Aflatoxin B1-induced DNA adduct formation and p53 mutations in CYP450- expressing human liver cell lines

Macé, Katherine; Aguilar, Fernando; Wang, Jia Sheng; Vautravers, P; Gómez-Lechón, Marı́a José; Gonzalez, Frank J.; Groopman, John D.; Harris, Curtis C.; Pfeifer, Andréa

doi:10.1093/carcin/18.7.1291

Cited by 186 publications

(118 citation statements)

References 10 publications

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“…In vitro studies exposing human liver cell lines to AFB 1 presented the same 249 ser mutational pattern of TP53 (Aguilar et al, 1993;Mace et al, 1997), as it has been reported in the epidemiological studies ( Figure 1c). There are at least two possible explanations for these findings.…”

Section: Aflatoxin Bsupporting

confidence: 77%

TP53 mutations and hepatocellular carcinoma: insights into the etiology and pathogenesis of liver cancer

et al. 2007

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Section: Aflatoxin Bsupporting

confidence: 77%

TP53 mutations and hepatocellular carcinoma: insights into the etiology and pathogenesis of liver cancer

et al. 2007

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“…THLE cells, obtained by transfection of the simian virus 40 large tumor antigen gene into primary hepatocytes (Pfeifer et al, 1995), did not express several important P450 isoenzymes, but clones expressing CYP3A4 (T5-3A4) or CYP2D6 (T5-2D6) were produced by subsequent transfection (Mace et al, 1997). Cell-culturing details are presented elsewhere (Molden et al, 2000).…”

Section: Methodsmentioning

confidence: 99%

Desacetyl-Diltiazem Displays Severalfold Higher Affinity to CYP2D6 Compared with CYP3A4

Molden

Åsberg²,

Christensen³

2002

Drug Metab Dispos

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This paper is available online at http://dmd.aspetjournals.org ABSTRACT:It has earlier been shown that the isoenzymes CYP2D6 and CYP3A4 are involved in O-and N-demethylation of diltiazem (DTZ), respectively. Apparently, CYP3A4 plays a more prominent role than CYP2D6 in the overall metabolism of DTZ. However, previous observations indicate that the opposite might be true for the pharmacologically active metabolite desacetyl-DTZ (M1). Thus, the aim of the present in vitro investigation was to study the relative affinity of M1 to CYP2D6 and CYP3A4. Immortalized human liver epithelial cells transfected with either CYP2D6 or CYP3A4 were used as a model system, and the presence of M1 and its metabolites in the cell culture medium was analyzed by high-performance liquid chromatography/UV detection both before and following 90 min of incubation. The estimated K m value for the CYP2D6-mediated Odemethylation of M1 was approximately 5 M. In comparison, the affinity of M1 to CYP3A4 (N-demethylation) was about 100 times lower (K m , Ϸ540 M) than to CYP2D6. These in vitro data suggest that M1 metabolism via CYP2D6, in contrast to the parent drug, probably is the preferred pathway in vivo. Metabolism mediated through CYP2D6 is associated with a substantial interindividual variability, and since M1 expresses pharmacological activity, individual CYP2D6 metabolic capacity might be an aspect to consider when using DTZ.

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“…These compounds are immunosuppressive, carcinogenic, teratogenic and mutagenic, and acute exposure to high levels of aflatoxin leads to aflatoxicosis, which can result in rapid death from liver failure. Symptoms of acute aflatoxicosis include, but are not limited to, swollen stomach, fatigue, swollen legs, and eyes turning yellowish [11,12]. In 2004, during the worst known outbreak of aflatoxicosis in Kenya, 317 cases were reported of which 125 died [13].…”

Section: Introductionmentioning

confidence: 99%

Aflatoxin variations in maize flour and grains collected from various regions of Kenya

Nduti¹

2017

AJFAND

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In Kenya, maize remains an important staple food in every household. Unfortunately, the fungus Aspergillus flavus can infect the maize and produce aflatoxins. While government efforts to remove contaminated maize from circulation are well intentioned, there remain concerns that consumers are still being inadvertently exposed to aflatoxin. The aim of this study was to sample maize in different parts of Kenya and determine if consumers were inadvertently being chronically exposed to aflatoxins. Seventy-five maize samples and 27 samples of maize flour from three regions of Kenya (Nairobi, Eastern and Western) were analysed using an ELISA assay followed by microtiter plate reader (Neogen model) where the optical density of each microwell was read using a 450nm filter. There was a significant difference in aflatoxin levels in maize grains between the three regions and five stores (P<0.05). Samples from Eastern Kenya had the highest contamination at 22.54±4.94 ppb, while those from Nairobi had the lowest (7.92±1.57 ppb). There was no significant difference in the total aflatoxin in maize flours from Nairobi, Western and Eastern regions (P>0.05) at 95% confidence interval. Aflatoxin in maize flours were slightly above international upper limit of 5ppb but all the results were lower than the Kenya standard whose upper limit is 10ppb, indicating good manufacturing practices (GMP) by the millers. Samples of maize flours from Eastern Kenya had the highest aflatoxins concentrations at 6.98± 0.53 ppb. In summary, the study found aflatoxin contamination in maize grains especially in Eastern Kenya. The study concluded that measures put in place by government agencies for millers appear to be working. However, samples of maize grains showed variation among the regions and between stores, perhaps due to storage practices, with some levels far exceeding health limits. Due to higher levels of aflatoxin contamination in maize grains in relation to maize flours, the government and relevant stakeholders need to establish further measures to protect consumers.

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Aflatoxin B1-induced DNA adduct formation and p53 mutations in CYP450- expressing human liver cell lines

Cited by 186 publications

References 10 publications

TP53 mutations and hepatocellular carcinoma: insights into the etiology and pathogenesis of liver cancer

TP53 mutations and hepatocellular carcinoma: insights into the etiology and pathogenesis of liver cancer

Desacetyl-Diltiazem Displays Severalfold Higher Affinity to CYP2D6 Compared with CYP3A4

Aflatoxin variations in maize flour and grains collected from various regions of Kenya

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