However, these studies are not fully comparable due to difference

However, these studies are not fully comparable due to differences regarding doses and species and the time point when the modified diet was introduced. Further Ryan et al. housed their mice in cages made of polycarbonate and used water bottles also made of polycarbonate, which might have been sources of BPA contamination in the control groups masking subtle effects, though it was otherwise a very sound study. The above mentioned studies were carried out with rodents which are said to be poor models for BPA in humans due to different toxicokinetics. According to a study by Tominaga et al. using nonhuman primates; chimpanzees (Pantroglodytes verus) and cynomolgus monkeys (Macaca

fascicularis), there are differences also among different primate species. In rodents the BPA T½ is longer, primarily explained by enterohepatic

recirculation in rodents but not in primates. The conjugation Dabrafenib rate in the liver is faster in rodents than in primates, primarily explained by a higher hepatic blood flow-rate in rodents ( Tominaga et al., 2006). However, there seem to be no differences in the metabolites formed e.g. it is a question of rate and time and not in the fate of BPA. The calculated mean exposure in humans is well below the TDI, but there are still uncertainties about the exact sources of exposure. Further, based on the WHO report: “Joint FAO/WHO Expert Meeting to Review Toxicological and Health Aspects of Bisphenol A Summary Report” (http://www.who.int/foodsafety/chem/chemicals/BPA_Summary2010.pdf), the most sensitive individuals – newborn babies – are also the ones with highest exposure. R428 clinical trial According to this report the highest estimated exposure occurs in infants 0–6 months of age who are fed with liquid formula out of PC bottles: 2.4 μg/kg bw per day (mean) and 4.5 μg/kg bw per day (95th percentile), which is very close to the lowest dose used in the present study. In children, teenagers and adults the mean exposure was <0.01–0.40 μg/kg bw per day. Prenatal exposure to BPA has been shown to increase expression of

lipogenic Idoxuridine genes and adipocyte size in rodents (Marmugi et al., 2012 and Somm et al., 2009). Studies on isolated cells have shown BPA to induce production of proinflammatory cytokines, such as IL-6 and TNF-alpha (Yamashita et al., 2005), and to induce expression of adipogenic transcription factors (Phrakonkham et al., 2008), including PPAR-gamma activation (Kwintkiewicz et al., 2010). How these in vitro findings relate to the present finding of an increase in liver fat infiltration in combined exposure to fructose and BPA is not understood. The above-mentioned study by Marmugi et al. further suggests that exposure to low BPA doses may influence de novo fatty acid synthesis and thereby contributing to hepatic steatosis in mice (Marmugi et al., 2012). Interestingly, fructose has also been pointed out as a possible contributor to similar effects on the liver by its interaction with the Glut5 receptor (Lustig, 2010).

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