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3. Dissecting the contribution of human chromosome 21 syntenic regions to recognition memory processes in adult and aged mouse models of Down syndrome.

Author

Canonica, Tara, Kidd, Emma J., Gibbins, Dorota, Lana-Elola, Eva, Fisher, Elizabeth M. C., Tybulewicz, Victor L. J., and Good, Mark

Subjects
RECOGNITION (Psychology), LABORATORY mice, DOWN syndrome, COGNITIVE ability, HUMAN chromosomes, ANIMAL cognition, FRAGILE X syndrome, PROTEIN receptors
Abstract

Background: Trisomy of human chromosome 21 (Hsa21) results in a constellation of features known as Down syndrome (DS), the most common genetic form of intellectual disability. Hsa21 is orthologous to three regions in the mouse genome on mouse chromosome 16 (Mmu16), Mmu17 and Mmu10. We investigated genotype-phenotype relationships by assessing the contribution of these three regions to memory function and age-dependent cognitive decline, using three mouse models of DS, Dp1Tyb, Dp(17)3Yey, Dp(10)2Yey, that carry an extra copy of the Hsa21-orthologues on Mmu16, Mmu17 and Mmu10, respectively. Hypothesis: Prior research on cognitive function in DS mouse models has largely focused on models with an extra copy of the Mmu16 region and relatively little is known about the effects of increased copy number on Mmu17 and Mmu10 on cognition and how this interacts with the effects of aging. As aging is is a critical contributor to cognitive and psychiatric changes in DS, we hypothesised that ageing would differentially impact memory function in Dp1Tyb, Dp(17)3Yey, and Dp(10)2Yey, models of DS. Methods: Young (12-13 months and old (18-20 months mice Dp1Tyb, Dp(17)3Yey and Dp(10)2Yey mice were tested on a battery of object recognition memory test that assessed object novelty detection, novel location detection and associative object-in place memory. Following behavioral testing, hippocampal and frontal cortical tissue was analysed for expression of glutamatergic receptor proteins using standard immunoblot techniques. Results: Young (12-13 months and old (18-20 months mice Dp1Tyb, Dp(17)3Yey and Dp(10)2Yey mice were tested on a battery of object recognition memory test that assessed object novelty detection, novel location detection and associative object-in place memory. Following behavioral testing, hippocampal and frontal cortical tissue was analysed for expression of glutamatergic receptor proteins using standard immunoblot techniques. Conclusion: Our results show that distinct Hsa21-orthologous regions contribute differentially to cognitive dysfunction in DS mouse models and that aging interacts with triplication of Hsa21-orthologous genes on Mmu10. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Characterization of Negative Allosteric Modulators of the Calcium-Sensing Receptor for Repurposing as a Treatment of Asthma

Author

Yarova, Polina L., primary, Huang, Ping, additional, Schepelmann, Martin W., additional, Bruce, Richard, additional, Ecker, Rupert, additional, Nica, Robert, additional, Telezhkin, Vsevolod, additional, Traini, Daniela, additional, Gomes dos Reis, Larissa, additional, Kidd, Emma J., additional, Ford, William R., additional, Broadley, Kenneth J., additional, Kariuki, Benson M., additional, Corrigan, Christopher J., additional, Ward, Jeremy P.T., additional, Kemp, Paul J., additional, and Riccardi, Daniela, additional

Published
2020
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7. 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
nervous system, Visual Perception, Cognitive Science
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 kf] 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 kf, but not with any differences in neurite microstructure. In women, age mediated the effects of VFF on fornix MPF and kf, 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.

Published
2019
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9. 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
Male, Amyloid, Aging, N-Methylaspartate, βCTF antibody, BACE1, Mice, Transgenic, Hippocampus, Receptors, N-Methyl-D-Aspartate, Article, Amyloid beta-Protein Precursor, amyloid, amyloid precursor protein, BACE1, hippocampus, memory, NMDA, βCTF antibody, NMDA, Memory, Alzheimer Disease, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Amyloid Precursor Protein Secretases
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

Published
2019

10. Warm-coding deficits and aberrant inflammatory pain in mice lacking P2X 3 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
Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Author(s): Veronika Souslova [1]; Paolo Cesare [1]; Yanning Ding [1]; Armen N. Akopian [1]; Louise Stanfa [2]; Rie Suzuki [2]; Katherine Carpenter [2]; Anthony Dickenson [2]; Susan Boyce [3]; Ray [...]

Published
2000
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11. Route of administration affects corticosteroid sensitivity of a combined ovalbumin and lipopolysaccharide model of asthma exacerbation in guinea-pigs

Author

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

Subjects
respiratory system, RS
Abstract

Lipopolysaccharide (LPS) contributes to asthma exacerbations and development of inhaled corticosteroid insensitivity. Complete resistance to systemic corticosteroids is rare and most patients lie on a continuum of steroid responsiveness. The objective of this study was to examine the sensitivity of combined ovalbumin- (Ova) and LPS-induced functional and inflammatory responses to inhaled and systemic corticosteroid in conscious guinea-pigs, to test the hypothesis that the route of administration affects its sensitivity. Guinea-pigs were sensitised to Ova and challenged with inhaled Ova alone or combined with LPS. Airways function was determined by measuring specific airways conductance via whole-body plethysmography. Airways hyperresponsiveness to histamine was determined pre- and 24h post-Ova challenge. Airways inflammation and underlying mechanisms were determined from bronchoalveolar lavage cell counts and lung tissue cytokines. Vehicle or dexamethasone was administered by once-daily intraperitoneal injection (5, 10 or 20 mg/kg) or twice-daily inhalation (4 or 20 mg/ml) for 6 days before Ova challenge or Ova with LPS. LPS exacerbated Ova-induced responses, elongating early asthmatic responses (EAR), prolonging bronchoconstriction by histamine and further elevating airways inflammation. Intraperitoneal dexamethasone (20 mg/kg) significantly reduced the elongated EAR and airways inflammation but not the increased bronchoconstriction to histamine. In contrast, inhaled dexamethasone (20 mg/ml), which inhibited responses to Ova alone, did not significantly reduce functional and inflammatory responses to combined Ova and LPS. Combined Ova and LPS-induced functional and inflammatory responses are insensitive to inhaled but only partially sensitive to systemic dexamethasone. These results suggest that the route of corticosteroid administration may be important in determining the sensitivity of asthmatic responses to these agents.

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
Cellular and Molecular Neuroscience
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.

Published
2016

15. correction: Warm-coding deficits and aberrant inflammatory pain in mice lacking P2X3

Author

Souslova, Veronika, Cesare, Paolo, Ding, Yanning, Akoplan, Armen N., Stanfa, Louise, Suzuki, Rie, Carpenter, Katherine, Nebenius-Oosthuizen, Daniela, Smith, Andrew J. H., Kidd, Emma J., and Wood, John N.

Subjects
Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Author(s): Veronika Souslova; Paolo Cesare; Yanning Ding; Armen N. Akoplan; Louise Stanfa; Rie Suzuki; Katherine Carpenter; Daniela Nebenius-Oosthuizen; Andrew J. H. Smith; Emma J. Kidd; John N. Wood Nature 407 [...]

Published
2001
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18. Effects of dietary amines on the gut and its vasculature.

Author

Broadley, Kenneth J., Akhtar Anwar, M., Herbert, Amy A., Fehler, Martina, Jones, Elen M., Davies, Wyn E., Kidd, Emma J., and Ford, William R.

Abstract

Trace amines, including tyramine and β-phenylethylamine (β-PEA), are constituents of many foods including chocolate, cheeses and wines and are generated by so-called ‘friendly’ bacteria such as Lactobacillus, Lactococcus and Enterococcus species, which are found in probiotics. We therefore examined whether these dietary amines could exert pharmacological effects on the gut and its vasculature. In the present study we examined the effects of tyramine and β-PEA on the contractile activity of guinea-pig and rat ileum and upon the isolated mesenteric vasculature and other blood vessels. Traditionally, these amines are regarded as sympathomimetic amines, exerting effects through the release of noradrenaline from sympathetic nerve endings, which should relax the gut. A secondary aim was therefore to confirm this mechanism of action. However, contractile effects were observed in the gut and these were independent of noradrenaline, acetylcholine, histamine and serotonin receptors. They were therefore probably due to the recently described trace amine-associated receptors. These amines relaxed the mesenteric vasculature. In contrast, the aorta and coronary arteries were constricted, a response that was also independent of a sympathomimetic action. From these results, we propose that after ingestion, trace amines could stimulate the gut and improve intestinal blood flow. Restriction of blood flow elsewhere diverts blood to the gut to aid digestion. Thus, trace amines in the diet may promote the digestive process through stimulation of the gut and improved gastrointestinal circulation. [ABSTRACT FROM PUBLISHER]

Published
2009
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20. Calcium-sensing receptor antagonists abrogate airway hyperresponsiveness and inflammation in allergic asthma

Author

Yarova, Polina L., Stewart, Alecia L., Sathish, Venkatachalem, Britt, Rodney D., Thompson, Michael A., Lowe, Alexander P. P., Freeman, Michelle, Aravamudan, Bharathi, Kita, Hirohito, Brennan, Sarah C., Schepelmann, Martin, Davies, Thomas, Yung, Sun, Cholisoh, Zakky, Kidd, Emma J., Ford, William R., Broadley, Kenneth J., Rietdorf, Katja, Chang, Wenhan, Bin Khayat, Mohd E., Ward, Donald T., Corrigan, Christopher J., T. Ward, Jeremy P., Kemp, Paul J., Pabelick, Christina M., Prakash, Y. S., Riccardi, Daniela, Yarova, Polina L., Stewart, Alecia L., Sathish, Venkatachalem, Britt, Rodney D., Thompson, Michael A., Lowe, Alexander P. P., Freeman, Michelle, Aravamudan, Bharathi, Kita, Hirohito, Brennan, Sarah C., Schepelmann, Martin, Davies, Thomas, Yung, Sun, Cholisoh, Zakky, Kidd, Emma J., Ford, William R., Broadley, Kenneth J., Rietdorf, Katja, Chang, Wenhan, Bin Khayat, Mohd E., Ward, Donald T., Corrigan, Christopher J., T. Ward, Jeremy P., Kemp, Paul J., Pabelick, Christina M., Prakash, Y. S., and Riccardi, Daniela

Abstract

Airway hyperresponsiveness and inflammation are fundamental hallmarks of allergic asthma that are accompanied by increases in certain polycations, such as eosinophil cationic protein. Levels of these cations in body fluids correlate with asthma severity. We show that polycations and elevated extracellular calcium activate the human recombinant and native calcium-sensing receptor (CaSR), leading to intracellular calcium mobilization, cyclic adenosine monophosphate breakdown, and p38 mitogen-activated protein kinase phosphorylation in airway smooth muscle (ASM) cells. These effects can be prevented by CaSR antagonists, termed calcilytics. Moreover, asthmatic patients and allergen-sensitized mice expressed more CaSR in ASMs than did their healthy counterparts. Indeed, polycations induced hyperreactivity in mouse bronchi, and this effect was prevented by calcilytics and absent in mice with CaSR ablation from ASM. Calcilytics also reduced airway hyperresponsiveness and inflammation in allergen-sensitized mice in vivo. These data show that a functional CaSR is up-regulated in asthmatic ASM and targeted by locally produced polycations to induce hyperresponsiveness and inflammation. Thus, calcilytics may represent effective asthma therapeutics.

21. Calcium-sensing receptor antagonists abrogate airway hyperresponsiveness and inflammation in allergic asthma

Author

Yarova, Polina L., Stewart, Alecia L., Sathish, Venkatachalem, Britt, Rodney D., Thompson, Michael A., Lowe, Alexander P. P., Freeman, Michelle, Aravamudan, Bharathi, Kita, Hirohito, Brennan, Sarah C., Schepelmann, Martin, Davies, Thomas, Yung, Sun, Cholisoh, Zakky, Kidd, Emma J., Ford, William R., Broadley, Kenneth J., Rietdorf, Katja, Chang, Wenhan, Bin Khayat, Mohd E., Ward, Donald T., Corrigan, Christopher J., T. Ward, Jeremy P., Kemp, Paul J., Pabelick, Christina M., Prakash, Y. S., Riccardi, Daniela, Yarova, Polina L., Stewart, Alecia L., Sathish, Venkatachalem, Britt, Rodney D., Thompson, Michael A., Lowe, Alexander P. P., Freeman, Michelle, Aravamudan, Bharathi, Kita, Hirohito, Brennan, Sarah C., Schepelmann, Martin, Davies, Thomas, Yung, Sun, Cholisoh, Zakky, Kidd, Emma J., Ford, William R., Broadley, Kenneth J., Rietdorf, Katja, Chang, Wenhan, Bin Khayat, Mohd E., Ward, Donald T., Corrigan, Christopher J., T. Ward, Jeremy P., Kemp, Paul J., Pabelick, Christina M., Prakash, Y. S., and Riccardi, Daniela

Abstract

Airway hyperresponsiveness and inflammation are fundamental hallmarks of allergic asthma that are accompanied by increases in certain polycations, such as eosinophil cationic protein. Levels of these cations in body fluids correlate with asthma severity. We show that polycations and elevated extracellular calcium activate the human recombinant and native calcium-sensing receptor (CaSR), leading to intracellular calcium mobilization, cyclic adenosine monophosphate breakdown, and p38 mitogen-activated protein kinase phosphorylation in airway smooth muscle (ASM) cells. These effects can be prevented by CaSR antagonists, termed calcilytics. Moreover, asthmatic patients and allergen-sensitized mice expressed more CaSR in ASMs than did their healthy counterparts. Indeed, polycations induced hyperreactivity in mouse bronchi, and this effect was prevented by calcilytics and absent in mice with CaSR ablation from ASM. Calcilytics also reduced airway hyperresponsiveness and inflammation in allergen-sensitized mice in vivo. These data show that a functional CaSR is up-regulated in asthmatic ASM and targeted by locally produced polycations to induce hyperresponsiveness and inflammation. Thus, calcilytics may represent effective asthma therapeutics.

22. Route of Administration Affects Corticosteroid Sensitivity of a Combined Ovalbumin and Lipopolysaccharide Model of Asthma Exacerbation in Guinea Pigs.

Author

Lowe APP, Thomas RS, Nials AT, Kidd EJ, Broadley KJ, and Ford WR

Subjects
Administration, Inhalation, Animals, Asthma metabolism, Bronchial Hyperreactivity chemically induced, Bronchial Hyperreactivity drug therapy, Bronchial Hyperreactivity metabolism, Drug Administration Routes, Drug Combinations, Guinea Pigs, Injections, Intraperitoneal, Lipopolysaccharides administration & dosage, Male, Ovalbumin administration & dosage, Respiratory Hypersensitivity chemically induced, Respiratory Hypersensitivity drug therapy, Respiratory Hypersensitivity metabolism, Adrenal Cortex Hormones administration & dosage, Asthma chemically induced, Asthma drug therapy, Lipopolysaccharides toxicity, Ovalbumin toxicity
Abstract

Lipopolysaccharide (LPS) contributes to asthma exacerbations and development of inhaled corticosteroid insensitivity. Complete resistance to systemic corticosteroids is rare, and most patients lie on a continuum of steroid responsiveness. This study aimed to examine the sensitivity of combined ovalbumin- (Ova) and LPS-induced functional and inflammatory responses to inhaled and systemic corticosteroid in conscious guinea pigs to test the hypothesis that the route of administration affects sensitivity. Guinea pigs were sensitized to Ova and challenged with inhaled Ova alone or combined with LPS. Airway function was determined by measuring specific airway conductance via whole-body plethysmography. Airway hyper-responsiveness to histamine was determined before and 24 hours post-Ova challenge. Airway inflammation and underlying mechanisms were determined from bronchoalveolar lavage cell counts and lung tissue cytokines. Vehicle or dexamethasone was administered by once-daily i.p. injection (5, 10, or 20 mg/kg) or twice-daily inhalation (4 or 20 mg/ml) for 6 days before Ova challenge or Ova with LPS. LPS exacerbated Ova-induced responses, elongating early asthmatic responses (EAR), prolonging histamine bronchoconstriction, and further elevating airway inflammation. Intraperitoneal dexamethasone (20 mg/kg) significantly reduced the elongated EAR and airway inflammation but not the increased bronchoconstriction to histamine. In contrast, inhaled dexamethasone (20 mg/ml), which inhibited responses to Ova alone, did not significantly reduce functional and inflammatory responses to combined Ova and LPS. Combined Ova and LPS-induced functional and inflammatory responses are insensitive to inhaled, but they are only partially sensitive to systemic, dexamethasone. This finding suggests that the route of corticosteroid administration may be important in determining corticosteroid sensitivity of asthmatic responses., (Copyright © 2017 by The Author(s).)

Published
2017
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