Search

Your search keyword '"V Sullivan"' showing total 1,022 results
Start Over Author "V Sullivan"

Refine your results

1,022 results on '"V Sullivan"'

1. Aging, HIV infection, and alcohol exert synergist effects on regional thalamic volumes resulting in functional impairment

Author

Adolf Pfefferbaum, Natalie M. Zahr, Stephanie A. Sassoon, Rosemary Fama, Manojkumar Saranathan, Kilian M. Pohl, and Edith V. Sullivan

Subjects
Brain, Age, Alcohol use disorder, HIV, Cognition, Motor, Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429
Abstract

Objective: Pharmacologically-treated people living with HIV infection have near-normal life spans with more than 50 % living into at-risk age for dementia and a disproportionate number relative to uninfected people engaging in unhealthy drinking. Accelerated aging in HIV occurs in some brain structures including the multinucleated thalamus. Unknown is whether aging with HIV affects thalamic nuclei and associated functions differentially and whether the common comorbidity of alcohol use disorder (AUD) + HIV accelerates aging. Methods: This mixed cross-sectional/longitudinal design examined 216 control, 69 HIV, and 74 HIV + AUD participants, age 25–75 years old at initial visit, examined 1–8 times. MRI thalamic volumetry, parcellated using THalamus Optimized Multi-Atlas Segmentation (THOMAS), identified 10 nuclei grouped into 4 functional regions for correlation with age and measures of neuropsychological, clinical, and hematological status. Results: Aging in the control group was best modeled with quadratic functions in the Anterior and Ventral regions and with linear functions in the Medial and Posterior regions. Relative to controls, age-related decline was even steeper in the Anterior and Ventral regions of the HIV group and in the Anterior region of the comorbid group. Anterior volumes of each HIV group declined significantly faster after age 50 (HIV = -2.4 %/year; HIV + AUD = -2.8 %/year) than that of controls (-1.8 %/year). Anterior and Ventral volumes were significantly smaller in the HIV + AUD than HIV-only group when controlling for infection factors. Although compared with controls HIV + AUD declined faster than HIV alone, the two HIV groups did not differ significantly from each other in aging rates. Declining Attention/Working Memory and Motor Skills performance correlated with Anterior and Posterior volume declines in the HIV + AUD group. Conclusions: Regional thalamic volumetry detected normal aging declines, differential and accelerated volume losses in HIV, relations between age-related nuclear and performance declines, and exacerbation of volume declines in comorbid AUD contributing to functional deficits.

Published
2024
Full Text
View/download PDF

5. Prior test experience confounds longitudinal tracking of adolescent cognitive and motor development

Author

Edith V. Sullivan, Wesley K. Thompson, Ty Brumback, Devin Prouty, Susan F. Tapert, Sandra A. Brown, Michael D. De Bellis, Kate B. Nooner, Fiona C. Baker, Ian M. Colrain, Duncan B. Clark, Bonnie J. Nagel, Kilian M. Pohl, and Adolf Pfefferbaum

Subjects
Longitudinal, Practice effects, Development, Cognition, Motor, Medicine (General), R5-920
Abstract

Abstract Background Accurate measurement of trajectories in longitudinal studies, considered the gold standard method for tracking functional growth during adolescence, decline in aging, and change after head injury, is subject to confounding by testing experience. Methods We measured change in cognitive and motor abilities over four test sessions (baseline and three annual assessments) in 154 male and 165 female participants (baseline age 12–21 years) from the National Consortium on Alcohol and NeuroDevelopment in Adolescence (NCANDA) study. At each of the four test sessions, these participants were given a test battery using computerized administration and traditional pencil and paper tests that yielded accuracy and speed measures for multiple component cognitive (Abstraction, Attention, Emotion, Episodic memory, Working memory, and General Ability) and motor (Ataxia and Speed) functions. The analysis aim was to dissociate neurodevelopment from testing experience by using an adaptation of the twice-minus-once tested method, which calculated the difference between longitudinal change (comprising developmental plus practice effects) and practice-free initial cross-sectional performance for each consecutive pairs of test sessions. Accordingly, the first set of analyses quantified the effects of learning (i.e., prior test experience) on accuracy and after speed domain scores. Then developmental effects were determined for each domain for accuracy and speed having removed the measured learning effects. Results The greatest gains in performance occurred between the first and second sessions, especially in younger participants, regardless of sex, but practice gains continued to accrue thereafter for several functions. For all 8 accuracy composite scores, the developmental effect after accounting for learning was significant across age and was adequately described by linear fits. The learning-adjusted developmental effects for speed were adequately described by linear fits for Abstraction, Emotion, Episodic Memory, General Ability, and Motor scores, although a nonlinear fit was better for Attention, Working Memory, and Average Speed scores. Conclusion Thus, what appeared as accelerated cognitive and motor development was, in most cases, attributable to learning. Recognition of the substantial influence of prior testing experience is critical for accurate characterization of normal development and for developing norms for clinical neuropsychological investigations of conditions affecting the brain.

Published
2022
Full Text
View/download PDF

17. The role of scientific evidence in decisions to adopt complex innovations in cancer care settings: a multiple case study in Nova Scotia, Canada

Author

R. Urquhart, C. Kendell, L. Geldenhuys, A. Ross, M. Rajaraman, A. Folkes, L. L. Madden, V. Sullivan, D. Rayson, and G. A. Porter

Subjects
Adoption, Innovation, Evidence, Case study methods, Medicine (General), R5-920
Abstract

Abstract Background Health care delivery and outcomes can be improved by using innovations (i.e., new ideas, technologies, and practices) supported by scientific evidence. However, scientific evidence may not be the foremost factor in adoption decisions and is rarely sufficient. The objective of this study was to examine the role of scientific evidence in decisions to adopt complex innovations in cancer care. Methods Using an explanatory, multiple case study design, we examined the adoption of complex innovations in five purposively sampled cases in Nova Scotia, Canada. Data were collected via documents and key informant interviews. Data analysis involved an in-depth analysis of each case, followed by a cross-case analysis to develop theoretically informed, generalizable knowledge on the role of scientific evidence in innovation adoption that may be applied to similar settings and contexts. Results The analyses identified key concepts alongside important caveats and considerations. Key concepts were (1) scientific evidence underpinned the adoption process, (2) evidence from multiple sources informed decision-making, (3) decision-makers considered three key issues when making decisions, and (4) champions were essential to eventual adoption. Caveats and considerations related to the presence of urgent problems and short-term financial pressures and minimizing risk. Conclusions The findings revealed the different types of issues decision-makers consider while making these decisions and why different sources of evidence are needed in these processes. Future research should examine how different types of evidence are legitimized and why some types are prioritized over others.

Published
2019
Full Text
View/download PDF

18. Episodic memory deficit in HIV infection: common phenotype with Parkinson’s disease, different neural substrates

Author

Rosemary Fama, Eva M. Müller-Oehring, Taylor F. Levine, Edith V. Sullivan, Stephanie A. Sassoon, Priya Asok, Helen M. Brontë-Stewart, Kathleen L. Poston, Kilian M. Pohl, Adolf Pfefferbaum, and Tilman Schulte

Subjects
Histology, General Neuroscience, Anatomy
Abstract

Episodic memory deficits occur in people living with HIV (PLWH) and individuals with Parkinson’s disease (PD). Given known effects of HIV and PD on frontolimbic systems, episodic memory deficits are often attributed to executive dysfunction. Although executive dysfunction, evidenced as retrieval deficits, is relevant to mnemonic deficits, learning deficits may also contribute. Here, the California Verbal Learning Test-II, administered to 42 PLWH, 41 PD participants, and 37 controls, assessed learning and retrieval using measures of free recall, cued recall, and recognition. Executive function was assessed with a composite score comprising Stroop Color-Word Reading and Backward Digit Spans. Neurostructural correlates were examined with MRI of frontal (precentral, superior, orbital, middle, inferior, supplemental motor, medial) and limbic (hippocampus, thalamus) volumes. HIV and PD groups were impaired relative to controls on learning and free and cued recall trials but did not differ on recognition or retention of learned material. In no case did executive functioning solely account for the observed mnemonic deficits or brain-performance relations. Critically, the shared learning and retrieval deficits in HIV and PD were related to different substrates of frontolimbic mnemonic neurocircuitry. Specifically, diminished learning and poorer free and cued recall were related to smaller orbitofrontal volume in PLWH but not PD, whereas diminished learning in PD but not PLWH was related to smaller frontal superior volume. In PD, poorer recognition correlated with smaller thalamic volume and poorer retention to hippocampal volume. Although memory deficits were similar, the neural correlates in HIV and PD suggest different pathogenic mechanisms.

Published
2023
Full Text
View/download PDF

24. Imaging of Brain Structural and Functional Effects in People With Human Immunodeficiency Virus

Author

Erin E O’Connor, Edith V Sullivan, Linda Chang, Dima A Hammoud, Tony W Wilson, Ann B Ragin, Christina S Meade, Jennifer Coughlin, and Beau M Ances

Subjects
Infectious Diseases, Immunology and Allergy
Abstract

Before the introduction of antiretroviral therapy, human immunodeficiency virus (HIV) infection was often accompanied by central nervous system (CNS) opportunistic infections and HIV encephalopathy marked by profound structural and functional alterations detectable with neuroimaging. Treatment with antiretroviral therapy nearly eliminated CNS opportunistic infections, while neuropsychiatric impairment and peripheral nerve and organ damage have persisted among virally suppressed people with HIV (PWH), suggesting ongoing brain injury. Neuroimaging research must use methods sensitive for detecting subtle HIV-associated brain structural and functional abnormalities, while allowing for adjustments for potential confounders, such as age, sex, substance use, hepatitis C coinfection, cardiovascular risk, and others. Here, we review existing and emerging neuroimaging tools that demonstrated promise in detecting markers of HIV-associated brain pathology and explore strategies to study the impact of potential confounding factors on these brain measures. We emphasize neuroimaging approaches that may be used in parallel to gather complementary information, allowing efficient detection and interpretation of altered brain structure and function associated with suboptimal clinical outcomes among virally suppressed PWH. We examine the advantages of each imaging modality and systematic approaches in study design and analysis. We also consider advantages of combining experimental and statistical control techniques to improve sensitivity and specificity of biotype identification and explore the costs and benefits of aggregating data from multiple studies to achieve larger sample sizes, enabling use of emerging methods for combining and analyzing large, multifaceted data sets. Many of the topics addressed in this article were discussed at the National Institute of Mental Health meeting “Biotypes of CNS Complications in People Living with HIV,” held in October 2021, and are part of ongoing research initiatives to define the role of neuroimaging in emerging alternative approaches to identifying biotypes of CNS complications in PWH. An outcome of these considerations may be the development of a common neuroimaging protocol available for researchers to use in future studies examining neurological changes in the brains of PWH.

Published
2023
Full Text
View/download PDF

26. Principles of diagnostic stewardship: A practical guide from the Society for Healthcare Epidemiology of America Diagnostic Stewardship Task Force

Author

Valeria Fabre, Angelina Davis, Daniel J. Diekema, Bruno Granwehr, Mary K. Hayden, Christopher F. Lowe, Christopher D. Pfeiffer, Anna C. Sick-Samuels, Kaede V. Sullivan, Trevor C. Van Schooneveld, and Daniel J. Morgan

Subjects
Microbiology (medical), Infectious Diseases, Epidemiology
Abstract

Executive summaryWe provide an overview of diagnostic stewardship with key concepts that include the diagnostic pathway and the multiple points where interventions can be implemented, strategies for interventions, the importance of multidisciplinary collaboration, and key microbiologic diagnostic tests that should be considered for diagnostic stewardship. The document focuses on microbiologic laboratory testing for adult and pediatric patients and is intended for a target audience of healthcare workers involved in diagnostic stewardship interventions and all workers affected by any step of the diagnostic pathway (ie, ordering, collecting, processing, reporting, and interpreting results of a diagnostic test). This document was developed by the Society for Healthcare Epidemiology of America Diagnostic Stewardship Taskforce.

Published
2023
Full Text
View/download PDF

27. Deep learning identifies morphological determinants of sex differences in the pre-adolescent brain

Author

Ehsan Adeli, Qingyu Zhao, Natalie M. Zahr, Aimee Goldstone, Adolf Pfefferbaum, Edith V. Sullivan, and Kilian M. Pohl

Subjects
Deep learning, Sex differences, Adolescents, Study confounders, Pubertal development, Cerebellum, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

The application of data-driven deep learning to identify sex differences in developing brain structures of pre-adolescents has heretofore not been accomplished. Here, the approach identifies sex differences by analyzing the minimally processed MRIs of the first 8144 participants (age 9 and 10 years) recruited by the Adolescent Brain Cognitive Development (ABCD) study. The identified pattern accounted for confounding factors (i.e., head size, age, puberty development, socioeconomic status) and comprised cerebellar (corpus medullare, lobules III, IV/V, and VI) and subcortical (pallidum, amygdala, hippocampus, parahippocampus, insula, putamen) structures. While these have been individually linked to expressing sex differences, a novel discovery was that their grouping accurately predicted the sex in individual pre-adolescents. Another novelty was relating differences specific to the cerebellum to pubertal development. Finally, we found that reducing the pattern to a single score not only accurately predicted sex but also correlated with cognitive behavior linked to working memory. The predictive power of this score and the constellation of identified brain structures provide evidence for sex differences in pre-adolescent neurodevelopment and may augment understanding of sex-specific vulnerability or resilience to psychiatric disorders and presage sex-linked learning disabilities.

Published
2020
Full Text
View/download PDF

28. Bias-Resilient Neural Network.

Author

Ehsan Adeli 0001, Qingyu Zhao, Adolf Pfefferbaum, Edith V. Sullivan, Li Fei-Fei 0001, Juan Carlos Niebles, and Kilian M. Pohl

Published
2019

29. Effects of prior testing lasting a full year in NCANDA adolescents: Contributions from age, sex, socioeconomic status, ethnicity, site, family history of alcohol or drug abuse, and baseline performance

Author

Edith V. Sullivan, Ty Brumback, Susan F. Tapert, Devin Prouty, Rosemary Fama, Wesley K. Thompson, Sandra A. Brown, Kevin Cummins, Ian M. Colrain, Fiona C. Baker, Duncan B. Clark, Tammy Chung, Michael D. De Bellis, Stephen R. Hooper, Bonnie J. Nagel, B. Nolan Nichols, Weiwei Chu, Dongjin Kwon, Kilian M. Pohl, and Adolf Pfefferbaum

Subjects
Neurophysiology and neuropsychology, QP351-495
Abstract

Longitudinal study provides a robust method for tracking developmental trajectories. Yet inherent problems of retesting pose challenges in distinguishing biological developmental change from prior testing experience. We examined factors potentially influencing change scores on 16 neuropsychological test composites over 1 year in 568 adolescents in the National Consortium on Alcohol and NeuroDevelopment in Adolescence (NCANDA) project. The twice-minus-once-tested method revealed that performance gain was mainly attributable to testing experience (practice) with little contribution from predicted developmental effects. Group mean practice slopes for 13 composites indicated that 60% to ∼100% variance was attributable to test experience; General Ability accuracy showed the least practice effect (29%). Lower baseline performance, especially in younger participants, was a strong predictor of greater gain. Contributions from age, sex, ethnicity, examination site, socioeconomic status, or family history of alcohol/substance abuse were nil to small, even where statistically significant. Recognizing that a substantial proportion of change in longitudinal testing, even over 1-year, is attributable to testing experience indicates caution against assuming that performance gain observed during periods of maturation necessarily reflects development. Estimates of testing experience, a form of learning, may be a relevant metric for detecting interim influences, such as alcohol use or traumatic episodes, on behavior. Keywords: Cognitive development, Motor development, Longitudinal, Alcohol, Adolescence, Practice effects

Published
2017
Full Text
View/download PDF

30. Poor subjective sleep predicts compromised quality of life but not cognitive impairment in abstinent individuals with Alcohol Use Disorder

Author

David Piekarski, Edith V. Sullivan, Adolf Pfefferbaum, and Natalie M. Zahr

Subjects
Male, Sleep Wake Disorders, Depressive Disorder, Major, Health (social science), Depression, General Medicine, Toxicology, Biochemistry, Article, Alcoholism, Behavioral Neuroscience, Neurology, Sleep Initiation and Maintenance Disorders, Quality of Life, Humans, Cognitive Dysfunction, Female, Sleep
Abstract

How disrupted sleep contributes to cognitive dysfunction over the dynamic course of Alcohol Use Disorder (AUD) is an emerging topic of investigation. Here, the Pittsburgh Sleep Quality Index (PSQI) was used to evaluate subjective sleep in 90 individuals with AUD sober for an average of 3 months and in 50 healthy controls. Relative to controls, AUD individuals had higher global PSQI scores (worse sleep), higher scores on the Beck Depression Inventory (BDI), worse Quality of Life (QoL) indicators, and poorer performance on cognitive composite tests (executive functioning, attention and working memory, visual and verbal learning or memory). Among AUD individuals, a higher PSQI score correlated with a higher BDI scores and worse QoL, but not with cognitive scales. Also noted in the AUD group were higher global PSQI scores in individuals also diagnosed with major depressive (MDD) or generalized anxiety (GAD) disorders. Together, the 4 variables explained 29.8% of the variance in AUD PSQI scores. In women with AUD, the 4 factors explained 39.3% of the variance in PSQI scores; in AUD men, the 4 measures explained 19.9% of the variance: MDD was salient in women, QoL in men with AUD suggesting differential factors associate with poor sleep in men and women with AUD even with sustained alcohol abstinence. Here, global PSQI scores were related to clinical diagnoses and life functioning but failed to predict cognitive performance in abstinent AUD individuals.

Published
2022
Full Text
View/download PDF

31. Multiplatform molecular analyses refine classification of gliomas arising in patients with neurofibromatosis type 1

Author

Calixto-Hope G. Lucas, Emily A. Sloan, Rohit Gupta, Jasper Wu, Drew Pratt, Harish N. Vasudevan, Ajay Ravindranathan, Jairo Barreto, Erik A. Williams, Anny Shai, Nicholas S. Whipple, Carol S. Bruggers, Ossama Maher, Burt Nabors, Michael Rodriguez, David Samuel, Melandee Brown, Jason Carmichael, Rufei Lu, Kanish Mirchia, Daniel V. Sullivan, Melike Pekmezci, Tarik Tihan, Andrew W. Bollen, Arie Perry, Anuradha Banerjee, Sabine Mueller, Nalin Gupta, Shawn L. Hervey-Jumper, Nancy Ann Oberheim Bush, Mariza Daras, Jennie W. Taylor, Nicholas A. Butowski, John de Groot, Jennifer L. Clarke, David R. Raleigh, Joseph F. Costello, Joanna J. Phillips, Alyssa T. Reddy, Susan M. Chang, Mitchel S. Berger, and David A. Solomon

Subjects
Cellular and Molecular Neuroscience, Neurology (clinical), Pathology and Forensic Medicine
Abstract

Gliomas arising in the setting of neurofibromatosis type 1 (NF1) are heterogeneous, occurring from childhood through adulthood, can be histologically low-grade or high-grade, and follow an indolent or aggressive clinical course. Comprehensive profiling of genetic alterations beyond NF1 inactivation and epigenetic classification of these tumors remain limited. Through next-generation sequencing, copy number analysis, and DNA methylation profiling of gliomas from 47 NF1 patients, we identified 2 molecular subgroups of NF1-associated gliomas. The first harbored biallelic NF1 inactivation only, occurred primarily during childhood, followed a more indolent clinical course, and had a unique epigenetic signature for which we propose the terminology “pilocytic astrocytoma, arising in the setting of NF1”. The second subgroup harbored additional oncogenic alterations including CDKN2A homozygous deletion and ATRX mutation, occurred primarily during adulthood, followed a more aggressive clinical course, and was epigenetically diverse, with most tumors aligning with either high-grade astrocytoma with piloid features or various subclasses of IDH-wildtype glioblastoma. Several patients were treated with small molecule MEK inhibitors that resulted in stable disease or tumor regression when used as a single agent, but only in the context of those tumors with NF1 inactivation lacking additional oncogenic alterations. Together, these findings highlight recurrently altered pathways in NF1-associated gliomas and help inform targeted therapeutic strategies for this patient population.

Published
2022
Full Text
View/download PDF

32. A prospective study revealing a compounded burden of COVID-19, sex, and clinical diagnosis of alcohol use disorder and HIV infection on quality of life, anxiety, and alcohol use

Author

Séverine Lannoy, Rosemary Fama, Stephanie A. Sassoon, Anne-Pascale Le Berre, Priya Asok, Natalie M. Zahr, Adolf Pfefferbaum, and Edith V. Sullivan

Subjects
Male, Alcoholism, Psychiatry and Mental health, Surveys and Questionnaires, Quality of Life, COVID-19, Humans, Female, HIV Infections, Prospective Studies, Anxiety, Pandemics, Biological Psychiatry
Abstract

The COVID-19 pandemic led to unprecedented restrictions to mitigate disease spread, leading to consequences affecting mental health. Many studies examining COVID-19 pandemic effects on well-being and mental health initiated inquiry after the pandemic onset, whereas we used self-report questionnaires obtained before the pandemic to re-assess the same functions during the pandemic. Participants were drawn from our ongoing longitudinal studies of people with HIV infection, alcohol use disorder (AUD), HIV + AUD comorbidity, and controls. We used phone or mail contact to invite all to participate in our COVID phone survey, which included three self-report questionnaires: Health-related Quality of Life (QoL), State-Trait Anxiety Inventory (STAI), and Alcohol Use Disorder Identification Test (AUDIT). Of 218 eligible participants, 86 responded (July 2020-March 2021): clinical (29 men, 23 women; 17 AUD, 21 HIV, 14 HIV + AUD); control (17 men, 17 women). QoL scores declined, and anxiety symptoms increased from pre-COVID surveys in all groups; clinical women reported greater negative changes than the other groups. QoL subscales revealed COVID-related declines in emotional well-being in all groups, with clinical women reporting additional declines in energy, physical and social functioning, health, and pain increase. Clinical men also reported health declines. Although AUDIT scores were stable in all groups between assessments, changes in AUDIT scores were inversely correlated with QoL scores in clinical women; in clinical men, changes in STAI scores were inversely correlated with QoL scores. Although all groups were adversely affected by the pandemic, the negative effects were greater in the clinical group regardless of diagnosis and greatest in clinical women.

Published
2022
Full Text
View/download PDF

34. Evaluation of Molecularly Imprinted Polymers as Synthetic Virus Neutralizing Antibody Mimics

Author

Simon P. Graham, Hazim F. El-Sharif, Sabha Hussain, Rieke Fruengel, Rebecca K. McLean, Philippa C. Hawes, Mark V. Sullivan, and Subrayal M. Reddy

Subjects
molecularly imprinted polymer, virus, porcine reproductive and respiratory syndrome virus, neutralization, synthetic antibody mimic, Biotechnology, TP248.13-248.65
Abstract

Rapid development of antibody-based therapeutics are crucial to the agenda of innovative manufacturing of macromolecular therapies to combat emergent diseases. Although highly specific, antibody therapies are costly to produce. Molecularly imprinted polymers (MIPs) constitute a rapidly-evolving class of antigen-recognition materials that act as synthetic antibodies. We report here on the virus neutralizing capacity of hydrogel-based MIPs. We produced MIPs using porcine reproductive and respiratory syndrome virus (PRRSV-1), as a model mammalian virus. Assays were performed to evaluate the specificity of virus neutralization, the effect of incubation time and MIP concentration. Polyacrylamide and N-hydroxymethylacrylamide based MIPs produced a highly significant reduction in infectious viral titer recovered after treatment, reducing it to the limit of detection of the assay. MIP specificity was tested by comparing their neutralizing effects on PRRSV-1 to the effects on the unrelated bovine viral diarrhea virus-1; no significant cross-reactivity was observed. The MIPs demonstrated effective virus neutralization in just 2.5 min and their effect was concentration dependent. These data support the further evaluation of MIPs as synthetic antibodies as a novel approach to the treatment of viral infection.

Published
2019
Full Text
View/download PDF

35. Convergence of three parcellation approaches demonstrating cerebellar lobule volume deficits in Alcohol Use Disorder

Author

Edith V. Sullivan, Natalie M. Zahr, Manojkumar Saranathan, Kilian M. Pohl, and Adolf Pfefferbaum

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429
Abstract

Recent advances in robust and reliable methods of MRI-derived cerebellar lobule parcellation volumetry present the opportunity to assess effects of Alcohol Use Disorder (AUD) on selective cerebellar lobules and relations with indices of nutrition and motor functions. In pursuit of this opportunity, we analyzed high-resolution MRI data acquired in 24 individuals with AUD and 20 age- and sex-matched controls with a 32-channel head coil using three different atlases: the online automated analysis pipeline volBrain Ceres, SUIT, and the Johns Hopkins atlas. Participants had also completed gait and balance examination and hematological analysis of nutritional and liver status, enabling testing of functional meaningfulness of each cerebellar parcellation scheme. Compared with controls, each quantification approach yielded similar patterns of group differences in regional volumes: All three approaches identified AUD-related deficits in total tissue and total gray matter, but only Ceres identified a total white matter volume deficit. Convergent volume differences occurred in lobules I-V, Crus I, VIIIB, and IX. Coefficients of variation (CVs) were

Published
2019
Full Text
View/download PDF

36. Hippocampal subfield CA2+3 exhibits accelerated aging in Alcohol Use Disorder: A preliminary study

Author

Natalie M. Zahr, Kilian M. Pohl, Manojkumar Saranathan, Edith V. Sullivan, and Adolf Pfefferbaum

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429
Abstract

The profile of brain structural dysmorphology of individuals with Alcohol Use Disorders (AUD) involves disruption of the limbic system. In vivo imaging studies report hippocampal volume loss in AUD relative to controls, but only recently has it been possible to articulate different regions of this complex structure. Volumetric analysis of hippocampal regions rather than total hippocampal volume may augment differentiation of disease processes. For example, damage to hippocampal subfield cornu ammonis 1 (CA1) is often reported in Alzheimer's disease (AD), whereas deficits in CA4/dentate gyrus are described in response to stress and trauma. Two previous studies explored the effects of chronic alcohol use on hippocampal subfields: one reported smaller volume of the CA2+3 in alcohol-dependent subjects relative to controls, associated with years of alcohol consumption; the other, smaller volumes of presubiculum, subiculum, and fimbria in alcohol-dependent relative to control men.The current study, conducted in 24 adults with DSM5-diagnosed AUD (7 women, 53.7 ± 8.8) and 20 controls (7 women, 54.1 ± 9.3), is the first to use FreeSurfer 6.0, which provides state-of-the art hippocampal parcellation, to explore the sensitivity of hippocampal sufields to alcoholism. T1- and T2- images were collected on a GE MR750 system with a 32-channel Nova head coil. FreeSurfer 6.0 hippocampal subfield analysis produced 12 subfields: parasubiculum; presubiculum; subiculum; CA1; CA2+3; CA4; GC-ML-DG (Granule Cell (GC) and Molecular Layer (ML) of the Dentate Gyrus (DG)); molecular layer; hippocampus-amygdala-transition-area (HATA); fimbria; hippocampal tail; hippocampal fissure; and whole volume for left and right hippocampi. A comprehensive battery of neuropsychological tests comprising attention, memory and learning, visuospatial abilities, and executive functions was administered.Multiple regression analyses of raw volumetric data for each subfields by group, age, sex, hemisphere, and supratentorial volume (svol) showed significant effects of svol (p

Published
2019
Full Text
View/download PDF

38. Common mission planning and situation awareness model for UxS Command and Control systems

Author

Teodor Hanchevici, Piotr Zaborowski, Donald V. Sullivan, and Alex Robin

Abstract

Multi-vendor operations of uncrewed vehicles as part of the observations, surveillance and surveying are already daily practice in many fields. The popularity of the integration platforms that manage multiple, sometimes simultaneously, systems is also already proven by the integration platforms' popularity. With new European regulations for the drone industry and the growing popularity of various (ground, water surface, underwater, aerial) systems exploitations, the need for situation awareness and planning that will be flexible and vendor lock-in free is leveraged. However, despite several recent efforts and some popular specifications that aim at becoming de-facto standards, civil operations' interoperability challenge is unsolved. To assess whether a shared data model is suitable for multi-domain, multi-heterogeneous vehicle use, and challenge it with real applications and demonstrate the exchange of command and control information, OGC members started an Interoperability Experiment in 2022. IE is based on a data model developed by Kongsberg Geospatial and partners under the Standards-based UxS Interoperability Test-bed (SUIT). The IE considers those other standards and specifications which were used in the SUIT work as well as other Command and Control practices from the aviation and marine communities. The presentation depicts selected use cases and scenarios and outlines the information model of the localized situation awareness and mission planning and operations. Being specific for autonomous vehicle operations, they extend the needs of generic geospatial representations. Authors will explain relations to other similar models like (LSTS, MavLink, UMAA, STANAG 4586, JAUS, C2INav) and modern geospatial data exchange standards like OGC SensorThings, Features, Moving Features, GeoPose.

Published
2023
Full Text
View/download PDF

39. Harmonizing DTI measurements across scanners to examine the development of white matter microstructure in 803 adolescents of the NCANDA study.

Author

Kilian M. Pohl, Edith V. Sullivan, Torsten Rohlfing, Weiwei Chu, Dongjin Kwon, B. Nolan Nichols, Yong Zhang 0004, Sandra A. Brown, Susan F. Tapert, Kevin Cummins, Wesley K. Thompson, Ty Brumback, Ian M. Colrain, Fiona C. Baker, Devin Prouty, Michael D. De Bellis, James T. Voyvodic, Duncan B. Clark, Claudiu V. Schirda, Bonnie J. Nagel, and Adolf Pfefferbaum

Published
2016
Full Text
View/download PDF

40. Big Data Analytics for Earth Sciences: the EarthServer approach.

Author

Peter Baumann 0001, Paolo Mazzetti, Joachim Ungar, Roberto Barbera, Damiano Barboni, Alan Beccati, Lorenzo Bigagli, Enrico Boldrini, Riccardo Bruno, Antonio Calanducci, Piero Campalani, D. Oliver Clements, Alex Mircea Dumitru, Mike Grant, Pasquale Herzig, George Kakaletris, John Laxton, Panagiota Koltsida, Kinga Lipskoch, Alireza Rezaei Mahdiraji, Simone Mantovani, Vlad Merticariu, Antonio Messina, Dimitar Misev, Stefano Natali, Stefano Nativi, Jelmer Oosthoek, Marco Pappalardo, James Passmore, Angelo Pio Rossi, Francesco Rundo, Marcus Sen, Vittorio Sorbera, Don V. Sullivan, Mario Torrisi, Leonardo Trovato, Maria Grazia Veratelli, and Sebastian Wagner 0003

Published
2016
Full Text
View/download PDF

42. Neurofunctional characteristics of executive control in older people with HIV infection: a comparison with Parkinson’s disease

Author

Eva M. Müller-Oehring, Jui-Yang Hong, Kathleen L. Poston, Helen M. Brontë-Stewart, Edith V. Sullivan, Lawrence McGlynn, and Tilman Schulte

Subjects
Cognitive Neuroscience, HIV Infections, Parkinson Disease, Neuropsychological Tests, Magnetic Resonance Imaging, Article, Executive Function, Behavioral Neuroscience, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Neurology, Humans, Radiology, Nuclear Medicine and imaging, Neurology (clinical), Aged
Abstract

Expression of executive dysfunctions is marked by substantial heterogeneity in people living with HIV infection (PLWH) and attributed to neuropathological degradation of frontostriatal circuitry with age and disease. We compared the neurophysiology of executive function in older PLWH and Parkinson’s disease (PD), both affecting frontostriatal systems. Thirty-one older PLWH, 35 individuals with PD, and 28 older healthy controls underwent executive task-activated fMRI, neuropsychological testing, and a clinical motor exam. fMRI task conditions distinguished cognitive control operations, invoking a lateral frontoparietal network, and motor control operations, activating a cerebellar-precentral-medial prefrontal network. HIV-specific findings denoted a prominent sensorimotor hypoactivation during cognitive control and striatal hypoactivation during motor control related to CD4(+) T cell count and HIV disease duration. Activation deficits overlapped for PLWH and PD, relative to controls, in dorsolateral frontal, medial frontal, and middle cingulate cortices for cognitive control, and in limbic, frontal, parietal, and cerebellar regions for motor control. Thus, despite well-controlled HIV infection, frontostriatal and sensorimotor activation deficits occurred during executive control in older PLWH. Overlapping activation deficits in posterior cingulate and hippocampal regions point toward similarities in mesocorticolimbic dopaminergic system aberrations among older PLWH and PD. The extent of pathophysiology in PLWH was associated with variations in immune system health, neural signature consistent with subclinical parkinsonism, and mild neurocognitive impairment. The failure to adequately engage these pathways could be an early sign for cognitive and motor functional decline in the aging population of PLWH.

Published
2022
Full Text
View/download PDF

43. Aging Accelerates Postural Instability in HIV Infection: Contributing Sensory Biomarkers

Author

Edith V. Sullivan, Natalie M. Zahr, Stephanie A. Sassoon, and Adolf Pfefferbaum

Subjects
Pharmacology, Immunology, Neuroscience (miscellaneous), Immunology and Allergy
Abstract

People living with HIV infection (PWH) who are adequately treated pharmacologically are now likely to have a near normal life span. Along with this benefit of the aging HIV population are potential physical problems attendant to aging, including postural stability. Whether aging with HIV accelerates age-related liability for postural instability and what sensory factors contribute to imbalance were examined in 227 PWH and 137 people living without HIV (PWoH), age 25 to 75 years. A mixed cross-sectional/longitudinal design revealed steeper aging trajectories of the PWH than PWoH in sway path length, measured as center-of-pressure micro-displacements with a force platform while a person attempted to stand still. Sway paths were disproportionately longer for PWH than PWoH when tested with eyes closed than open. Multiple regression identified objective measures of sensory perception as unique predictors of sway path length, whereas age, sway path length, and self-reports of falls were predictors of standing on one leg, a common measure of ataxia. Knowledge about sensory signs and symptoms of imbalance in postural stability with and without visual information may serve as modifiable risk factors for averting instability and liability for falls in the aging HIV population.

Published
2022
Full Text
View/download PDF

45. Thallium isotopes as indicators of ore mineralization at the Zn-rich sediment-hosted massive sulfide TL Deposit, British Columbia, Canada

Author

Derek R. Knaack, K. V. Sullivan, M. I. Leybourne, C. E. Dunn, and D. Layton-Matthews

Subjects
Geochemistry and Petrology, General Earth and Planetary Sciences, General Chemistry, General Environmental Science
Abstract

Few studies have focused on the application of the Tl isotopic system for geochemical exploration. We report ε 205 Tl values of rock samples from the TL Deposit, British Columbia, Canada – a sediment-hosted massive sulfide (SHMS) deposit with characteristics of a Broken Hill-type deposit – and investigate relationships with major and trace element geochemistry. Maps generated using Tl isotope and trace element data indicate that ε 205 Tl values can potentially be used to fingerprint ore mineralization at the TL Deposit. The sources of Tl and other metals (Ag, Pb, Zn) are assessed using Tl isotope data. Measured ε 205 Tl values exhibit positive correlations with Pb, sedimentary exhalative metal index (Zn + 100*Pb + 100*Tl), and the redox proxy, U/Th, and negative correlations with Be, Cd, Ce, La, Ni and Th. Individual lithologies have distinct Tl isotopic compositions. Metal-rich heavily altered samples have relatively high ε 205 Tl values (−5.0 to −2.5 ε -units) reflecting the euxinic conditions of the global Paleoproterozoic ocean and hydrothermal influence. Samples with lower ε 205 Tl values (−15 to −7.6 ε -units) reflect a combination of their mineralogy (phyllosilicate minerals such as biotite and clinochlore), Tl from sediments reflecting the Tl isotopic composition of modern seawater, and possible low-temperature alteration processes. Samples with high Pb and Ag contents have high ε 205 Tl values, indicating a hydrothermal origin of these metals, whereas Zn is highest in samples with low ε 205 Tl values, indicating a low-temperature or sedimentary origin. Thallium isotopes, paired with conventional geochemical data, show promise as a useful tool for exploration of SHMS deposits with Broken Hill-type characteristics. Supplementary material: Major, minor and trace element contents of samples and reference materials, blank values, correlation coefficient values, and XRD patterns are available at https://doi.org/10.6084/m9.figshare.c.6370671 Thematic collection: This article is part of the Geochemical processes related to mined, milled, or natural metal deposits collection available at: https://www.lyellcollection.org/topic/collections/geochemical-processes-related-to-mined-milled-or-natural-metal-deposits

Published
2023
Full Text
View/download PDF

48. Jacobian Maps Reveal Under-reported Brain Regions Sensitive to Extreme Binge Ethanol Intoxication in the Rat

Author

Qingyu Zhao, Michael Fritz, Adolf Pfefferbaum, Edith V. Sullivan, Kilian M. Pohl, and Natalie M. Zahr

Subjects
alcohol, addiction, rodent, colliculus, thalamus, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Human anatomy, QM1-695
Abstract

Individuals aged 12–20 years drink 11% of all alcohol consumed in the United States with more than 90% consumed in the form of binge drinking. Early onset alcohol use is a strong predictor of future alcohol dependence. The study of the effects of excessive alcohol use on the human brain is hampered by limited information regarding the quantity and frequency of exposure to alcohol. Animal models can control for age at alcohol exposure onset and enable isolation of neural substrates of exposure to different patterns and quantities of ethanol (EtOH). As with humans, a frequently used binge exposure model is thought to produce dependence and affect predominantly corticolimbic brain regions. in vivo neuroimaging enables animals models to be examined longitudinally, allowing for each animal to serve as its own control. Accordingly, we conducted 3 magnetic resonance imaging (MRI) sessions (baseline, binge, recovery) to track structure throughout the brains of wild type Wistar rats to test the hypothesis that binge EtOH exposure affects specific brain regions in addition to corticolimbic circuitry. Voxel-based comparisons of 13 EtOH- vs. 12 water- exposed animals identified significant thalamic shrinkage and lateral ventricular enlargement as occurring with EtOH exposure, but recovering with a week of abstinence. By contrast, pretectal nuclei and superior and inferior colliculi shrank in response to binge EtOH treatment but did not recover with abstinence. These results identify brainstem structures that have been relatively underreported but are relevant for localizing neurocircuitry relevant to the dynamic course of alcoholism.

Published
2018
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results