Your search keyword '"Kidd, Emma J."' showing total 27 results

1. P2X[sub7] Receptors Are Redistributed on Human Monocytes after Pore Formation in Response to Prolonged Agonist Exposure.

Author

Young, Robert D., Kidd, Emma J., and Connon, Che J.

Subjects

*CATIONS, *ADENOSINE triphosphate, *CELL membranes, *ELECTRON microscopy, *MONOCYTES, *AGGLOMERATION (Materials), *IMMUNOGOLD labeling

Abstract

The P2X[sub7] cell surface receptor is responsible for adenosine triphosphate-dependent lysis of immune cells following the formation of non-selective membrane pores. This study examined changes in P2X[sub7] receptor distribution following agonist treatment. Human THP-1 monocytes were exposed to the agonist 2′-3′-O-(4-benzoylbenzoyl) adenosine 5′-triphosphate for 1—40 min after which P2X[sub7] receptors were immunogold labelled. The number and distribution of P2X7 receptors on the cell membrane were quantified using transmission electron microscopy. Increasing the time of agonist exposure resulted in clustering of P2X[sub7] receptors, a decrease in individual P2X[sub7] receptors and no change in the total number of P2X[sub7] receptors. These results suggest that pore formation does not involve further insertion or initial movement of receptors in the membrane but that P2X[sub7] receptors do cluster together after prolonged activation. [ABSTRACT FROM AUTHOR]

Published

2003

2. Proteins Involved in Endocytosis Are Upregulated by Ageing in the Normal Human Brain: Implications for the Development of Alzheimer's Disease.

Author

Alsaqati, Mouhamed, Thomas, Rhian S., and Kidd, Emma J.

Subjects

*ALZHEIMER'S disease, *BRAIN, *SENILE dementia, *HEAD, *NEURODEGENERATION, *AGING, *BIOCHEMISTRY, *CARRIER proteins, *COMPARATIVE studies, *ENDOCYTOSIS, *HYDROLASES, *PHENOMENOLOGY, *RESEARCH methodology, *MEDICAL cooperation, *MEMBRANE proteins, *NERVE tissue proteins, *PEPTIDES, *PROTEIN precursors, *RESEARCH, *RESEARCH funding, *EVALUATION research, BRAIN metabolism

Abstract

The greatest risk factor for Alzheimer's disease (AD) is advanced age, but the reason for this association remains unclear. Amyloid-β (Aβ) is produced from amyloid precursor protein (APP) primarily after APP is internalized by clathrin-mediated or clathrin-independent endocytosis. Changes in endocytosis in AD have been identified. We hypothesized that endocytic protein expression is altered during ageing, thus influencing the likelihood of developing AD by increasing Aβ production. We explored how levels of endocytic proteins, APP, its metabolites, secretase enzymes, and tau varied with age in cortical brain samples from men of three age ranges (young [20-30], middle aged [45-55], and old [70-90]) with no symptoms of dementia. Aβ40 and Aβ42 were significantly increased in old brains, while APP and secretase expression was unaffected by age. Phosphorylated GSK3β increased significantly with age, a possible precursor for neurofibrillary tangle production, although phosphorylated tau was undetectable. Significant increases in clathrin, dynamin-1, AP180, Rab-5, caveolin-2, and flotillin-2 were seen in old brains. Rab-5 also increased in middle-aged brains prior to changes in Aβ levels. This age-related increase in endocytic protein expression, not described previously, suggests an age-related upregulation of endocytosis which could predispose older individuals to develop AD by increasing APP internalization and Aβ generation. [ABSTRACT FROM AUTHOR]

Published

2018

3. Effects of nebulised magnesium sulphate on inflammation and function of the guinea-pig airway.

Author

Turner, Dawn L., Ford, William R., Kidd, Emma J., Broadley, Kenneth J., and Powell, Colin

Subjects

*INFLAMMATION, *MAGNESIUM sulfate, *AEROSOLS, *ASTHMA treatment, *LABORATORY swine, *DOSE-effect relationship in pharmacology, *THERAPEUTICS

Abstract

Magnesium sulphate is a potential treatment for acute severe asthma. However, the mechanisms and dose-response relationships are poorly understood. The first objective of this study was to examine whether inhaled magnesium sulphate exerts bronchodilator activity measured as bronchoprotection against histamine-induced bronchoconstriction in conscious guinea-pigs alone and combined with salbutamol. Secondly, we examined whether inhaled magnesium sulphate inhibits airways inflammation and function in models of neutrophilic and eosinophilic lung inflammation induced, respectively, by inhaled lipopolysaccharide or the inhaled antigen, ovalbumin (OVA). Airway function was measured in conscious guinea-pigs as specific airway conductance (sG aw ) by whole-body plethysmography. Anti-inflammatory activity was measured against lung inflammatory cell influx induced by OVA inhalation in OVA-sensitised animals or by lipopolysaccharide (LPS) exposure of non-sensitised animals. Airway function (sG aw ) was measured over 24 h after OVA exposure. Airway hyperresponsiveness to inhaled histamine and inflammatory cells in bronchoalveolar lavage fluid were recorded 24 h after OVA or LPS challenge. Histamine-induced bronchoconstriction was inhibited by inhaled magnesium sulphate or salbutamol alone and in combination, they produced synergistic bronchoprotection. LPS-induced neutrophil influx was inhibited by 6 days pretreatment with magnesium sulphate. Early and late asthmatic responses in OVA sensitised and challenged animals were attenuated by magnesium sulphate. Lung inflammatory cells were increased by OVA, macrophages being significantly reduced by magnesium sulphate. Nebulised magnesium sulphate protects against histamine-induced bronchoconstriction in conscious guinea-pigs and exerts anti-inflammatory activity against pulmonary inflammation induced by allergen (OVA) or LPS. These properties of magnesium sulphate explain its beneficial actions in acute asthma. [ABSTRACT FROM AUTHOR]

Published

2017

4. The role of menopausal symptoms on future health and longevity: A systematic scoping review of longitudinal evidence.

Author

Andrews, Robin, Lacey, Arron, Bache, Kate, and Kidd, Emma J.

Subjects

*BONE density, *JOINT pain, *SLEEP, *FATIGUE (Physiology), *COGNITION disorders, *PREMATURE menopause

Abstract

• This scoping review found that menopausal symptoms are highly associated with future health and longevity. • Cardiovascular disease, psychiatric disorders, diabetes, and reduced bone mineral density are positively associated with menopausal symptoms. • Psychological menopausal symptoms and cognitive decline improve after menopause, except among women from low socioeconomic backgrounds. • Future work should assess whether cognitive decline is associated with developing dementia and investigate the long-term effects of underexplored menopausal symptoms such as sleep issues, fatigue, urogenital symptoms, period irregularities, joint pain, and headaches. • Future work should also endeavour to explore whether improving menopausal symptoms, as and when they arise, can reduce future health risks. Women live longer than men but spend more years in poor health. Menopausal symptoms are not generally associated with adverse health outcomes. However, increasingly, evidence suggests they can significantly impact future health and longevity. Understanding the long-term effects of menopausal symptoms will enable clinicians to identify risk factors and intervene with modifications to support healthy aging. This review examined the scope of research investigating the association between menopausal symptoms and future health outcomes. We searched for longitudinal cohort studies. Date and geographical restrictions were not applied. Articles were screened and data extracted using standardised methods. Included studies examined the role of menopausal symptoms on future health developments using a sample who had experienced menopause and were deemed healthy at baseline, with clear reporting of their menopausal status at symptom assessment. We identified 53 eligible studies with data from over 450,000 women enrolled in 28 longitudinal cohorts. Cardiovascular disease, psychiatric disorders, diabetes, and reduced bone mineral density were positively associated with menopausal symptoms. Breast cancer was associated with an asymptomatic menopause. Psychological menopausal symptoms and cognitive decline improved after menopause, except among women from low socioeconomic backgrounds. These findings demonstrate that menopausal symptoms are important indicators for future health risks. Future work should investigate the impact of underexplored menopausal symptoms on future health, such as sleeping problems and urogenital issues, and evaluate whether treating menopausal symptoms could lead to improvements in future health outcomes. Should future research continue to support these findings, clinical guidelines should be updated to support clinical decision-making in menopause care. [ABSTRACT FROM AUTHOR]

Published

2024

5. Outcome-Specific Satiety Reveals a Deficit in Context-Outcome, but Not Stimulus- or Action-Outcome, Associations in Aged Tg2576 Mice.

Author

Lelos, Mariah J., Thomas, Rhian S., Kidd, Emma J., and Good, Mark A.

Subjects

*ANIMAL models of Alzheimer's disease, *AMYLOID beta-protein, *AMYGDALOID body, *CLASSICAL conditioning, *ACTION theory (Psychology)

Abstract

The onset of Alzheimer's disease (AD) is often accompanied by changes in emotion, motivation, and goal-directed behavior. The production of beta-amyloid is thought to be a major and early contributor to the pathogenesis of AD. The present study tested the hypothesis that amyloid pathology present in the amygdala, frontal cortex, and hippocampus of Tg2576 mice would disrupt the development of instrumentaland/or Pavlovian-outcome associations. The results showed that both instrumentaland Pavlovian-conditioned behaviors were sensitive to Outcome devaluation (Experiments 1 & 2) and that Pavlovian cues influenced goal-directed actions associated with the same outcome (Experiment 2) in Tg2576 mice. In contrast, context mediated Pavlovian-conditioned behaviors in aged (Experiment 3a) but not young (Experiment 3b) Tg2576 mice were insensitive to outcome devaluation. Aged Tg2576, nevertheless, successfully acquired a simple context discrimination at the same rate as control mice. We conclude that amyloid pathology in aged Tg2576 mice may specifically disrupt context-outcome associations supported by the hippocampus and/or its interaction with the amygdala. [ABSTRACT FROM AUTHOR]

Published

2011

6. Anti-amyloid precursor protein immunoglobulins inhibit amyloid-β production by steric hindrance.

Author

Thomas, Rhian S., Liddell, J. Eryl, and Kidd, Emma J.

Subjects

*AMYLOID beta-protein precursor, *STERIC hindrance, *ALZHEIMER'S disease, *MONOCLONAL antibodies, *EXTRACELLULAR matrix, *BIODEGRADATION, *BINDING sites

Abstract

The cleavage of amyloid precursor protein (APP) by β- and γ-secretases results in the production of amyloid-β (Aβ) in Alzheimer's disease. We raised two monoclonal antibodies, 2B3 and 2B12, that recognize the β-secretase cleavage site on APP but not Aβ. We hypothesized that these antibodies would reduce Aβ levels via steric hindrance of β-secretase. Both antibodies decreased extracellular Aβ levels from astrocytoma cells, but 2B3 was more potent than 2B12. Levels of soluble sAPPα from the nonamyloidogenic α-secretase pathway and intracellular APP were not affected by either antibody nor were there any effects on cell viability. 2B3 exhibited a higher affinity for APP than 2B12 and its epitope appeared to span the cleavage site, whereas 2B12 bound slightly upstream. Both of these factors probably contribute to its greater effect on Aβ levels. After 60 min incubation at pH 4.0, most 2B3 and 2B12 remained bound to their antigen, suggesting that the antibodies will remain bound to APP in the acidic endosomes where β-secretase cleavage probably occurs. Only 2B3 and 2B12, but not control antibodies, inhibited the cleavage of sAPPα by β-secretase in a cell-free assay where the effects of antibody internalization and intracellular degradation were excluded. 2B3 virtually abolished this cleavage. In addition, levels of C-terminal APP fragments, generated following β-secretase cleavage (βCTF), were significantly reduced in cells after incubation with 2B3. These results strongly suggest that anti-cleavage site IgGs can generically reduce Aβ levels via inhibition of β-secretase by steric hindrance and may provide a novel alternative therapy for Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2011

7. Distribution of P2X[sub 1] and P2X[sub 3] Receptors in the Rat and Human Urinary Bladder.

Author

Elneil, Sohier, Skepper, Jeremy N., Kidd, Emma J., Williamson, John G., and Ferguson, Douglas R.

Subjects

*ADENOSINE triphosphatase, *BLADDER, *RECEPTOR antibodies, *NEUROTRANSMITTERS, *CALCITONIN gene-related peptide, *SMOOTH muscle, *IMMUNOFLUORESCENCE, *IMMUNOLOGY, *SENSORY stimulation

Abstract

Adenosine 5′-triphosphate (ATP) is known to play a significant role as a neurotransmitter in smooth muscle. There is evidence to show that ATP can cause bladder contractions and may also be involved in the processing of sensory information in the urinary bladder. These effects are likely to be mediated by P2X receptors, namely P2X[sub 1] and P2X[sub 3] , respectively. This study set out to investigate their distribution in rat and human urinary bladders. P2X[sub 1] receptor immunoreactivity was found on detrusor muscle fibres and P2X[sub 3] receptor immunoreactivity was found in the urothelium of both species. This is the first demonstration of a non-neuronal localisation for P2X[sub 3] receptors. No clear evidence was found for the presence of P2X[sub 3] receptors on calcitonin gene-related peptide-containing sensory nerves and therefore P2X[sub 3] receptors may not have a direct role in the mediation of sensory responses to ATP in the urinary bladder.Copyright © 2001 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2001

8. ACE2 activation protects against cognitive decline and reduces amyloid pathology in the Tg2576 mouse model of Alzheimer's disease.

Author

Evans, Charles E., Miners, James S., Piva, Giulia, Willis, Christine L., Heard, David M., Kidd, Emma J., Good, Mark A., and Kehoe, Patrick G.

Subjects

*ALZHEIMER'S disease, *RENIN-angiotensin system, *COGNITION disorders, *ANIMAL disease models, *TRANSGENIC mice, *MICE, *ANIMAL models in research

Abstract

Mid-life hypertension and cerebrovascular dysfunction are associated with increased risk of later life dementia, including Alzheimer's disease (AD). The classical renin–angiotensin system (cRAS), a physiological regulator of blood pressure, functions independently within the brain and is overactive in AD. cRAS-targeting anti-hypertensive drugs are associated with reduced incidence of AD, delayed onset of cognitive decline, and reduced levels of Aβ and tau in both animal models and human pathological studies. cRAS activity is moderated by a downstream regulatory RAS pathway (rRAS), which is underactive in AD and is strongly associated with pathological hallmarks in human AD, and cognitive decline in animal models of CNS disease. We now show that enhancement of brain ACE2 activity, a major effector of rRAS, by intraperitoneal administration of diminazene aceturate (DIZE), an established activator of ACE2, lowered hippocampal Aβ and restored cognition in mid-aged (13–14-month-old) symptomatic Tg2576 mice. We confirmed that the protective effects of DIZE were directly mediated through ACE2 and were associated with reduced hippocampal soluble Aβ42 and IL1-β levels. DIZE restored hippocampal MasR levels in conjunction with increased NMDA NR2B and downstream ERK signalling expression in hippocampal synaptosomes from Tg2576 mice. Chronic (10 weeks) administration of DIZE to pre-symptomatic 9–10-month-old Tg2576 mice, and acute (10 days) treatment in cognitively impaired 12–13-month-old mice, prevented the development of cognitive impairment. Together these data demonstrate that ACE2 enhancement protects against and reverses amyloid-related hippocampal pathology and cognitive impairment in a preclinical model of AD. [ABSTRACT FROM AUTHOR]

Published

2020

9. Sex-specific effects of central adiposity and inflammatory markers on limbic microstructure.

Author

Metzler-Baddeley, Claudia, Mole, Jilu P., Leonaviciute, Erika, Sims, Rebecca, Kidd, Emma J., Ertefai, Benyamin, Kelso-Mitchell, Aurora, Gidney, Florence, Fasano, Fabrizio, Evans, John, Jones, Derek K., and Baddeley, Roland J.

Subjects

*OBESITY, *VISCERAL pain, *WAIST-hip ratio, *MICROSTRUCTURE

Abstract

Abstract Midlife obesity is a risk factor of late onset Alzheimer's disease (LOAD) but why this is the case remains unknown. As systemic inflammation is involved in both conditions, obesity-related neuroinflammation may contribute to damage in limbic structures important in LOAD. Here, we investigated the hypothesis that systemic inflammation would mediate central obesity related effects on limbic tissue microstructure in 166 asymptomatic individuals (38–71 years old). We employed MRI indices sensitive to myelin and neuroinflammation [macromolecular proton fraction (MPF) and k f ] from quantitative magnetization transfer (qMT) together with indices from neurite orientation dispersion and density imaging (NODDI) to investigate the effects of central adiposity on the fornix, parahippocampal cingulum, uncinate fasciculus (compared with whole brain white matter and corticospinal tract) and the hippocampus. Central obesity was assessed with the Waist Hip Ratio (WHR) and abdominal visceral and subcutaneous fat area fractions (VFF, SFF), and systemic inflammation with blood plasma concentrations of leptin, adiponectin, C-reactive protein and interleukin 8. Men were significantly more centrally obese and had higher VFF than women. Individual differences in WHR and in VFF were negatively correlated with differences in fornix MPF and k f , but not with any differences in neurite microstructure. In women, age mediated the effects of VFF on fornix MPF and k f , whilst in men differences in the leptin and adiponectin ratio fully mediated the effect of WHR on fornix MPF. These results suggest that visceral fat related systemic inflammation may damage myelin-related properties of the fornix, a key limbic structure known to be involved in LOAD. Highlights • Central adiposity is linked to apparent myelin/inflammatory damage in the fornix. • Central adiposity is not linked to differences in apparent neurite microstructure. • Men were more centrally obese and had higher visceral fat fractions than women. • In women, age mediated the correlation between visceral fat and fornix myelin. • In men, adipokines mediated the correlation between WHR and fornix myelin. [ABSTRACT FROM AUTHOR]

Published

2019

10. Selective reduction of APP-BACE1 activity improves memory via NMDA-NR2B receptor-mediated mechanisms in aged PDAPP mice.

Author

Evans, Charles E., Thomas, Rhian S., Freeman, Thomas J., Hvoslef-Eide, Martha, Good, Mark A., and Kidd, Emma J.

Subjects

*MEMORY, *METHYL aspartate receptors, *INTRAPERITONEAL injections, *PLATELET-derived growth factor, *GROWTH factors

Abstract

Abstract β-Amyloid (Aβ) accumulation is an early event of Alzheimer's disease (AD) pathogenesis. Inhibition of Aβ production by β-secretase (BACE) has been proposed as a potential therapeutic strategy for AD. However, BACE inhibitors lack specificity and have had limited clinical benefit. To better study the consequences of reducing BACE metabolism, specifically of APP, we used an antibody, 2B3, that binds to APP at the BACE cleavage site, inhibiting Aβ production. 2B3 was administered either directly into the lateral ventricles or by intraperitoneal injection to (platelet-derived growth factor promoter hAPP717V (PDAPP) mice and WT mice. 2B3 reduced soluble Aβ40 and βCTF (β-amyloid derived C-terminal fragment) and improved memory for object-in-place associations and working memory in a foraging task in PDAPP mice. 2B3 also normalized the phosphorylation of the N-methyl-D-aspartate receptor NR2B subunit and subsequent extracellular signal–regulated kinase signaling. The importance of this NR2B pathway for OiP memory was confirmed by administering the NR2B antagonist, Ro25-6981, to 18-month-old WT. In contrast, 2B3 impaired associative recognition memory in young WT mice. These data provide novel insights into the mechanism by which selective modulation of APP metabolism by BACE influences synaptic and cognitive processes in both normal mice and aged APP transgenic mice. Highlights • Inhibition of APP metabolism by ICV 2B3 reduced Aβ and βCTF production • 2B3 prevented the onset of memory impairments in PDAPP mice • 2B3 restored NR2B receptor phosphorylation and subsequent ERK activity • NMDA-NR2B receptor mechanisms contributed to object-in-place memory • Directly inhibiting APP-BACE metabolism provides a therapeutic strategy for AD [ABSTRACT FROM AUTHOR]

Published

2019

11. Death Receptor 3 regulates distinct pathological attributes of acute versus chronic murine allergic lung inflammation.

Author

Singh, Ravinder Kaur, Perks, William Victor, Twohig, Jason Peter, Kidd, Emma J., Broadley, Kenneth, Farrow, Stuart N., Williams, Anwen Sian, Taylor, Philip Russel, and Wang, Eddie Chung Yern

Subjects

*LUNG diseases, *DEATH receptors, *AUTOIMMUNE diseases, *LABORATORY mice, *DISEASE progression, *PATHOGENIC microorganisms

Abstract

The Death Receptor 3 (DR3)/Tumour Necrosis Factor-like cytokine 1A (TL1A) axis stimulates effector T cells and type 2 innate lymphocytes (ILC2) that trigger cytokine release and drive disease pathology in several inflammatory and autoimmune diseases, including murine models of acute allergic lung inflammation (ALI). The aim of this study was to elucidate the role of DR3 in chronic ALI compared to acute ALI, using mice genetically deficient in the DR3 gene (DR3 ko ). Results showed DR3 expression in the lungs of wild-type mice was up-regulated following induction of acute ALI and this increased expression was maintained in chronic disease. DR3 ko mice were resistant to cellular accumulation within the alveolar passages in acute, but not chronic ALI. However, DR3 ko mice displayed reduced immuno-histopathology and goblet cell hyperplasia; hallmarks of the asthmatic phenotype; in chronic, but not acute ALI. These data suggest DR3 is a potential therapeutic target, involved in temporally distinct aspects of ALI progression and pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2017

12. Decreasing the expression of PICALM reduces endocytosis and the activity of β-secretase: implications for Alzheimer's disease.

Author

Thomas, Rhian S., Henson, Alex, Gerrish, Amy, Jones, Lesley, Williams, Julie, and Kidd, Emma J.

Subjects

*ALZHEIMER'S disease, *ENDOCYTOSIS, *PHOSPHATIDYLINOSITOL 3-kinases, *AMYLOID beta-protein precursor, *SECRETASES, *RNA metabolism, *CELL lines, *ENZYME-linked immunosorbent assay, *FLOW cytometry, *IMMUNOHISTOCHEMISTRY, *MEMBRANE proteins, *PEPTIDES, *PROTEIN precursors, *PROTEINS, *PROTEOLYTIC enzymes, *RESEARCH funding, *RNA, *TRANSFERRIN, *WESTERN immunoblotting, BRAIN metabolism

Abstract

Background: Polymorphisms in the gene for phosphatidylinositol binding clathrin assembly protein (PICALM), an endocytic-related protein, are associated with a small, increased risk of developing Alzheimer's disease (AD), strongly suggesting that changes in endocytosis are involved in the aetiology of the disease. We have investigated the involvement of PICALM in the processing of amyloid precursor protein (APP) to understand how PICALM could be linked to the development of AD. We used siRNA to deplete levels of PICALM, its isoforms and clathrin heavy chain in the human brain-derived H4 neuroglioma cell line that expresses endogenous levels of APP. We then used Western blotting, ELISA and immunohistochemistry to detect intra- and extracellular protein levels of endocytic-related proteins, APP and APP metabolites including β-amyloid (Aβ). Levels of functional endocytosis were quantified using ALEXA 488-conjugated transferrin and flow cytometry as a marker of clathrin-mediated endocytosis (CME).Results: Following depletion of all the isoforms of PICALM by siRNA in H4 cells, levels of intracellular APP, intracellular β-C-terminal fragment (β-CTF) and secreted sAPPβ (APP fragments produced by β-secretase cleavage) were significantly reduced but Aβ40 was not affected. Functional endocytosis was significantly reduced after both PICALM and clathrin depletion, highlighting the importance of PICALM in this process. However, depletion of clathrin did not affect APP but did reduce β-CTF levels. PICALM depletion altered the intracellular distribution of clathrin while clathrin reduction affected the subcellular pattern of PICALM labelling. Both PICALM and clathrin depletion reduced the expression of BACE1 mRNA and PICALM siRNA reduced protein levels. Individual depletion of PICALM isoforms 1 and 2 did not affect APP levels while clathrin depletion had a differential effect on the isoforms, increasing isoform 1 while decreasing isoform 2 expression.Conclusions: The depletion of PICALM in brain-derived cells has significant effects on the processing of APP, probably by reducing CME. In particular, it affects the production of β-CTF which is increasingly considered to be an important mediator in AD independent of Aβ. Thus a decrease in PICALM expression in the brain could be beneficial to slow or prevent the development of AD. [ABSTRACT FROM AUTHOR]

Published

2016

13. Pulmonary edema measured by MRI correlates with late-phase response to allergen challenge.

Author

Evans, Rhys L., Changani, Kumar K., Hotee, Sarah, Pindoria, Kashmira, Campbell, Simon, Nials, Anthony T., Ford, William R., Broadley, Kenneth J., and Kidd, Emma J.

Subjects

*PULMONARY edema, *EDEMA, *ALLERGENS, *OVALBUMINS, *GUINEA pigs

Abstract

Purpose: Asthma is associated with reversible airway obstruction, leucocyte infiltration, airways hyperresponsiveness (AHR), and airways remodeling. Fluid accumulation causes pulmonary edema contributing to airways obstruction. We examined the temporal relationship between the late asthmatic response (LAR) following allergen challenge of sensitized guinea-pigs and pulmonary edema measured by magnetic resonance imaging (MRI). Materials and Methods: Ovalbumin (OVA) sensitized guinea-pigs received either a single OVA inhalation (acute) or nine OVA inhalations at 48 h intervals (chronic). Airways obstruction was measured as specific airways conductance (s Gaw) by whole body plethysmography. AHR to inhaled histamine and bronchoalveolar lavage for leucocyte counts were measured 24 h after a single or the final chronic ovalbumin challenges. MRI was performed at intervals after OVA challenge and high-intensity edemic signals were quantified. Results: Ovalbumin caused early bronchoconstriction, followed at 7 h by an LAR and at 24 h AHR and leucocyte influx. The bright-intensity MRI edema signal, peaking at 7 h, was significantly ( P < .05) greater after chronic (9.0 ± 0.7 × 103 mm3) than acute OVA (7.6 ± 0.2 × 103 mm3). Dexamethasone treatment before acute OVA abolished the AHR and LAR and significantly reduced eosinophils and the bright-intensity MRI edema from 9.1 ± 1.0 to 6.4 ± 0.3 × 103 mm3. Conclusion: We show a temporal relationship between edema and the LAR and their parallel reduction, along with eosinophils and AHR, by dexamethasone. This suggests a close causative association between pulmonary edema and impaired airways function. [ABSTRACT FROM AUTHOR]

Published

2015

14. Adjustment of sensitisation and challenge protocols restores functional and inflammatory responses to ovalbumin in guinea-pigs.

Author

Lowe, Alexander P.P., Broadley, Kenneth J., Nials, Anthony T., Ford, William R., and Kidd, Emma J.

Subjects

*INFLAMMATION, *OVALBUMINS, *ANTIGENS, *ASTHMA, *AIRWAY (Anatomy), *LABORATORY swine, *DISEASES

Abstract

Introduction Inhalation of antigen in atopic asthma induces early (EAR) and late asthmatic responses (LARs), inflammatory cell infiltration and airways hyperresponsiveness (AHR). Previously, we have established a protocol of sensitisation and subsequent ovalbumin (Ova) inhalation challenge in guinea-pigs which induced these 4 features (Smith & Broadley, 2007). However, the responses of guinea-pigs to Ova challenge have recently declined, producing no LAR or AHR and diminished EAR and cells. By making cumulative modifications to the protocol, we sought to restore these features. Methods Guinea-pigs were sensitised with Ova (i.p. 100 or 150 μg) on days 1 and 5 or days 1, 4 and 7 and challenged with nebulised Ova (100 or 300 μg/ml, 1 h) on day 15. Airway function was measured in conscious guinea-pigs by whole-body plethysmography to record specific airway conductance (sGaw). Airway responsiveness to aerosolized histamine (0.3 mM) was determined before and 24 h after Ova challenge. Bronchoalveolar lavage was performed for total and differential inflammatory cell counts. Lung sections were stained for counting of eosinophils. Results Lack of AHR and LAR with the original protocol was confirmed. Increasing the Ova challenge concentration from 100 to 300 μg/ml restored AHR and eosinophils and increased the peak of the EAR. Increasing the number of sensitisation injections from 2 to 3 did not alter the responses. Increasing the Ova sensitisation concentration from 100 to 150 μg significantly increased total cells, particularly eosinophils. A LAR was revealed and lymphocytes and eosinophils increased when either the Al(OH) 3 concentration was increased or the duration between the final sensitisation injection and Ova challenge was extended from 15 to 21 days. Discussion This study has shown that declining allergic responses to Ova in guinea-pigs could be restored by increasing the sensitisation and challenge conditions. It has also demonstrated an important dissociation between EAR, LAR, AHR and inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

15. Human parainfluenza type 3 virus impairs the efficacy of glucocorticoids to limit allergy-induced pulmonary inflammation in guinea-pigs.

Author

FORD, William R., BLAIR, Alan E., EVANS, Rhys L., JOHN, Elinor, BUGERT, Joachim J., BROADLEY, Kenneth J., and KIDD, Emma J.

Subjects

*PARAINFLUENZA viruses, *GLUCOCORTICOIDS, *PNEUMONIA, *OVALBUMINS, *PLETHYSMOGRAPHY

Abstract

Viral exacerbations of allergen-induced pulmonary inflammation in pre-clinical models reportedly reduce the efficacy of glucocorticoids to limit pulmonary inflammation and airways hyper-responsiveness to inhaled spasmogens. However, exacerbations of airway obstruction induced by allergen challenge have not yet been studied. hPIV-3 (human parainfluenza type 3 virus) inoculation of guinea-pigs increased inflammatory cell counts in BAL (bronchoalveolar lavage) fluid and caused hyper-responsiveness to inhaled histamine. Both responses were abolished by treatment with either dexamethasone (20 mg/kg of body weight, subcutaneous, once a day) or fluticasone propionate (a 0.5 mg/ml solution aerosolized and inhaled over 15 min, twice a day). In ovalbumin-sensitized guinea-pigs, allergen (ovalbumin) challenge caused two phases of airway obstruction [measured as changes in sGaw (specific airways conductance) using whole body plethysmography]: an immediate phase lasting between 4 and 6 h and a late phase at about 7 h. The late phase, airway hyper-responsiveness to histamine and inflammatory cell counts in BAL were all significantly reduced by either glucocorticoid. Inoculation of guinea-pigs sensitized to ovalbumin with hPIV-3 transformed the allergen-induced airway obstruction from two transient phases into a single sustained response lasting up to 12 h. This exacerbated airway obstruction and airway hyper-responsiveness to histamine were unaffected by treatment with either glucocorticoid whereas inflammatory cell counts in BAL were only partially inhibited. Virus- or allergen-induced pulmonary inflammation, individually, are glucocorticoid-sensitive, but in combination generate a phenotype where glucocorticoid efficacy is impaired. This suggests that during respiratory virus infection, glucocorticoids might be less effective in limiting pulmonary inflammation associated with asthma. [ABSTRACT FROM AUTHOR]

Published

2013

16. Functional evaluation of the receptors mediating vasoconstriction of rat aorta by trace amines and amphetamines.

Author

Broadley, Kenneth J., Fehler, Martina, Ford, William R., and Kidd, Emma J.

Subjects

*VASOCONSTRICTION, *LABORATORY rats, *AMPHETAMINES, *PHENETHYLAMINES, *PHARMACOLOGY, *SYMPATHOMIMETIC agents, *ECSTASY (Drug), *THERAPEUTICS

Abstract

Abstract: Trace amines including β-phenylethylamine (β-PEA) and amphetamines classically exert pharmacological actions via indirect sympathomimetic mechanisms. However, there is evidence for other mechanisms and this study explores the receptors mediating vasoconstriction in rat aorta. β-PEA, d-amphetamine, MDMA, cathinone and methylphenidate caused concentration-dependent contractions of rat isolated aortic rings which were unaffected by prazosin (1μM), ICI-118,551 (1μM), cocaine (10μM) and pargyline (10μM), to inhibit α1- and β2-adrenoceptors, neuronal transport and monoamine oxidase (MAO), respectively. Octopamine concentration–response curves, however, were shifted to the right. In the presence of the inhibitors, the rate of onset of octopamine contractions was slowed. Lineweaver–Burk analysis of the kinetics of the response generated different K M values for octopamine in the absence (2.35×10−6 M) and presence (6.09×10−5 M) of inhibitors, indicating mediation by different receptors. Tryptamine-induced vasoconstriction also resisted blockade by adrenergic inhibitors and the 5-HT1A, 1B, 1D and 5-HT2A receptor antagonists, methiothepin (50nM) and ketanserin (30nM), respectively. Trace amines and amphetamines therefore exert vasoconstriction independently of adrenoceptors, neuronal transport and 5-HT receptor activation. There was no evidence of tachyphylaxis or cross-tachyphylaxis of the vasoconstriction to these amines. Tyramine was a partial agonist and in its presence, β-PEA, d-amphetamine and octopamine were antagonised indicating that they all act through a common receptor for which tyramine serves as an antagonist. We conclude that the vasoconstriction is via TAAR-1, because of structural similarities between amines, ability to stimulate recombinant trace amine-associated receptor 1 (TAAR-1) and the presence of TAAR-1 in rat aorta. [Copyright &y& Elsevier]

Published

2013

17. Protective role of β2- and β3-adrenoceptors at reperfusion in isolated rat heart

Author

Penson, Peter E., Ford, William R., Kidd, Emma J., and Broadley, Kenneth J.

Published

2008

18. A comparison of antiasthma drugs between acute and chronic ovalbumin-challenged guinea-pig models of asthma

Author

Evans, Rhys L., Nials, Anthony T., Knowles, Richard G., Kidd, Emma J., Ford, William R., and Broadley, Kenneth J.

Subjects

*ANTIASTHMATIC agents, *OVALBUMINS, *GUINEA pigs as laboratory animals, *ASTHMA, *COMPARATIVE studies, *RESPIRATORY infections, *CHRONIC diseases, *ACUTE diseases

Abstract

Abstract: Pre-clinical evaluation of asthma therapies requires animal models of chronic airways inflammation, airway hyperresponsiveness (AHR) and lung remodelling that accurately predict drug effectiveness in human asthma. However, most animal models focus on acute allergen challenges where chronic inflammation and airway remodelling are absent. Chronic allergen challenge models have been developed in mice but few studies use guinea-pigs which may be more relevant to humans. We tested the hypothesis that a chronic rather than acute pulmonary inflammation model would best predict clinical outcome for asthma treatments. Guinea-pigs sensitized with ovalbumin (OVA) received single (acute) or nine OVA inhalation challenges at 48 h intervals (chronic). Airways function was recorded as specific airways conductance (sGaw) in conscious animals for 12 h after OVA challenge. AHR to inhaled histamine, inflammatory cell influx and lung histology were determined 24 h after the single or 9th OVA exposure. The inhaled corticosteroid, fluticasone propionate (FP), the phosphodiesterase 4 inhibitor, roflumilast, and the inducible nitric oxide synthase (iNOS) inhibitor, GW274150, orally, were administered 24 and 0.5 h before and 6 h after the single or final chronic OVA exposure. Both models displayed early (EAR) and late (LAR) asthmatic responses to OVA challenge, as falls in sGaw, AHR, as increased histamine-induced bronchoconstriction, and inflammatory cell influx. Tissue remodelling, seen as increased collagen and goblet cell hyperplasia, occurred after multiple OVA challenge. Treatment with FP and roflumilast inhibited the LAR, cell influx and AHR in both models, and the remodelling in the chronic model. GW274150 also inhibited the LAR, AHR and eosinophil influx in the acute model, but not, together with the remodelling, in the chronic model. In the clinical setting, inhaled corticosteroids and phosphodiesterase 4 inhibitors are relatively effective against most features of asthma whereas the iNOS inhibitor GW274150 was ineffective. Thus, while there remain certain differences between our data and clinical effectiveness of these antiasthma drugs, a chronic pulmonary inflammation guinea-pig model does appear to be a better pre-clinical predictor of potential asthma therapeutics than an acute model. [Copyright &y& Elsevier]

Published

2012

19. Clathrin-mediated endocytic proteins are upregulated in the cortex of the Tg2576 mouse model of Alzheimer’s disease-like amyloid pathology

Author

Thomas, Rhian S., Lelos, Mariah J., Good, Mark A., and Kidd, Emma J.

Subjects

*ALZHEIMER'S disease, *AMYLOID, *ENDOCYTOSIS, *GENE expression, *CLATHRIN, *LABORATORY mice

Abstract

Abstract: Amyloid-β (Aβ) is cleaved from amyloid precursor protein (APP) predominantly after APP has trafficked through the secretory pathway and then become re-internalised by endocytosis. Clathrin-mediated and, more recently, clathrin-independent endocytosis have both been implicated in this process. Furthermore, endocytic abnormalities have been identified in cases of Alzheimer’s disease (AD), however, the relevance of these changes to the aetiology of the disease remains unclear. We therefore examined the expression of proteins related to these endocytic processes in the cortex of Tg2576 mice that overexpress the Swedish mutation in APP, and consequently overexpress Aβ, to determine if there were any changes in their associated pathways. We identified significant increases in the levels of clathrin, dynamin and PICALM, all proteins intimately involved with the clathrin-mediated endocytic pathway, in the transgenic animals. However, levels of proteins associated with flotillin or caveolin-mediated endocytic pathways remained unchanged. These results emphasise the importance of clathrin-mediated endocytosis in the aetiology of AD and reinforce the results of the recent GWAS studies that identified genes for clathrin-mediated endocytosis as susceptibility genes for AD. Such studies in transgenic mice will allow us to learn more about the role of clathrin-mediated endocytosis in AD. [Copyright &y& Elsevier]

Published

2011

20. Actions of Artemisia vulgaris extracts and isolated sesquiterpene lactones against receptors mediating contraction of guinea pig ileum and trachea

Author

Natividad, Gaudencio M., Broadley, Kenneth J., Kariuki, Benson, Kidd, Emma J., Ford, William R., and Simons, Claire

Subjects

*ALTERNATIVE medicine, *AMINES, *ANALYSIS of variance, *ANIMAL experimentation, *BIOLOGICAL models, *CELL receptors, *DOSE-effect relationship in pharmacology, *GASTROINTESTINAL system, *GUINEA pigs, *HISTAMINE, *ILEUM, *LUNGS, *MEDICINAL plants, *SMOOTH muscle, *TRACHEA, *PLANT extracts

Abstract

Abstract: Aim of the study: The present study evaluates the Philippine medicinal plant Artemisia vulgaris for antagonistic activity at selected biogenic amine receptors on smooth muscle of the airways and gastrointestinal tract in order to explain its traditional use in asthma and hyperactive gut. Materials and methods: The antagonistic activity of chloroform crude extract (AV-CHCl3) and methanol crude extract (AV-MeOH) of Artemisia vulgaris was studied against concentration–response curves for contractions of the guinea pig ileum and trachea to 5-hydroxytrptamine (5-HT2 receptors), methacholine (M3 muscarinic receptors), histamine (H1 receptors) and β-phenylethylamine (trace amine-associated receptors, TAAR1). Results and discussion: The Artemisia vulgaris chloroform (AV-CHCl3) and methanol (AV-MeOH) extract showed histamine H1 antagonism in the ileum and trachea. Further analysis of AV-CHCl3 isolated two major components, yomogin and 1,2,3,4-diepoxy-11(13)-eudesmen-12,8-olide. Yomogin, a sesquiterpene lactone, exhibited a novel histamine H1 receptor antagonism in the ileum. Conclusion: The presence of a specific, competitive histamine receptor antagonist and smooth muscle relaxant activity in Artemisia vulgaris extracts on the smooth muscle in ileum and trachea explains its traditional use in the treatment of asthma and hyperactive gut. [Copyright &y& Elsevier]

Published

2011

21. Paracetamol reduces influenza-induced immunopathology in a mouse model of infection without compromising virus clearance or the generation of protective immunity.

Author

Lauder, Sarah N., Taylor, Philip R., Clark, Stephen R., Evans, Rhys L., Hindley, James P., Smart, Kathryn, Leach, Heather, Kidd, Emma J., Broadley, Kenneth J., Jones, Simon A., Wise, Matt P., Godkin, Andrew J., O'Donnell, Valerie, and Gallimore, Awen M.

Subjects

*ACETAMINOPHEN, *INFLUENZA A virus, *CELECOXIB, *MICE, *IMMUNITY, *RESPIRATORY infections

Abstract

BACKGROUND: Seasonal influenza A infection affects a significant cohort of the global population annually, resulting in considerable morbidity and mortality. Therapeutic strategies are of limited efficacy, and during a pandemic outbreak would only be available to a minority of the global population. Over-the-counter medicines are routinely taken by individuals suffering from influenza, but few studies have been conducted to determine their effectiveness in reducing pulmonary immunopathology or the influence they exert upon the generation of protective immunity. METHODS: A mouse model of influenza infection was utilised to assess the efficacy of paracetamol (acetaminophen) in reducing influenza-induced pathology and to examine whether paracetamol affects generation of protective immunity. RESULTS: Administration (intraperitoneal) of paracetamol significantly decreased the infiltration of inflammatory cells into the airway spaces, reduced pulmonary immunopathology associated with acute infection and improved the overall lung function of mice, without adversely affecting the induction of virus-specific adaptive responses. Mice treated with paracetamol exhibited an ability to resist a second infection with heterologous virus comparable with that of untreated mice. CONCLUSIONS: Our results demonstrate that paracetamol dramatically reduces the morbidity associated with influenza but does not compromise the development of adaptive immune responses. Overall, these data support the utility of paracetamol for reducing the clinical symptoms associated with influenza virus infection. [ABSTRACT FROM AUTHOR]

Published

2011

22. TPI 1020, a novel anti-inflammatory, nitric oxide donating compound, potentiates the bronchodilator effects of salbutamol in conscious guinea-pigs

Author

Turner, Dawn L., Ferrari, Nicolay, Ford, William R, Kidd, Emma J., Paquet, Luc, Renzi, Paulo, and Broadley, Kenneth J.

Subjects

*ANTI-inflammatory agents, *NITRIC oxide, *BRONCHODILATOR agents, *GUINEA pigs as laboratory animals, *HISTAMINE, *DRUG administration

Abstract

Abstract: Inhaled corticosteroids are regularly co-administered with β2-adrenoceptor agonists. This study evaluates in conscious guinea-pigs the bronchodilator effect, alone or combined with salbutamol, of TPI 1020, a novel anti-inflammatory corticosteroid and nitric oxide (NO) donor derived from budesonide. Guinea-pigs received inhaled histamine (3mM) and specific airway conductance (sGaw) measured. Responses to histamine were measured before and on the next day 15min after a 15min inhalation of vehicle, salbutamol, TPI 1020, budesonide, the NO-donor, S-nitroso-N-acetylpenicillamine (SNAP), or combinations of these drugs. Salbutamol and TPI 1020 caused concentration-dependent bronchodilatation measured as inhibition of histamine-induced bronchoconstriction. TPI 1020-induced bronchodilatation was blocked by the guanylyl cyclise inhibitor, ODQ, indicating cGMP-dependence through released NO. While salbutamol at 80μM did not exert significant bronchodilatation, significant inhibitions were observed when co-administered with TPI 1020, 0.11 and 0.33mM. The combined effects of TPI 1020 and salbutamol lasted significantly longer than either drug alone. Inhaled budesonide was a weak bronchodilator and when co-administered with salbutamol there was enhanced bronchodilatation. Addition of the NO-donor, SNAP (0.1mM), to the budesonide/salbutamol combination, also improved the inhibition of histamine-induced bronchoconstriction. This study has shown that TPI 1020 potentiates the bronchodilator activity of salbutamol, and their combination lasted longer than either drug administered individually. Both the corticosteroid and NO-releasing activities of TPI 1020 appear to be required for the potentiation of salbutamol. Combination of TPI 1020 with a β2-adrenoceptor agonist may therefore be useful against acute bronchoconstriction episodes in asthma, and may offer an opportunity for reducing doses of inhaled β2-adrenoceptor agonists. [Copyright &y& Elsevier]

Published

2010

23. Increased muscarinic receptor activity of airway smooth muscle isolated from a mouse model of allergic asthma

Author

Fernandez-Rodriguez, Sofia, Broadley, Kenneth J., Ford, William R., and Kidd, Emma J.

Subjects

*MUSCARINIC receptors, *AIRWAY (Anatomy), *SMOOTH muscle, *LABORATORY mice, *ASTHMA, *PNEUMONIA, *MUSCLE contraction, *IMMUNOGLOBULIN G

Abstract

Abstract: The mechanisms leading to airway hyper-responsiveness (AHR) in asthma are still not fully understood. AHR could be produced by hypersensitivity of the airway smooth muscle or hyperreactivity of the airways. This study was conducted to ascertain whether AHR in a murine model of asthma is produced by changes at the level of the airway smooth muscle. Airway smooth muscle responses were characterised in vitro in isolated trachea spirals from naive mice and from an acute ovalbumin (OVA) challenge model of allergic asthma. AHR was investigated in vivo in conscious, freely moving mice. Inflammatory cell influx into the lungs and antibody responses to the antigen were also measured. In vitro study of tracheal airway smooth muscle from naïve mice demonstrated concentration-related contractions to methacholine and 5-HT, but no responses to histamine or adenosine or its stable analogue, 5′-N-ethyl-carboxamidoadenosine. The contractions to 5-HT were inhibited by ketanserin and alosetron indicating involvement of 5-HT2A and 5-HT3 receptors, respectively. In an acute model of allergic asthma, OVA-treated mice were shown to be atopic by inflammatory cell influx to the lungs after OVA challenge, increases in total IgE and OVA-specific IgG levels and contractions to OVA in isolated trachea. In the asthmatic model, AHR to methacholine was demonstrated in conscious, freely moving mice in vivo and in isolated trachea in vitro 24 and 72h after OVA challenge. No AHR in vitro was seen for 5-HT, histamine or adenosine. These results suggest that, in our mouse model of asthma, changes occur at the level of the muscarinic receptor transduction pathway of coupling to airway smooth muscle contraction. These changes are maintained when tissues are removed from the inflammatory environment and for at least 3 days. [Copyright &y& Elsevier]

Published

2010

24. Establishing the phenotype in novel acute and chronic murine models of allergic asthma

Author

Fernandez-Rodriguez, Sofia, Ford, William R., Broadley, Kenneth J., and Kidd, Emma J.

Subjects

*ALLERGIES, *ASTHMA, *IMMUNOGLOBULINS, *ASTHMATICS, *IMMUNOGLOBULIN E

Abstract

Abstract: Allergic asthma is a chronic disease of the airways, with superimposed acute inflammatory episodes which correspond to exacerbations of asthma. Two novel models of allergic asthma have been developed in mice receiving the same allergen sensitisation, but with acute or chronic allergen exposures, the latter to mimic the human situation more closely. Ovalbumin-sensitised mice were challenged by ovalbumin inhalation twice on the same day for the acute model, and 18 times over a period of 6 weeks for the chronic model. Lung function was monitored in conscious, unrestrained mice immediately after the last challenge for up to 12 h. Airway responsiveness to inhaled methacholine and serum antibody levels were determined 24 h after challenge. Bronchoalveolar inflammatory cell recruitment was determined at 2 or 24 h. Acute and chronically treated mice had similar early and late asthmatic responses peaking at 2 h and 7---8 h, respectively. IgE and IgG antibody levels, compared with naïve mice, and eosinophil infiltration, compared with naïve and saline challenge, were elevated. Airway hyperresponsiveness to methacholine was observed 24 h after challenge in both models. The acute model had higher levels of eosinophilia, whereas the chronic model showed hyperresponsiveness to lower doses of methacholine and had higher levels of total IgE and ovalbumin-specific IgG antibodies. Both novel murine models of allergic asthma bear a close resemblance to human asthma, each offering particular advantages for studying the mechanisms underlying asthma and for evaluating existing and novel therapeutic agents. [Copyright &y& Elsevier]

Published

2008

25. An antibody to the β-secretase cleavage site on amyloid-β-protein precursor inhibits amyloid-β production.

Author

Thomas, Rhian S., Liddell, J. Eryl, Murphy, Lynne S., Pache, David M., and Kidd, Emma J.

Subjects

*ALZHEIMER'S disease, *MONOCLONAL antibodies, *AMYLOID, *GLYCOPROTEINS, *MEDICAL research

Abstract

Proteolytic cleavage of amyloid-β-protein precursor (AβPP) by β- and γ-secretases results in production of the amyloid-β peptide (Aβ) that accumulates in the brains of sufferers of Alzheimer's disease (AD). We have developed a monoclonal antibody, 2B12, which binds in the vicinity of the β-secretase cleavage site on AβPP but does not bind within the Aβ region. We hypothesised that this antibody, directed against the substrate rather than the enzyme, could inhibit cleavage of AβPP by β-secretase via steric hindrance and thus reduce downstream production of Aβ. The antibody would enter cells by binding to AβPP when it is at the cell surface and then be internalised with the protein. We subsequently demonstrated that, after addition of 2B12 to standard growth media, this antibody was indeed capable of inhibiting Aβ40 production in neuroblastoma and astrocytoma cells expressing native AβPP, as measured by an ELISA. This inhibition was both concentration- and time-dependent and was specific to 2B12. We were only able to inhibit approximately 50% of Aβ40 production suggesting that not all AβPP is trafficked to the cell surface. We propose that this antibody could be used as a novel, putative therapy for the treatment of AD. [ABSTRACT FROM AUTHOR]

Published

2006

26. Correction to: ACE2 activation protects against cognitive decline and reduces amyloid pathology in the Tg2576 mouse model of Alzheimer's disease.

Author

Evans, Charles E., Miners, James S., Piva, Giulia, Willis, Christine L., Heard, David M., Kidd, Emma J., Good, Mark A., and Kehoe, Patrick G.

Subjects

*ALZHEIMER'S disease, *SPINAL tuberculosis, *TRANSGENIC mice, *MICE, *PATHOLOGY

Abstract

Unfortunately, the acknowledgement section was not included in the original publication. [ABSTRACT FROM AUTHOR]

Published

2020

27. Warm-coding deficits and aberrant inflammatory pain in mice lacking P2X[sub3] receptors.

Author

Souslova, Veronika, Cesare, Paolo, Ding, Yanning, Akopian, Armen N., Stanfa, Louise, Suzuki, Rie, Carpenter, Katherine, Dickenson, Anthony, Boyce, Susan, Hill, Ray, Nebenius-Oosthuizen, Daniela, Smith, Andrew J.H., Kidd, Emma J., and Wood, John N.

Subjects

*ADENOSINE triphosphate, *GENETICS, *NEURAL transmission, *PAIN, *HYPERALGESIA

Abstract

Demonstrates the results of ablation and deletion of the ATP receptor P2X[sub3] gene. Effect of ablation on the function of ganglion neurons, sensorimotor function, responses to noxious mechanical and thermal stimuli, and formalin-induced pain behavior; Deletion of the P2X[sub3] receptor, which causes thermal hyperalgesia in chronic inflammation and other abnormal thermal responses.

Published

2000