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Comparative pathogenicity of single and mixed drug-resistant Trypanosoma brucei brucei and Trypanosoma congolense infections in rats
被引:1
|作者:
Obi, Chukwunonso F.
[1
]
Okpala, Michael I.
[1
]
Anyogu, Davinson C.
[2
]
Onyeabo, Amaechi
[3
]
Aneru, Ganiyu E.
[1
]
Ezeh, Ikenna O.
[1
]
Ezeokonkwo, Romanus C.
[1
]
机构:
[1] Univ Nigeria, Fac Vet Med, Dept Vet Parasitol & Entomol, Nsukka, Enugu, Nigeria
[2] Univ Nigeria, Fac Vet Med, Dept Vet Pathol & Microbiol, Nsukka, Enugu, Nigeria
[3] Michael Okpara Univ Agr, Coll Vet Med, Dept Vet Parasitol & Entomol, Umudike, Abia, Nigeria
关键词:
Drug -resistant trypanosomes;
Pathogenicity;
Clinical findings;
Haematology;
Rats;
CATTLE;
D O I:
10.1016/j.rvsc.2023.104946
中图分类号:
S85 [动物医学(兽医学)];
学科分类号:
0906 ;
摘要:
Drug-resistant trypanosomes are widespread in sub-Saharan Africa and in conjunction with the drug-sensitive phenotypes cause a serious endemic wasting disease in animals. We evaluated the pathogenicity of single and mixed drug-resistant Trypanosoma brucei brucei and T. congolense isolates in 35 female rats, randomly divided into seven groups (1-7) of five rats. Group 1 was the uninfected control. Groups 2 and 3 were infected with drugsensitive T. brucei brucei and T. congolense, respectively, whereas groups 4 and 5 were infected with multidrug-resistant T. brucei brucei and T. congolense respectively. Group 6 were infected with drug-sensitive T. brucei brucei and T. congolense while group 7 were infected with multidrug-resistant T. brucei brucei and T. congolense. Parasitaemia kinetics, haematological parameters, body weight, clinical signs, survival time, gross and histopathological changes in the spleen were evaluated. Parasitaemia occurred between day 3-9 postinfection in all the infected groups. Rats in groups 4 and 7 had markedly prolonged (p < 0.05) pre-patent period, days to first peak parasitaemia, survival time, and lower (p < 0.05) parasitaemia level than groups 2 and 6 rats while these parameters were comparable for groups 3 and 5 rats. Anaemia was noted in the infected groups but the severity did not vary amongst the infected groups. Severe clinical signs and splenic lesions were noted in rats infected with drug-sensitive trypanosome species compared to the multidrug-resistant species. Therefore, we conclude that the trypanosome isolates were pathogenic. However, the drug-sensitive T. brucei brucei and mixed drug-sensitive trypanosome infections were more pathogenic than their multidrug-resistant counterparts.
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