4.5 Article

Differential appearance of placentomes and expression of prostaglandin H synthase type 2 in placentome subtypes after betamethasone treatment of sheep late in gestation

期刊

PLACENTA
卷 32, 期 4, 页码 295-303

出版社

W B SAUNDERS CO LTD
DOI: 10.1016/j.placenta.2011.01.012

关键词

Glucocorticoids; Betamethasone; Placenta; Placentomes; Prostaglandin H synthase; PGHS-2

资金

  1. Raine Medical Research Foundation [74301003]
  2. NHMRC [139026, 303261, 254502]
  3. Canadian Institutes of Health Research

向作者/读者索取更多资源

Inappropriate fetal exposure to maternal glucocorticoid (GC) has been proposed as a mechanism for fetal programming where the effects of GC may be mediated by the placenta. However, the consequences of maternal GC on placental morphology and enzyme expression are unclear. Objectives: We used betamethasone (BET) to determine effects on placentome subtype distribution and expression of prostaglandin H synthase type 2 (PGHS-2) enzyme. Methods: Pregnant sheep carrying male fetuses were randomized to receive injections of saline (n = 30) or one (104 days of gestation, (dG); n = 6), two (104, 111 dG; n = 6) or three (104, 111, 118 dG; n = 11) doses of BET (0.5 mg/kg). Placental tissue was collected prior to (75, 84,101 dG), during (109, 116 dG) and after BET (122, 132, 146 dG). Results: Total number of placentomes was not different between gestational ages. A- and B-subtypes were most affected by prenatal BET exposure; numbers of A-subtypes were increased and numbers of B-subtypes were decreased compared to controls at 116 dG. At term numbers of A-subtypes were lower after BET, but the weight range distribution was similar to controls. In controls, placental PGHS-2 protein levels increased with gestational age and PGHS-2 localized primarily to uninuclear trophoblast cells. After BET, PGHS-2 protein in C-subtypes at term was significantly increased compared to A-subtypes. Conclusions: Maternal BET treatment in late gestation affects the proportions of placentome subtypes and their differential expression of PGHS-2. Our data do not support previous hypotheses that A-subtypes develop into B-, C- and D-subtypes over the course of gestation. (C) 2011 Elsevier Ltd. All rights reserved.

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