4.7 Article

Regulation of mRNA expression encoding chaperone and co-chaperone proteins of the glucocorticoid receptor in peripheral blood: association with depressive symptoms during pregnancy

期刊

PSYCHOLOGICAL MEDICINE
卷 42, 期 5, 页码 943-956

出版社

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S0033291711002121

关键词

Co-chaperone; gene expression; glucocorticoid receptor; peripartum depression; peripheral blood; steroid hormones

资金

  1. Specialized Center for Research [P50 MH 68036]
  2. Pfizer
  3. Doris Duke Charitable foundation
  4. Eli Lilly
  5. GSK
  6. Janssen
  7. Wyeth
  8. NARSAD
  9. NIH
  10. NIDA
  11. NIMH
  12. NINDS
  13. Roche
  14. Schering-Plough
  15. Behrens-Weise Foundation
  16. PharmaNeuroBoost
  17. [R21 MH076024-01]

向作者/读者索取更多资源

Background. Major depressive disorder during pregnancy associates with potentially detrimental consequences for mother and child. The current study examined peripheral blood gene expression as a potential biomarker for prenatal depressive symptoms. Method. Maternal RNA from whole blood, plasma and the Beck Depression Inventory were collected longitudinally from preconception through the third trimester of pregnancy in 106 women with a lifetime history of mood or anxiety disorders. The expression of 16 genes in whole blood involved in glucorticoid receptor (GR) signaling was assessed using real-time polymerase chain reaction. In parallel, plasma concentrations of progesterone, estradiol and cortisol were measured. Finally, we assessed ex vivo GR sensitivity in peripheral blood cells from a subset of 29 women. Results. mRNA expression of a number of GR-complex regulating genes was up-regulated over pregnancy. Women with depressive symptoms showed significantly smaller increases in mRNA expression of four of these genes - FKBP5, BAG1, NCOA1 and PPID. Ex vivo stimulation assays showed that GR sensitivity diminished with progression of pregnancy and increasing maternal depressive symptoms. Plasma concentrations of gonadal steroids and cortisol did not differ over pregnancy between women with and without clinically relevant depressive symptoms. Conclusions. The presence of prenatal depressive symptoms appears to be associated with altered regulation of GR sensitivity. Peripheral expression of GR co-chaperone genes may serve as a biomarker for risk of developing depressive symptoms during pregnancy. The presence of such biomarkers, if confirmed, could be utilized in treatment planning for women with a psychiatric history.

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