Pharmacokinetics of propylthio-benzimidazole anthelmintics : modulation of liver biotransformation in sheep and cattle

Lanusse, Carlos Edmundo

January 1991

The aim of this research was to determine the influence of route of administration, drug formulation and modified-liver metabolism on the pharmacokinetic and metabolic patterns of benzimidazole anthelmintics in ruminants. Both route of administration and formulation dramatically affected the bioconversion of netobimin (NTB) pro-drug, N-methoxycarbonyl-N$ sp prime$-(2-nitro-5-propylphenylthio)-${ rm N} sp{ prime prime}$-(2-ethyl sulphonic acid) guanidine, and the bioavailability and disposition kinetics of its active albendazole (ABZ) metabolites in both sheep and cattle. The efficacy of NTB conversion by the gastrointestinal (GI) microflora, was markedly lower after subcutaneous (SC) administration of NTB pro-drug compared with enteral administrations in both species. Although trisamine and zwitterion formulations of NTB were bioequivalent after SC treatment, the zwitterion suspension was two-fold more bioavailable in terms of ABZ metabolites, after oral administration to cattle. ABZ sulphoxide (ABZSO) and ABZ sulphone (ABZSO$ sb2$), the main metabolites found in plasma, were reversibly exchanged between plasma and GI compartments and concentrated in the abomasum. ABZ, ABZSO and ABZSO$ sb2$ were detected in the GI tract for 72 h post-NTB administration to cattle. In vitro, ABZ was oxidized into ABZSO and ABZSO$ sb2$ by liver microsomes and ruminal and ileal fluids. However, only ABZSO was reduced (back to ABZ) by these GI fluids. The rate of ABZ sulphoxidation by liver microsomes was significantly lower in cattle compared to sheep. However, while the oxidizing activity was greater in GI fluids of cattle, the reducing activity was prevalent in those of sheep. This was consistent with the higher ABZSO$ sb2$/ABZSO ratio and the markedly faster disposition of both metabolites in cattle compared to sheep. The co-administration of NTB with different oxidation-impairing compounds, largely methimazole (MTZ), in both species, resulted in an increased bioavailability and/o

Benzimidazoles -- Pharmacokinetics.

Anthelmintics -- Pharmacokinetics.

Sheep -- Parasites -- Control.

Cattle -- Parasites -- Control.

Pharmacokinetics of propylthio-benzimidazole anthelmintics : modulation of liver biotransformation in sheep and cattle

Lanusse, Carlos Edmundo

January 1991

No description available.

Anthelmintics -- Pharmacokinetics.

Sheep -- Parasites -- Control.

Benzimidazoles -- Pharmacokinetics.

Cattle -- Parasites -- Control.

"The mode of action of Bacillus thuringiensis (Berliner) against the sheep louse, Bovicola ovis (Schrank)"

Hill, Catherine Alexandra.

January 1998

Bibliography: leaves 120-145. Reports Bt crystal protein toxicity to a phthirapteran species. Although Bt strain WB3516 may produce other unidentified toxins effective against B. ovis, the results provide strong evidence that the [delta]-endotoxin crystal proteins of strain WB3516 significantly contribute to the lousicidal toxicity of this strain.

Sheep lice

Sheep Parasites Control

Endotoxins Pathophysiology

Bacillus thuringiensis

Microbial insecticides

Pesticide resistance

"The mode of action of Bacillus thuringiensis (Berliner) against the sheep louse, Bovicola ovis (Schrank)" / by Catherine Alexandra Hill.

Hill, Catherine Alexandra

January 1998

Bibliography: leaves 120-145. / vii, 145, [43] leaves, [23] leaves of plates : ill. (some col.) ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Reports Bt crystal protein toxicity to a phthirapteran species. Although Bt strain WB3516 may produce other unidentified toxins effective against B. ovis, the results provide strong evidence that the [delta]-endotoxin crystal proteins of strain WB3516 significantly contribute to the lousicidal toxicity of this strain. / Thesis (Ph.D.)--University of Adelaide, Dept. of Crop Protection, 1998?

636.3/069/44324 21

Sheep lice.

Sheep Parasites Control.

Endotoxins Pathophysiology.

Bacillus thuringiensis.

Microbial insecticides.

Pesticide resistance.