| Literature DB >> 23710083 |
Sayed Hassan Seif El-Din1, Abdel-Nasser Abdel-Aal Sabra, Olfat Ali Hammam, Naglaa Mohamed El-Lakkany.
Abstract
The fear that schistosomes will become resistant to praziquantel (PZQ) motivates the search for alternatives to treat schistosomiasis. The antimalarials quinine (QN) and halofantrine (HF) possess moderate antischistosomal properties. The major metabolic pathway of QN and HF is through cytochrome P450 (CYP) 3A4. Accordingly, this study investigates the effects of CYP3A4 inhibitor, ketoconazole (KTZ), on the antischistosomal potential of these quinolines against Schistosoma mansoni infection by evaluating parasitological, histopathological, and biochemical parameters. Mice were classified into 7 groups: uninfected untreated (I), infected untreated (II), infected treated orally with PZQ (1,000 mg/kg) (III), QN (400 mg/kg) (IV), KTZ (10 mg/kg)+QN as group IV (V), HF (400 mg/kg) (VI), and KTZ (as group V)+HF (as group VI) (VII). KTZ plus QN or HF produced more inhibition (P<0.05) in hepatic CYP450 (85.7% and 83.8%) and CYT b5 (75.5% and 73.5%) activities, respectively, than in groups treated with QN or HF alone. This was accompanied with more reduction in female (89.0% and 79.3%), total worms (81.4% and 70.3%), and eggs burden (hepatic; 83.8%, 66.0% and intestinal; 68%, 64.5%), respectively, and encountering the granulomatous reaction to parasite eggs trapped in the liver. QN and HF significantly (P<0.05) elevated malondialdehyde levels when used alone or with KTZ. Meanwhile, KTZ plus QN or HF restored serum levels of ALT, albumin, and reduced hepatic glutathione (KTZ+HF) to their control values. KTZ enhanced the therapeutic antischistosomal potential of QN and HF over each drug alone. Moreover, the effect of KTZ+QN was more evident than KTZ+HF.Entities:
Keywords: CYP3A4; Schistosoma mansoni; glutathione; halofantrine; ketoconazole; malondialdehyde; quinine
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Year: 2013 PMID: 23710083 PMCID: PMC3662059 DOI: 10.3347/kjp.2013.51.2.165
Source DB: PubMed Journal: Korean J Parasitol ISSN: 0023-4001 Impact factor: 1.341
Effects of QN or HF alone and in addition to KTZ on the number of male and female worms in S. mansoni-infected mice at week 9 post-infection (i.e., week 2 post-treatment)
No. of animals in each group; 8 mice. Values are presented as the mean±SD. Numbers in the parentheses indicate the percentage of reduction from infected control.
aSignificant difference from infected group at P<0.05.
bSignificant difference from QN group at P<0.05.
Effects of QN or HF alone and in addition to KTZ on the percentage of egg developmental stages and tissue egg load in S. mansoni-infected mice at week 9 post-infection (i.e., week 2 post-treatment)
No. of animals in each group; 8 mice. Values are presented as the mean±SD. Numbers in the parentheses indicate the percentage of reduction from infected control.
aSignificant difference from infected group at P<0.05; bSignificant difference from QN group at P<0.05; cSignificant difference from HF group at P<0.05.
Effect of QN or HF alone and in addition to KTZ on granuloma diameter and associated histopathological changes in S. mansoni-infected mice 9 weeks post-infection (i.e., 2 weeks post treatment)
No. of animals in each group; 8 mice. Values are presented as the mean±SD. Numbers in the parentheses indicate the percentage of reduction from infected group.
aSignificant difference from infected group at P<0.05; bSignificant difference from QN group at P<0.05.
Fig. 1Masson's trichrome stained liver sections of (A) S. mansoni-infected untreated mice showing irregularly outlined large fibrocellular granuloma formed of a central egg (with a living miracidium; arrow), surrounded mainly by lymphocytes, eosinophils, and extensive collagen depositions as concentric collagen fibers. (B) PZQ-treated group showing medium circumscribed fibrocellular granuloma (arrow) with eggs starting degeneration. (C, D) QN and KTZ+QN-treated groups, respectively, showing the smallest size and well-demarcated fibrocellular granuloma, formed of central degenerated egg (D; arrow), surrounded by lymphocytes, eosinophils, neutrophils, scattered macrophages, and fewer collagen depositions (C; arrow). (E, F) HF and KTZ+HF-treated groups, respectively, showing small fibrocellular granuloma formed of central degenerated egg (E; arrow), surrounded mainly by lymphocytes, eosinophils, neutrophils, and few concentric collagen fibers (F; arrow) (×200).
Effect of QN or HF alone and in addition to KTZ on liver antioxidant capacity, CYP450 and CYT b5 activities and hepatic function in S. mansoni-infected mice 9 weeks post-infection (i.e., 2 weeks post treatment)
Units: GSH, µmole/g liver; SOD, µmole/min/g liver; MDA, nmole/g liver; CYP450 and CYT b5, nmole/mg protein; ALT, U/L; Albumin, g/100 ml.
No. of animals in each group; 8 mice. Values are presented as the mean±SD.
aSignificant difference from uninfected group at P<0.05; bSignificant difference from QN group at P<0.05; cSignificant difference from HF group at P<0.05.
Fig. 2Effect of QN or HF alone and in addition to KTZ on percent inhibitions in hepatic CYP450 and CYT b5 relative to uninfected group in S. mansoni-infected mice at week 9 PI (i.e., week 2 post treatment). No. of animals in each group; 8 mice. Values are presented as the mean±SD. aSignificant difference from uninfected group at P<0.05. bSignificant difference from QN group at P<0.05. cSignificant difference from HF group at P<0.05.