Elucidating the combined toxicity of aflatoxin B1 and fumonisin B1 on HepG2 cells based on respirometry and transcriptome analyses

Xiangrong Chen; Mohamed F. Abdallah; Charlotte Grootaert; Filip Van Nieuwerburgh; Andreja Rajkovic

doi:10.1101/2023.01.19.524737

Abstract

Aflatoxin B1 (AFB1) and fumonisin B1 (FB1) are two toxic mycotoxins widely found in food contaminants, and known for their hepatotoxicity in human. However, their combined toxicity still needs to be deeply investigated especially for their harmful effect. Therefore, the current work aimed at investigating the (combined) effect of AFB1 and FB1 on mitochondrial and glycolytic activity of HepG2 cell line, a well-recognized in vitro model system to study liver cell function. In our previous work, we studied the impact of a short term exposure to different doses of AFB1, FB1, and their binary mixture (MIX) on the bioenergetic status of HepG2 cells. Seahorse respirometry analysis revealed that the co-exposure, especially at high doses (8 µg/mL for AFB1 and 160 µg/mL for FB1), is more toxic as a result of more inhibition of all parameters of mitochondrial respiration. RNA transcriptome sequencing showed that the p53 signaling pathway, which is a major orchestrator of mitochondrial apoptosis, was differentially expressed. Moreover, the co-exposure has significantly downregulated Cx I, Cx II, Cx III, and Cx IV genes, which represent the onset of the suppressed mitochondrial respiration in HepG2 cells. It was found that FB1 is contributed more to the MIX effects than AFB1.⍰

Environmental Implication Aflatoxin B1 (AFB1) and fumonisin B1 (FB1) are two main mycotoxins that frequently (co-)contaminate maize and maize-based ingredients in several parts of the world. Both toxins are well-known for their hepatotoxicity in humans as the liver is their main target organ. However, the combined toxicity of AFB1 and FB1 still needs to be deeply investigated especially for their effect on cellular respiration. In this study, we proved that a binary mixture of AFB1 and FB1 is more toxic on mitochondrial respiration, and disrupted the p53 signaling pathway to induce apoptosis, which promised a novel insight of hazardous materials-induced hepatic damage.

Competing Interest Statement

The authors have declared no competing interest.

Abbreviations

AFB1: Aflatoxin B1
FB1: fumonisin B1
MIX: their binary mixture
CON: control
HepG2: human hepatocellular carcinoma
IARC: International Agency for Research on Cancer
ATP: adenosine triphosphate
ROS: reactive oxygen species
DMEM: Dulbecco’s modified Eagle’s medium
NEAA: non-essential amino acids
FBS: Fetal Bovine Serum
PBS: Phosphate buffer saline
MTT: tetrazolium salt
MMP: mitochondrial membrane potential
OXPHOS: oxidative phosphorylation
ECAR: extracellular acidification rate
OCR: oxygen consumption rate
DEGs: differentially expressed genes
FC: fold change
FDR: false discovery rate
GO: Gene Ontology
KEGG: Kyoto Encyclopedia of Genes and Genomes
ETC: electron transport chain
IMM: the inner mitochondrial membrane
AFBO: AFB1-exo28,9-epoxide
PPP: pentose phosphate pathway
G6P: glucose-6-phosphate
G6PD: glucose-6-phosphate dehydrogenase.

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