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1. Unilateral hindlimb ischaemia‐induced systemic inflammation is associated with non‐ischaemic skeletal muscle inflammation

Author

William S. Evans, Gabriel S. Pena, Beata Gelman, Sarah Kuzmiak‐Glancy, and Steven J. Prior

Subjects
angiogenesis, macrophage, muscle atrophy, neutrophil, Physiology, QP1-981
Abstract

Abstract Skeletal muscle atrophy and dysfunction commonly accompany cardiovascular diseases such as peripheral arterial disease and may be partially attributable to systemic inflammation. We sought to determine whether acute systemic inflammation in a model of hindlimb ischaemia (HLI) could affect skeletal muscle macrophage infiltration, fibre size, or capillarization, independent of the ischaemia. Eight‐week‐old C57BL/6 male mice underwent either Sham or HLI surgery, and were killed 1, 3, or 7 days post‐surgery. Circulating inflammatory cytokine concentrations were measured, as well as immune cell infiltration and morphology of skeletal muscle from both limbs of HLI and Sham mice. In HLI compared with Sham mice at day 1, plasma interleukin‐1β levels were 216% higher (0.48 ± 0.10 vs. 0.15 ± 0.01 pg/μL, P = 0.005) and decreased by day 3. This was followed by increased macrophage presence in muscle from both ischaemic and non‐ischaemic limbs of HLI mice by day 7 (7.3‐ and 2.3‐fold greater than Sham, respectively, P

Published
2024
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2. A tool for integrating agrometeorological observation data for digital agriculture: A Minnesota case study

Author

Logan Gall, Tom Glancy, Michael Kantar, and Bryan C. Runck

Subjects
Agriculture, Environmental sciences, GE1-350
Abstract

Abstract Agrometeorological data are essential for understanding production using digital agriculture techniques. However, integrating agrometerological observations from multiple sources remains a challenge. Often, digital agriculture scientists download and clean the same datasets many times. We present a prototype system that simplifies the process of collecting, cleaning, integrating, and aggregating data from meteorological data sources by providing a simplified user interface, database, and application programming interface. The prototype provides a standard interface for querying multiple geospatial formats (raster and vector) and integrates observation networks including the National Oceanic and Atmospheric Administration Global Historical Climatology Network (NOAA GHCN), NOAA NClim‐Grid (NOAA's Gridded Climate Normals), and Ameriflux BASE. The system automatically checks and updates data, saving storage space and processing time, and allows users to summarize data spatially and temporally. Provided as open source code and browser‐based user interface, the application and integration system can be run across Windows, Linux, and Mac environments to support broader use of multi‐source agrometeorology data.

Published
2024
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4. Addition of hyaluronic acid to the FIB‐4 liver fibrosis score improves prediction of incident cirrhosis and hepatocellular carcinoma in type 2 diabetes: The Edinburgh Type 2 Diabetes Study

Author

Sheila M. Grecian, Stela McLachlan, Jonathan A. Fallowfield, Peter C. Hayes, Indra Neil Guha, Joanne R. Morling, Stephen Glancy, Rachel M. Williamson, Rebecca M. Reynolds, Brian M. Frier, Nicola N. Zammitt, Jackie F. Price, and Mark W. J. Strachan

Subjects
hyaluronic acid, NAFLD, risk prediction, type 2 diabetes, Internal medicine, RC31-1245
Abstract

Abstract Background Type 2 diabetes (T2D) is associated with increased risk of progression to cirrhosis and hepatocellular carcinoma (HCC) in people with chronic liver diseases, particularly non‐alcoholic fatty liver disease (NAFLD). However, the absolute risk of progression is low. So, it is crucial to accurately identify patients who would benefit most from hepatology referral and intensified management. Current risk‐stratification tools are suboptimal and perform worse in people with diabetes. Aims To determine whether the addition of complementary biomarker(s) to current NAFLD risk‐stratification tools in people with T2D could improve the identification of people who are at increased risk of developing incident cirrhosis or HCC. Methods The Edinburgh Type 2 diabetes Study (ET2DS) is a cohort study of men and women with T2D (n = 1066, age 60–75 at baseline). Cases of cirrhosis and HCC were identified over 11 years of follow‐up. Biomarkers were measured at baseline and year 1 and association with incident disease was assessed using logistic regression. Results Of existing risk‐stratification scores tested, the Fibrosis‐4 (FIB‐4) index and the AST:platelet ratio index (APRI) performed best in this cohort. Addition of hyaluronic acid (cut‐point ≥ 50 μ g/L) to FIB‐4 (cut‐point ≥ 1.3) maintained a false negative rate of ≤25% and reduced the number of people incorrectly identified as “high risk” for incident disease by ∼50%. Conclusions The addition of hyaluronic acid to FIB‐4 reduced the proportion of people inappropriately identified as “high risk” for development of cirrhosis/HCC in a community population of otherwise asymptomatic people with T2D. These findings require a validation in independent cohorts.

Published
2021
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5. Prevalence of opioid dependence in Scotland 2015–2020: A multi‐parameter estimation of prevalence (MPEP) study

Author

Markoulidakis, Andreas, primary, Hickman, Matthew, additional, McAuley, Andrew, additional, Barnsdale, Lee R., additional, Welton, Nicky J., additional, Glancy, Megan, additional, Shivaji, Tara, additional, Collins, Craig, additional, Lang, Jaroslaw, additional, de Wit, Femke, additional, Hunt, Gordon, additional, Wilkinson, Levin, additional, Fraser, Rosalyn, additional, Yeung, Alan, additional, Horsburgh, Kirsten, additional, Priyadarshi, Saket, additional, Hutchinson, Sharon J., additional, and Jones, Hayley E., additional

Published
2024
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7. Cover Image, Volume 239, Number 4, April 2024

Author

Hinton, Antentor, primary, Katti, Prasanna, additional, Mungai, Margaret, additional, Hall, Duane D., additional, Koval, Olha, additional, Shao, Jianqiang, additional, Vue, Zer, additional, Lopez, Edgar Garza, additional, Rostami, Rahmati, additional, Neikirk, Kit, additional, Ponce, Jessica, additional, Streeter, Jennifer, additional, Schickling, Brandon, additional, Bacevac, Serif, additional, Grueter, Chad, additional, Marshall, Andrea, additional, Beasley, Heather K., additional, Do Koo, Young, additional, Bodine, Sue C., additional, Nava, Nayeli G. Reyes, additional, Quintana, Anita M., additional, Song, Long‐Sheng, additional, Grumbach, Isabella M., additional, Pereira, Renata O., additional, Glancy, Brian, additional, and Abel, E. Dale, additional

Published
2024
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9. ATF4‐dependent increase in mitochondrial‐endoplasmic reticulum tethering following OPA1 deletion in skeletal muscle

Author

Hinton, Antentor, primary, Katti, Prasanna, additional, Mungai, Margaret, additional, Hall, Duane D., additional, Koval, Olha, additional, Shao, Jianqiang, additional, Vue, Zer, additional, Lopez, Edgar Garza, additional, Rostami, Rahmati, additional, Neikirk, Kit, additional, Ponce, Jessica, additional, Streeter, Jennifer, additional, Schickling, Brandon, additional, Bacevac, Serif, additional, Grueter, Chad, additional, Marshall, Andrea, additional, Beasley, Heather K., additional, Do Koo, Young, additional, Bodine, Sue C., additional, Nava, Nayeli G. Reyes, additional, Quintana, Anita M., additional, Song, Long‐Sheng, additional, Grumbach, Isabella M., additional, Pereira, Renata O., additional, Glancy, Brian, additional, and Abel, E. Dale, additional

Published
2024
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11. 3D reconstruction of murine mitochondria reveals changes in structure during aging linked to the MICOS complex

Author

Vue, Zer, primary, Garza‐Lopez, Edgar, additional, Neikirk, Kit, additional, Katti, Prasanna, additional, Vang, Larry, additional, Beasley, Heather, additional, Shao, Jianqiang, additional, Marshall, Andrea G., additional, Crabtree, Amber, additional, Murphy, Alexandria C., additional, Jenkins, Brenita C., additional, Prasad, Praveena, additional, Evans, Chantell, additional, Taylor, Brittany, additional, Mungai, Margaret, additional, Killion, Mason, additional, Stephens, Dominique, additional, Christensen, Trace A., additional, Lam, Jacob, additional, Rodriguez, Benjamin, additional, Phillips, Mark A., additional, Daneshgar, Nastaran, additional, Koh, Ho‐Jin, additional, Koh, Alice, additional, Davis, Jamaine, additional, Devine, Nina, additional, Muhammod, Saleem, additional, Scudese, Estevão, additional, Arnold, Kenneth Ryan, additional, Vanessa Chavarin, Valeria, additional, Daniel Robinson, Ryan, additional, Chakraborty, Moumita, additional, Gaddy, Jennifer A., additional, Sweetwyne, Mariya T., additional, Wilson, Genesis, additional, Zaganjor, Elma, additional, Kezos, James, additional, Dondi, Cristiana, additional, Reddy, Anilkumar K., additional, Glancy, Brian, additional, Kirabo, Annet, additional, Quintana, Anita M., additional, Dai, Dao‐Fu, additional, Ocorr, Karen, additional, Murray, Sandra A., additional, Damo, Steven M., additional, Exil, Vernat, additional, Riggs, Blake, additional, Mobley, Bret C., additional, Gomez, Jose A., additional, McReynolds, Melanie R., additional, and Hinton, Antentor, additional

Published
2023
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13. A Comprehensive Approach to Sample Preparation for Electron Microscopy and the Assessment of Mitochondrial Morphology in Tissue and Cultured Cells

Author

Hinton, Antentor, primary, Katti, Prasanna, additional, Christensen, Trace A., additional, Mungai, Margaret, additional, Shao, Jianqiang, additional, Zhang, Liang, additional, Trushin, Sergey, additional, Alghanem, Ahmad, additional, Jaspersen, Adam, additional, Geroux, Rachel E., additional, Neikirk, Kit, additional, Biete, Michelle, additional, Lopez, Edgar Garza, additional, Shao, Bryanna, additional, Vue, Zer, additional, Vang, Larry, additional, Beasley, Heather K., additional, Marshall, Andrea G., additional, Stephens, Dominique, additional, Damo, Steven, additional, Ponce, Jessica, additional, Bleck, Christopher K. E., additional, Hicsasmaz, Innes, additional, Murray, Sandra A., additional, Edmonds, Ranthony A. C., additional, Dajles, Andres, additional, Koo, Young Do, additional, Bacevac, Serif, additional, Salisbury, Jeffrey L., additional, Pereira, Renata O., additional, Glancy, Brian, additional, Trushina, Eugenia, additional, and Abel, E. Dale, additional

Published
2023
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14. Systematic Transmission Electron Microscopy‐Based Identification and 3D Reconstruction of Cellular Degradation Machinery

Author

Neikirk, Kit, primary, Vue, Zer, additional, Katti, Prasanna, additional, Rodriguez, Ben I., additional, Omer, Salem, additional, Shao, Jianqiang, additional, Christensen, Trace, additional, Garza Lopez, Edgar, additional, Marshall, Andrea, additional, Palavicino‐Maggio, Caroline B., additional, Ponce, Jessica, additional, Alghanem, Ahmad F., additional, Vang, Larry, additional, Barongan, Taylor, additional, Beasley, Heather K., additional, Rodman, Taylor, additional, Stephens, Dominique, additional, Mungai, Margaret, additional, Correia, Marcelo, additional, Exil, Vernat, additional, Damo, Steven, additional, Murray, Sandra A., additional, Crabtree, Amber, additional, Glancy, Brian, additional, Pereira, Renata O., additional, Abel, E. Dale, additional, and Hinton, Antentor O., additional

Published
2023
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15. Development, preliminary validation and reliability of the colourful ‘My Feelings Form’ self‐report for young children

Author

Aisling Mulligan, Natthaphol Sresthaporn, Sinead Mulroy, Tara Rudd, Anne Coffey, Maria Joyce, Veselina Gadancheva, and Caoimhe Glancy

Subjects
Psychiatry and Mental health, Pediatrics, Perinatology and Child Health
Abstract

Patient-reported outcome measures place the patient at the centre of his/her care. There are calls to introduce child-reported outcome measures to mental health services. We aimed to (a) develop an age-appropriate patient-reported outcome measure for children's mental health, and (b) validate this in a primary school and Child and Adolescent Mental Health Service (CAMHS).A list of items to measure children's mental health was proposed (Draft 1) and revised to 14 items following focus group and user consultation (Draft 2). A colourful, cartoon and emoji version was created in consultation with children (Draft 3); a professional cartoon artist created the final 'My Feelings Form' (MFF), with usability feedback (Draft 4). The MFF was tested by 317 children aged 4-13 years from one mixed-gender primary school at two time points in 1 day, and 25 children aged 4-13 years from CAMHS. Results were analysed using test-retest reliability and exploratory factor analysis; a receiver operator characteristic curve was constructed.The CAMHS group scored significantly higher than the school group for the mean total score (23.5 ± 11.3 vs. 16.1 ± 6.2) and for 10 items. Test-retest reliability was acceptable (correlation = 0.74, p .001). Exploratory factor analysis using 10 informative items identified two factors - emotional factor (Cronbach's alpha = 0.74) and function factor (Cronbach's alpha = 0.59). The revised 10-item form has a Cronbach's alpha of 0.77; a cut-off of 12 has a sensitivity of 80% and specificity of 60%, indicating that it correctly identified 80% of those who were attending CAMHS and gave 60% of the schoolchildren a negative result.The colourful MFF was co-produced with children, and preliminary data suggest that it is a useful patient-reported outcome measure for children's mental health.

Published
2022
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16. A Comprehensive Approach to Sample Preparation for Electron Microscopy and the Assessment of Mitochondrial Morphology in Tissue and Cultured Cells

Author

Antentor Hinton, Prasanna Katti, Trace A. Christensen, Margaret Mungai, Jianqiang Shao, Liang Zhang, Sergey Trushin, Ahmad Alghanem, Adam Jaspersen, Rachel E. Geroux, Kit Neikirk, Michelle Biete, Edgar Garza Lopez, Bryanna Shao, Zer Vue, Larry Vang, Heather K. Beasley, Andrea G. Marshall, Dominique Stephens, Steven Damo, Jessica Ponce, Christopher K. E. Bleck, Innes Hicsasmaz, Sandra A. Murray, Ranthony A. C. Edmonds, Andres Dajles, Young Do Koo, Serif Bacevac, Jeffrey L. Salisbury, Renata O. Pereira, Brian Glancy, Eugenia Trushina, and E. Dale Abel

Subjects
Biomaterials, Biomedical Engineering, General Biochemistry, Genetics and Molecular Biology
Published
2023
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19. Mitochondrial lactate metabolism: history and implications for exercise and disease

Author

Matthew L. Goodwin, Wayne T. Willis, Daniel A. Kane, L. Bruce Gladden, Brian Glancy, and Andreas N. Kavazis

Subjects
0301 basic medicine, Physiology, Mitochondrial disease, Oxidative phosphorylation, Mitochondrion, Oxidative Phosphorylation, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Glycolysis, ATP synthase, biology, Chemiosmosis, Chemistry, NAD, medicine.disease, Electron transport chain, Mitochondria, 030104 developmental biology, Mitochondrial matrix, Biophysics, biology.protein, Energy Metabolism, Oxidation-Reduction, 030217 neurology & neurosurgery
Abstract

Mitochondrial structures were probably observed microscopically in the 1840s, but the idea of oxidative phosphorylation (OXPHOS) within mitochondria did not appear until the 1930s. The foundation for research into energetics arose from Meyerhof’s experiments on oxidation of lactate in isolated muscles recovering from electrical contractions in an O(2) atmosphere. Today, we know that mitochondria are actually reticula and that the energy released from electron pairs being passed along the electron transport chain from NADH to O(2) generates a membrane potential and pH gradient of protons that can enter the molecular machine of ATP Synthase to resynthesize ATP. Lactate stands at the crossroads of glycolytic and oxidative energy metabolism. Based on reported research and our own modeling in silico, we contend that lactate is not directly oxidized in the mitochondrial matrix. Instead, the interim glycolytic products (pyruvate and NADH) are held in cytosolic equilibrium with the products of the lactate dehydrogenase (LDH) reaction and the intermediates of the malate-aspartate and glycerol 3-phosphate shuttles. This equilibrium supplies the glycolytic products to the mitochondrial matrix for OXPHOS. LDH in the mitochondrial matrix is not compatible with the cytoplasmic/matrix redox gradient; its presence would drain matrix reducing power and substantially dissipate the proton motive force. OXPHOS requires O(2) as the final electron acceptor, but O(2) supply is sufficient in most situations, including exercise and often acute illness. Recent studies suggest that atmospheric normoxia may constitute a cellular hyperoxia in mitochondrial disease. As research proceeds appropriate oxygenation levels should be carefully considered.

Published
2020
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22. Systematic Transmission Electron Microscopy‐Based Identification and 3D Reconstruction of Cellular Degradation Machinery

Author

Kit Neikirk, Zer Vue, Prasanna Katti, Ben I. Rodriguez, Salem Omer, Jianqiang Shao, Trace Christensen, Edgar Garza Lopez, Andrea Marshall, Caroline B. Palavicino‐Maggio, Jessica Ponce, Ahmad F. Alghanem, Larry Vang, Taylor Barongan, Heather K. Beasley, Taylor Rodman, Dominique Stephens, Margaret Mungai, Marcelo Correia, Vernat Exil, Steven Damo, Sandra A. Murray, Amber Crabtree, Brian Glancy, Renata O. Pereira, E. Dale Abel, and Antentor O. Hinton

Subjects
Biomaterials, Biomedical Engineering, General Biochemistry, Genetics and Molecular Biology
Published
2023
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27. MitoRACE: evaluating mitochondrial function in vivo and in single cells with subcellular resolution using multiphoton NADH autofluorescence

Author

Duck-Yeon Lee, Alessio Andreoni, Jay R. Knutson, Yingfan Zhang, Brian Glancy, and T. Bradley Willingham

Subjects
Male, 0301 basic medicine, Cell type, Physiology, Cell, Oxidative phosphorylation, Mitochondrion, Fluorescence, Article, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Animals, Cyanides, Chemistry, NAD, Mitochondria, Mitochondria, Muscle, Mice, Inbred C57BL, Kinetics, Autofluorescence, 030104 developmental biology, medicine.anatomical_structure, Biophysics, Energy Metabolism, Oxidation-Reduction, Flux (metabolism), 030217 neurology & neurosurgery, Function (biology)
Abstract

Key points We developed a novel metabolic imaging approach that provides direct measures of the rate of mitochondrial energy conversion with single-cell and subcellular resolution by evaluating NADH autofluorescence kinetics during the mitochondrial redox after cyanide experiment (mitoRACE). Measures of mitochondrial NADH flux by mitoRACE are sensitive to physiological and pharmacological perturbations in vivo. Metabolic imaging with mitoRACE provides a highly adaptable platform for evaluating mitochondrial function in vivo and in single cells with potential for broad applications in the study of energy metabolism. Abstract Mitochondria play a critical role in numerous cell types and diseases, and structure and function of mitochondria can vary greatly among cells or within different regions of the same cell. However, there are currently limited methodologies that provide direct assessments of mitochondrial function in vivo, and contemporary measures of mitochondrial energy conversion lack the spatial resolution necessary to address cellular and subcellular heterogeneity. Here, we describe a novel metabolic imaging approach that provides direct measures of mitochondrial energy conversion with single-cell and subcellular resolution by evaluating NADH autofluorescence kinetics during the mitochondrial redox after cyanide experiment (mitoRACE). MitoRACE measures the rate of NADH flux through the steady-state mitochondrial NADH pool by rapidly inhibiting mitochondrial energetic flux, resulting in an immediate, linear increase in NADH fluorescence proportional to the steady-state NADH flux rate, thereby providing a direct measure of mitochondrial NADH flux. The experiments presented here demonstrate the sensitivity of this technique to detect physiological and pharmacological changes in mitochondrial flux within tissues of living animals and reveal the unique capability of this technique to evaluate mitochondrial function with single-cell and subcellular resolution in different cell types in vivo and in cell culture. Furthermore, we highlight the potential applications of mitoRACE by showing that within single neurons, mitochondria in neurites have higher energetic flux rates than mitochondria in the cell body. Metabolic imaging with mitoRACE provides a highly adaptable platform for evaluating mitochondrial function in vivo and in single cells, with potential for broad applications in the study of energy metabolism.

Published
2019
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28. Protein composition of the muscle mitochondrial reticulum during postnatal development

Author

Yuho Kim, Daniel S. Yang, Brian Glancy, and Prasanna Katti

Subjects
0301 basic medicine, Physiology, Chemistry, Skeletal muscle, Oxidative phosphorylation, Mitochondrion, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Mitochondrial biogenesis, Downregulation and upregulation, Mitophagy, medicine, Glycolysis, 030217 neurology & neurosurgery, Calcium signaling
Abstract

Key points Muscle mitochondrial networks changed from a longitudinal, fibre parallel orientation to a perpendicular configuration during postnatal development. Mitochondrial dynamics, mitophagy and calcium uptake proteins were abundant during early postnatal development. Mitochondrial biogenesis and oxidative phosphorylation proteins were upregulated throughout muscle development. Postnatal muscle mitochondrial network formation is accompanied by a change in protein expression profile from mitochondria designed for co-ordinated cellular assembly to mitochondria highly specialized for cellular energy metabolism. Abstract Striated muscle mitochondria form connected networks capable of rapid cellular energy distribution. However, the mitochondrial reticulum is not formed at birth and the mechanisms driving network development remain unclear. In the present study, we aimed to establish the network formation timecourse and protein expression profile during postnatal development of the murine muscle mitochondrial reticulum. Two-photon microscopy was used to observe mitochondrial network orientation in tibialis anterior (TA) muscles of live mice at postnatal days (P) 1, 7, 14, 21 and 42, respectively. All muscle fibres maintained a longitudinal, fibre parallel mitochondrial network orientation early in development (P1-7). Mixed networks were most common at P14 but, by P21, almost all fibres had developed the perpendicular mitochondrial orientation observed in mature, glycolytic fibres. Tandem mass tag proteomics were then applied to examine changes in 6869 protein abundances in developing TA muscles. Mitochondrial proteins increased by 32% from P1 to P42. In addition, both nuclear- and mitochondrial-DNA encoded oxidative phosphorylation (OxPhos) components were increased during development, whereas OxPhos assembly factors decreased. Although mitochondrial dynamics and mitophagy were induced at P1-7, mitochondrial biogenesis was enhanced after P14. Moreover, calcium signalling proteins and the mitochondrial calcium uniporter had the highest expression early in postnatal development. In conclusion, mitochondrial networks transform from a fibre parallel to perpendicular orientation during the second and third weeks after birth in murine glycolytic skeletal muscle. This structural transition is accompanied by a change in protein expression profile from mitochondria designed for co-ordinated cellular assembly to mitochondria highly specialized for cellular energy metabolism.

Published
2019
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33. Addition of hyaluronic acid to the FIB‐4 liver fibrosis score improves prediction of incident cirrhosis and hepatocellular carcinoma in type 2 diabetes: The Edinburgh Type 2 Diabetes Study

Author

Grecian, Sheila M., primary, McLachlan, Stela, additional, Fallowfield, Jonathan A., additional, Hayes, Peter C., additional, Guha, Indra Neil, additional, Morling, Joanne R., additional, Glancy, Stephen, additional, Williamson, Rachel M., additional, Reynolds, Rebecca M., additional, Frier, Brian M., additional, Zammitt, Nicola N., additional, Price, Jackie F., additional, and Strachan, Mark W. J., additional

Published
2021
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38. Non‐invasive risk scores do not reliably identify future cirrhosis or hepatocellular carcinoma in Type 2 diabetes: The Edinburgh type 2 diabetes study

Author

Grecian, Sheila M., primary, McLachlan, Stela, additional, Fallowfield, Jonathan A., additional, Kearns, Patrick K. A., additional, Hayes, Peter C., additional, Guha, Neil I., additional, Morling, Joanne R., additional, Glancy, Stephen, additional, Williamson, Rachel M., additional, Reynolds, Rebecca M., additional, Frier, Brian M., additional, Zammitt, Nicola N., additional, Price, Jackie F., additional, and Strachan, Mark W. J., additional

Published
2020
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41. KATPchannel inhibition blunts electromechanical decline during hypoxia in left ventricular working rabbit hearts

Author

Matthew W. Kay, Kara Garrott, Anastasia M. Wengrowski, Sarah Kuzmiak-Glancy, Hanyu Zhang, and Jack M. Rogers

Subjects
0301 basic medicine, medicine.medical_specialty, Physiology, Chemistry, Oxygenation, 030204 cardiovascular system & hematology, Hypoxia (medical), Potassium channel, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Tolbutamide, Internal medicine, Optical mapping, Cardiology, medicine, Ventricular pressure, Myocyte, Sinus rhythm, medicine.symptom, medicine.drug
Abstract

Key points Heart function is critically dependent upon the balance of energy production and utilization. Sarcolemmal ATP-sensitive potassium channels (KATP channels) in cardiac myocytes adjust contractile function to compensate for the level of available energy. Understanding the activation of KATP channels in working myocardium during high-stress situations is crucial to the treatment of cardiovascular disease, especially ischaemic heart disease. Using a new optical mapping approach, we measured action potentials from the surface of excised contracting rabbit hearts to assess when sarcolemmal KATP channels were activated during physiologically relevant workloads and during gradual reductions in myocardial oxygenation. We demonstrate that left ventricular pressure is closely linked to KATP channel activation and that KATP channel inhibition with a low concentration of tolbutamide prevents electromechanical decline when oxygen availability is reduced. As a result, KATP channel inhibition probably exacerbates a mismatch between energy demand and energy production when myocardial oxygenation is low. Abstract Sarcolemmal ATP-sensitive potassium channel (KATP channel) activation in isolated cells is generally understood, although the relationship between myocardial oxygenation and KATP activation in excised working rabbit hearts remains unknown. We optically mapped action potentials (APs) in excised rabbit hearts to test the hypothesis that hypoxic changes would be more severe in left ventricular (LV) working hearts (LWHs) than Langendorff (LANG) perfused hearts. We further hypothesized that KATP inhibition would prevent those changes. Optical APs were mapped when measuring LV developed pressure (LVDP), coronary flow rate and oxygen consumption in LANG and LWHs. Hearts were paced to increase workload and perfusate was deoxygenated to study the effects of myocardial hypoxia. A subset of hearts was perfused with 1 μm tolbutamide (TOLB) to identify the level of AP duration (APD) shortening attributed to KATP channel activation. During sinus rhythm, APD was shorter in LWHs compared to LANG hearts. APD in both LWHs and LANG hearts dropped steadily during deoxygenation. With TOLB, APDs in LWHs were longer at all workloads and APD reductions during deoxygenation were blunted in both LWHs and LANG hearts. At 50% perfusate oxygenation, APD and LVDP were significantly higher in LWHs perfused with TOLB (199 ± 16 ms; 92 ± 5.3 mmHg) than in LWHs without TOLB (109 ± 14 ms, P = 0.005; 65 ± 6.5 mmHg, P = 0.01). Our results indicate that KATP channels are activated to a greater extent in perfused hearts when the LV performs pressure–volume work. The results of the present study demonstrate the critical role of KATP channels in modulating myocardial function over a wide range of physiological conditions.

Published
2017
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47. A Model-based approach for microvasculature structure distortion correction in two-photon fluorescence microscopy images

Author

Lam Dao, Li-Yueh Hsu, Lin-Ching Chang, Bertrand M. Lucotte, Robert S. Balaban, and Brian Glancy

Subjects
Blind deconvolution, Distortion function, Histology, Materials science, Image quality, business.industry, Imaging phantom, Pathology and Forensic Medicine, Distortion, Microscopy, Computer vision, Deconvolution, Artificial intelligence, business, Image restoration
Abstract

Summary This paper investigates a postprocessing approach to correct spatial distortion in two-photon fluorescence microscopy images for vascular network reconstruction. It is aimed at in vivo imaging of large field-of-view, deep-tissue studies of vascular structures. Based on simple geometric modelling of the object-of-interest, a distortion function is directly estimated from the image volume by deconvolution analysis. Such distortion function is then applied to subvolumes of the image stack to adaptively adjust for spatially varying distortion and reduce the image blurring through blind deconvolution. The proposed technique was first evaluated in phantom imaging of fluorescent microspheres that are comparable in size to the underlying capillary vascular structures. The effectiveness of restoring three-dimensional (3D) spherical geometry of the microspheres using the estimated distortion function was compared with empirically measured point-spread function. Next, the proposed approach was applied to in vivo vascular imaging of mouse skeletal muscle to reduce the image distortion of the capillary structures. We show that the proposed method effectively improve the image quality and reduce spatially varying distortion that occurs in large field-of-view deep-tissue vascular dataset. The proposed method will help in qualitative interpretation and quantitative analysis of vascular structures from fluorescence microscopy images. Lay Description Image distortion in fluorescence microscopy affects qualitative interpretation and particularly quantitative comparison of biological structures. Conventional image deconvolution approaches using empirically measured point-spread function (PSF) from submicron beads have limitations in correcting for large structural distortion in in vivo deep-tissue scans that require spatially varying models of the PSF. In this paper, we present a model-based image restoration approach to reduce spatial distortion and image blurring of microvascular structures in two-photon fluorescence microscopy images. Our results showed significant improvement in quantitative geometry measurements of the microsphere phantom compared to conventional measured PSF approach. We also showed that the method improve the image quality of vessel structures in mouse skeletal muscle. This image restoration approach can assist in qualitative and quantitative analysis of large field-of-view deep-tissue two photon fluorescence microscopy images.

Published
2015
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48. Oxygen demand of perfused heart preparations: how electromechanical function and inadequate oxygenation affect physiology and optical measurements

Author

Rafael Jaimes, Matthew W. Kay, Sarah Kuzmiak-Glancy, and Anastasia M. Wengrowski

Subjects
Isolated Heart Preparation, Electrophysiology, chemistry, In vivo, Myocardial oxygenation, Optical measurements, chemistry.chemical_element, Physiology, General Medicine, Oxygenation, Biology, Oxygen, Ex vivo
Abstract

New Findings What is the topic of this review? This review discusses how the function and electrophysiology of isolated perfused hearts are affected by oxygenation and energy utilization. The impact of oxygenation on fluorescence measurements in perfused hearts is also discussed. What advances does it highlight? Recent studies have illuminated the inherent differences in electromechanical function, energy utilization rate and oxygen requirements between the primary types of excised heart preparations. A summary and analysis of how these variables affect experimental results are necessary to elevate the physiological relevance of these approaches in order to advance the field of whole-heart research. The ex vivo perfused heart recreates important aspects of in vivo conditions to provide insight into whole-organ function. In this review we discuss multiple types of ex vivo heart preparations, explain how closely each mimic in vivo function, and discuss how changes in electromechanical function and inadequate oxygenation of ex vivo perfused hearts may affect measurements of physiology. Hearts that perform physiological work have high oxygen demand and are likely to experience hypoxia when perfused with a crystalloid perfusate. Adequate myocardial oxygenation is critically important for obtaining physiologically relevant measurements, so when designing experiments the type of ex vivo preparation and the capacity of perfusate to deliver oxygen must be carefully considered. When workload is low, such as during interventions that inhibit contraction, oxygen demand is also low, which could dramatically alter a physiological response to experimental variables. Changes in oxygenation also alter the optical properties of cardiac tissue, an effect that may influence optical signals measured from both endogenous and exogenous fluorophores. Careful consideration of oxygen supply, working condition, and wavelengths used to acquire optical signals is critical for obtaining physiologically relevant measurements during ex vivo perfused heart studies.

Published
2015
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49. NGSS and the landscape of engineering in K-12 state science standards

Author

Aran W. Glancy, Tamara J. Moore, Kristina Maruyama Tank, and Jennifer A. Kersten

Subjects
Engineering, business.industry, 4. Education, Comparative case, media_common.quotation_subject, Next Generation Science Standards, Science education, National Science Education Standards, Education, Engineering education, ComputingMilieux_COMPUTERSANDEDUCATION, Mathematics education, Engineering ethics, Quality (business), Science, technology, society and environment education, business, Research question, media_common
Abstract

Recent documents pertaining to K-12 education have fostered a connection between engineering and science education to help better prepare our students and future citizens to better meet the current and future challenges of our modern and technological society. With that connection, there has been a concerted effort to raise the visibility of engineering within K-12 science education, which is reflected in the Framework for K-12 Science Education and the recently released Next Generation Science Standards. As states look towards the adoption and implementation of the Next Generation Science Standards, it is important to take a deeper look at the shift in K-12 science education that is being suggested by these documents and what that means in terms of the potential changes for states that have chosen to adopt these standards. The main research question that has guided the work for this paper is: What is the extent and quality of the engineering that is present in state science standards and the Next Generation Science Standards? This paper will present a detailed analysis of the landscape of engineering in K-12 policy before and after the release of the NGSS through a comparative case study of academic state science standards and Next Generation Science Standards. This comparison provides insight into what the widespread adoption of the NGSS would mean in terms of potential changes in the way we implement science education in the United States. © 2015 Wiley Periodicals, Inc. J Res Sci Teach 52: 296–318, 2015

Published
2015
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50. Use of independent component analysis to improve signal-to-noise ratio in multi-probe fluorescence microscopy

Author

Lam Dao, Li-Yueh Hsu, Bertrand M. Lucotte, Robert S. Balaban, Lin-Ching Chang, and Brian Glancy

Subjects
Physics, Histology, business.industry, Image quality, Bandwidth (signal processing), Detector, Filter (signal processing), Independent component analysis, Cutoff frequency, Pathology and Forensic Medicine, Optics, Microscopy, Dichroic filter, business
Abstract

Summary In conventional multi-probe fluorescence microscopy, narrow bandwidth filters on detectors are used to avoid bleed-through artefacts between probes. The limited bandwidth reduces the signal-to-noise ratio of the detection, often severely compromising one or more channels. Herein, we describe a process of using independent component analysis to discriminate the position of different probes using only a dichroic mirror to differentiate the signals directed to the detectors. Independent component analysis was particularly effective in samples where the spatial overlap between the probes is minimal, a very common case in cellular microscopy. This imaging scheme collects nearly all of the emitted light, significantly improving the image signal-to-noise ratio. In this study, we focused on the detection of two fluorescence probes used in vivo, NAD(P)H and ANEPPS. The optimal dichroic mirror cutoff frequency was determined with simulations using the probes spectral emissions. A quality factor, defined as the cross-channel contrast-to-noise ratio, was optimized to maximize signals while maintaining spatial discrimination between the probes after independent component analysis post-processing. Simulations indicate that a ∼3 fold increase in signal-to-noise ratio using the independent component analysis approach can be achieved over the conventional narrow-band filtering approach without loss of spatial discrimination. We confirmed this predicted performance from experimental imaging of NAD(P)H and ANEPPS in mouse skeletal muscle, in vivo. For many multi-probe studies, the increased sensitivity of this ‘full bandwidth’ approach will lead to improved image quality and/or reduced excitation power requirements. Lay Description Signal to noise ratio (SNR) is a limiting factor in many fluorescence microscopy techniques to image multiple fluorescence probes simultaneously. Conventional approaches using band-pass filters to minimize cross-talk between channels can significantly reduce SNR by limiting the number of emitted photons that are detected. Using the assumption that the fluorescent probes are not present in the same regions of the cell or tissue, a common feature for many but not all probes, a technique is presented where most of the emitted light is collected and then discriminated using Independent Component Analysis. To illustrate this approach increased the SNR by a factor of ∼3 over the conventional filter scheme in the skeletal muscle of a live mouse. This improvement in SNR can be used to improve image quality or decrease the power and time required to collect a fluorescent image if the probes are spatially distinct.

Published
2014
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