In vivo analysis of trypanocidal drug resistance in sahelian goats infected by Trypanosoma vivax strains collected in northern Togo

被引:1
|
作者
Boma, Soudah [1 ]
Vitouley, Sena Herve [1 ,2 ]
Somda, Martin Bienvenu [1 ,2 ]
Bengaly, Zakaria [1 ]
Houaga, Isidore [3 ]
Lombo, Yao [4 ]
Tchamdja, Eyaba [4 ]
Dayo, Guiguigbaza-Kossigan [1 ]
机构
[1] Ctr Int Rech Dev Elevage Zone Subhumide CIRDES, Unite Rech Malad Vecteurs & Biodiversite UMaVeB, 01POB 454, Bobo Dioulasso 01, Burkina Faso
[2] Univ Nazi BONI UNB, 01 BP 1 091, Bobo Dioulasso 01, Burkina Faso
[3] Univ Edinburgh, Ctr Trop Livestock Genet & Hlth CTLGH, Roslin Inst, Edinburgh EH25 9RG, Midlothian, Scotland
[4] Inst Togolais Rech Agron ITRA Togo, Programme Prod & Sante Anim, BP 1163, Lome, Togo
关键词
Trypanosoma vivax; Goats; Diminazen aceturate; Isometamidium chloride; Togo; SSU-RDNA AMPLIFICATION; CATTLE; DIAGNOSIS; ISOMETAMIDIUM; EPIDEMIOLOGY; POPULATIONS; CONGOLENSE; BRUCEI; REGION; MICE;
D O I
10.1016/j.vetpar.2022.109723
中图分类号
R38 [医学寄生虫学]; Q [生物科学];
学科分类号
07 ; 0710 ; 09 ; 100103 ;
摘要
Trypanosoma (T.) vivax is one of the animal trypanosomes species causing calf mortality and economic losses in Togo. Despite its importance as the most widely distributed trypanosome species, T. vivax has received little attention because it is difficult to cultivate most field isolates in rodents. No molecular diagnostic tools for the identification of drug-resistant in T. vivax are currently available. Herein, four field isolates of T. vivax from Togo were cryopreserved and assessed for susceptibility to diminazene aceturate (DA) and isometamidium chloride (ISM) in goats. For field isolate preparation, 1 ml of blood from an infected goat was diluted in 111 mu l of phosphate-buffered-saline and stored in liquid nitrogen. The in vivo experiment drug test was performed using twenty Sahelian goats with six-month of age and weighing 14.5 +/- 1.6 kg. These experimental goats were purchased from a tsetse free-area Dori, a Sahelian region of Burkina Faso. The cryopreserved T. vivax isolates with unknowns, DA, and ISM sensitivity was inoculated to five goats and one goat was used as control. Each animal was inoculated by intravenously route 1 x 10(5) trypanosomes from the donor goat. Relapses were earlier in the first phase of treatment (14.85 +/- 1.08 days) compared with the second phase (20 +/- 3.39 days). The overall mean PCV of the control group decreased from 32% to 17% at day-60 (P-value < 0.001). Three isolates were phenotypically resistant to 0.5 mg per kg body weight (BW) ISM and one for 3.5 mg per kg BW of DA. There were no relapses with the 7 mg per kg BW dose DA. This study shows the resistance of T. vivax to two main trypanocidal drugs in different villages of Mango. The results suggest the extension of surveillance strategies to remote villages in Togo and will guide the veterinarian or herder in choosing a mass treatment strategy. Further studies will be needed to better understand the molecular basis of the observed resistance.
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