Steroid Receptor Coactivator-1 Is Not Required for Androgen-Mediated Sexual Differentiation of Spinal Motoneurons

Monks, D. Ashley; Xu, Jianming; O’Malley, Bert W.; Jordan, Cynthia L.

doi:10.1159/000071705

Cited by 17 publications

(14 citation statements)

References 35 publications

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“…Similar observations have been made in white-footed mice (Forger and Breedlove, 1987), gerbils (Ulibarri et al, 1995), and several strains of Mus musculus (Wee and Clemens, 1987;Park et al, 2002;Monks et al, 2003;Zuloago et al, 2007). Larger somata likely reflect differences in electrophysiological properties, protein synthesis, and more robust dendritic organization, all of which are androgen sensitive in SNB motoneurons (see below).…”

Section: Snb Soma Size Effects Of Androgens During Development and Insupporting

confidence: 74%

“…Although SNB motoneurons express several steroid receptor coactivators (SRC-1, SCR-2, CBP, p300, cJUN), most other lumbar motoneurons, including those that do not respond morphologically to changes in androgen, also do (O'Bryant and Jordan, 2005). In addition, soma size of SNB motoneurons in SRC-1 knockout mice does not differ from that of wild-type controls (Monks et al, 2003). Thus, at this point, the molecular basis of the unusual androgen responsiveness of SNB motoneurons is not clear.…”

Section: Molecular Mechanismsmentioning

confidence: 99%

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The spinal nucleus of the bulbocavernosus: Firsts in androgen-dependent neural sex differences

Sengelaub

Forger

2008

Hormones and Behavior

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Cell number in the spinal nucleus of the bulbocavernosus (SNB) of rats was the first neural sex difference shown to differentiate under the control of androgens, acting via classical intracellular androgen receptors. SNB motoneurons reside in the lumbar spinal cord and innervate striated muscles involved in copulation, including the bulbocavernosus (BC) and levator ani (LA). SNB cells are much larger and more numerous in males than in females, and the BC/LA target muscles are reduced or absent in females. The relative simplicity of this neuromuscular system has allowed for considerable progress in pinpointing sites of hormone action, and identifying the cellular bases for androgenic effects. It is now clear that androgens act at virtually every level of the SNB system, in development and throughout adult life. In this review we focus on effects of androgens on developmental cell death of SNB motoneurons and BC/LA muscles; the establishment and maintenance of SNB motoneuron soma size and dendritic length; BC/LA muscle morphology and physiology; and behaviors controlled by the SNB system. We also describe new data on neurotherapeutic effects of androgens on SNB motoneurons after injury in adulthood.

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Section: Snb Soma Size Effects Of Androgens During Development and Insupporting

confidence: 74%

Section: Molecular Mechanismsmentioning

confidence: 99%

The spinal nucleus of the bulbocavernosus: Firsts in androgen-dependent neural sex differences

Sengelaub

Forger

2008

Hormones and Behavior

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“…Another study, however, demonstrated a profound inhibition of lordosis in female rats treated with SRC-1 antisense (Apostolakis et al, 2002). Studies of SRC-1 knock-out mice also found no effect on the development of the androgen-dependent motoneurons within the spinal nucleus of the bulbocavernosus (Monks et al, 2003), suggesting that this cofactor may not be important for androgendependent neuroendocrine processes. The present study clearly indicates that SRC-1 alone is important for the activational effects of testosterone on many aspects of male-typical sexual behaviors (Figs.…”

Section: Discussionmentioning

confidence: 97%

Inhibition of Steroid Receptor Coactivator-1 Blocks Estrogen and Androgen Action on Male Sex Behavior and Associated Brain Plasticity

Charlier¹,

Ball²,

Balthazart³

2005

J. Neurosci.

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“…Coincident with receptivity is a period of time when females exhibit a series of 'courtship' behaviors that foster behavioral interactions with the males and facilitate the electrophysiological properties of the neurons in the female hypothalamus. It is likely that these behaviors, while not reflex, are due to hormonal modulation of the serial neurocircuitry via ER (Pfaff & Schwartz-Giblin 1998), inducible PR (Monks et al 2001), and at least SRC-1 (Monks et al 2003). To verify this, the incidence of proceptive behaviors by the females was quantified.…”

Section: Receptivity Scorementioning

confidence: 99%

Hypothalamic progesterone receptor-A mediates gonadotropin surges, self priming and receptivity in estrogen-primed female mice

White

Sheffer²,

Teeter³

et al. 2007

Journal of Molecular Endocrinology

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Ovarian progesterone (Prog) is an essential steroid hormone for the secretion of GnRH and reproductive behavior. It exerts primary effects through the progesterone receptor (PR). When analyzed separately in vitro, PR isoforms (PR-A, PR-B) display striking differences in transcriptional activity. The present study was undertaken to determine the in vivo impact of each isoform on hypothalamic function in female mice with ablation of a single isoform, either PR-A or PR-B. To this end, we used single-cell RNA analyses, reverse transcriptase real-time (q)PCR mRNA analyses of punched-out tissue, immunohistochemistry, and reproductive behavior. We provide evidence for the requirement of PR-A in individual ventrolateral ventromedial nucleus (vlVMN) neurons for Prog-facilitated proceptive and receptive behaviors in estrogen benzoate (EB)-primed females and the reciprocal male interactions. We clarify histological and molecular mechanisms of PR isoform activity by showing that (1) PR-A is predominant in individual vlVMN neurons controlling female lordosis circuitry, whilst (2) PR-B is predominant in those VMN subdivisions that provide for amplification of PR-A activity. We go on to demonstrate that PR-A is dominant in the anteroventral periventricular nucleus but not the arcuate nucleus that feed fibers into and around the VMN. In the medial preoptic area, high levels of GnRH RNA in EB-primed PR-A-expressing mice were seen coincident with increased plasma LH levels. Two consecutive GnRH pulses enhanced LH only in primed PR-A-expressing females. In all, the findings are consistent with the hypothesis that hypothalamic PR-A-mediated genomic activities result in reproductive behavior coordinated with ovulation.

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Steroid Receptor Coactivator-1 Is Not Required for Androgen-Mediated Sexual Differentiation of Spinal Motoneurons

Cited by 17 publications

References 35 publications

The spinal nucleus of the bulbocavernosus: Firsts in androgen-dependent neural sex differences

The spinal nucleus of the bulbocavernosus: Firsts in androgen-dependent neural sex differences

Inhibition of Steroid Receptor Coactivator-1 Blocks Estrogen and Androgen Action on Male Sex Behavior and Associated Brain Plasticity

Hypothalamic progesterone receptor-A mediates gonadotropin surges, self priming and receptivity in estrogen-primed female mice

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