developed further to be a sanative drug for T. vivax in non-tsetse infested areas like South Americas.
Afficher plus [+] Moins [-]Ascofuranone antibiotic is a promising trypanocidal drug for nagana
2024
Suganuma, Keisuke(Obihiro University of Agriculture and Veterinary Medicine National Research Center for Protozoan Diseases) | Mochabo, Kennedy M.(Egerton University Faculty of Veterinary Medicine and Surgery Department of Veterinary Public Health, Pharmacology) | Chemuliti, Judith K.(Kenya Agricultural Research Organization Biotechnology Research Institute) | Kiyoshi, Kita(Nagasaki University Institute of Tropical Medicine Department of Host-Defense Biochemistry) | Noboru, Inoue(Obihiro University of Agriculture and Veterinary Medicine National Research Center for Protozoan Diseases) | Kawazu, Shin-ichiro(Obihiro University of Agriculture and Veterinary Medicine National Research Center for Protozoan Diseases)
Trypanosomosis is a disease complex which affects both humans and animals in sub-Saharan Africa, transmitted by the tsetse fly and distributed within the tsetse belt of Africa. But some trypanosome species, for example, Trypanosoma brucei evansi, T. vivax, T. theileri and T. b. equiperdum are endemic outside the tsetse belt of Africa transmitted by biting flies, for example, Tabanus and Stomoxys, or venereal transmission, respectively. Trypanocidal drugs remain the principal method of animal trypanosomosis control in most African countries. However, there is a growing concern that their effectiveness may be severely curtailed by widespread drug resistance. A minimum number of six male cattle calves were recruited for the study. They were randomly grouped into two (T. vivax and T. congolense groups) of three calves each. One calf per group served as a control while two calves were treatment group. They were inoculated with 10(5) cells/mL parasites in phosphate buffered solution (PBS) in 2 mL. When parasitaemia reached 1 × 10(7.8) cells/mL trypanosomes per mL in calves, treatment was instituted with 20 mL (25 mg/kg in 100 kg calf) ascofuranone (AF) for treatment calves, while the control ones were administered a placebo (20 mL PBS) intramuscularly. This study revealed that T. vivax was successfully cleared by AF but the T. congolense group was not cleared effectively. CONTRIBUTION: There is an urgent need to develop new drugs which this study sought to address. It is suggested that the AF compound can be developed further to be a sanative drug for T. vivax in non-tsetse infested areas like South Americas
Afficher plus [+] Moins [-]The susceptibility of Trypanosoma congolense isolated in Zambezia Province, Mozambique, to isometamidium chloride, diminazene aceturate and homidium chloride
2005
Jamal, S. | Sigauque, I. | Macuamule, C. (National Directorate of Livestock, Maputo (Mozambique)) | Neves, L. | Penzhorn, B.L. | Marcotty, T. | Van den Bossche, P.
Parasitological prevalence of bovine trypanosomosis in Kindo Koisha district, Wollaita zone, south Ethiopia
2002
Kidanemariam, A. (National Animal Health Research Centre, Sebeta (Ethiopia)) | Hadgu, K. | Sahle, M.
Heterophile antibodies to chicken erythrocytes in sheep infected with Trypanosoma congolense
1996
Joshua, R.A. | Neils, J.S. (Zimbabwe Univ., Harare (Zimbabwe). Paraclinical Veterinary Studies) | Oladosu, L.A.