4.4 Article

Effects of androgen and leptin on behavioral and cellular responses in female rats

Journal

HORMONES AND BEHAVIOR
Volume 60, Issue 4, Pages 427-438

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.yhbeh.2011.07.012

Keywords

Dihydrotestosterone; Leptin; Brain; Adipose tissue; Behavior; Anxiety; Depression; Polycystic ovary syndrome

Funding

  1. Swedish Medical Research Council [2008-72VP-15445-01A, 5859]
  2. Novo Nordisk Foundation
  3. Wilhelm and Martina Lundgrens's Science Fund
  4. Adlerbert Research Foundation
  5. Swedish federal government under the LUA/ALF [ALFFGBG-10984]
  6. Fredrik and Ingrid Thurings Foundation
  7. Goteborgs Lakaresallskap
  8. Hjalmar Svensson Foundation
  9. Anna Cederbergs Foundation
  10. Emil and Maria Palm Foundation
  11. Tore Nilson Foundation
  12. Chinese Special Fund for Postdoc [200801170]
  13. National Natural Science Foundation of China [81001544/H2718]
  14. Swedish Institute
  15. China Scholarship Council
  16. Center for Mouse Physiology and Bio-Imaging (University of Gothenburg)

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The causes of anxiety and depression in women with polycystic ovary syndrome (PCOS) remain elusive. To identify steps linking androgen signaling to the regulation of affective symptoms in vivo, we compared behavioral responses in female rats continuously exposed to DHT from puberty (a model of DHT-induced PCOS) and in rats exposed to DHT for 1 week. Continuous and 1 week of DHT exposure resulted in a general decrease in locomotor activity and time spent on the open arms in the elevated plus maze, indicating anxiety-like behavior. Rats with DHT-induced PCOS have increases in adiposity and circulating leptin levels accompanied by leptin resistance. One week of DHT exposure decreased androgen receptor (AR) expression in the hypothalamus and leptin synthesis and function in adipocytes; it also inhibited signal transducer and activator of transcription 3 (STAT3) and attenuated leptin activity by increasing levels of soluble leptin receptor, a leptin-binding protein, in the hypothalamus. This may affect the androgen-induced anxiety-related behavior in female rats. In conclusion, our results highlight the central role of androgens in behavioral function in female rats and suggest that androgens directly regulate the AR by decreasing its hypothalamic expression. Androgens also increase leptin synthesis in adipocytes, which drives central leptin signaling, and may regulate anxiety-related behaviors. Elucidating mechanisms by which androgens modulate female anxiety-like behavior may uncover useful approaches for treating women with PCOS who have symptoms of anxiety. (C) 2011 Elsevier Inc. All rights reserved.

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