GABAergic contribution to rat bladder hyperactivity after middle cerebral artery occlusion

Kanie, Sayoko; Yokoyama, Osamu; Komatsu, Kazuto; Kodama, K.; Yotsuyanagi, Satoshi; Niikura, Susumu; Nagasaka, Yasuhiro; Miyamoto, Ken‐ichi; Namiki, Mikio

doi:10.1152/ajpregu.2000.279.4.r1230

Cited by 38 publications

(25 citation statements)

References 24 publications

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“…Various cortical lesions are thought to lead to these symptoms due to damage to the cerebral inhibitory centers leading to uninhibited detrusor contractions [26]. Other cerebral infarction-induced factors that may lead to OAB include alterations in N-methyl-D-aspartic acid glutamatergic mechanisms [27], dopamine D2 receptor excitatory mechanisms [28], dopaminergic-glutamatergic interactions in the brain [29], a central mechanism sensitive to nitric oxide [30], and a decreased GAGA-mediated inhibition of micturition [31]. Other neurological entities that are known to cause OAB syndrome include Parkinson's disease, multiple sclerosis, and spinal cord injuries.…”

Section: Neurologic Factors Of Oabmentioning

confidence: 99%

Pathophysiology of overactive bladder

2012

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Overactive bladder (OAB) is a common disorder that negatively affects the quality of life of our patients and carries a large socioeconomic burden. According to the International Continence Society, it is characterized as urinary urgency, with or without urge incontinence, usually, with frequency and nocturia in the absence of causative infection. The pathophysiology of this disease entity varies between neurogenic, myogenic, or idiopathic factors. This paper provides a review of the contemporary theories behind the pathophysiology of OAB.

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Section: Neurologic Factors Of Oabmentioning

confidence: 99%

Pathophysiology of overactive bladder

2012

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“…These proteins and receptors may be involved in the regulation of nociceptive processing. Indeed, systemic or central administration of nociceptin, 28 enkephalins (intrathecal naloxone, 29 ), and GABA, 30 inhibits the micturition reflex. Interestingly, peripheral inflammation induces nociceptin in primary sensory neurons 31 and increases pro-dynorphin mRNA in dorsal horn neurons.…”

Section: Genes Involved In Bladder Physiologymentioning

confidence: 99%

Gene Expression Profiling of Mouse Bladder Inflammatory Responses to LPS, Substance P, and Antigen-Stimulation

Saban

Nguyen

Hammond

et al. 2002

The American Journal of Pathology

110

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Inflammatory bladder disorders such as interstitial cystitis (IC) deserve attention since a major problem of the disease is diagnosis. IC affects millions of women and isClinical and animal models of acute and chronic urinary bladder inflammation have provided several lines of evidence suggesting a central role of mast cells, sensory nerves, and neurokinin (NK)-1 receptors. Fundamental work regarding the participation of sensory nerves and mast cells in cystitis provides indirect evidence, such as increased numbers of mast cells in the detrusor and submucosa, and morphological evidence of mast cell activation and degranulation. [1][2][3][4] In addition, the extensive tissue remodeling seen in some clinical forms of bladder inflammation such as interstitial cystitis, 4 along with increased urinary levels of histamine and tryptase 5 suggest a role for mast cells. Because both mast cells 6 -8 and NK-1 receptors are increased in bladder biopsies of interstitial cystitis (IC) patients, 9,10 it is tempting to propose a role for sensory peptides-mast cell communication in the pathogenesis of this disorder.Experimentally, we have used classical morphometric analysis and microarray technology to determine the role of mast cells, NK-1 receptors, and bacterial toxins in animal models of cystitis. Time-course experiments indicated early and late genes involved in bladder inflammatory responses. 11 The availability of mice genetically deficient in neurokinin-1 receptor (NK-1R Ϫ/Ϫ ) allowed us to propose a mandatory role of SP receptors in cystitis. 12 We also determined genes that depend on the presence of tissue mast cells for their expression by comparing inflammatory responses in mast cell-deficient (Kit W /

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“…Blok et al 18 demonstrated a direct pathway from the pontine micturition center to the dorsal gray commissure of the sacral cord in cats, 18 and suggested that the pathway relaxed the external striated sphincter during micturition via inhibitory modulation through GABA neurons in Onuf's nucleus. Furthermore, Kanie et al, 16 who performed many experiments on the mechanisms underlying bladder overactivity in CI rats, suggested that the impairment of the inhibitory GABAergic pathway that originates in the forebrain Neurourology and Urodynamics DOI 10.1002/nau Fig. 4.…”

Section: Discussionmentioning

confidence: 99%