Literature DB >> 19406239

Assisted reproduction technologies impair placental steroid metabolism.

Abby C Collier1, Shogo J Miyagi, Yasuhiro Yamauchi, Monika A Ward.   

Abstract

The placenta plays a vital role in pregnancy by facilitating steroid passage from maternal to fetal circulation and/or direct production of hormones. Using a murine model, we demonstrated the differences in placental steroid metabolism between pregnancies conceived naturally and with assisted reproduction technologies (ART): in vitro fertilization (IVF) and intracytoplasmic sperm injection (ICSI). While the ovarian steroid production was similar (estrone, 17beta-estradiol) or higher (estriol) in ART pregnancies compared to mating, the levels of placental estriol were significantly lower in ART group. Placentas from ART had significantly higher activities of the steroid metabolizing enzymes UDP-glucuronosyltransferase (UGT) and sulfotransferase (SULT), which in ICSI were also coupled with decreased activity of the steroid regenerating enzymes beta-glucuronidase (beta-G) and aryl sulfatase (AS). Levels of steroid metabolites androstane-3alpha-17beta-diol glucuronide and dehydroepiandrosterone sulfate were higher in fetal compared to maternal blood in ART, but not in mating. This study demonstrates that in murine ART pregnancies, higher metabolism and clearance of steroids by the placenta may seriously affect the passage of essential hormones to the fetus. If a similar phenomenon exists in humans, this could provide a plausible explanation for obstetric and neonatal complications associated with ART, including the higher incidence of low birth weight babies.

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Year:  2009        PMID: 19406239      PMCID: PMC2702461          DOI: 10.1016/j.jsbmb.2009.04.005

Source DB:  PubMed          Journal:  J Steroid Biochem Mol Biol        ISSN: 0960-0760            Impact factor:   4.292


  43 in total

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Authors:  R I Silver; R Rodriguez; T S Chang; J P Gearhart
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Journal:  Pediatr Pathol       Date:  1993 Jul-Aug

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  26 in total

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2.  Placental inflammation and oxidative stress in the mouse model of assisted reproduction.

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3.  Single blastomere removal from murine embryos is associated with activation of matrix metalloproteinases and Janus kinase/signal transducers and activators of transcription pathways of placental inflammation.

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4.  Effect of the method of conception and embryo transfer procedure on mid-gestation placenta and fetal development in an IVF mouse model.

Authors:  L Delle Piane; W Lin; X Liu; A Donjacour; P Minasi; A Revelli; E Maltepe; P F Rinaudo
Journal:  Hum Reprod       Date:  2010-06-24       Impact factor: 6.918

5.  Upregulation of Ugt1a genes in placentas and fetal livers in a murine model of assisted reproduction.

Authors:  A C Collier; K A Milam; L R A Rougée; A Sugawara; Y Yamauchi; M A Ward
Journal:  Placenta       Date:  2011-11-25       Impact factor: 3.481

6.  Assisted reproductive technologies induce temporally specific placental defects and the preeclampsia risk marker sFLT1 in mouse.

Authors:  Lisa A Vrooman; Eric A Rhon-Calderon; Olivia Y Chao; Duy K Nguyen; Laren Narapareddy; Asha K Dahiya; Mary E Putt; Richard M Schultz; Marisa S Bartolomei
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Review 7.  Predisposing Factors to Abnormal First Trimester Placentation and the Impact on Fetal Outcomes.

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Journal:  Semin Reprod Med       Date:  2015-12-22       Impact factor: 1.303

8.  Assisted reproduction technologies alter steroid delivery to the mouse fetus during pregnancy.

Authors:  Jefferey M Raunig; Yasuhiro Yamauchi; Monika A Ward; Abby C Collier
Journal:  J Steroid Biochem Mol Biol       Date:  2010-12-28       Impact factor: 4.292

Review 9.  Morphologic and molecular changes in the placenta: what we can learn from environmental exposures.

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10.  Does rapid metabolism ensure negligible risk from bisphenol A?

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