Social stress-induced bladder dysfunction: potential role of corticotropin-releasing factor

Wood, Susan K.; Baez, Madelyn A.; Bhatnagar, Seema; Valentino, Rita J.

doi:10.1152/ajpregu.91013.2008

Cited by 109 publications

(143 citation statements)

References 52 publications

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“…Thus, discrete chemical activation of Barrington's nucleus neurons elicited bladder contractions that were increased by intrathecal administration of a CRF antagonist, and conversely, decreased by intrathecal CRF. An inhibitory role for CRF in Barrington's nucleus regulation of the bladder is consistent with reports that social stress in rodents leads to urinary retention, abnormal urodynamics, and bladder hypertrophy (4,6,12,13,45), and this is associated with increased expression of CRF in Barrington's nucleus neurons (45). These findings suggest that pharmacological manipulation of CRF may improve bladder dysfunctions associated with stress or other conditions.…”

supporting

confidence: 88%

“…Brain sections collected on slides were postfixed by incubation in 10% formalin and processed to quantify CRF mRNA, as previously described (42). Sections containing Barrington's nucleus were hybridized with an antisense riboprobe to CRF mRNA (Dr. Audrey F. Seasholtz, University of Michigan) and coated with Kodak NTB2 liquid autoradiographic emulsion (7-day exposure at 4°C) identical to that previously published (45). The tissue was lightly stained with cresyl violet, and bright-field images were cap-tured and magnified using Open Lab software to identify cresyl violet-stained cells containing silver grains greater than 2-4 times background.…”

mentioning

confidence: 99%

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A corticotropin-releasing factor receptor antagonist improves urodynamic dysfunction produced by social stress or partial bladder outlet obstruction in male rats

Wood

McFadden

Griffin

et al. 2013

American Journal of Physiology-Regulatory, Integrative and Comp

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Wood SK, McFadden K, Griffin T, Wolfe JH, Zderic S, Valentino RJ. A corticotropin-releasing factor receptor antagonist improves urodynamic dysfunction produced by social stress or partial bladder outlet obstruction in male rats. Am J Physiol Regul Integr Comp Physiol 304: R940 -R950, 2013. First published April 3, 2013 doi:10.1152/ajpregu.00257.2012.-Barrington's nucleus, in the pons, regulates micturition through spinal projections to preganglionic parasympathetic neurons. The stress neuropeptide CRF is prominent in these projections and has an inhibitory influence. Social stress in rats causes urinary retention and abnormal urodynamics resembling those produced by partial bladder outlet obstruction (pBOO), and this is associated with CRF upregulation in Barrington's nucleus. Here, we examined the role of CRF in social stress-and pBOO-induced urodynamic dysfunction by assessing the ability of a CRF 1 receptor antagonist to alter these effects. Male rats exposed to repeated resident-intruder stress were administered vehicle or a CRF1 antagonist (NBI-30775) daily prior to the stress. Urodynamic function was recorded in the unanesthetized state 72 h after the final stress. NBI-30775 prevented the increased intermicturition interval, micturition volume, and bladder capacity produced by social stress, but not the increase in CRF expression in Barrington's nucleus neurons. The urinary dysfunction was also partly prevented by shRNA targeting of CRF in Barrington's nucleus, suggesting that stress-induced urinary dysfunction results, in part, from CRF upregulation in Barrington's nucleus and enhanced postsynaptic effects in the spinal cord. Finally, NBI-30775 improved urodynamic function of rats that had pBOO of 2-wk duration when administered daily during the second week but did not block the increase in CRF expression in Barrington's nucleus neurons. These findings implicate a role for Barrington's nucleus CRF in stress-and pBOO-induced urodynamic changes and suggest that CRF1 antagonists may be useful therapeutic agents for the treatment of urinary dysfunction. cystometry; resident-intruder; Barrington's nucleus; urinary BARRINGTON'S NUCLEUS IN THE pons regulates the descending limb of the micturition reflex through its axonal projections to preganglionic neurons of the lumbosacral spinal cord that provide the parasympathetic input to the detrusor muscle (21). Electrical and chemical stimulation of Barrington's nucleus elicits detrusor contraction, and conversely, lesions disrupt the micturition reflex (1,27,29). More recent anatomical and physiological evidence suggests that Barrington's nucleus plays a key role in coordinating central and visceral responses during micturition (39) (for review, see Ref. 41). In addition to its connections to the bladder, Barrington's nucleus neurons are transsynaptically linked to the distal colon and other pelvic viscera, suggesting a broader role for this nucleus in the regulation of pelvic visceral functions (23,24,33,40,44). Elucidating the function of neuromodulators expresse...

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confidence: 88%

mentioning

confidence: 99%

A corticotropin-releasing factor receptor antagonist improves urodynamic dysfunction produced by social stress or partial bladder outlet obstruction in male rats

Wood

McFadden

Griffin

et al. 2013

American Journal of Physiology-Regulatory, Integrative and Comp

Self Cite

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“…For example, rats exposed to various types of stress (water avoidance, intruder stress) exhibit symptoms of bladder dysfunction including increased micturition frequency as well as anxiety-like behavior (257,299). Furthermore, an exaggerated acoustic startle response has been demonstrated in both cats diagnosed with FIC as well as in BPS/IC patients (279,296).…”

Section: A Bladder Pain Syndromementioning

confidence: 99%

Urothelial Signaling

Birder

Andersson

2013

Physiological Reviews

399

362

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The urothelium, which lines the inner surface of the renal pelvis, the ureters, and the urinary bladder, not only forms a high-resistance barrier to ion, solute and water flux, and pathogens, but also functions as an integral part of a sensory web which receives, amplifies, and transmits information about its external milieu. Urothelial cells have the ability to sense changes in their extracellular environment, and respond to chemical, mechanical and thermal stimuli by releasing various factors such as ATP, nitric oxide, and acetylcholine. They express a variety of receptors and ion channels, including P2X3 purinergic receptors, nicotinic and muscarinic receptors, and TRP channels, which all have been implicated in urothelial-neuronal interactions, and involved in signals that via components in the underlying lamina propria, such as interstitial cells, can be amplified and conveyed to nerves, detrusor muscle cells, and ultimately the central nervous system. The specialized anatomy of the urothelium and underlying structures, and the possible communication mechanisms from urothelial cells to various cell types within the bladder wall are described. Changes in the urothelium/ lamina propria ("mucosa") produced by different bladder disorders are discussed, as well as the mucosa as a target for therapeutic interventions.

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“…Studies on molecular mechanisms through which CRH is stimulated in these areas lag behind compared to that of PVH. It has been shown that psychosocial stress increases CRH mRNA levels in the CeA (Hsu et al 1998, Kalin et al 1994 and laterodorsal (oval) subnucleus of BNST (Makino et al 1999) and in the Barrington's nucleus (Wood et al 2009). Although CRH mRNA is elevated in both of…”

Section: Regulation and Function Of Central (Extrahypophyseotropic) Crhmentioning

confidence: 99%

“…Expression of CRH mRNA in these neurons is upregulated in response to stress (Wood et al 2009), but not to ADX (Imaki et al 1991). Increase of CRH in Barrington's nucleus by social stress has been linked to stress-induced bladder disfunction (Wood et al 2009, Wood et al 2013.…”

Section: Regulation and Function Of Central (Extrahypophyseotropic) Crhmentioning

confidence: 99%

CRH: The link between hormonal-, metabolic- and behavioral responses to stress

Kovács

2013

Journal of Chemical Neuroanatomy

108

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Two major and mutually interconnected brain systems are recruited during stress reaction. One is the hypothalamic paraventricular nucleus (PVH) and the second is the extended amygdala. PVH governs the neuroendocrine stress response while CeA regulates most of the autonomic and behavioral stress reactions. The common neurohormonal mediator of these responses is the corticotropin-releasing hormone, CRH, which is expressed in both centers. CRH belongs to a larger family of neuropeptides that also includes urocortins 1, 2, and 3 all have different affinity towards the two types of CRHR receptors and have been implicated in regulation of stress and HPA axis activity. One functionally relevant aspect of CRH systems is their differential regulation by glucocorticoids. While corticosterone inhibits CRH transcription in the PVH, stress-induced glucocorticoids stimulate CRH expression in the extended amygdala. This review summarizes past and recent findings related to CRH gene regulation and its involvement in the neuroendocrine, autonomic and behavioral stress reaction.Key words: Corticotropin-releasing hormone, paraventricular nucleus, central amygdala, bed nucleus of stria terminalis, corticosterone, cAMP-response element.

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Social stress-induced bladder dysfunction: potential role of corticotropin-releasing factor

Cited by 109 publications

References 52 publications

A corticotropin-releasing factor receptor antagonist improves urodynamic dysfunction produced by social stress or partial bladder outlet obstruction in male rats

A corticotropin-releasing factor receptor antagonist improves urodynamic dysfunction produced by social stress or partial bladder outlet obstruction in male rats

Urothelial Signaling

CRH: The link between hormonal-, metabolic- and behavioral responses to stress

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