Diagnostic guidelines for ruminant toxicoses.

Management of poisoning is best accomplished when an accurate diagnosis is made and enhanced by attention to five major diagnostic criteria: history, clinical signs, clinical laboratory evaluation, lesions, and chemical analysis. Used properly, all of these factors allow for a better understanding of clinical poisoning. Although not all of these are possible for individual incidents, a systematic approach to support these criteria will bring a more useful assessment of risk and an accurate diagnosis.

Evaluation of XPC and prototypes on aflatoxin-challenged broilers.

Various products and prototypes were added to poultry diets during an aflatoxin challenge on growth and histological parameters. Male broiler chicks were randomly assigned to 8 treatment groups with 8 replicates/treatment and 3 birds/replicate. Treatments were as follows: 1) negative control containing no aflatoxin (NC); 2) positive control containing aflatoxin (PC); 3) 0.

Fumonisin B-glucose reaction products are less toxic when fed to swine.

The effects of fumonisin B-glucose reaction products in swine diets was examined. Pigs were fed diets containing 528 micromol of total fumonisin B/kg (FB), 528 micromol of total FB-glucose adducts/kg (FB-G, 122 micromol of unreacted FB/kg), or 0 micromol of total FB/kg for 15 days to test the efficacy of the FB-G reaction products in detoxifying FB. Weight gain in FB pigs was lower than in FB-G or controls, which was correlated with feed intake reduction in FB pigs.

Glucose reaction with fumonisin B1 partially reduces its toxicity in swine.

Acute and subacute intraperitoneal doses of fumonisin B(1) (FB(1)) were administered to test the efficacy of the FB(1)-glucose reaction products in detoxifying FB(1) in swine. In the acute study at 11 mumol of FB(1)/kg of body weight, five of six pigs administered FB(1) and four of six pigs administered FB(1)-glucose died from acute pulmonary edema. Analysis of weight gain, serum aspartate aminotransferase and gamma-glutamyltransferase, total cholesterol, and pathological evaluation did not provide evidence of protection against FB(1) toxicity by the FB(1)-glucose reaction products.