Search

Your search keyword '"Page, Amanda"' showing total 9 results
Start Over Author "Page, Amanda" Publisher american physiological society
9 results on '"Page, Amanda"'

1. Opioid modulation of ferret vagal afferent mechanosensitivity

Author

Page, Amanda J., O'Donnell, Traeey A., and Blaekshaw, L. Ashley

Subjects
Opioids -- Physiological aspects, Esophageal diseases -- Care and treatment, Biological sciences
Abstract

Despite universal use of opioids in the clinic to inhibit pain, there is relatively little known of their peripheral actions on sensory nerve endings, where in fact they may be better targeted with more widespread applications. Here we show differential effects of [micro]-, [kappa]-, and [delta]-opioids on mechanosensitive ferret esophageal vagal afferent endings investigated in vitro. The effects of selective agonists [D-[Ala.sup.2],N-Me-[Phe.sup.4],[Gly-ol.sup.S]]-enkephalin (DAMGO), 2-(3, 4-dichloropbenyl)-N-methyl-N-[(1S)- 1 phenyl-2-(1-pyrrolidinyl) ethyl] acetamide hydrochlorine (ICI 199441), and (+)-4-[([alpha]R)-[alpha]-((2S,5R)-4-allyl-2, 5-dimethyl-l-piperazinyl)-3-methoxybenzyl]-N,N-diethylbenz- amide (SNC-80), respectively, on mechanosensory stimulus-response functions were quantified. DAMGO ([10.sup.-7] to [10.sup.-5] M) reduced the responses of tension receptors to circumferential tension (1-5 g) by up to 50%, and the responses of mucosal receptors to mucosal stroking (10-1,000 mg von Frey hair) by >50%. DAMGO effects were reversed by naloxone ([10.sup.-5] M). Tension/mucosal (TM) receptor responses to tension and stroking were unaffected by DAMGO. ICI 199441 ([10.sup.-6] to [10.sup.-5] M) potently inhibited all responses except TM receptor responses to tension, and SNC-80 ([10.sup.-5] to [10.sup.-3] M) had no effect other than a minor inhibition of mucosal receptor responses to intense stimuli at [10.sup.-3] M. We conclude that [micro]- and [kappa]-opioids have potent and selective peripheral effects on esophageal vagal afferents that may have applications in treatment of disorders of visceral sensation. vagal afferents; neuromodulation; esophagus more...

Published
2008

2. Ghrelin selectively reduces mechanosensitivity of upper gastrointestinal vagal afferents

Author

Page, Amanda J., Slattery, James A., Milte, Catherine, Laker, Rhianna, O'Donnell, Tracey, Dorian, Camilla, Brierley, Stuart M., and Blackshaw, L. Ashley

Subjects
Ghrelin -- Research, Metabolic regulation -- Research, Gastrointestinal system -- Motility, Gastrointestinal system -- Research, Physiological research, Biological sciences
Abstract

Ghrelin is a peptide released from gastric endocrine cells that has an orexigenic effect via a vagal pathway. Here we determine the effect of ghrelin on mechanosensitivity of upper-intestinal vagal afferent fibers in ferret and mouse. The responses of gastroesophageal vagal afferents to graded mechanical stimulation were determined in vitro before and during application of ghrelin to their peripheral endings. Three types of vagal afferent were tested: tension receptors responding to circumferential tension, mucosal receptors responding only to mucosal stroking, and tension/mucosal (TM) receptors in ferret esophagus that responded to both stimuli. In the mouse, ghrelin did not significantly affect the response of mucosal receptors to mucosal stroking with calibrated von Frey hairs. However, it significantly reduced responses of tension receptors to circumferential tension (P < 0.005; two-way ANOVA) by up to 40%. This inhibition was reversed by the ghrelin receptor antagonist [D-Lys-3]-growth hormone-releasing peptide (GHRP)-6. In the ferret, ghrelin significantly reduced the response of mucosal and TM receptors to mucosal stroking with calibrated von Frey hairs. Surprisingly, ghrelin did not significantly alter the response to circumferential tension in either tension or TM receptors. RT-PCR analysis indicated that both ghrelin and its receptor are expressed in vagal afferent cell bodies in mouse nodose ganglia. In conclusion, ghrelin selectively inhibits subpopulations of mechanically sensitive gastroesophageal vagal afferents; there is also potential for ghrelin release from vagal afferents. However, the subpopulation of afferents inhibited differs between species. These data have broad implications for ghrelin's role in food intake regulation and reflex control of gastrointestinal function. in vitro gastroesophageal preparation; neuromodulation; mechanoreceptor doi:10.1152/ajpgi.00536.2006. more...

Published
2007

Catalog

Books, media, physical & digital resources
See catalog results

3. Peripheral versus central modulation of gastric vagal pathways by metabotropic glutamate receptor 5

Author

Young, Richard L., Page, Amanda J., O'Donnell, Tracey A., Cooper, Nicole J., and Blackshaw, L. Ashley

Subjects
Immunohistochemistry -- Research, Afferent pathways -- Analysis, Metabolic regulation -- Analysis, Biological sciences
Abstract

Metabotropic glutamate receptors (mGluR) are classified into group I, II, and III mGluR. Group I (mGluR1, mGluR5) are excitatory, whereas group II and III are inhibitory, mGluR5 antagonism potently reduces triggering of transient lower esophageal sphincter relaxations and gastroesophageal reflux. Transient lower esophageal sphincter relaxations are mediated via a vagal pathway and initiated by distension of the proximal stomach. Here, we determined the site of action of mGluR5 in gastric vagal pathways by investigating peripheral responses of ferret gastroesophageal vagal afferents to graded mechanical stimuli in vitro and central responses of nucleus tractus solitarius (NTS) neurons with gastric input in vivo in the presence or absence of the mGluR5 antagonist 2-methyl-6-(phenylethynyl)pyridine (MPEP). mGluR5 were also identified immunohistochemically in the nodose ganglia and NTS after extrinsic vagal inputs had been traced from the proximal stomach. Gastroesophageal vagal afferents were classified as mucosal, tension, or tension-mucosal (TM) receptors. MPEP (1-10 [micro]M) inhibited responses to circumferential tension of tension and TM receptors. Responses to mucosal stroking of mucosal and TM receptors were unaffected. MPEP (0.001-10 nmol icv) had no major effect on the majority of NTS neurons excited by gastric distension or on NTS neurons inhibited by distension, mGluR5 labeling was abundant in gastric vagal afferent neurons and sparse in fibers within NTS vagal subnuclei. We conclude that mGluR5 play a prominent role at gastroesophageal vagal afferent endings but a minor role in central gastric vagal pathways. Peripheral mGluR5 may prove a suitable target for reducing mechanosensory input from the periphery, for therapeutic benefit. metabotropic glutamate receptor 5; immunohistochemistry; retrograde tracing; nucleus tractus solitarius; vagal afferent mechanosensitivity more...

Published
2007

7. Pregnancy-related plasticity of gastric vagal afferent signals in mice.

Author

Hui Li, Clarke, Georgia S., Christie, Stewart, Ladyman, Sharon R., Kentish, Stephen J., Young, Richard L., Gatford, Kathryn L., and Page, Amanda J.

Subjects
AFFERENT pathways, SOMATOTROPIN, CENTRAL nervous system, INGESTION, FETAL development
Abstract

Gastric vagal afferents (GVAs) sense food-related mechanical stimuli and signal to the central nervous system, to integrate control of meal termination. Pregnancy is characterized by increased maternal food intake, which is essential for normal fetal growth and to maximize progeny survival and health. However, it is unknown whether GVA function is altered during pregnancy to promote food intake. This study aimed to determine the mechanosensitivity of GVAs and food intake during early, mid-, and late stages of pregnancy in mice. Pregnant mice consumed more food compared with nonpregnant mice, notably in the light phase during mid- and late pregnancy. The increased food intake was predominantly due to light-phase increases in meal size across all stages of pregnancy. The sensitivity of GVA tension receptors to gastric distension was significantly attenuated in mid- and late pregnancy, whereas the sensitivity of GVA mucosal receptors to mucosal stroking was unchanged during pregnancy. To determine whether pregnancy-associated hormonal changes drive these adaptations, the effects of estradiol, progesterone, prolactin, and growth hormone on GVA tension receptor mechanosensitivity were determined in nonpregnant female mice. The sensitivity of GVA tension receptors to gastric distension was augmented by estradiol, attenuated by growth hormone, and unaffected by progesterone or prolactin. Together, the data indicate that the sensitivity of GVA tension receptors to tension is reduced during pregnancy, which may attenuate the perception of gastric fullness and explain increased food intake. Further, these adaptations may be driven by increases in maternal circulating growth hormone levels during pregnancy. NEW & NOTEWORTHY This study provides first evidence that gastric vagal afferent signaling is attenuated during pregnancy and inversely associated with meal size. Growth hormone attenuated mechanosensitivity of gastric vagal afferents, adding support that increases in maternal growth hormone may mediate adaptations in gastric vagal afferent signaling during pregnancy. These findings have important implications for the peripheral control of food intake during pregnancy. [ABSTRACT FROM AUTHOR] more...

Published
2021
Full Text
View/download PDF

9. Activation of CRF2 receptor increases gastric vagal afferent mechanosensitivity.

Author

Hui Li and Page, Amanda J.

Abstract

Gastric vagal afferent (GVA) sensing of food-related mechanical stimuli is a crucial mechanism in the control of feeding behavior and gastric function. Stress is an important factor contributing to eating disorders and gastric diseases. Chronic stress has been shown to increase the mechanosensitivity of GVAs in mice and to reduce food intake and body weight. Whether the mechanosensitivity of GVAs is modulated by stress hormones is not known. This study aimed to determine the effect of stress hormones on GVA mechanosensitivity. The expression of stress hormone receptors in GVA cell bodies was determined in 8-wk-old male C57BL/6 mice using quantitative RT-PCR combined with laser capture microdissection. The mechanosensitivity of GVAs was determined in the absence and presence of stress hormones using an in vitro single-fiber recording preparation. NR3C1 and CRHR2 (mRNA isoforms of glucocorticoid receptor and CRF2 receptor, respectively) were expressed in GVA neurons. The glucocorticoid receptor agonist corticosterone had no effect on the mechanosensitivity of either tension or mucosal GVAs. Activation of CRF2 receptor by its specific analog, urocortin 3, significantly increased the mechanosensitivity of both tension and mucosal GVAs, an effect prevented by the CRF2 receptor antagonist astressin 2B. In conclusion, activation of CRF2 receptor increases the mechanosensitivity of GVAs. This may contribute to the stress- and CRF2 receptor-associated changes in feeding behavior and gastric function, possibly contributing to the hypersensitivity of GVAs in chronic stress conditions.NEW & NOTEWORTHY Gastric vagal afferents (GVAs) relay food-related signals to the central nervous system, where they are processed, eventually leading to modulation of food intake and gastric function. GVA signaling can be modulated by an array of hormones. Stress has been shown to induce GVA hypersensitivity. This study demonstrates that GVA neurons express subtypes of stress hormone receptors, specifically CRF2. Furthermore, activation of CRF2 receptor increases GVA mechanosensitivity, which could have implications for food intake and gastric function. [ABSTRACT FROM AUTHOR] more...

Published
2019
Full Text
View/download PDF