Awardee OrganizationUNIVERSITY OF MICHIGAN AT ANN ARBOR
Description
Abstract Text
Future studies proposed in this application will continue to explore
hormonal abnormalities in depression, with a shift in focus from solely
HPA axis hormones to include interactions between the gonadal hormone axis
and the stress axis. Depression is a disorder with a strong predilection
for women. Abnormalities of several hormonal axes particularly the adrenal
(stress) and thyroid axes have been well documented in depressed women,
but few studies have explored the hypothalamic pituitary gonadal (HPG)
axis. The occurrence of sex bias in the expression of depressive illness
after the onset of puberty, as well as anecdotal studies suggesting an
association between mood and cyclic gonadal steroid changes suggest that
gonadal axis hormones may modulate the onset and course of depression.
Hormones of the hypothalamic pituitary adrenal (HPA) axis have been
demonstrated to affect the hypothalamic pituitary gonadal axis,
particularly the secretion of gonadotropin releasing hormone (GnRH) from
the hypothalamus. Hypothalamic amenorrhea, exercise induced amenorrhea and
anorexia nervosa all demonstrate activation of the HPA axis accompanying
the abnormalities in GnRH and LH secretion. This suggests that activation
of the HPA axis is closely linked to abnormal GnRH secretion in humans.
This project proposes to study the interactions between these two hormonal
axes (stress and gonadal) to determine if depression in women is
accompanied by abnormalities in reproductive axis hormones and if
abnormalities in the reproductive axis are linked to abnormalities in the
HPA axis, or if the two abnormalities can co-exist independently. To
characterize baseline secretion in these two axes,l2 hour studies using 3
minute sampling will be conducted in depressed women to examine pulsatile
secretion of the gonadal hormones (LH, FSH, estradiol and progesterone) as
well as pulsatile secretion of the stress axis hormones (ACTH and
cortisol). These data will be compared with data from control women
matched for age and menstrual cycle day. In depressed women pulse
frequency and amplitude of LH secretion will each be examined, as well as
frequency and amplitude of ACTH and cortisol pulses. GnRH secretion, as
assessed by LH secretion in the periphery, appears to be the most
sensitive index of disruptions in HPG axis secretion, but gonadal steroid
hormones will also be evaluated. HPA axis pulsatility data will determine
if secretory drive in depressed women increases in the zenith and nadir of
the circadian rhythm, and if the onset of circadian driven secretory
episodes shift in depressed women. In normal women, the influence of
gonadal axis hormones on HPA axis function will be explored by comparing
the two axes and the response to dexamethasone at different phases of the
menstrual cycle in a subgroup of the control women. In rats, we will
examine the effect of ovariectomy and replacement with gonadal steroids on
the negative feedback effects of exogenous glucocorticoids at multiple
levels of the HPA axis as well as the effects on stress.
No Sub Projects information available for 2K02MH000427-11
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