| Literature DB >> 27133914 |
Celal Güven1, Fulya Dal2, Müfide Aydoğan Ahbab3, Eylem Taskin4, Süleyman Ahbab5, Suzan Adin Çinar6, Sema Sırma Ekmekçi7, Çağrı Güleç8, Neslihan Abacı7, Handan Akçakaya9.
Abstract
Phthalate plasticizers used in a wide range of common plastic products are released into the environment and may pose a risk of increased incidence of type 2 diabetes. In this work, we studied the effects of monoethyl phthalate (MEP), the metabolite of diethyl phthalate, exposure on 1.1B4 human pancreatic beta cells at low doses (1-1000 nM). We showed that MEP treatment induced proliferation in 1.1B4 cells. Also PCNA protein expression levels were increased related to proliferation induction. It has been noted that phthalates can exert estrogen mediated response by interacting with ER. In our study 24 h MEP treatment decreased ERα protein expression level conversely it increased the same protein expression level after 72 h treatment. Also MEP treatment decreased ERβ expression after 72 h at 1.1B4 cells. Our results further show that insulin content of 1.1B4 cells were increased with low dose MEP treatment. Along with our insulin content results, PDX- 1 expression levels were also increased at 1.1B4 cells with MEP treatment. These findings suggest that MEP acts as an estrogenic compound and PPARγ agonist at lower concentrations. Also it should be noted that PDX-1 may be a critical regulator of 1.1B4 cells treated with MEP.Entities:
Keywords: 1.1B4 cells; Diabetes; Mechanisms; Monoethyl phthalate; PDX-1; Toxicity
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Year: 2016 PMID: 27133914 DOI: 10.1016/j.fct.2016.04.023
Source DB: PubMed Journal: Food Chem Toxicol ISSN: 0278-6915 Impact factor: 6.023