Risk Assessment of Ochratoxin A in Food

Overview

Journal EFSA J

Date 2023 Aug 31

PMID 37649524

Authors

Dieter Schrenk

Laurent Bodin

James Kevin Chipman

Jesus Del Mazo

Bettina Grasl-Kraupp

Christer Hogstrand

Laurentius Ron Hoogenboom

Jean-Charles Leblanc

Carlo Stefano Nebbia

Elsa Nielsen

Evangelia Ntzani

Annette Petersen

Salomon Sand

Tanja Schwerdtle

Christiane Vleminckx

Heather Wallace

Jan Alexander

Chiara DallAsta

Angela Mally

Manfred Metzler

Marco Binaglia

Zsuzsanna Horvath

Hans Steinkellner

Margherita Bignami

Affiliations

Soon will be listed here.

Abstract

The European Commission asked EFSA to update their 2006 opinion on ochratoxin A (OTA) in food. OTA is produced by fungi of the genus and and found as a contaminant in various foods. OTA causes kidney toxicity in different animal species and kidney tumours in rodents. OTA is genotoxic both and ; however, the mechanisms of genotoxicity are unclear. Direct and indirect genotoxic and non-genotoxic modes of action might each contribute to tumour formation. Since recent studies have raised uncertainty regarding the mode of action for kidney carcinogenicity, it is inappropriate to establish a health-based guidance value (HBGV) and a margin of exposure (MOE) approach was applied. For the characterisation of non-neoplastic effects, a BMDL of 4.73 μg/kg body weight (bw) per day was calculated from kidney lesions observed in pigs. For characterisation of neoplastic effects, a BMDL of 14.5 μg/kg bw per day was calculated from kidney tumours seen in rats. The estimation of chronic dietary exposure resulted in mean and 95th percentile levels ranging from 0.6 to 17.8 and from 2.4 to 51.7 ng/kg bw per day, respectively. Median OTA exposures in breastfed infants ranged from 1.7 to 2.6 ng/kg bw per day, 95th percentile exposures from 5.6 to 8.5 ng/kg bw per day in average/high breast milk consuming infants, respectively. Comparison of exposures with the BMDL based on the non-neoplastic endpoint resulted in MOEs of more than 200 in most consumer groups, indicating a low health concern with the exception of MOEs for high consumers in the younger age groups, indicating a possible health concern. When compared with the BMDL based on the neoplastic endpoint, MOEs were lower than 10,000 for almost all exposure scenarios, including breastfed infants. This would indicate a possible health concern if genotoxicity is direct. Uncertainty in this assessment is high and risk may be overestimated.

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