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152. Linguistic Understanding and Knowledge of Truth-Conditions

Author

Chase B. Wrenn

Subjects
Philosophy of mind, Philosophy, Argument, Metaphysics, Truth condition, Meaning (non-linguistic), Psychology, Semantics, Linguistics, Sentence, Epistemology
Abstract

What do you know when you know what a sentence means? According to some theories, understanding a sentence is, in part, knowing its truth-conditions. Dorit Bar-On, Claire Horisk, and William Lycan have defended such theories on the grounds of an “epistemic determination argument” (“EDA”). That argument turns on the ideas (a) that understanding a sentence, along with knowledge of the non-linguistic facts, suffices to know its truth-value, and (b) that being able to determine a sentence’s truth-value given knowledge of the non-linguistic facts is knowing its truth-conditions. I argue that the EDA withstands the objections recently raised by Daniel Cohnitz and Jaan Kangilaski, but fails for other reasons. It equivocates between a fine-grained and a coarse grained conception of “facts.”

Published
2016

153. The interaction between fibrinogen and zymogen FXIII-A2B2 is mediated by fibrinogen residues γ390-396 and the FXIII-B subunits

Author

Helen Philippou, Matthew J. Flick, James R. Byrnes, Clare Wilson, Alisa S. Wolberg, Anthony M. Boutelle, and Chase B. Brandner

Subjects
0301 basic medicine, Tissue transglutaminase, Amino Acid Motifs, Immunology, Plasma protein binding, 030204 cardiovascular system & hematology, Fibrinogen, Biochemistry, Thrombosis and Hemostasis, law.invention, Mice, 03 medical and health sciences, 0302 clinical medicine, law, Zymogen, medicine, Animals, Humans, Surface plasmon resonance, Mice, Knockout, Enzyme Precursors, Factor XIII, biology, Chemistry, Cell Biology, Hematology, Surface Plasmon Resonance, Recombinant Proteins, Fibronectins, 030104 developmental biology, Coagulation, Recombinant DNA, biology.protein, Protein Binding, medicine.drug
Abstract

Coagulation transglutaminase factor XIII (FXIII) exists in circulation as heterotetrameric proenzyme FXIII-A2B2 Effectively all FXIII-A2B2 circulates bound to fibrinogen, and excess FXIII-B2 circulates in plasma. The motifs that mediate interaction of FXIII-A2B2 with fibrinogen have been elusive. We recently detected reduced binding of FXIII-A2B2 to murine fibrinogen that has γ-chain residues 390-396 mutated to alanines (Fibγ390-396A). Here, we evaluated binding features using human components, including recombinant fibrinogen variants, FXIII-A2B2, and isolated FXIII-A2 and -B2 homodimers. FXIII-A2B2 coprecipitated with wild-type (γA/γA), alternatively-spliced (γ'/γ'), and αC-truncated (Aα251) fibrinogens, whereas coprecipitation with human Fibγ390-396A was reduced by 75% (P

Published
2016

154. Raising a big tent: Internal party composition and leadership selectorate expansion

Author

Brett N. Odom and Chase B. Meyer

Subjects
021110 strategic, defence & security studies, Political science, 05 social sciences, Political Science and International Relations, 050602 political science & public administration, 0211 other engineering and technologies, Opposition (politics), 02 engineering and technology, Public administration, 0506 political science
Abstract

The trend amongst many parties toward the inclusion of rank-and-file members in the leadership selection process has often been attributed to opposition status and electoral defeat. However, these explanations are typical events for parties and hardly seem sufficient for party elites to willingly cede their authority over the selection of party leaders. This paper proposes that the electoral regionalization of the party contributes to the decision to expand the leadership selectorate. In the event a party is defeated to an extent in which their support is reduced to its regional base, this situation necessitates the bringing in of new voices to avoid further marginalization. This paper finds that regionalization plays a significant role in the decision of parties to expand leadership selectorates and that the role of opposition status and electoral setbacks have been overstated.

Published
2016

155. It's Not Race, It's Politics! A Natural Experiment Examining the Influence of Race in Electoral Politics*

Author

Chase B. Meyer and J. David Woodard

Subjects
White (horse), Natural experiment, media_common.quotation_subject, 05 social sciences, General Social Sciences, 050109 social psychology, Electoral politics, 0506 political science, Race (biology), Politics, Feeling, Political science, Scale (social sciences), 050602 political science & public administration, 0501 psychology and cognitive sciences, Racial resentment, Social psychology, media_common
Abstract

Objective Minority candidates for office must overcome numerous hurdles in order to win elective office, with one such hurdle being the racial resentment of voters. This article tests the impact racial resentment has on white support for a minority candidate in relation to a similar white candidate. Method This article employs a natural experiment provided by the 2014 South Carolina Senate elections. Examining these elections, this article examines what impact a voter's racial resentment has on his or her support for the two candidates. Results The results show that voters who score highly on the racial resentment scale are just as likely to support a minority Republican as they are to support a white Republican. Conclusion These findings indicate that racial resentment scores may not adequately measure a person's true feelings on race, particularly when the minority candidate is a Republican.

Published
2016

156. Differential signalling and glutamate receptor compositions in the OFF bipolar cell types in the mouse retina

Author

Tomomi Ichinose and Chase B. Hellmer

Subjects
0301 basic medicine, Retina, Cell type, Physiology, Cell, Glutamate receptor, Kainate receptor, Retinal, AMPA receptor, Biology, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, chemistry, medicine, Excitatory postsynaptic potential, Neuroscience, 030217 neurology & neurosurgery
Abstract

Key points Using whole-cell clamp methods, we characterized the temporal coding in each type of OFF bipolar cell. We found that type 2 and 3a cells are transient, type 1 and 4 cells are sustained, and type 3b cells are intermediate. The light-evoked excitatory postsynaptic potentials in some types were rectified, suggesting that they provide inputs to the non-linear ganglion cells. Visual signalling from the photoreceptors was mediated exclusively through the kainate receptors in the transient OFF bipolar cells, whereas both kainate and AMPA receptors contributed in the other cells. This study demonstrates, for the first time, that parallel visual encoding starts at the OFF bipolar cells in a type-specific manner. Abstract The retina is the entrance to the visual system, which receives various kinds of image signals and forms multiple encoding pathways. The second-order retinal neurons, the bipolar cells, are thought to initiate multiple neural streams by encoding various visual signals in different types of cells. However, the functions of each bipolar cell type have not been fully understood. We investigated whether OFF bipolar cells encode visual signals in a type-dependent manner. We recorded the changes in the bipolar cell voltage in response to two input functions: step and sinusoidal light stimuli. Type 1 and 4 OFF bipolar cells were sustained cells and responded to sinusoidal stimuli over a broad range of frequencies. Type 2 and 3a cells were transient and exhibited band-pass filtering. Type 3b cells were in the middle of these two groups. The distinct temporal responses might be attributed to different types of glutamate receptors. We examined the AMPA and kainate glutamate receptor composition in each bipolar cell type. The light responses in the transient OFF bipolar cells were exclusively mediated by kainate receptors. Although the kainate receptors mediated the light responses in the sustained cells, the AMPA receptors also mediated a portion of the responses in sustained cells. Furthermore, we found that some types of cells were rectified more than other types. Taken together, we found that the OFF bipolar cells encode diverse temporal image signals in a type-dependent manner, confirming that each type of OFF bipolar cell initiates diverse temporal visual processing in parallel.

Published
2015

157. Évaluation objective de la qualité du sommeil chez les patients souffrant d’une rupture de la coiffe des rotateurs

Author

Chase B. Ansok, Stephanie Muh, and Lafi S. Khalill

Subjects
medicine.medical_specialty, business.industry, Actigraphy, Sleep in non-human animals, medicine.anatomical_structure, Cohort, Physical therapy, Medicine, Orthopedics and Sports Medicine, Surgery, Sleep diary, Rotator cuff, Sleep onset latency, Sleep onset, business, Prospective cohort study
Abstract

Introduction Sleep dysfunction in patients with rotator cuff tears has been previously evaluated only using subjective measures. Objective parameters of sleep quality amongst rotator cuff tear patients are scarce in the literature. The aim of this study is to compare objective sleep data to historical controls and to subjective patient reported sleep quality in patients with rotator cuff tears. Hypothesis We hypothesized that patients with rotator cuff tears would demonstrate objectively poor sleep quality based on actigraphy when compared to a historical control group. Secondarily, we hypothesize that objective sleep quality measures will correlate poorly with traditionally used questionnaires and other subjective assessments. Materials and methods Twenty patients with full-thickness rotator cuff tears wore a highly validated activity monitor for 2 consecutive weeks for objective assessment and completed a sleep diary during the same period. Patients completed multiple questionnaires pertaining to their shoulder function and subjective assessment of sleep quality. Objective sleep assessments were compared to patients’ sleep diary data and to subjective sleep data from a historical cohort of 969 healthy adults aged 57–97 years. Results Mean total sleep time, sleep onset latency, wake after sleep onset (WASO), and sleep efficiency were all significantly worse in the study cohort compared to the historical cohort (p = 0.0338, p = 0.0040, p Discussion This study of objective sleep measures demonstrated poor sleep quality in patients with rotator cuff tears with shorter sleep duration, frequent awakenings, and decreased efficiency. Subjective assessments of sleep did not correlate with objective findings. Level of evidence Level II, prospective cohort study.

Published
2020

158. Observations of insect visitors to Price’s Potato Bean (Apios priceana, Fabaceae) in North Alabama, USA

Author

Paula Galvan, Chase B. Kimmel, Hadi Sutarno, Joshua W. Campbell, and Brittany E. Campbell

Subjects
0106 biological sciences, media_common.quotation_subject, Apios priceana, Plant Science, Insect, Fabaceae, Potato-bean, Biology, biology.organism_classification, 010603 evolutionary biology, 01 natural sciences, food.food, food, Pollinator, Reproductive biology, Botany, Flowering plant, Megachile sculpturalis, 010606 plant biology & botany, media_common
Abstract

Background and aims Apios priceana is a rare flowering plant that can only be found in parts of the Southeastern United States. Little is known about the reproductive biology of this plant and only a

Published
2016

159. Better Understanding the Potential Importance of Florida Roadside Breeding Habitat for the Monarch

Author

Jaret C. Daniels, Simon McClung, Samm Epstein, Chase B. Kimmel, Jonathan S. Bremer, and Kristin Rossetti

Subjects
0106 biological sciences, vegetation management, Population, Wildlife, migration, 010603 evolutionary biology, 01 natural sciences, Article, Danaus, Monarch butterfly, monarch butterfly, education, lcsh:Science, Restoration ecology, mowing, Asclepias, education.field_of_study, biology, Ecology, conservation, biology.organism_classification, 010602 entomology, Habitat, Insect Science, Butterfly, milkweed, lcsh:Q, roadside habitat
Abstract

The North American monarch butterfly (Danaus plexippus) population has declined significantly over the past two decades. Among the many other factors, loss of breeding habitat has been implicated as a potential leading driver. In response, wildlife agencies and conservation practitioners have made a strong push to restore and conserve milkweeds on both wild and managed landscapes including agricultural lands as well as transportation and utility rights-of-way. Roadsides in particular have been emphasized as a targeted landscape for monarch habitat restoration. While much attention has been focused on habitat in California, along the I-35 corridor from Texas to Minnesota, and more broadly across the agricultural Midwest, research on the occurrence of roadside breeding habitat and the development of best vegetative management practices conducted in the Deep South has been limited. We sampled roadside verges in north-central Florida for the presence of two early season milkweed species, that are particularly important for early season monarch recolonization, Asclepias tuberosa and Asclepias humistrata. Our findings suggest that roadsides harbor extensive populations of the target milkweeds with the vast majority of plants occurring on the back slope of the verge. Alterations to current roadside mowing frequency and scope are needed to effectively conserve these populations and ensure that they are available for use by the monarch.

Published
2018

160. Secondary-Structure-Mediated Hierarchy and Mechanics in Polyurea-Peptide Hybrids

Author

Bingrui Li, Chase B. Thompson, Richard S. Tomazin, Jonathan E. Cowen, Jong K. Keum, LaShanda T. J. Korley, and Lindsay E. Matolyak

Subjects
Protein Conformation, alpha-Helical, Polymers and Plastics, Polymers, Bioengineering, Peptide, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Polyethylene Glycols, Biomaterials, chemistry.chemical_compound, Crystallinity, PEG ratio, Materials Chemistry, Polylysine, Protein secondary structure, Polyurea, Mechanical Phenomena, chemistry.chemical_classification, Mechanics, 021001 nanoscience & nanotechnology, 0104 chemical sciences, chemistry, Covalent bond, Network covalent bonding, Protein Conformation, beta-Strand, 0210 nano-technology, Crystallization, Ethylene glycol
Abstract

Peptide-polymer hybrids combine the hierarchy of biological species with synthetic concepts to achieve control over molecular design and material properties. By further incorporating covalent cross-links, the enhancement of molecular complexity is achieved, allowing for both a physical and covalent network. In this work, the structure and function of poly(ethylene glycol) (PEG)-network hybrids are tuned by varying peptide block length and overall peptide content. Here the impact of poly(ε-carbobenzyloxy-l-lysine) (PZLY) units on block interactions and mechanics is explored by probing secondary structure, PEG crystallinity, and hierarchical organization. The incorporation of PZLY reveals a mixture of α-helices and β-sheets at smaller repeat lengths ( n = 5) and selective α-helix formation at a higher peptide molecular weight ( n = 20). Secondary structure variations tailored the solid-state film hierarchy, whereby nanoscale fibers and microscale spherulites varied in size depending on the amount of α-helices and β-sheets. This long-range ordering influenced mechanical properties, resulting in a decrease in elongation-at-break (from 400 to 20%) with increasing spherulite diameter. Furthermore, the reduction in soft segment crystallinity with the addition of PZLY resulted in a decrease in moduli. It was determined that, by controlling PZLY content, a balance of physical associations and self-assembly is obtained, leading to tunable PEG crystallinity, spherulite formation, and mechanics.

Published
2018

161. Functional and Morphological Analysis of OFF Bipolar Cells

Author

Chase B. Hellmer and Tomomi Ichinose

Subjects
0301 basic medicine, Retinal Bipolar Cells, Microscopy, Confocal, Patch-Clamp Techniques, genetic structures, Biotin, Retinal, Biology, Immunohistochemistry, Article, Membrane Potentials, 03 medical and health sciences, chemistry.chemical_compound, Mice, 030104 developmental biology, 0302 clinical medicine, chemistry, Mouse Retina, Morphological analysis, Animals, Patch clamp, sense organs, Neuroscience, 030217 neurology & neurosurgery, Photic Stimulation
Abstract

Retinal first-order neurons, photoreceptors, receive visual inputs and convert them to neural signals. The second-order neurons, bipolar cells then sort out the visual signals and encode them through multiple neural streams. Approximately 15 morphological types of bipolar cells have been identified, which are thought to encode different aspects of visual signals such as motion and color (Ichinose et al. J Neurosci 34(26):8761-8771, 2014; Euler et al. Nat Rev Neurosci 15(8):507-519, 2014). To investigate functional aspects of OFF bipolar cells, single cell recordings are preferred; however, bipolar cells in the mouse retina are small and hard to distinguish from other types of cells. Here, we describe our methodology and tips for immunohistochemistry and patch clamp recordings for analyzing light-evoked responses in each type of OFF bipolar cell.

Published
2018

162. A group I metabotropic glutamate receptor controls synaptic gain between rods and rod bipolar cells in the mouse retina

Author

Scott Nawy, Tomomi Ichinose, Chase B. Hellmer, and Melissa Rampino Clemons

Subjects
0301 basic medicine, Male, Retinal Bipolar Cells, retina, Physiology, metabotropic glutamate receptors, Receptor, Metabotropic Glutamate 5, Receptors, Metabotropic Glutamate, 03 medical and health sciences, Mice, 0302 clinical medicine, Retinal Rod Photoreceptor Cells, Physiology (medical), Animals, Protein kinase C, Protein Kinase C, Original Research, Light response, Phospholipase C, Chemistry, Glutamate receptor, Metabotropic glutamate receptor 6, Long-term potentiation, Synaptic Potentials, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Metabotropic glutamate receptor, Type C Phospholipases, Metabotropic glutamate receptor 1, Calcium, Female, sense organs, 030217 neurology & neurosurgery, Intracellular
Abstract

The canonical mGluR6‐Trpm1 pathway that generates the sign‐inverting signal between photoreceptors and ON bipolar cells has been well described. However, one type of ON bipolar cell, the rod bipolar cell (RBC), additionally is thought to express the group I mGluRs whose function is unknown. We examined the role of group I mGluRs in mouse RBCs and here provide evidence that it controls synaptic gain between rods and RBCs. In dark‐adapted conditions, the mGluR1 antagonists LY367385 and (RS)‐1‐Aminoindan‐1,5‐dicarboxylic acid, but not the mGluR5 antagonist 2‐Methyl‐6‐(phenylethynyl)pyridine hydrochloride reduced the light‐evoked responses in RBCs indicating that mGluR1, but not mGluR5, serves to potentiate RBC responses. Perturbing the downstream phospholipase C (PLC)‐protein kinase C (PKC) pathway by inhibiting PLC, tightly buffering intracellular Ca2+, or preventing its release from intracellular stores reduced the synaptic potentiation by mGluR1. The effect of mGluR1 activation was dependent upon adaptation state, strongly increasing the synaptic gain in dark‐, but not in light‐adapted retinas, or in the presence of a moderate background light, consistent with the idea that mGluR1 activation requires light‐dependent glutamate release from rods. Moreover, immunostaining revealed that protein kinase Cα (PKC α) is more strongly expressed in RBC dendrites in dark‐adapted conditions, revealing an additional mechanism behind the loss of mGluR1 potentiation. In light‐adapted conditions, exogenous activation of mGluR1 with the agonist 3,5‐Dihydroxyphenylglycine increased the mGluR6 currents in some RBCs and decreased it in others, suggesting an additional action of mGluR1 that is unmasked in the light‐adapted state. Elevating intracellular free Ca2+, consistently resulted in a decrease in synaptic gain. Our results provide evidence that mGluR1 controls the synaptic gain in RBCs.

Published
2018

163. Optimal management of glenohumeral osteoarthritis

Author

Ansok,Chase B and Muh,Stephanie J

Subjects
Orthopedic Research and Reviews
Abstract

Chase B Ansok, Stephanie J Muh Department of Orthopaedic Surgery, Henry Ford Hospital, Detroit, MI, USA Abstract: Glenohumeral osteoarthritis (OA) is defined as progressive loss of articular cartilage, resulting in bony erosion, pain, and decreased function. This article provides a gross overview of this disease, along with peer-reviewed research by experts in the field. The pathology, diagnosis, and classification of this condition have been well described. Treatment begins with non-operative measures, including oral and topical anti-inflammatory agents, physical therapy, and intra-­articular injections of either a corticosteroid or a viscosupplementation agent. Operative treatment is based on the age and function of the affected patient, and treatment of young individuals with glenohumeral OA remains controversial. Various methods of surgical treatment, ranging from arthroscopy to resurfacing, are being evaluated. The roles of hemiarthroplasty, total shoulder arthroplasty, and reverse shoulder arthroplasty are similarly reviewed with supporting data. Keywords: glenohumeral, osteoarthritis, hyaluronic acid, hemiarthroplasty, total shoulder arthroplasty

Published
2018

164. Socius

Author

Boyle, Kaitlin M. and Meyer, Chase B.

Subjects
affect control theory, Gender, elections, politics, culture
Abstract

In 2016, Hillary Clinton was the first woman to gain the presidential nomination from a major political party in the United States, yet she was unsuccessful. The current study explores barriers to being elected as president for women generally and Hillary Clinton specifically. Using the propositions and tools of affect control theory, we demonstrate how women’s political representation shapes cultural sentiments about women and the president. In a nationwide sample of Americans surveyed shortly before the election, we find women’s representation on the state level influences voter preferences through these cultural sentiments: More women in politics makes a woman president feel less deflecting, which is associated with a greater likelihood of voting for Clinton. We also demonstrate how sentiments about Clinton—as an individual, not merely a woman running for president—conflict with Democratic voters’ expectations for presidential qualities and behaviors, which may have further prevented victory in 2016. OASF

Published
2018

165. A Plea for Immodesty: Alethic Pluralism, Logical Pluralism, and Mixed Inferences

Author

Chase B. Wrenn

Subjects
Plea, Alethic modality, Dead end, Logical conjunction, Logical pluralism, Philosophy, Classical logic, Pluralism (philosophy), Intuitionistic logic, Epistemology
Abstract

The problem of mixed inferences is a bugbear for alethic pluralism and logical pluralism alike. Michael Lynch’s alethic functionalism is meant to solve the problem for alethic pluralists. But, as Lynch observes, it is tempting to combine alethic and logical pluralism, and doing so threatens to reintroduce the problem. Lynch proposes a way out of the problem for alethic cum logical pluralists. I argue that Lynch’s way out is a dead end, and the combination of logical and alethic pluralism is unattractive.

Published
2018

166. 94. Cost analysis of primary single-level lumbar discectomies

Author

Chase B. Grover, Nicholas Spina, Darrel S. Brodke, Trevor R. Mordhorst, Richard E. Nelson, W. Ryan Spiker, and Ali Jalali

Subjects
Univariate analysis, Multivariate statistics, medicine.medical_specialty, Multivariate analysis, business.industry, Univariate, Context (language use), Indirect costs, Standard error, Emergency medicine, Medicine, Surgery, Orthopedics and Sports Medicine, Neurology (clinical), Activity-based costing, business
Abstract

BACKGROUND CONTEXT Improving value in surgical care requires a detailed understanding of the true costs of surgical and operating room resources. PURPOSE In this study, we sought to identify predictors of health care costs and operating room resource use for patients undergoing initial single-level discectomies using a unique institutional cost dataset from the value driven outcomes (VDO) program developed by the University of Utah. STUDY DESIGN/SETTING A retrospective cost analysis of primary single-level lumbar discectomies. PATIENT SAMPLE A total of 622 patients undergoing initial single-level lumbar discectomy between January 2014 to April 2016 at the University of Utah Orthopaedic Center. OUTCOME MEASURES Health care costs, clinical length of stay, and operating room time. METHODS Univariate and multivariate generalized linear models (GLM) performed to identify predictors of health care costs, clinical length of stay (LOS, days) and operating room time (OR, minutes) using a unique costing tool. Modified park test procedure was implemented to determine GLM error distribution specifications and standard errors were clustered by provider. Cost outcomes were normalized using mean costs for a patient with normal body mass index (BMI) and a healthy American Society of Anesthesiologists (ASA) classification system. Average marginal effects in multivariate analysis were reported as percentage of normalized costs. RESULTS Advanced age, male gender, Hispanic, Black, unemployment, and being retired were significant positive predictors of costs in univariate analysis. Asian, Native American, outpatient procedures, and being a student were significant negative predictors of costs. Univariate analysis also showed that obesity, higher ASA class and insurance status were also positive and significant predictors of costs. In multivariate analysis, we found that obesity led to higher average marginal total direct (9%), total facility (15%), and facility OR costs (22%), as well as an average marginal effect of 24 more OR minutes per surgery. Conversely, being underweight was associated with lower average marginal total direct (-23%), total non-facility (-54%), total facility (-8%), facility OR costs (-15%), as well as lower clinical LOS (-.42 days), and 18 less OR minutes. While being overweight was not significantly associated with greater total direct costs, it was associated with higher total facility (8%), and facility OR costs (12%), with an average marginal effect of 11 more OR minutes per surgery. Age was associated with a longer LOS but not with OR costs in multivariate analysis. As expected, outpatient surgical costs, LOS and OR time were significantly lower than inpatient procedures. Patients with incapacitating disease ASA Class had the highest predicted OR time in GLM estimates with an average marginal effect of 28 minutes, while severe systematic disease was associated with greater total and nonfacility costs. In addition, Medicare patients had higher facility costs (14%) compared to privately insured patients. CONCLUSIONS Although many of our observed variables were significant predictors of costs in univariate analysis, multivariate GLM estimates showed that the main variables determining cost and operating room time and resource use were obesity (BMI), general health (ASA class), Medicare status and advanced age, and whether the surgery was an outpatient or inpatient procedure. FDA DEVICE/DRUG STATUS This abstract does not discuss or include any applicable devices or drugs.

Published
2019

172. Challenging the norm: further psychometric investigation of the neck disability index

Author

Christine Cheng, Chase B. Grover, Jeremy D. Franklin, Darrel S. Brodke, Man Hung, Ashley Neese, Brandon D. Lawrence, and Shirley D. Hon

Subjects
education.field_of_study, Neck pain, medicine.medical_specialty, Neck Pain, Trauma Severity Indices, Rasch model, Psychometrics, business.industry, Population, Context (language use), Disability Evaluation, Physical medicine and rehabilitation, Floor effect, medicine, Physical therapy, Humans, Raw score, Ceiling effect, Surgery, Orthopedics and Sports Medicine, Neurology (clinical), medicine.symptom, education, business
Abstract

Background context The neck disability index (NDI) was the first patient-reported outcome (PRO) instrument specific to patients with neck pain, and it remains one of the most widely used PROs for the neck population. The NDI is an appealing measure as it is a short and well-known PRO measure. Currently, there are conflicting data on the performance and applicability of the NDI in patients undergoing either operative or nonoperative treatment for neck-related conditions. Purpose This study investigates the psychometric properties, performance, and applicability of the NDI in the spine patient population. Study design A total of 865 patients visiting a university-based spine clinic with neck complaints, with or without radiating upper extremity pain, numbness, or weakness were enrolled in the study. Visit types included new and follow-up visits to both operative and nonoperative treatments. Questionnaires were administered electronically on a tablet computer, and all patients answered all 10 questions of the NDI. Methods Standard descriptive statistics were performed to describe the demographic characteristics of the patients. Rasch modeling was applied to examine the psychometric properties of the NDI. Results The NDI demonstrated insufficient unidimensionality (ie, unexplained variance after accounting for the first dimension=9.4%). Person reliability was 0.85 and item reliability was 1.00 for the NDI. The overall item fit for the NDI was good with an outfit mean square of 1.03. The NDI had a floor effect of 35.5% and ceiling effect of 4.6%. The raw score to measure correlation of the NDI was 0.019. Conclusions Although the NDI had good person and item reliability, it did not demonstrate strong evidence of unidimensionality. The NDI exhibited a very large floor effect. Because of the poor raw score to measure correlation, the sum score should not be used in interpretation of findings. Despite great investment by physicians and other stakeholders in the NDI, this evaluation and previous research have demonstrated that the NDI needs further investigation and refinement.

Published
2015

173. Truth is not (Very) Intrinsically Valuable

Author

Chase B. Wrenn

Subjects
Instrumental and intrinsic value, 060302 philosophy, 05 social sciences, 0501 psychology and cognitive sciences, 06 humanities and the arts, 0603 philosophy, ethics and religion, 050105 experimental psychology, Mathematics, Epistemology
Abstract

We might suppose it is not only instrumentally valuable for beliefs to be true, but that it is intrinsically valuable – truth makes a non-derivative, positive contribution to a belief's overall value. Some intrinsic goods are better than others, though, and this article considers the question of how good truth is, compared to other intrinsic goods. I argue that truth is the worst of all intrinsic goods; every other intrinsic good is better than it. I also suggest the best explanation for truth's inferiority is that it is not really an intrinsic good at all. It is intrinsically neutral.

Published
2015

174. Who Is Presidential? Women’s Political Representation, Deflection, and the 2016 Election

Author

Boyle, Kaitlin M., Meyer, Chase B., Boyle, Kaitlin M., and Meyer, Chase B.

Abstract

In 2016, Hillary Clinton was the first woman to gain the presidential nomination from a major political party in the United States, yet she was unsuccessful. The current study explores barriers to being elected as president for women generally and Hillary Clinton specifically. Using the propositions and tools of affect control theory, we demonstrate how women’s political representation shapes cultural sentiments about women and the president. In a nationwide sample of Americans surveyed shortly before the election, we find women’s representation on the state level influences voter preferences through these cultural sentiments: More women in politics makes a woman president feel less deflecting, which is associated with a greater likelihood of voting for Clinton. We also demonstrate how sentiments about Clinton—as an individual, not merely a woman running for president—conflict with Democratic voters’ expectations for presidential qualities and behaviors, which may have further prevented victory in 2016.

Published
2018
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175. Maternal CXCR4 deletion results in placental defects and pregnancy loss mediated by immune dysregulation

Author

Fang Lyu, Chase Burzynski, Yuan yuan Fang, Aya Tal, Alice Y. Chen, Jacqueline Kisa, Kriti Agrawal, Yuval Kluger, Hugh S. Taylor, and Reshef Tal

Subjects
Reproductive biology, Medicine
Abstract

CXCR4 is a key regulator of the development of NK cells and DCs, both of which play an important role in early placental development and immune tolerance at the maternal-fetal interface. However, the role of CXCR4 in pregnancy is not well understood. Our study demonstrates that adult-induced global genetic CXCR4 deletion, but not uterine-specific CXCR4 deletion, was associated with increased pregnancy resorptions and decreased litter size. CXCR4-deficient mice had decreased NK cells and increased granulocytes in the decidua, along with increased leukocyte numbers in peripheral blood. We found that CXCR4-deficient mice had abnormal decidual NK cell aggregates and NK cell infiltration into trophoblast areas beyond the giant cell layer. This was associated with low NK cell expression of granzyme B, a NK cell granule effector, indicative of NK cell dysfunction. Pregnancy failure in these mice was associated with abnormalities in placental vascular development and increased placental expression of inflammatory genes. Importantly, adoptive BM transfer of WT CXCR4+ BM cells into CXCR4-deficient mice rescued the reproductive deficits by normalizing NK cell function and mediating normal placental vascular development. Collectively, our study found an important role for maternal CXCR4 expression in immune cell function, placental development, and pregnancy maintenance.

Published
2023
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176. Varenicline Combined With Oral Nicotine Replacement Therapy and Smartphone-Based Medication Reminders for Smoking Cessation: Feasibility Randomized Controlled Trial

Author

Munjireen Sifat, Emily T Hébert, Jasjit S Ahluwalia, Michael S Businelle, Joseph J C Waring, Summer G Frank-Pearce, Chase Bryer, Lizbeth Benson, Stefani Madison, Lourdes G Planas, Irina Baranskaya, and Darla E Kendzor

Subjects
Medicine
Abstract

BackgroundVarenicline and oral nicotine replacement therapy (NRT) have each been shown to increase the likelihood of smoking cessation, but their combination has not been studied. In addition, smoking cessation medication adherence is often poor, thus, challenging the ability to evaluate medication efficacy. ObjectiveThis study examined the effects of combined varenicline and oral NRT and smartphone medication reminders on pharmacotherapy adherence and smoking abstinence among adults enrolled in smoking cessation treatment. MethodsA 2×2 factorial design was used. Participants (N=34) were randomized to (1) varenicline + oral NRT (VAR+NRT) or varenicline alone (VAR) and (2) smartphone medication reminder messages (REM) or no reminder messages (NREM) over 13 weeks. Participants assigned to VAR+REM received varenicline reminder prompts, and those assigned to VAR+NRT+REM also received reminders to use oral NRT. The other 2 groups (VAR+NREM and VAR+NRT+NREM) did not receive medication reminders. Participants were not blinded to intervention groups. All participants received tobacco cessation counseling. Smartphone assessments of smoking as well as varenicline and NRT use (if applicable) were prompted daily through the first 12 weeks after a scheduled quit date. Descriptive statistics were generated to characterize the relations between medication and reminder group assignments with daily smoking, daily varenicline adherence, and daily quantity of oral NRT used. Participants completed follow-up assessments for 26 weeks after the quit date. ResultsParticipants were predominantly White (71%), and half were female (50%). On average, participants were 54.2 (SD 9.4) years of age, they smoked an average of 19.0 (SD 9.0) cigarettes per day and had smoked for 34.6 (SD 12.7) years. Descriptively, participants assigned to VAR+NRT reported more days of smoking abstinence compared to VAR (29.3 vs 26.3 days). Participants assigned to REM reported more days of smoking abstinence than those assigned to NREM (40.5 vs 21.8 days). Participants assigned to REM were adherent to varenicline on more days compared to those assigned to NREM (58.6 vs 40.5 days), and participants assigned to VAR were adherent to varenicline on more days than those assigned to VAR + NRT (50.7 vs 43.3 days). In the subsample of participants assigned to VAR+NRT, participants assigned to REM reported more days where ≥5 pieces of NRT were used than NREM (14.0 vs 7.4 days). Average overall medication adherence (assessed via the Medication Adherence Questionnaire) showed the same pattern as the daily smartphone-based adherence assessments. ConclusionsPreliminary findings indicated that smoking cessation interventions may benefit from incorporating medication reminders and combining varenicline with oral NRT, though combining medications may be associated with poorer adherence. Further study is warranted. Trial RegistrationClinicalTrials.gov NCT03722966; https://classic.clinicaltrials.gov/ct2/show/NCT03722966

Published
2023
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177. A Guide to Planting Wildflower Enhancements in Florida

Author

Josh Campbell, Mary C. Bammer, Jaret C. Daniels, James D. Ellis, and Chase B. Kimmel

Subjects
Agronomy, Wildflower, Sowing, Biology
Abstract

The establishment of native wildflower plantings in Florida can benefit agricultural producers as well as native pollinators and other beneficial insects (predators and parasitoids). The plantings do this by: providing forage and nesting sites for bees, butterflies, and other pollinators, increasing wild bee numbers possibly across the farm, and increasing natural enemies of insect pests (that also depend on forage and nesting sites). This document discusses choosing the right mix of native plant species to benefit many pollinator species, as well as proper site selection, planting practices, and weed control techniques. Wildflower plots should be practical to manage, maximize benefits to wildlife, and fit into the overall management practices of the property.

Published
2017

178. Sporadic Creutzfeldt–Jakob disease infected human cerebral organoids retain the original human brain subtype features following transmission to humanized transgenic mice

Author

Bradley R. Groveman, Brent Race, Simote T. Foliaki, Katie Williams, Andrew G. Hughson, Chase Baune, Gianluigi Zanusso, and Cathryn L. Haigh

Subjects
Sporadic CJD, Subtype, Prion, PrP, Cerebral organoid, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Human cerebral organoids (COs) are three-dimensional self-organizing cultures of cerebral brain tissue differentiated from induced pluripotent stem cells. We have recently shown that COs are susceptible to infection with different subtypes of Creutzfeldt–Jakob disease (CJD) prions, which in humans cause different manifestations of the disease. The ability to study live human brain tissue infected with different CJD subtypes opens a wide array of possibilities from differentiating mechanisms of cell death and identifying neuronal selective vulnerabilities to testing therapeutics. However, the question remained as to whether the prions generated in the CO model truly represent those in the infecting inoculum. Mouse models expressing human prion protein are commonly used to characterize human prion disease as they reproduce many of the molecular and clinical phenotypes associated with CJD subtypes. We therefore inoculated these mice with COs that had been infected with two CJD subtypes (MV1 and MV2) to see if the original subtype characteristics (referred to as strains once transmitted into a model organism) of the infecting prions were maintained in the COs when compared with the original human brain inocula. We found that disease characteristics caused by the molecular subtype of the disease associated prion protein were similar in mice inoculated with either CO derived material or human brain material, demonstrating that the disease associated prions generated in COs shared strain characteristics with those in humans. As the first and only in vitro model of human neurodegenerative disease that can faithfully reproduce different subtypes of prion disease, these findings support the use of the CO model for investigating human prion diseases and their subtypes.

Published
2023
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179. Second passage experiments of chronic wasting disease in transgenic mice overexpressing human prion protein

Author

Brent Race, Chase Baune, Katie Williams, James F. Striebel, Andrew G. Hughson, and Bruce Chesebro

Subjects
RT-QuIC, prion, cross-species transmission, barrier, chronic wasting disease, transgenic mice, Veterinary medicine, SF600-1100
Abstract

Abstract Chronic wasting disease (CWD) is a prion disease of cervids including deer, elk, reindeer, and moose. Human consumption of cervids is common, therefore assessing the risk potential of CWD transmission to humans is critical. In a previous study, we tested CWD transmission via intracerebral inoculation into transgenic mice (tg66 and tgRM) that over-expressed human prion protein. Mice screened by traditional prion detection assays were negative. However, in a group of 88 mice screened by the ultrasensitive RT-QuIC assay, we identified 4 tg66 mice that produced inconsistent positive RT-QuIC reactions. These data could be false positive reactions, residual input inoculum or indicative of subclinical infections suggestive of cross species transmission of CWD to humans. Additional experiments were required to understand the nature of the prion seeding activity in this model. In this manuscript, second passage experiments using brains from mice with weak prion seeding activity showed they were not infectious to additional recipient tg66 mice. Clearance experiments showed that input CWD prion seeding activity was eliminated by 180 days in tg66 mice and PrPKO mice, which are unable to replicate prion protein, indicating that the weak positive levels of seeding activity detected at later time points was not likely residual inoculum. The failure of CWD prions to cause disease in tg66 after two sequential passages suggested that a strong species barrier prevented CWD infection of mice expressing human prion protein.

Published
2022
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181. Bipolar Cell Type-Specific Expression and Conductance of Alpha-7 Nicotinic Acetylcholine Receptors in the Mouse Retina

Author

Christina C. Koehler, Chase B. Hellmer, Tomomi Ichinose, and Leo M Hall

Subjects
0301 basic medicine, Agonist, Retinal Bipolar Cells, alpha7 Nicotinic Acetylcholine Receptor, medicine.drug_class, Cell, Motion Perception, Stem cell marker, patch clamp, Synaptic Transmission, Bridged Bicyclo Compounds, Mice, 03 medical and health sciences, 0302 clinical medicine, mental disorders, medicine, Animals, Nicotinic Agonists, Acetylcholine receptor, Retina, acetylcholine receptor, Chemistry, mouse retina, Ganglion, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Nicotinic agonist, nervous system, immunohistochemistry, Benzamides, Models, Animal, sense organs, Visual Neuroscience, 030217 neurology & neurosurgery, Acetylcholine, medicine.drug
Abstract

Purpose Motion detection is performed by a unique neural network in the mouse retina. Starburst amacrine cells (SACs), which release acetylcholine and gamma-aminobutyric acid (GABA) into the network, are key neurons in the motion detection pathway. Although GABA contributions to the network have been extensively studied, the role of acetylcholine is minimally understood. Acetylcholine receptors are present in a subset of bipolar, amacrine, and ganglion cells. We focused on α7-nicotinic acetylcholine receptor (α7-nAChR) expression in bipolar cells, and investigated which types of bipolar cells possess α7-nAChRs. Methods Retinal slice sections were prepared from C57BL/6J and Gus8.4-GFP mice. Specific expression of α7-nAChRs in bipolar cells was examined using α-bungarotoxin (αBgTx)-conjugated Alexa dyes co-labeled with specific bipolar cell markers. Whole-cell recordings were conducted from bipolar cells in retinal slice sections. A selective α7-nAChR agonist, PNU282987, was applied by a puff and responses were recorded. Results αBgTx fluorescence was observed primarily in bipolar cell somas. We found that α7-nAChRs were expressed by the majority of type 1, 2, 4, and 7 bipolar cells. Whole-cell recordings revealed that type 2 and 7 bipolar cells depolarized by PNU application. In contrast, α7-nAChRs were not detected in most of type 3, 5, 6, and rod bipolar cells. Conclusions We found that α7-nAChRs are present in bipolar cells in a type-specific manner. Because these bipolar cells provide synaptic inputs to SACs and direction selective ganglion cells, α7-nAChRs may play a role in direction selectivity by modulating these bipolar cells' outputs.

Published
2019

182. Design of the ILC Crab Cavity System

Author

Adolphsen, C., primary, Beard, C., additional, Bellantoni, L., additional, Burt, G., additional, Carter, R., additional, Chase, B., additional, Church, M., additional, Dexter, A., additional, Dykes, M., additional, Edwards, H., additional, Goudket, P, additional, Jenkins, R., additional, Jones, R.M., additional, Kalinin, A., additional, Khabiboulline, T., additional, Ko, K., additional, Latina, A., additional, Li, Z., additional, Ma, L., additional, McIntosh, P., additional, and Ng, C., additional

Published
2007
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185. Record high-gradient SRF beam acceleration at Fermilab

Author

Broemmelsiek, D, primary, Chase, B, additional, Edstrom, D, additional, Harms, E, additional, Leibfritz, J, additional, Nagaitsev, S, additional, Pischalnikov, Y, additional, Romanov, A, additional, Ruan, J, additional, Schappert, W, additional, Shiltsev, V, additional, Thurman-Keup, R, additional, and Valishev, A, additional

Published
2018
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194. Advanced silicon photonics technology platform leveraging a semiconductor supply chain

Author

De Dobbelaere, P., primary, Dahl, A., additional, Mekis, A., additional, Chase, B., additional, Weber, B., additional, Welch, B., additional, Foltz, D., additional, Armijo, G., additional, Masini, G., additional, McGee, G., additional, Wong, G., additional, Balardeta, J., additional, Dotson, J., additional, Schramm, J., additional, Hon, K., additional, Khauv, K., additional, Robertson, K., additional, Stechschulte, K., additional, Yokoyama, K., additional, Planchon, L., additional, Tullgren, L., additional, Eker, M., additional, Mack, M., additional, Peterson, M., additional, Rudnick, N., additional, Milton, P., additional, Sun, P., additional, Bruck, R., additional, Zhou, R., additional, Denton, S., additional, Fath-pour, S., additional, Gloeckner, S., additional, Jackson, S., additional, Pang, S., additional, Sahni, S., additional, Wang, S., additional, Yu, S., additional, Pinguet, T., additional, De Koninck, Y., additional, Chi, Y., additional, and Liang, Y., additional

Published
2017
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195. Multi-tissue DNA methylation microarray signature is predictive of gene function

Author

Xiavan Renaldo Roopnarinesingh, Hunter Porter, Cory Giles, Chase Brown, Constantin Georgescu, and Jonathan Wren

Subjects
dna methylation, epigenetics, gene function prediction, Genetics, QH426-470
Abstract

Background Transcriptional correlation networks derived from publicly available gene expression microarrays have been previously shown to be predictive of known gene functions, but less is known about the predictive capacity of correlated DNA methylation at CpG sites. Guilt-by-association co-expression methods can adapted for use with DNA methylation when a representative methylation value is created for each gene. We examine how methylation compares to expression in predicting Gene Ontology terms using both co-methylation and traditional machine learning approaches across different types of representative methylation values per gene. Methods We perform guilt-by-association gene function prediction with a suite of models called Methylation Array Network Analysis, using a network of correlated methylation values derived from over 24,000 samples. In generating the correlation matrix, the performance of different methods of collapsing probe-level data effect on the resulting gene function predictions was compared, along with the use of different regions surrounding the gene of interest. Results Using mean comethylation of a given gene to its annotated term had an overall highest prediction macro-AUC of 0.60 using mean gene body methylation, across all Gene Ontology terms. This was increased using the logistic regression approach with the highest macro-AUC of 0.82 using mean gene body methylation, compared to the naive predictor of 0.72. Conclusion Genes correlated in their methylation state are functionally related. Genes clustered in co-methylation space were enriched for chromatin state, PRC2, immune response, and development-related terms.

Published
2022
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196. A global multiproxy database for temperature reconstructions of the Common Era

Author

Emile-Geay, J., McKay, N., Kaufman, D., Von Gunten, L., Wang, J., Anchukaitis, K., Abram, N., Addison, J., Curran, M., Evans, M., Henley, B., Hao, Z., Martrat, B., McGregor, H., Neukom, R., Pederson, G., Stenni, B., Thirumalai, K., Werner, J., Xu, C., Divine, D., Dixon, B., Gergis, J., Mundo, I., Nakatsuka, T., Phipps, S., Routson, C., Steig, E., Tierney, J., Tyler, J., Allen, K., Bertler, N., Björklund, J., Chase, B., Chen, M., Cook, E., De Jong, R., DeLong, K., Dixon, D., Ekaykin, A., Ersek, V., Filipsson, H., Francus, P., Freund, M., Frezzotti, M., Gaire, N., Gajewski, K., Ge, Q., Goosse, H., Gornostaeva, A., Grosjean, M., Horiuchi, K., Hormes, A., Husum, K., Isaksson, E., Kandasamy, S., Kawamura, K., Kilbourne, K., Koç, N., Leduc, G., Linderholm, H., Lorrey, A., Mikhalenko, V., Mortyn, P., Motoyama, H., Moy, A., Mulvaney, R., Munz, P., Nash, D., Oerter, H., Opel, T., Orsi, A., Ovchinnikov, D., Porter, T., Roop, H., Saenger, C., Sano, M., Sauchyn, D., Saunders, K., Seidenkrantz, M., Severi, M., Shao, X., Sicre, M., Sigl, M., Sinclair, K., St George, S., St Jacques, J., Thamban, M., Thapa, U., Thomas, E., Turney, C., Uemura, R., Viau, A., Vladimirova, D., Wahl, E., White, J., Yu, Z., Zinke, Jens, Emile-Geay, J., McKay, N., Kaufman, D., Von Gunten, L., Wang, J., Anchukaitis, K., Abram, N., Addison, J., Curran, M., Evans, M., Henley, B., Hao, Z., Martrat, B., McGregor, H., Neukom, R., Pederson, G., Stenni, B., Thirumalai, K., Werner, J., Xu, C., Divine, D., Dixon, B., Gergis, J., Mundo, I., Nakatsuka, T., Phipps, S., Routson, C., Steig, E., Tierney, J., Tyler, J., Allen, K., Bertler, N., Björklund, J., Chase, B., Chen, M., Cook, E., De Jong, R., DeLong, K., Dixon, D., Ekaykin, A., Ersek, V., Filipsson, H., Francus, P., Freund, M., Frezzotti, M., Gaire, N., Gajewski, K., Ge, Q., Goosse, H., Gornostaeva, A., Grosjean, M., Horiuchi, K., Hormes, A., Husum, K., Isaksson, E., Kandasamy, S., Kawamura, K., Kilbourne, K., Koç, N., Leduc, G., Linderholm, H., Lorrey, A., Mikhalenko, V., Mortyn, P., Motoyama, H., Moy, A., Mulvaney, R., Munz, P., Nash, D., Oerter, H., Opel, T., Orsi, A., Ovchinnikov, D., Porter, T., Roop, H., Saenger, C., Sano, M., Sauchyn, D., Saunders, K., Seidenkrantz, M., Severi, M., Shao, X., Sicre, M., Sigl, M., Sinclair, K., St George, S., St Jacques, J., Thamban, M., Thapa, U., Thomas, E., Turney, C., Uemura, R., Viau, A., Vladimirova, D., Wahl, E., White, J., Yu, Z., and Zinke, Jens

Abstract

Reproducible climate reconstructions of the Common Era (1 CE to present) are key to placing industrial-era warming into the context of natural climatic variability. Here we present a community-sourced database of temperature-sensitive proxy records from the PAGES2k initiative. The database gathers 692 records from 648 locations, including all continental regions and major ocean basins. The records are from trees, ice, sediment, corals, speleothems, documentary evidence, and other archives. They range in length from 50 to 2000 years, with a median of 547 years, while temporal resolution ranges from biweekly to centennial. Nearly half of the proxy time series are significantly correlated with HadCRUT4.2 surface temperature over the period 1850-2014. Global temperature composites show a remarkable degree of coherence between high- and low-resolution archives, with broadly similar patterns across archive types, terrestrial versus marine locations, and screening criteria. The database is suited to investigations of global and regional temperature variability over the Common Era, and is shared in the Linked Paleo Data (LiPD) format, including serializations in Matlab, R and Python.

Published
2017

197. Use of a handheld Doppler to measure brachial and femoral artery occlusion pressure

Author

Pat R. Vehrs, Shay Richards, Chase Blazzard, Hannah Hart, Nicole Kasper, Ryan Lacey, Daniela Lopez, and Luke Baker

Subjects
arterial occlusion pressure, Doppler ultrasound, occlusion training, KAATSU, blood flow restriction, Physiology, QP1-981
Abstract

Objective: Measurement of arterial occlusion pressure (AOP) is essential to the safe and effective use of blood flow restriction during exercise. Use of a Doppler ultrasound (US) is the “gold standard” method to measure AOP. Validation of a handheld Doppler (HHDOP) device to measure AOP could make the measurement of AOP more accessible to practitioners in the field. The purpose of this study was to determine the accuracy of AOP measurements of the brachial and femoral arteries using an HHDOP.Methods: We simultaneously measured AOP using a “gold standard” US and a HHDOP in the dominant and non-dominant arms (15 males; 15 females) and legs (15 males; 15 females).Results: There were no differences in limb circumference or limb volume in the dominant and non-dominant arms and legs between males and females or between the dominant and non-dominant arms and legs of males and females. The differences between US and HHDOP measures of AOP in the dominant and non-dominant arms and legs were either not significant or small ( 0.60). Bland–Altman analysis yielded an average bias (−0.65 mmHg; −2.93 mmHg) and reasonable limits of agreement (±5.56 mmHg; ±5.58 mmHg) between US and HHDOP measures of brachial and femoral artery AOP, respectively.Conclusion: HHDOP yielded acceptable measures of AOP of the brachial and femoral arteries and can be used to measure AOP by practitioners for the safe and effective use of blood flow restriction. Due to the potential differences in AOP between dominant and non-dominant limbs, AOP should be measured in each limb.

Published
2023
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198. Temporary alteration of neuronal network communication is a protective response to redox imbalance that requires GPI-anchored prion protein

Author

Simote T. Foliaki, Aleksandar Wood, Katie Williams, Anna Smith, Ryan O. Walters, Chase Baune, Bradley R. Groveman, and Cathryn L. Haigh

Subjects
Oxidative stress, PrP, Prion disease, Prion protein, Neuronal cytoskeleton, Hippocampal CA1 long-term potentiation, Medicine (General), R5-920, Biology (General), QH301-705.5
Abstract

Cellular prion protein (PrPC) protects neurons against oxidative stress damage. This role is lost upon its misfolding into insoluble prions in prion diseases, and correlated with cytoskeletal breakdown and neurophysiological deficits. Here we used mouse neuronal models to assess how PrPC protects the neuronal cytoskeleton, and its role in network communication, from oxidative stress damage. Oxidative stress was induced extrinsically by potassium superoxide (KO2) or intrinsically by Mito-Paraquat (MtPQ), targeting the mitochondria. In mouse neural lineage cells, KO2 was damaging to the cytoskeleton, with cells lacking PrPC (PrP-/-) damaged more than wild-type (WT) cells. In hippocampal slices, KO2 acutely inhibited neuronal communication in WT controls without damaging the cytoskeleton. This inhibition was not observed in PrP-/- slices. Neuronal communication and the cytoskeleton of PrP-/- slices became progressively disrupted and degenerated post-recovery, whereas the dysfunction in WT slices recovered in 5 days. This suggests that the acute inhibition of neuronal activity in WT slices in response to KO2 was a neuroprotective role of PrPC, which PrP-/- slices lacked. Heterozygous expression of PrPC was sufficient for this neuroprotection. Further, hippocampal slices from mice expressing PrPC without its GPI anchor (PrPGPI-/-) displayed acute inhibition of neuronal activity by KO2. However, they failed to restore normal activity and cytoskeletal formation post-recovery. This suggests that PrPC facilitates the depressive response to KO2 and its GPI anchoring is required to restore KO2-induced damages. Immuno spin-trapping showed increased radicals formed on the filamentous actin of PrP-/- and PrPGPI-/- slices, but not WT and PrP+/- slices, post-recovery suggesting ongoing dysregulation of redox balance in the slices lacking GPI-anchored PrPC. The MtPQ treatment of hippocampal slices temporarily inhibited neuronal communication independent of PrPC expression. Overall, GPI-anchored PrPC alters synapses and neurotransmission to protect and repair the neuronal cytoskeleton, and neuronal communication, from extrinsically induced oxidative stress damages.

Published
2023
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199. Colaboradores

Author

Abidi, Nadia Y., Abzug, Mark J., Adams, David R., Adams, Nicholas S., Adelson, Stewart L., Ahlfeld, Shawn K., Ahmad, Osman Z., Aiken, John J., Akdis, Cezmi A., Alessandrini, Evaline A., Alexander, Michael A., Ali, Omar, Anderson, Karl E., Anthony, Kelly K., Antoon, Alia Y., Apkon, Susan D., Ardoin, Stacy P., Arkader, Alexandre, Armangué, Thaís, Arndt, Carola A.S., Aronson, Paul L., Asher, David M., Ashworth, Ann, Assa, Amit, Asselin, Barbara L., Astley, Christina M., Ater, Joann L., Atkinson, Norrell, Augustine, Erika U., Augustyn, Marilyn C., Avitzur, Yaron, Bacino, Carlos A., Bailey, Zinzi D., Balakrishnan, Binod, Balamuth, Frances B., Baldassano, Robert N., Baldwin, Keith D., Bales, Christina, Balistreri, William F., Ballantine, Allison, Baltimore, Robert S., Balwani, Manisha, Bamba, Vaneeta, Banwell, Brenda L., Barclay, Sarah F., Barnes-Davis, Maria E., Barron, Karyl S., Basel, Donald, Bass, Dorsey M., Bassett, Mary T., Bauerfeld, Christian P., Baum, Rebecca A., Bell, Michael J., Bender, Nicole R., Benjamin, Daniel K., Jr, Bennett, Michael J., Bernstein, Daniel, Bernstein, Henry H., Bharucha-Goebel, Diana X., Biggs, Holly M., Blanchard, Samra S., Blatter, Joshua A., Bleyer, Archie, Blum, Nathan J., Boas, Steven R., Bockting, Walter O., Boguniewicz, Mark, Boivin, Michael J., Bonthius, Daniel J., Bordini, Brett J., Bosse, Kristopher R., Bostwick, Bret L., Boyer, Kenneth M., Brady, Jennifer M., Brady, Patrick W., Brady, Rebecca C., Brady, Samuel L., Brandow, Amanda M., Breault, David T., Breuner, Cora Collette, Bridgemohan, Carolyn, Britt, William J., Brower, Laura, Brown, Rebeccah L., Brownell, J. Naylor, Browning, Meghen B., Brunetti-Pierri, Nicola, Bryant, Phillip R., Buckley, Rebecca H., Budek, Cynthia Etzler, Bunyavanich, Supinda, Burnham, Carey-Ann D., Burstein, Gale R., Bustinduy, Amaya L., Buyon, Jill P., Cabada, Miguel M., Cada, Michaela, Caglar, Derya, Cairo, Mitchell S., Calello, Diane P., Camarda, Lauren E., Cameron, Lindsay Hatzenbuehler, Camitta, Bruce M., Campbell, Angela J.P., Carlin, Rebecca F., Carr, Michael R., Carrigan, Robert B., Carroll, Michael S., Carter, Rebecca G., Caserta, Mary T., Chapman, Jennifer I., Cheifetz, Ira M., Chelimsky, Gisela G., Chelimsky, Thomas C., Chemaitilly, Wassim, Chen, Yuan-Tsong, Chiriboga, Jennifer A., Chiu, Yvonne E., Cho, Christine B., Chong, Hey Jin, Chou, Stella T., Christenson, John C., Chun, Robert H., Chusid, Michael J., Cieslak, Theodore J., Claes, Donna J., Clark, Jeff A., Clemens, John David, Coates, Thomas D., Coffin, Susan E., Cohen, Joanna S., Cohen, Mitchell B., Cohen-Wolkowiez, Michael, Colbert, Robert A., Cole, F. Sessions, III, Collaco, J. Michael, Colombo, John L., Congeni, Joseph A., Conner, Lindsay N., Creighton, Sarah M., Crowe, James E., Jr, Czinn, Steven J., Dalal, Aarti S., Dalmau, Josep O., Danziger-Isakov, Lara A., Darville, Toni, Daum, Robert S., Davidson, Loren T., Davidson, Richard S., Davies, H. Dele, Daw, Najat C., Dean, Shannon L., Toro, Helen M. Oquendo Del, DeMaso, David R., Denison, Mark R., Dent, Arlene E., Desnick, Robert J., Deterding, Robin R., Devarajan, Prasad, deVeber, Gabrielle A., Dhar, Vineet, Dhawan, Anil, Dick, André A.S., Dietz, Harry C., III, Diiorio, Daren A., DiMeglio, Linda A., Dixon, Bradley P., Dlamini, Nomazulu, Dodhia, Sonam N., Donohoue, Patricia A., Downes, Kevin J., Doyle, Alexander J., Doyle, Daniel A., Doyle, Jefferson J., Dreskin, Stephen C., Driscoll, Sherilyn W., Dror, Yigal, D'souza, Jill N., Dubowitz, Howard, Dumler, J. Stephen, Duncan, Janet, Dvergsten, Jeffrey A., Earing, Michael G., Eberly, Matthew D., Eddy, S. Derrick, Egan, Marie E., Elder, Jack S., Englander, Elizabeth, Enlow, Elizabeth, Eppes, Stephen C., Ericson, Jessica, Erkan, Elif, Ermias, Yokabed, Eskew, Ashley M., Etzel, Ruth A., Fahrenkopf, Matthew P., Falk, Marni J., Faria, John J., Fargo, John H., Feemster, Kristen A., Feigelman, Susan, Feinstein, Jeffrey A., Feldman, Amy G., Felner, Eric I., Fels, Edward C., Feng, Sing-Yi, Ferkol, Thomas W., Jr, Finberg, Karin E., Finder, Jonathan D., Finkelstein, Laura H., Fiorino, Kristin N., Fischer, Philip R., Fisher, Brian T., Flood, Veronica H., Flores, Francisco X., Flynn, Joseph T., Flynn, Patricia M., Forman, Joel A., Frank, Michael M., Frenck, Robert W., Jr, Friedman, Deborah M., Friehling, Erika, Fritz, Stephanie A., Frush, Donald P., Gadomski, Anne M., Gaensbauer, James T., Gahagan, Sheila, Gahl, William A., Gallagher, Patrick G., Gans, Hayley A., Garcia-mauriño, Cristina, Gardiner, Paula M., Garibaldi, Luigi R., Gauthier, Gregory M., Gerber, Jeffrey S., Gershon, Anne A., Ghadersohi, Saied, Gibson, Mark, Gigliotti, Francis, Gilliam, Walter S., Ginde, Salil, Girotto, John A., Goldfarb, Samuel B., Goldman, David L., Goldman, Stanton C., Goldstein, Neal D., Goldstein, Stuart L., Gonzalez-Heydrich, Joseph, Goodman, Denise M., Goodman, Tracy S., Gordon, Catherine M., Gordon, Leslie B., Goto, Collin S., Gower, W. Adam, Goyal, Neera K., Goyeneche, Nicholas P., Graepel, Kevin W., Graham, Robert J., Greally, John M., Green, Cori M., Green, Michael, Greenbaum, Larry A., Greenbaum, V. Jordan, Greenberg, James M., Griffiths, Anne G., Grizzle, Kenneth L., Groner, Judith A., Guarino, Alfredo, Gurria, Juan P., Guz-Mark, Anat, Haddad, Gabriel G., Haddad, Joseph, Jr, Hagan, Joseph F., Jr, Hagood, James S., Haider, Suraiya K., Haliloglu, Goknur, Halstead, Scott B., Hammer, Allison R., Hammerschlag, Margaret R., Hamvas, Aaron, Harris, James C., Harrison, Douglas J., Hartman, Corina, Hartman, Mary E., Haslam, David B., Hassan, H. Hesham Abdel-Kader, Hauck, Fern R., Havers, Fiona P., Hayes, Ericka V., Hecht, Jacqueline T., Heidemann, Sabrina M., Heimall, Jennifer R., Hemingway, Cheryl, Hendley, J. Owen, Hernandez, Michelle L., Hershey, Andrew D., Herzog, Cynthia E., Hirner, Jesse P., Hochberg, Jessica, Hodes, Deborah, Hoefgen, Holly R., Holinger, Lauren D., Holland-Hall, Cynthia M., Hooper, David K., Hoover-Fong, Julie E., Hord, Jeffrey D., Horn, B. David, Horstmann, Helen M., Horton, William A., Hotez, Peter J., House, Samantha A., Hsu, Evelyn, Hsu, Katherine, Huang, Felicia A. Scaggs, Huddleston, Heather G., Huepenbecker, Sarah P., Huff, Vicki, Huh, Winston W., Humphrey, Stephen R., Hunger, Stephen P., Hunstad, David A., Hunt, Carl E., Huppert, Stacey S., Huppler, Anna R., Ibeziako, Patricia I., Ibrahim, Samar H., Jackson, Allison M., Jackson, Elizabeth C., Jackson, Mary Anne, Jaffe, Ashlee, Janowski, Andrew B., Jatlaoui, Tara C., Jelsing, Elena J., Jensen, M. Kyle, Jenssen, Brian P., Jerardi, Karen E., John, Chandy C., Johnston, Brian D., Johnston, Michael V., Johnston, Richard B., Jr, Jones, Bridgette L., Joselow, Marsha, Josephson, Cassandra D., Jospe, Nicholas, Joyce, Joel C., Kabbouche, Marielle A., Kacperski, Joanne, Kamat, Deepak, Kamath-Rayne, Beena D., Kansra, Alvina R., Kanter, David M., Karlin, Aaron M., Kattan, Jacob, Kazura, James W., Kearns, Gregory L., Kelly, Andrea, Kelly, Desmond P., Kelly, Kevin J., Kelly, Matthew S., Kelly, Michael, Ken, Kimberly M., Kennedy, Melissa A., Kerem, Eitan, Kerschner, Joseph E., Khan, Seema, Khatami, Ameneh, Khatua, Soumen, Kilinsky, Alexandra, Kim, Chong-Tae, Kim, Wendy E., King, Charles H., Kingma, Paul S., Kinsman, Stephen L., Kishnani, Priya S., Klein, Bruce L., Klein, Bruce S., Kliegman, Robert M., Koch, William C., Kochanek, Patrick M., Kodish, Eric, Kohlhoff, Stephan A., Kostic, Mark A., Kotloff, Karen L., Krane, Elliot J., Krause, Peter J., Kreipe, Richard E., Krug, Steven E., Kwiatkowski, Janet L., Kwon, Jennifer M., Lachenauer, Catherine S., Ladisch, Stephan, Lakser, Oren J., Landrigan, Philip J., Landry, Gregory L., Lane, Wendy G., Larson, A. Noelle, LaRussa, Phillip S., Lawrence, J. Todd R., Lee, Brendan, Lee, K. Jane, Leeder, J. Steven, Leiding, Jennifer W., Lentze, Michael J., Lestrud, Steven O., Leung, Donald Y.M., Levas, Michael N., Levy, Rona L., Li, B U.K., Liacouras, Chris A., Liebig, Christopher W., Lipkin, Paul H., Liptzin, Deborah R., Liu, Andrew H., Lo, Lucinda, Lo, Stanley F., Long, Kathleen A., Long, Sarah S., Lopez, Anna Lena, Lopez, Santiago M.C., Lossef, Steven V., Lowry, Jennifer A., Macumber, Ian R., Magnusson, Mark R., Magoulas, Pilar L., Mahajan, Prashant V., Majzoub, Joseph A., Mann, Robert J., Manoli, Irini, Maqbool, Asim, Maranich, Ashley M., Marcantuono, Nicole, Margolis, David, Marin, Mona, Marini, Joan C., Markello, Thomas C., Markowitz, Morri, Maroushek, Stacene R., Marsh, Justin D., Martin, Kari L., Martinez, Maria G., Mason, Wilbert H., Maalon, Reuben K., Matta, Sravan Kumar Reddy, Maybank, Aletha, Mazor, Robert L., McAllister, Jennifer, McCabe, Megan E., McClean, Megan E., McColley, Susanna A., McGann, Patrick T., McGovern, Margaret M., McGrath-Morrow, Sharon A., McKinney, Jeffrey S., McLaughlin, Matthew J., McLeod, Rima, Mejias, Asuncion, Melby, Peter C., Melzer-Lange, Marlene D., Merguerian, Matthew D., Merhar, Stephanie L., Merritt, Diane F., Messacar, Kevin, Michaels, Marian G., Michniacki, Thomas F., Mikati, Mohad A., Milgrom, Henry, Mink, Jonathan W., Mistovich, R. Justin, Mitchell, Jonathan A., Mitsnefes, Mark M., Mohandas, Sindhu, Moon, Rachel Y., Moran, Joan P., Morava, Eva, Moreno, Megan A., Morgan, Esi, Morrison, Peter E., Moseley, Lovern R., Mozer-Glassberg, Yael, Muglia, Louis J., Murphy, Kevin P., Murphy, Timothy F., Murray, Karen F., Murray, Thomas S., Narula, Sona, Natale, Mindo J., Nathan, Amy T., Navsaria, Dipesh, Neal, William A., Nehme, Grace, Nehus, Edward J., Nelson, Maureen R., Neri, Caitlin M., Neuman, Mark I., Nevin, Mary A., Newburger, Jane W., NewMark, Jonathan, Nield, Linda S., Niss, Omar, Noah, Zehava L., Nocton, James J., Nogee, Lawrence M., Noje, Corina, Norton, Laura E., Nowak-Węgrzyn, Anna, Obaro, Stephen K., Obeid, Makram M., O’Brien, Hope L., Okwo-Bele, Jean-Marie, Oleszek, Joyce L., Olitsky, Scott E., Olsson, John M., Ombrello, Amanda K., O’Neill, Meghan E., Onigbanjo, Mutiat T., Orenstein, Walter A., Orscheln, Rachel C., Osorio, Marisa, Otto, Christian A., Owens, Judith A., Özen, Seza, Pachter, Lee M., Padhye, Amruta, Pak-Gorstein, Suzinne, Panganiban, Jennifer, Pappas, Diane E., Parent, John J., Parker, Alasdair P.J., Parks, Elizabeth Prout, Patterson, Briana C., Patterson, Maria Jevitz, Peters, Anna L., Peters, Timothy R., Phelan, Rachel A., Pinto, Anna, Poindexter, Brenda B., Pollard, Andrew J., Preciado, Diego, Proctor, Mark R., II, Howard I. Pryor, Pyles, Lee A., Quinn, Molly, Quint, Elisabeth H., Rabatin, Amy E., Rabinovich, C. Egla, Raffini, Leslie J., Ralston, Shawn L., Ram, Sanjay, Ramilo, Octavio, Ramirez, Kacy A., Rand, Casey M., Ratner, Adam J., Ratner, Lee, Raymond, Gerald V., Reed, Ann M., Reif, Shimon, Reller, Megan E., Reuter, Caroline H., Reyes, Jorge D., Rinawi, Firas, Ritchey, A. Kim, Rivara, Frederick P., Robinette, Eric, Robinson, Angela Byun, Rodrigues, Kristine Knuti, Rodriguez-Buritica, David F., Rodríguez-Fernández, Rosa, Roosevelt, Genie E., Rosenberg, David R., Roskind, Cindy Ganis, Ross, A. Catharine, Rossano, Joseph W., Rothman, Jennifer A., Rozenfeld, Ranna A., Ryan, Colleen A., Ryan, Monique M., Ryu, Julie, Sachdev, H.P.S., Sadarangani, Manish, Sadun, Rebecca E., Sahin, Mustafa, Sainath, Nina N., Salata, Robert A., Salvana, Edsel Maurice T., Sampson, Hugh A., Samsel, Chase B., Sandora, Thomas J., Sandritter, Tracy L., Sankar, Wudbhav N., Sarkissian, Eric J., Sarnaik, Ajit A., Sarnaik, Ashok P., Sarnat, Harvey B., Schaffzin, Joshua K., Schanberg, Laura E., Schechter, Michael S., Schleiss, Mark R., Schor, Nina F., Schroeder, James W., Jr, Schulte, Elaine E., Schuster, Mark A., Scott, Daryl A., Scott, J. Paul, Scott, John P., Seed, Patrick C., Serwint, Janet R., Shah, Apurva S., Shah, Dheeraj, Shah, Samir S., Shaikhkhalil, Ala, Shamir, Raanan, Shanti, Christina M., Shapiro, Bruce K., Shaughnessy, Erin E., Shaywitz, Bennett A., Shaywitz, Sally E., Shchelochkov, Oleg A., Sheanon, Nicole M., Shneider, Benjamin L., Shulman, Stanford T., Sicherer, Scott H., Simms, Mark D., Simmons, Jeffery M., Simões, Eric A.F., Simonsen, Kari A., Sinclair-McBride, Keneisha, Sivaraman, Vidya, Slavotinek, Anne M., Smith, Jessica R., Smith, Stephanie H., Smith-Whitley, Kim, Son, Mary Beth F., Sosinsky, Laura Stout, Souder, Emily, Spahn, Joseph D., Spearman, Paul, Sperling, Mark A., Spiegel, David A., Spitzer, Jaclyn B., Spranger, Jürgen W., Squires, James E., Srivastava, Siddharth, Geme, Joseph W. St, III, Stallings, Amy P., Stallings, Virginia A., Stambough, Kathryn C., Stanberry, Lawrence R., Stanley, Charles A., Starke, Jeffrey R., Starr, Taylor B., Steenhoff, Andrew P., Stein, Ronen E., Steinbach, William J., Stewart, Janet, Storch, Gregory A., Strauss, Ronald G., Sucato, Gina S., Suchy, Frederick J., Suhrie, Kristen R., Sullivan, Kathleen E., Szilagyi, Moira, Tabbah, Sammy M., Tanz, Robert R., Tarango, Cristina, Tarek, Nidale, Tasker, Robert C., Tchapyjnikov, Dmitry, Tesini, Brenda L., Theobald, Jillian L., Thielen, Beth K., Thomas, Anita A., Thomas, Cameron W., Thornburg, Courtney D., Tieder, Joel S., Tifft, Cynthia J., Todd, James K., Tolentino, Victor R., Jr, Toro, Camilo, II, Richard L. Tower, Trapasso, Joseph M., Troncone, Riccardo, Tsao, Elaine, Tubergen, David G., Tuchman, Lisa K., Turk, Margaret A., Turner, David A., Ullrich, Christina, Ullrich, Nicole, Upadhya, Krishna K., Urion, David K., Valika, Taher, Van Hare, George F., Van Mater, Heather A., Varnell, Charles D., Jr, Vaughan, Ana M., Vece, Timothy J., Vemana, Aarthi P., Venditti, Charles P., Vepraskas, Sarah, Verbsky, James W., Vermilion, Jennifer A., Vickery, Brian P., Vitola, Bernadette E., Voynow, Judith A., Wagner, Jonathan B., Waguespack, Steven G., Walker, David M., Walkovich, Kelly J., Walter, Heather J., Wambach, Jennifer A., Wang, Julie, Wangler, Michael F., Ware, Russell E., Ware, Stephanie M., Washam, Matthew C., Wassner, Ari J., Wattier, Rachel, Weber, David R., Weese-Mayer, Debra E., Weinberg, Jason B., Weinman, Jason P., Weise, Kathryn L., Weiss, Anna K., Weiss, Pamela F., Weitzman, Carol, Welebir, Morgan P., Wells, Lawrence, Wen, Jessica W., Wendel, Danielle, Werlin, Steven L., Wessels, Michael R., Wetmore, Ralph F., Wexelblatt, Scott L., Wexler, Isaiah D., Clinton White, A., Jr, White, Perrin C., Williams, John V., Willoughby, Rodney E., Jr, Wilschanski, Michael, Wilson, Karen M., Wilson, Pamela, Winell, Jennifer J., Winnie, Glenna B., Wissow, Lawrence, Witters, Peter, Wolf, Joshua, Wolfgram, Peter M., Wolfe, Joanne, Woods, Brandon T., Wright, Benjamin L., Wright, Joseph L., Wright, Terry W., Wu, Eveline Y., Yagupsky, Pablo, Yeh, E. Ann, Yeshokumar, Anusha K., Zaky, Wafik, Zapata, Lauren B., Zeltzer, Lonnie K., Zhou, Amy, and Zuckerman, Barry S.

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2020
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