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Toxicity of bisphenol A (BPA) on urchin embryo gene expression and
morphology
Ivana Bošnjak, PhDLaboratory for Biology and Molecular GeneticsFaculty of Food Technology and BiotechnologyUniversity of Zagreb, Croatia
2nd International Symposium “VERA JOHANIDES”Zagreb, Croatia, May 10-11 2013
Bisphenol A (BPA)
1891: Chemical synthesis of BPA in the laboratory (A. Dianin, Russia)1953: Start of BPA global production polycarbonate polymers and epoxy resins
2011: 5.5 million metric tons per year (Greiner et al., 2007)
2015: 7 million metric tons per year (China Chemical Industry News 2005)BPA plastic:
•Cheap, useful, tough, resistible, transparent….….
IUPAC: 4,4'-(propane-2,2-diyl)diphenol
Resin identification code
Toxicity of BPA to aquatic biota• Reported EC50 and LC50 values: 1 – 10 mg/L [4.4 –
43.8 µM]
Flint et al., 2012 Journal of Environmental Management 104: 19-34
“moderately toxic” and “toxic” to aquatic biota[European Commission & United States Environmental Protection Agency
(US EPA)]
! Harmful even at environmentally relevant concentrations:
12 µg/L or lower [52.6 nM or lower]BPA toxicity studies: endocrine-related measurement endpoints- e.g. enlarged sex glands, oviduct deformities, increased fecundity, additional female organs, development arrest…
AIMs:
Paracentrotus lividus: 2-cell pluteus
1. Real time quantitative PCR (qPCR) measurement:
2. Insight of ultramorphological changes of treated embryos by:A. transmission electron microscopy (TEM)B. scanning electron microscopy (SEM)
BPA exposure
Cellular mechanism Protein Target gene expressions
A. multixenobitoic resistance (MXR) mechanismchemical defensome
P-glycoprotein/P-gp abcb1
B. endocrine disruption orphan Steroid Hormone Receptor/SHR2 shr2
C. cell-cycle regulation Cyclin BCdk (Cyclin-dependent kinase)
cyccdk
ABC (ATP-Binding Cassette) transportersuse ATP for active transport of toxic compound across cell membrane (“efflux transporters”)P-glycoprotein/P-gp ABCB1 member of ABCB subfamily (abcb1 gene)
! high expression throughout sea urchin embryo development [Hamdoun et al., 2004; Shipp et al., 2012]
MXR mechanism Protection from vast variety of natural and anthropogenic toxic compounds present in aquatic environment. [Kurelec, 1992]
FIRST LINE OF
DEFENSE
0' 25' 30'
Fertilization
egg
Embryonic development (T = 16 °C)Time Post
Fertilization (PF):
Active MXR mechanism [Hamdoun et al.,
2004]
ADD BPA
1h35'
spermFertilization
envelop
96h
EXPERIMENTAL APPROACH:
Sample collection for:qPCR
TEM & SEM
100 nM [22.8 µg/L]
4 µM [910 µg/L]
100 nM [22.8 µg/L]
4 µM [910 µg/L]
EC50 = 2.5 µM [570 µg/L]
Toxicity of BPA on first cell division:
means ± SDs of 5 batches of embryos
qPCR results:
abcb1 (P-glycoprotein)
cyc (Cyclin B) shr2 (Shr2)
cdk (Cdk)
**
**
three independent RNA isolations of each egg culture normalised to ubiquitin mRNA bars represent means ±SD; * p < 0.05
5.3-fold
6.2-fold
2.7-fold 2.2 -
fold
1h 35’96h
Endocrine disruption
Cell cycle regulation
MXR mechanism
4 μM BPA2-cell stage
control
4 μM BPApluteus stage
control
Conclusions: EC50 = 2.5 µM BPA [570 µg/L]
cell-cycle arrest or delay
Target genes expression (qPCR): 100 nM & 4 µM BPA significant upregulation of abcb1
gene (P-gp expression) = involvement of MXR mechanism!
4 µM BPA = upregulation of other target genes: shr2, cyc and cdk
SEM & TEM results: higher sublethal concentration of BPA (4 µM) induces disorder in karyokinesis and developmental retardation
Endocrine disruption
Cell cycle regulation
Acknowledgements:
1 Ivona Mladineo, PhD
2Maria Ina Arnone, PhD2Rossella Annunziata , PhD
2 Marco Borra, PhD
2 Giovanna Benvenuto, PhD2 Davide Ciaramiello, facility
technician
1Institute of Oceanography and Fisheries, Split, Croatia
2Stazione Zoologica Anton Dohrn, Napoli, Italy
Endocrine disruptor:•Cause hormone chaos•Metabolism disorder, immunity disorder, affects growth and development during childhood, affects behavior, nerve and cardiovascular system disorder, cause breast cancer and prostate cancer, thyroid gland disorder…..
2008: Canada2009: USA2011: EuropeEmbargo for BPA in baby bottles!
BPA is toxic!