Oncogenic and tumor suppressor pathways in subchronic aflatoxicosis in rats: Association with serum and urinary aflatoxin exposure biomarkers

In this study, the changes in oncogenic and tumor suppressor signaling pathways in liver and their association with serum and urinary biomarkers of aflatoxin exposure were evaluated in Wistar rats fed diets containing aflatoxin B-1 (AFB(1)) for 90 days. Rats were divided into four groups (n = 15 per group) and assigned to dietary treatments containing 0 (control), 50 (AFB50), 100 (AFB100) and 200 mu g AFB(1) kg(-1) diet (AFB200). Multiple preneoplastic foci of hepatocytes marked with glutathione-S-transferase-placental form (GST-P) were identified in AFB100 and AFB200 groups. Hepatocellular damage induced by AFB(1) resulted in overexpression of cyclin D1 and beta-catenin. The liver expression of retinoblastoma (Rb) and p27(Kip1) decreased in AFB100 and AFB200 groups, confirming the favorable conditions for neoplastic progression to hepatocellular carcinoma. All samples from rats fed AFB(1)-contaminated diets had quantifiable AFB(1)-lysine in serum or urinary AFM(1) and AFB(1)-N-7-guanine, with mean levels of 20.42-50.34 ng mL(-1), 5.31-37.68 and 39.15-126.37 ng mg(-1) creatinine, respectively. Positive correlations were found between AFB(1)-lysine, AFM(1) or AFB(1)-N-7-guanine and GST-P+, beta-catenin+ and cyclin D1+ hepatocytes, while Rb + cells negatively correlated with those AFB(1) exposure biomarkers. The pathways evaluated are critical molecular mechanisms of AFB(1)-induced hepatocarcinogenesis in rats. (AU)