Altered drug influx/efflux and enhanced metabolic activity in triclabendazole-resistant liver flukes

被引:78
作者
Alvarez, LI
Solana, HD
Mottier, ML
Virkel, GL
Fairweather, I
Lanusse, CE
机构
[1] UNCPBA, Fac Ciencias Vet, Farmacol Lab, RA-7000 Tandil, Argentina
[2] Consejo Nacl Invest Cient & Tecn, RA-1033 Buenos Aires, DF, Argentina
[3] CICPBA, Buenos Aires, DF, Argentina
[4] Queens Univ Belfast, Ctr Med Biol, Sch Biol & Biochem, Belfast, Antrim, North Ireland
关键词
Fasciola hepatica; triclabendazole; resistance mechanisms; drug diffusion and metabolism;
D O I
10.1017/S0031182005007997
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
Triclabendazole (TCBZ) is a halogenated benzimidazole Compound that possesses high activity against immature and adult stages of the liver fluke, Fasciola hepatica. The intensive use of TCBZ in endemic areas of fascioliasis has resulted in the development of liver flukes resistant to this compound. TCBZ sulphoxide (TCBZSO) and TCBZ sulphone (TCBZSO(2)) are the main molecules recovered in the bloodstream of TCBZ-treated animals. In order to gain some insight into the possible mechanisms of resistance to TCBZ, the goals of the work described here were: to compare the ex vivo transtegumental diffusion of TCBZ parent drug and its sulpho-metabolites (TCBZSO and TCBZSO(2)) into 'I'CBZ-susceptible and -resistant liver flukes; and to assess the comparative pattern of TCBZ biotransformation by 'I'CBZ-susceptible and -resistant F. hepatica. For the tegumental diffusion studies, TCBZ-susceptible (Cullompton) and -resistant (Sligo) adult flukes collected from untreated infected sheep were incubated (15-180 min) in KRT buffer containing either TCBZ, TCBZSO or TCBZSO(2) (5 nmol.ml(-1)). For the metabolism studies, microsomal fractions obtained from TCBZ-susceptible and -resistant flukes were incubated for 60 min with TCBZ (40 gamma M), and the amount of the formed metabolic product (TCBZSO) was measured. Drug/metabolite concentrations were quantified by HPLC. All the assayed TCBZ-related molecules penetrated through the tegument of both TCBZ-susceptible and -resistant flukes. However, significantly lower (approximately, 50%) concentrations of TCBZ and TCBZSO were recovered within the TCBZ-resistant flukes compared to the TCBZ-susceptible ones over the 180 min incubation period. The rate of TCBZ sulphoxidative metabolism into TCBZSO was significantly higher (39%) in TCBZ-resistant flukes. The flavin-monooxigenase (FMO) enzyme system appears to be the main metabolic pathway involved in the formation of TCBZSO in both TCBZ-susceptible and -resistant flukes. The altered drug influx/efflux and enhanced metabolic capacity identified in TCBZ-resistant liver flukes may account for the development of resistance to TCBZ.
引用
收藏
页码:501 / 510
页数:10
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