Motor skill development of children with Down syndrome

Passarini, John Richard

January 2001

Thesis (Ed.D.)--Boston University / This study was conducted for the purpose of determining the effectiveness of a home-based motor activity program on children with Down syndrome 6 to 10 years of age. Twenty-six children with Down syndrome and their respective families participated in this twelve-week study. The Circles Of Learning instructional program was created, and fieldtested. The Test of Gross Motor Development (TGMD) provided base-line data for measures of progress in fundamental motor skills. Parents were instructed in how to teach locomotor skills and object control skills as measured by the TGMD. The methods required seven distinct activities: the creation of an instructional manual; recruitment and instruction of project assistants; identification and recruitment of the subjects and their families; pretest and posttest assessment of subjects; instructional training of parents; and the twelve week intervention. The comparison (C) group received the Handwriting Without Tears program during the 12 week intervention period. When compared with the (C) group, all subjects in the experimental (E) group showed statistically significant improvement in the acquisition of fundamental motor skills as measured by the TGMD. Four (E) group subjects improved to the "average" range for typically developing children. Ten of the 11 (E) group subjects continued to improved their demonstrated fundamental motor skill performance two weeks after the intervention, while one subject maintained his gains. Weekly parent comments during the intervention gave testimony to the effectiveness of the intervention supporting primary and secondary gains for the subjects. Parents reported that interactions between family members and the subjects increased and fundamental motor skills improved during spontaneous unstructured play and during organized activities at home and at school. This study challenges the previous research suggesting children with Down syndrome need specialized motor development programs. Furthermore, this study demonstrates that the acquisition of fundamental motor skills for children with Down syndrome can be accelerated.

Down syndrome

Child

Motor skills

Child development

Physical activity in individuals with Down syndrome: A qualitative examination of the perspectives of guardians and health professionals

Schultz, Emma

13 May 2022

Identifying factors that influence physical activity (PA) among individuals with Down syndrome (DS) is essential for PA promotion. Insight can be gained from guardians and health professionals. The purpose was to compare guardians and health professional perspectives on facilitators and barriers of PA in individuals with DS. Interviews were conducted with 11 guardians (5 mothers, 4 fathers, 2 legal guardians) and 11 professionals (4 PA specialists, 3 physical therapists, 4 occupational therapists). Grounded Theory was applied to data analysis. Barriers and facilitators fit the levels of the Ecological Model of Health Behavior: (a) Intrapersonal (perceived rewards); (b) Interpersonal (interaction); (c) Community (availability of programs); (d) Organizational (school systems); (e) Policy (education). Guardians and professionals agreed on the importance of enjoyment, interaction, and programs to promote PA. Differences were found among organizational and policy levels. PA in persons with DS is influenced by interactions between individual and environmental factors.

Physical activity

Down syndrome

Barriers

Facilitators

Kinesiology

Prediction of Energy Expenditure from Accelerometers During Physical Activity in Adults with Down Syndrome: The Effect of Accelerometer Placement

Allred, Anthony T

14 December 2018

There is a need to examine the difference in the relationship between oxygen uptake (VO2) and output from hip- and wrist-worn accelerometers in adults with Down syndrome (DS). The purpose of this study is to identify if that relationship is different between adults with and without DS. Hip- and wrist-worn accelerometer accuracy was also assessed. The sample included 16 adults with DS (10 men; age 31±15 years) and 19 adults without DS (10 men; age 24±6 years). We measured VO2 with a portable spirometer and accelerometer output (Vector Magnitude [VM]) with a hip- and a wrist-worn accelerometer. VM and group were significant predictors of VO2 (p?0.021). BMI became a significant predictor in the second model and DS was no longer significant for both accelerometer models. The Bland-Altman plots indicated nearly zero mean error for both groups. Hip-worn accelerometers showed greater accuracy, and showed less error based on 95% confidence intervals.

Accelerometers

Physical Activity

Energy Expenditure

Down Syndrome

Examining Postnatal Retinal Thickness and Retinal Ganglion Cell Count in the Ts65Dn Mouse Model of Down Syndrome

Folz, Andrew

05 1900

Indiana University-Purdue University Indianapolis (IUPUI) / Down syndrome (DS) is a genetic condition caused by the triplication of human chromosome 21 and presents with many phenotypes including decreased brain size, hypocellularity in the brain, and assorted ocular phenotypes. Some of the ocular phenotypes seen are increased risk of cataracts, accommodation difficulties, increased risk of refractive errors, and increased retinal thickness. The Ts65Dn mouse model of DS is a classically used mouse model as it presents a number of phenotypes also seen in those with DS. Some of these phenotypes include decreased brain volume, abnormal synaptic plasticity, and ocular phenotypes. These ocular phenotypes include decreased visual acuity, cataracts, and increased retinal thickness. The Ts65Dn mouse model is trisomic for Dyrk1a, a gene of interest in DS research. We hypothesize that there will be a genotypic and sex effect of retinal thickness and retinal ganglion cell (RGC) count at postnatal day 15 in the Ts65Dn mouse model of DS. Retinal slices were taken from male and female trisomic and euploid Ts65Dn mice at P15 and fluorescently labeled for RGCs and bipolar cells via immunohistochemistry. The retinas were measured for total retinal thickness and RNA-binding protein (RBPMS) positive cells in the RGC layer were counted. There was no genotypic or sex effect when comparing retinal thickness in trisomic mice as compared to euploid mice. There was a genotypic effect of RBPMS positive cell count in which the trisomic mice had a higher number of RBPMS positive cells than euploid mice. Increased retinal thickness along with increased RGC number have both been implicated with decreased apoptosis in the retina. In the Ts65Dn mouse model along with in individuals with DS, this could be due to an increase in DYRK1A protein levels reducing apoptosis. In future studies, determining DYRK1A’s influence in retinal thickness and RGC number could result in a treatment for overactive DYRK1A that could normalize retinal thickness and RGC number in those with DS.

Down syndrome

Retina

Retina Ganglion Cells

Ts65Dn

Design of a Low Power and Area Efficient Digital Down Converter and SINC Filter in CMOS 90-nm Technology

Billman, Steven John

27 June 2011

No description available.

Electrical Engineering

Digital Down Converter

SINC Filter

Potent Broad-Spectrum Antibacterial Activity of Bismuth-Based NPs Prepared by a Top-Down Method

Pant, Bishnu Datt

22 September 2022

No description available.

Chemistry

DYRK1A Dynamics: The Influence of Gene Copy Number on Neurodevelopment in the Ts65Dn Mouse Model of Down Syndrome

Laura E Hawley (8755629)

03 June 2024

<p dir="ltr">Down syndrome (DS) arises from the triplication of human chromosome 21 (Hsa21), leading to a spectrum of phenotypes characterized by neurodevelopmental and cognitive abnormalities. The Ts65Dn mouse model emulates DS by harboring three copies of genes found on Hsa21 resulting in trisomy 21 (Ts21)- like traits, including disruptions in neuronal pathways, delays in sensorimotor and behavior milestones, and deficits in learning and memory tasks. There is no cure for DS and available therapies primarily address symptoms stemming from Ts21-associated phenotypes. <i>DYRK1A</i>, a gene triplicated in Ts21, has a pivotal role in pathways of neurodevelopment and has been a focus of inhibition treatment research aimed at preempting abnormal brain phenotypes. This study aimed to find a point of substantial <i>Dyrk1a </i>expression dysregulation during a period of critical neonatal neurodevelopment and employ targeted pharmacological and genetic knockdown methods to alleviate the presence or severity of characteristically abnormal brain and behavior phenotypes. The hypothesis of this study was that administering a targeted intervention prior to a point of known overexpression in trisomic pups would ameliorate molecular, sensorimotor, and neurobehavioral deficits, redirecting growth trajectories of Ts65Dn neonatal pups towards more neurotypical outcomes. To test this hypothesis, the spatiotemporal pattern of DYRK1A expression was quantified during the first three weeks of neonatal development across the hippocampus, cerebral cortex, and cerebellum of the Ts65Dn mouse model and found to fluctuate according to the genotype, age, sex, and brain region of the subject. <i>Dyrk1a </i>protein and mRNA expression levels were delineated in trisomic animals by age, exploring the correlation between expression and age, sex, genotype, and brain region. Next a constitutive <i>Dyrk1a </i>knockdown model was integrated with the Ts65Dn model to investigate the impact of gene copy number reduction on protein and mRNA expression levels during phases of known DYRK1A dysregulation. On postnatal day 6, protein expression was rescued in all three brain regions of male animals but was rescued only in the cerebellum of females. There were no significant differences in mRNA transcript levels in either sex at this age. Finally, genetic elements were introduced into the Ts65Dn model to facilitate a spatiotemporally controlled functional reduction of <i>Dyrk1a</i> and discern how the timing of gene copy number reduction affects molecular and neurobehavioral development in a trisomic system. Results from these studies suggest that only functionally reducing <i>Dyrk1a </i>gene copy number on the day of birth is not sufficient to rescue the majority of deficits and delays present in the Ts65Dn mouse model of DS. These findings significantly enhance the understanding of trisomic <i>Dyrk1a </i>expression dynamics during neonatal development and shed light on tailored therapeutic approaches to modulate intrinsic DS characteristics based on age, sex, and phenotypic considerations.</p>

Neurogenetics

Ts65Dn

Down syndrome

DYRK1A

Neurodevelopment

Reálná hodnota v účetnictví / Fair value in accounting

Benáčková, Lenka

January 2010

The thesis is focused on using fair value in accounting in the context of other metods of measurement. There is summarized the application of fair value in Czech Republic and in IAS/IFRS. At the end of this thesis is discussed about presentation of the statements, if the fair value is applicated, next about latent pensions and about gains and losses and push-down effect.

Avaliação do estado nutricional, do consumo alimentar e do nível sérico do zinco de crianças com a síndrome de Down.

Domingues, Natália Tonon

January 2019

Orientador: Cátia Regina Branco da Fonseca / Resumo: A criança com a Síndrome de Down (SD) apresenta maior incidência de diversas complicações clínicas e a deficiência de zinco tem sido considerada problema de saúde pública, levando a maiores prejuízos e repercussões negativas em funções bioquímicas, imunológicas e clínicas. O quadro clínico pode variar dentro de um amplo espectro de manifestações. Não se conhece, ao certo, a magnitude desta deficiência no Brasil. A avaliação criteriosa da alimentação é importante para que possamos avaliar as necessidades nutricionais específicas e realizar uma orientação visando a alimentação mais equilibrada. O objetivo foi avaliar o estado nutricional e o consumo alimentar, e verificar se há deficiência sérica de zinco em crianças com a Síndrome de Down. Estudo aprovado pelo Comitê de Ética em Pesquisa. Análise estatística realizada através do programa SPSS. Método: Estudo clínico transversal, em crianças com SD que realizam o seguimento no ambulatório de Pediatria Genética do Hospital das Clínicas de Botucatu (HCFMB). Foram realizados entrevista semiestruturada, recordatório alimentar de 24 horas (R24), avaliação nutricional (classificação segundo as curvas para SD) e dosagem de zinco sérica. Resultados: 84% dos incluídos receberam diagnóstico de eutrofia. No R24, verificou-se excesso do consumo de calorias e carboidratos, e sem deficiência no consumo de zinco. Quanto ao nível sérico do zinco, em 94,3% houve deficiência (considerado insuficiente valores abaixo de 65 μg/dL) com valor médio d... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Children with Down Syndrome (DS) presents a higher frequency of clinical complications and the Zinc deficiency has been considered a public health problem, that may cause important damage to the biochemical, immunological and clinical functions. The clinical presentation may vary in a broad spectrum of manifestations. The magnitude of this deficiency in Brazil is unknown. The careful evaluation of the diet is essential to access the specific nutritional needs and to guide the best medical conduct and orientations for a more balanced diet. The aim of this study was to evaluate the nutritional status and diet of children with DS, and research serum zinc deficiency. The study was approved by the Research Ethics Committe and statistical analysis was performed with SPSS program. Method: Cross-sectional clinical study with children with DS who performed follow-up at the Genetic Pediatrics outpatient clinics of Hospital das Clínicas de Botucatu (HCFMB). It was performed a semi-structured interview, 24-hour food diary (R24), nutritional assessment (classification according to the charts for DS) and serum zinc blood test. Results: 84% of the patients were diagnosed eutrophic. In the 24-hour food diary evaluation was detected an excess of calories and carbohydrate consumption, and no deficiency in zinc consumption. Regarding the serum zinc level, 94.3% had a deficiency (considered insufficient levels below 65 ug / dL) with a mean value of 50.40 ug / dL, median of 49.24 ug / dL (dp-10.0... (Complete abstract click electronic access below) / Mestre

Nutrição.

Zinco.

Síndrome de Down.

Crianças.

Consumo alimentar e alimentação

Nutrition

Food consumption and food

Zinc

Síndrome de Down.

Children

Perfil proteômico salivar e degradação de histatinas em indivíduos com síndrome de Down e doença periodontal /

Domingues, Natália Bertolo.

January 2019

Orientador: Elisa Maria Aparecida Giro / Resumo: O objetivo deste trabalho foi avaliar o perfil proteômico e a proteólise da histatina 1 e da histatina 5 na saliva total estimulada de indivíduos com síndrome de Down (SD) e não-sindrômicos (NS) na presença e na ausência da doença periodontal (DP). Foram selecionados 24 indivíduos, os quais foram divididos em 4 grupos experimentais (n=6): SD com DP (SDcDP), SD sem DP (SDsDP), não sindrômicos com DP (NScDP) e não sindrômicos sem DP (NSsDP - controle). Inicialmente, os participantes passaram por exame clínico intra-bucal para avaliação da condição periodontal e determinação do índice CPO-D. Foi realizada a coleta da saliva estimulada até a obtenção de 3,0 mL. Parte da saliva foi utilizada para a análise microbiológica e parte foi centrifugada para obtenção do sobrenadante da saliva total (SST), aliquotada e armazenada em freezer -80ºC para as análises proteômica e de degradação. Os níveis salivares de Aggregatibacter actinomycetemcomitans e Porphyromonas gingivalis foram quantificados pela Reação em Cadeia da Polimerase em Tempo Real (qPCR). A análise espectrométrica foi realizada com os pools de saliva de cada um dos quatro grupos, os quais foram submetidos a nLC-ESI-MS/MS (Cromatografia Líquida por ionização electrospray Tandem Espectrometria de Massas). A degradação proteica foi realizada pela adição de histatina 1 e histatina 5 sintéticas ao SST diluído (1:10) e incubação à 37ºC pelos tempos 0, 0,5, 1,5, 4, 6, 8, 24 e 48 horas. Em seguida, foram realizadas as análises d... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: This study aimed to evaluate the proteomic profile and histatins 1 and 5 proteolysis in stimulated whole saliva of individuals with Down syndrome (DS) and non-syndromics (NS) in the presence and absence of periodontal disease (PD). Twenty-four individuals were selected and divided in the following groups (n=6): DS with PD (DSwPD), DS without PD (DSwtPD), NS with PD (NSwPD) and NS without PD (NSwtPD - control). First, periodontal condition and DMFT index were evaluated and 3.0 mL of stimulated whole saliva was collected. Then, part of whole saliva was used to microbiological analysis and the remaining samples were centrifuged in order to obtain the whole saliva supernatant (WSS), aliquoted and stored at -80ºC to proteomic and degradation assays. Levels of Porphyromonas gingivalis (Pg) and Aggregatibacter actinomycetemcomitans (Aa) were quantified by real-time polymerase chain reaction (qPCR). Spectrophotometric analyses were carried out with saliva pools of each group by using nLC-ESI-MS/MS (Liquid chromatography electrospray ionization tandem mass spectrometry). Protein degradation assay was carried out with synthetic histatins 1 or 5 added to WSS (1:10) followed by samples incubation at 37°C for 0, 0.5, 1.5, 4, 6, 8, 24 and 48 hours. Next, polyacrylamide cationic gel electrophoresis (PAGE) analysis and measurement of bands density (%) were performed. Kruskal-Wallis test complemented by Dunn's test was applied to analyze clinical and microbiological data. Total protein and hi... (Complete abstract click electronic access below) / Doutor

Síndrome de Down.

Saliva.

Proteólise

Doenças periodontais.

Down syndrome

Proteolysis

Periodontal diseases