Your search keyword '"Burton KL"' showing total 9 results

1. Factors affecting the summer carbon dioxide budget of subarctic wetland tundra

Author

Burton, KL, primary, Rouse, WR, additional, and Boudreau, LD, additional

Published

1996

2. Structural Racism and Racial Trauma Among African Americans at Elevated Risk for HIV Infection.

Author

Burton KL, Ritchwood TD, and Metzger IW

Subjects

Humans, Black or African American, Systemic Racism, Racial Groups, HIV Infections, Racism

Published

2023

3. An expanded mammal mitogenome dataset from Southeast Asia.

Author

Mohd Salleh F, Ramos-Madrigal J, Peñaloza F, Liu S, Mikkel-Holger SS, Riddhi PP, Martins R, Lenz D, Fickel J, Roos C, Shamsir MS, Azman MS, Burton KL, Stephen JR, Wilting A, and Gilbert MTP

Subjects

Animals, Asia, Southeastern, Biodiversity, Computational Biology methods, DNA Barcoding, Taxonomic, Genetic Variation, Genomics methods, Molecular Sequence Annotation, Phylogeny, Phylogeography, Reproducibility of Results, Databases, Nucleic Acid, Genome, Mitochondrial, Mammals genetics

Abstract

Southeast (SE) Asia is 1 of the most biodiverse regions in the world, and it holds approximately 20% of all mammal species. Despite this, the majority of SE Asia's genetic diversity is still poorly characterized. The growing interest in using environmental DNA to assess and monitor SE Asian species, in particular threatened mammals-has created the urgent need to expand the available reference database of mitochondrial barcode and complete mitogenome sequences. We have partially addressed this need by generating 72 new mitogenome sequences reconstructed from DNA isolated from a range of historical and modern tissue samples. Approximately 55 gigabases of raw sequence were generated. From this data, we assembled 72 complete mitogenome sequences, with an average depth of coverage of ×102.9 and ×55.2 for modern samples and historical samples, respectively. This dataset represents 52 species, of which 30 species had no previous mitogenome data available. The mitogenomes were geotagged to their sampling location, where known, to display a detailed geographical distribution of the species. Our new database of 52 taxa will strongly enhance the utility of environmental DNA approaches for monitoring mammals in SE Asia as it greatly increases the likelihoods that identification of metabarcoding sequencing reads can be assigned to reference sequences. This magnifies the confidence in species detections and thus allows more robust surveys and monitoring programmes of SE Asia's threatened mammal biodiversity. The extensive collections of historical samples from SE Asia in western and SE Asian museums should serve as additional valuable material to further enrich this reference database., (© The Author 2017. Published by Oxford University Press.)

Published

2017

4. Shared versus distinct genetic contributions of mental wellbeing with depression and anxiety symptoms in healthy twins.

Author

Routledge KM, Burton KL, Williams LM, Harris A, Schofield PR, Clark CR, and Gatt JM

Subjects

Adolescent, Adult, Anxiety diagnosis, Anxiety psychology, Depression diagnosis, Depression psychology, Diseases in Twins diagnosis, Diseases in Twins psychology, Female, Health Status, Humans, Male, Middle Aged, Surveys and Questionnaires, Twins, Dizygotic psychology, Twins, Monozygotic psychology, Young Adult, Anxiety genetics, Depression genetics, Diseases in Twins genetics, Mental Health, Twins, Dizygotic genetics, Twins, Monozygotic genetics

Abstract

Mental wellbeing and mental illness symptoms are typically conceptualized as opposite ends of a continuum, despite only sharing about a quarter in common variance. We investigated the normative variation in measures of wellbeing and of depression and anxiety in 1486 twins who did not meet clinical criteria for an overt diagnosis. We quantified the shared versus distinct genetic and environmental variance between wellbeing and depression and anxiety symptoms. The majority of participants (93%) reported levels of depression and anxiety symptoms within the healthy range, yet only 23% reported a wellbeing score within the "flourishing" range: the remainder were within the ranges of "moderate" (67%) or "languishing" (10%). In twin models, measures of wellbeing and of depression and anxiety shared 50.09% of variance due to genetic factors and 18.27% due to environmental factors; the rest of the variance was due to unique variation impacting wellbeing or depression and anxiety symptoms. These findings suggest that an absence of clinically-significant symptoms of depression and anxiety does not necessarily indicate that an individual is flourishing. Both unique and shared genetic and environmental factors may determine why some individuals flourish in the absence of symptoms while others do not., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

5. Sex differences in the shared genetics of dimensions of self-reported depression and anxiety.

Author

Burton KL, Williams LM, Richard Clark C, Harris A, Schofield PR, and Gatt JM

Subjects

Adolescent, Adult, Australia epidemiology, Comorbidity, Diseases in Twins genetics, Environment, Female, Humans, Male, Middle Aged, Models, Genetic, Self Report, Twins, Dizygotic genetics, Twins, Monozygotic genetics, Young Adult, Anxiety epidemiology, Anxiety genetics, Depression epidemiology, Depression genetics, Registries, Sex Characteristics

Abstract

Background: The prevalence of depression and anxiety symptoms and their comorbidity varies between males and females for reasons still unknown. This study aims to test whether differences between males and females in self-reported symptoms and their covariation are caused by variations in the magnitude of genetic and environmental factors., Methods: 750 monozygotic and dizygotic healthy twin pairs (18-60 years; M=39.77 years) participated in the TWIN-E project. Univariate and multivariate genetic modelling was undertaken using the Depression Anxiety Stress Scale (DASS-42)., Results: Additive genetics and unique environment contributed to self-reported depression (heritability, h(2): 34%), anxiety (h(2): 30%) and stress (h(2): 34%) scores in univariate models, and to the common latent factor (h(2): 39%) in the multivariate model. No sex differences in magnitude of estimates for DASS-42 scores were found in the univariate model. However when considering correlated depression and anxiety symptomatology only shared genetic factors between depression and anxiety contributed to depression scores in males, but both specific and shared genetic factors contributed to depression scores in females., Limitations: The results are limited to the sample of healthy, community, adult, same sex twin pairs who participated in the study., Conclusions: Differences in males and females in genetic aetiology of self-reported dimensions of depression are only apparent when taking into consideration the covariation with self-reported anxiety. This difference is highlighted by the finding that both common and specific genetic factors contribute to self-reported depression in females but not males. This novel finding may help explain the increased incidence of depression symptoms in females., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

6. Specific and common genes implicated across major mental disorders: a review of meta-analysis studies.

Author

Gatt JM, Burton KL, Williams LM, and Schofield PR

Subjects

Adult, Anxiety Disorders genetics, Bipolar Disorder genetics, Depressive Disorder, Major genetics, Female, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Schizophrenia genetics, Apolipoproteins E genetics, Brain-Derived Neurotrophic Factor genetics, Catechol O-Methyltransferase genetics, Genetic Variation, Mental Disorders genetics, Peptidyl-Dipeptidase A genetics

Abstract

Major efforts have been directed at family-based association and case-control studies to identify the involvement of candidate genes in the major disorders of mental health. What remains unknown is whether candidate genes are associated with multiple disorders via pleiotropic mechanisms, and/or if other genes are specific to susceptibility for individual disorders. Here we undertook a review of genes that have been identified in prior meta-analyses examining specific genes and specific mental disorders that have core disruptions to emotional and cognitive function and contribute most to burden of illness- major depressive disorder (MDD), anxiety disorders (AD, including panic disorder and obsessive compulsive disorder), schizophrenia (SZ) and bipolar disorder (BD) and attention deficit hyperactivity disorder (ADHD). A literature review was conducted up to end-March 2013 which included a total of 1519 meta-analyses across 157 studies reporting multiple genes implicated in one or more of the five disorders studied. A total of 134 genes (206 variants) were identified as significantly associated risk variants for MDD, AD, ADHD, SZ or BD. Null genetic effects were also reported for 195 genes (426 variants). 13 genetic variants were shared in common between two or more disorders (APOE e4, ACE Ins/Del, BDNF Val66Met, COMT Val158Met, DAOA G72/G30 rs3918342, DAT1 40-bp, DRD4 48-bp, SLC6A4 5-HTTLPR, HTR1A C1019G, MTHR C677T, MTHR A1298C, SLC6A4 VNTR and TPH1 218A/C) demonstrating evidence for pleiotrophy. Another 12 meta-analyses of GWAS studies of the same disorders were identified, with no overlap in genetic variants reported. This review highlights the progress that is being made in identifying shared and unique genetic mechanisms that contribute to the risk of developing several major psychiatric disorders, and identifies further steps for progress., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

7. The heritability of mental health and wellbeing defined using COMPAS-W, a new composite measure of wellbeing.

Author

Gatt JM, Burton KL, Schofield PR, Bryant RA, and Williams LM

Subjects

Adolescent, Adult, Australia, Factor Analysis, Statistical, Female, Humans, Male, Mental Disorders psychology, Middle Aged, Psychometrics, Reproducibility of Results, Mental Disorders genetics, Mental Health, Personal Satisfaction, Psychiatric Status Rating Scales statistics & numerical data, Surveys and Questionnaires standards

Abstract

Mental health is not simply the absence of mental illness; rather it is a distinct entity representing wellness. Models of wellbeing have been proposed that emphasize components of subjective wellbeing, psychological wellbeing, or a combination of both. A new 26-item scale of wellbeing (COMPAS-W) was developed in a cohort of 1669 healthy adult twins (18-61 years). The scale was derived using factor analysis of multiple scales of complementary constructs and confirmed using tests of reliability and convergent validity. Bivariate genetic modeling confirmed its heritability. From an original 89 items we identified six independent subcomponents that contributed to wellbeing. The COMPAS-W scale and its subcomponents showed construct validity against psychological and physical health behaviors, high internal consistency (average r=0.71, Wellbeing r=0.84), and 12-month test-retest reliability (average r=0.62, Wellbeing r=0.82). There was a moderate contribution of genetics to total Wellbeing (heritability h(2)=48%) and its subcomponents: Composure (h(2)=24%), Own-worth (h(2)=42%), Mastery (h(2)=40%), Positivity (h(2)=42%), Achievement (h(2)=32%) and Satisfaction (h(2)=43%). Multivariate genetic modeling indicated genetic variance was correlated across the scales, suggesting common genetic factors contributed to Wellbeing and its subcomponents. The COMPAS-W scale provides a validated indicator of wellbeing and offers a new tool to quantify mental health., (Copyright © 2014 Elsevier Ireland Ltd. All rights reserved.)

Published

2014

8. Postnatal changes in the expression pattern of the imprinted signalling protein XLαs underlie the changing phenotype of deficient mice.

Author

Krechowec SO, Burton KL, Newlaczyl AU, Nunn N, Vlatković N, and Plagge A

Subjects

Animals, Animals, Newborn, Base Sequence, Biomarkers metabolism, Brain drug effects, Chromogranins, GTP-Binding Protein alpha Subunits, Gs metabolism, Gene Silencing drug effects, Gene Targeting, Genetic Loci genetics, Genomic Imprinting drug effects, Hypothalamus drug effects, Hypothalamus metabolism, Insulin pharmacology, Leptin pharmacology, Mice, Mice, Inbred C57BL, Mice, Knockout, Molecular Sequence Data, Muscles drug effects, Muscles metabolism, Myocytes, Smooth Muscle drug effects, Myocytes, Smooth Muscle metabolism, Neuropeptides metabolism, Phenotype, Signal Transduction drug effects, Spinal Cord drug effects, Spinal Cord metabolism, Brain growth & development, Brain metabolism, GTP-Binding Protein alpha Subunits, Gs deficiency, GTP-Binding Protein alpha Subunits, Gs genetics, Gene Expression Regulation, Developmental drug effects, Genomic Imprinting genetics, Signal Transduction genetics

Abstract

The alternatively spliced trimeric G-protein subunit XLαs, which is involved in cAMP signalling, is encoded by the Gnasxl transcript of the imprinted Gnas locus. XLαs deficient mice show neonatal feeding problems, leanness, inertia and a high mortality rate. Mutants that survive to weaning age develop into healthy and fertile adults, which remain lean despite elevated food intake. The adult metabolic phenotype can be attributed to increased energy expenditure, which appears to be caused by elevated sympathetic nervous system activity. To better understand the changing phenotype of Gnasxl deficient mice, we compared XLαs expression in neonatal versus adult tissues, analysed its co-localisation with neural markers and characterised changes in the nutrient-sensing mTOR1-S6K pathway in the hypothalamus. Using a newly generated conditional Gnasxl lacZ gene trap line and immunohistochemistry we identified various types of muscle, including smooth muscle cells of blood vessels, as the major peripheral sites of expression in neonates. Expression in all muscle tissues was silenced in adults. While Gnasxl expression in the central nervous system was also developmentally silenced in some midbrain nuclei, it was upregulated in the preoptic area, the medial amygdala, several hypothalamic nuclei (e.g. arcuate, dorsomedial, lateral and paraventricular nuclei) and the nucleus of the solitary tract. Furthermore, expression was detected in the ventral medulla as well as in motoneurons and a subset of sympathetic preganglionic neurons of the spinal cord. In the arcuate nucleus of Gnasxl-deficient mice we found reduced activity of the nutrient sensing mTOR1-S6K signalling pathway, which concurs with their metabolic status. The expression in these brain regions and the hypermetabolic phenotype of adult Gnasxl-deficient mice imply an inhibitory function of XLαs in energy expenditure and sympathetic outflow. By contrast, the neonatal phenotype of mutant mice appears to be due to a transient role of XLαs in muscle tissues.

Published

2012

9. The Minnesota dental practice analysis system.

Author

Meskin L, Gooch BF, Davidson GB, Burton KL, and Oliver RC

Subjects

Adult, Dental Care statistics & numerical data, Health Services Needs and Demand, Humans, Middle Aged, Minnesota, Dentistry, Practice Management, Dental trends, Professional Practice trends

Abstract

The Minnesota Dental Practice Analysis System (DPAS) is a three-year project sponsored cooperatively by the University of Minnesota's School of Dentistry, Health Services Research Center, and the Minnesota Dental Association. The primary intent of the DPAS is to generate timely, reliable information on dental practice conditions for dental work force planning efforts. The system semiannually collects data from a representative sample of Minnesota dentists to monitor trends in such important areas as practice productivity, auxiliary utilization, types of procedures performed, payment mechanisms, and dental fees. Preliminary results of the project indicate that, in comparison with 1980 indicators, overall practice conditions among established Minnesota dentists have declined.

Published

1983