The Diabetes Risk Assessment study: Elucidating the inflammatory profile of the Metabolically Healthy Obese

Perreault, Maude

27 August 2013

This thesis investigates the complexity of the obesity phenotype by characterizing the inflammatory status of Metabolically Healthy Obese (MHO) individuals. More specifically, this work has examined circulating inflammatory markers in MHO individuals and compared it to Lean Healthy (LH) and Metabolically Abnormal Obese (MAO) subjects. Thirty participants (n=10/group) were recruited as part of the Diabetes Risk Assessment (DRA) study, and classified according to adiposity and metabolic status. Despite a similar level of adiposity compared to MAO individuals, MHO subjects presented a more favourable inflammatory profile. Specifically, MHO individuals had levels of hsCRP and IL-6 comparable to LH subjects and lower than MAO subjects. Also, MHO subjects presented similar levels of high molecular weight adiponectin as the MAO group, but PDGF-ββ levels were intermediate to those of the LH and MAO groups. Overall, the distinct inflammatory profile observed in MHO subjects demonstrates the unique status of these individuals, reinforcing that obesity is a complex and heterogeneous phenotype. / Public Health Agency of Canada, Ontario Graduate Scholarships, Queen Elizabeth II Graduate Scholarships in Science and Technology, Canada Foundation for Innovation

Obesity

Diabetes

Clinical study

Body composition

Anthropometric profile

Bioclinical profile

Inflammatory profile

Metabolically healthy obese

Metabolically obese normal weight

Insulin resistance

Dyslipidemia

Metabolic status

Adiposity status

Metabolically abnormal obese

Efficacy and safety of various tooth-whitening products, with special reference to the three dimensional colour space (L*a*b*) measurements and the microhardness tests

Majeed, Abdul

January 2011

Tooth-whitening or tooth-bleaching has become an integral part of modern dental practice. Today, a large number of whitening products are available on the market which are commonly categorized into dentist-supervised home bleaching, in-office bleaching and over-the-counter bleaching products according to their mode of application. This thesis looks into safety and efficacy of various tooth-whitening products and methods.

Tooth whitening

Tooth bleaching

Hydrogen peroxide

Carbamide peroxide

Sodium chlorite

Microhardness

Enamel

Spectrophotometer

Tooth colour

CIE L*a*b*

Clinical study

Dentist-supervised home bleaching

In-office bleaching

Over-the-counter bleaching.

Efeito da suplementação de L-carnitina combinada ao exercício aeróbio sobre a composição corporal, lipidemia, gasto energético e desempenho físico de adultos do sexo masculino e feminino / The effect of combined L-carnitine supplementation to aerobic exercise on body composition, lipid, energy expenditure and adult physical performance of male and female

Christianne de Faria Coelho

30 November 2004

O uso de suplementos alimentares à base de carnitina tem se tornado bastante popular dentre atletas. Nos seus possíveis efeitos biológicos, constam o emagrecimento e o melhor condicionamento aeróbio frente ao exercício físico. Embora o uso difundido também entre não-atletas, há poucas evidências científicas nestes grupos populacionais, particularmente adultos. O objetivo deste estudo foi avaliar os efeitos da suplementação de L-carnitina associada ao exercício físico aeróbio sobre a composição corporal e lipídica sanguínea, gasto energético de repouso e desempenho aeróbio de adultos clinicamente saudáveis. Foram selecionados 21 indivíduos voluntários de 40 a 58 anos de idade, de ambos os sexos (9 homens e 12 mulheres), com índice de Massa Corporal (IMC) entre 25 e 35 kg/m2, participantes de protocolo de exercícios físicos aeróbios supervisionados (80min/sessão, 3-5x/semana, 70 a 80% da freqüência cardíaca máxima para idade) há pelo menos 12 semanas. Após avaliação inicial (M0), foram divididos aleatoriamente em grupos: suplementado (G1; N=11), recebeu 1,8g/dia de L-carnitina e placebo (G2; N=10), recebeu maltodextrina, ambos mantidos nesta intervenção dietética por 30 dias consecutivos. Concluído o período dietético (M1), foram repetidas as avaliações de M0, nas situações de repouso (peso, estatura para cálculo do IMC, circunferência de abdômen, % de gordura, gasto energético de repouso, ingestão alimentar, colesterol e frações e triglicerídios) e esforço físico em esteira ergométrica (VO2máx, limiar anaeróbio, quociente respiratório e variação dos ácidos graxos livres plasmáticos). Houve ligeiro aumento do V02máx e limiar anaeróbio em ambos os grupos e reclassificação do LDL-c no grupo placebo. Os demais valores de ingestão alimentar, composição corporal, lipidemia e gasto energético não sofreram influência significativa do período de exercício ou tratamento dietético. As concentrações de ácidos graxos livres aumentaram durante o esforço físico em esteira, mas sem significância. Conclui-se que o efeito adicional da suplementação de L-carnitina em adultos exercitados regularmente é mínimo nas variações da composição corporal e sanguínea, no gasto energético, uso de substratos energéticos e no condicionamento aeróbio. / The use of nutritional supplements such as carnitine has been widely spread over among athletes. The refered advantages are related to possible weight loss and cardiorespiratory fitness. However, besides widely used in active people (non athletes) there has been little scientific based evidences in this group, specifically in adults. The purpose of the study was to investigate the additional effects of L-carnitine supplemented to exercised subjects on their body composition, blood lipid profile, resting metabolic rate and aerobic performance. Twenty-one volunteers (9 males and 12 females), 40 to 58 years old, body mass index (BMI) values between 25 and 35 kg/m2, were engaged in aerobic exercise program (80 min/session, 3-5 days/week, 70 a 80% of maximum heart rate-HRmáx) at least 12 weeks. After the first test (M0) the subjects were randomly assigned in two groups: L-carnitine (G1; N=11), receiving orally L-carnitine (1,8g/day) or placebo (G2; N=10), receiving maltodextrine during 30 consecutive days. After the dietary intervention (M 1), the assessment tests were repeated in both, resting (body mass, height, BMI calculation, resting energy expenditure, dietary intake, body fat and lipid profile) and exercised condition in a treadmill (VO2max, anaerobic threshold, respiratory exchange ratio and the variation on free fatty acids levels). VO2max and anaerobic threshold were increased in both groups and LDL-c downgraded in the placebo group. No significant changes were found due to either training or dietary supplementation in dietary intake, body composition, lipid profile and energy expenditure. Plasma free fatty acids levels increased, but not significantly, during the 30 min treadmill exercise. Thus, the additional effects of L-carnitine supplementation in moderate active adults were not enough to promote significant changes in body composition, lipid profile, energy expenditure, substrate utilization and aerobic fitness.

Composição corporal

Desempenho físico

Dieta para esportistas

Exercício físico (Efeitos)

L-carnitina

Nutrição humana (Estudo clínico)

Suplementação alimentar (Efeitos)

Body composition

Diet for sports

Human Nutrition (Clinical study)

L-carnitine

Performance

Physical exercise (Effects)

Physical performance

Supplementary feeding (Effects)

Avaliação da resposta imune de anticorpos contra proteínas recombinantes derivadas do Antígeno 1 de Membrana Aplical (AMA-1) de Plasmodium vivax em indivíduos de áreas endêmicas de malária do Brasil / Evaluation of immune response antibodies against recombinant proteins derived from the Apical Membrane Antigen 1 (AMA-1) of Plasmodium vivax in individuals of malaria-endemic areas of Brazil

Bruno Corrêa Múfalo

26 October 2007

O Antígeno 1 de Membrana Apical (AMA-1) de Plasmodium sp tem sido sugerido como candidato a compor uma vacina contra a malária. No presente estudo geramos cinco proteínas recombinantes baseadas em diferentes regiões do ectodomínio de AMA-1 de Plasmodium vivax, o qual compreende os domínios I a III, com intuito de mapear regiões particularmente imunogênicas da proteína. Cada uma das cinco proteínas recombinantes foi expressa em Eschericha coli a partir do vetor pET-28a em fusão com a cauda de histidina e purificadas por cromatografia de afinidade. As diferentes proteínas recombinantes foram comparadas, por ELISA, quanto ao reconhecimento por anticorpos IgM, IgG e subclasses de IgG de 100 indivíduos infectados por P. vivax procedentes de áreas endêmicas do Estado do Pará e 32 indivíduos não infectados que relataram terem sido acometidos de mais de 10 episódios prévios de malária procedentes do município de Terra Nova do Norte (MT). As freqüências de indivíduos que apresentaram anticorpos IgM foram mais baixas e variaram de 4% (DIII) a 36% (DII-III). Por outro lado, as freqüências de indivíduos que apresentaram anticorpos IgG para DI, DII, DIII, DI-II e DII-III foram 13%, 65%, 12%, 59% e 58%, respectivamente. Podemos observar que as proteínas recombinantes contendo o DII foram particularmente imunogênicas durante a infecção natural. Com o objetivo de avaliar se os epítopos reconhecidos nas cinco proteínas baseadas nos diferentes domínios estão expostos na proteína recombinante correspondente ao ectodomínio (DI-III) gerada previamente, realizamos ensaios de inibição por ELISA utilizando placas sensibilizadas com a proteína DI-III. Nossos resultados sugerem a presença de um maior número de epítopos comuns entre as proteínas recombinantes baseadas nos domínios I-II e ectodomínio de AMA-1. Além disso, observamos que a proporção de indivíduos que apresentaram anticorpos contra DII, DI-II e DII-III aumentou de acordo com o maior número de exposições prévias ao P. vivax. As subclasses de IgG que predominaram contra todas as proteínas foram IgG1, IgG3 e IgG4. Em conjunto, nossos resultados sugerem que as proteínas recombinantes contendo o DII podem ser exploradas em futuros estudos de indução de imunidade protetora contra malária vivax em primatas não-humanos. / The Apical Membrane Antigen 1 (AMA-1) of Plasmodium sp has been suggested as a vaccine candidate against malaria. Herein, to identify novel antigenic epitopes on the Plasmodium vivax AMA-1 ectodomain, we have generated five recombinant proteins, comprising domains I to III. All recombinant proteins were expressed in Escherichia coli using the pET-28a vector system fused to hexahistidine tag for purification by affinity chromatography. Recognition of recombinant proteins by antibodies was evaluated using a panel of sera collected from onehundred P. vivax -infected patients resident in the State of Pará and from thirty-two non-infected individuals, living in the State of Mato Grosso and who have faced a minimum of ten malaria episodes. ELISA analyses demonstrated that protein recognition was highly dependent on IgG antibodies, raging from 13%, 65%, 12%, 59% up to 58%, respectively for DI, DII, DIII, DI-II and DII-III domains. Indeed, we have noticed a lower frequency of recognition, ranging from 4% (DIII) to 36% (DII-III), by sera from those individuals that presented IgM antibodies. Collectively, these data suggest that the DII domain is particularly immunogenic during natural infections. Next, to verify whether the epitopes recognized in these five different recombinant proteins were also expressed in a recombinant protein spanning domains I through III (DI-III), we carried out ELISA inhibition assays using plates coated with the DI-III recombinant protein. Our findings revealed the presence of a higher number of common epitopes among recombinant proteins based on domains I-II and the AMA-1 ectodomain. Moreover, we observed that the proportion of individuals who had presented antibodies against DII, DI-II and DII-III domains increased according to the previous number of P. vivax episodes. Overall, IgG1, IgG3 and IgG4 antibodies were prevalent to all proteins. Taken together, our results demonstrated that DII domain is highly recognized, mainly by IgG antibodies; and open promising perspectives to use this region as an experimental vaccine in non-human primates capable to induce protective immunity against vivax malaria.

AMA-1

Antígenos de bactérias

Imunologia (Pesquisa)

Malária (Estudo clínico)-Brasil

Malária Humana

Plasmodium vivax

Proteínas recombinantes (Avaliação)

AMA-1

Antigens of bacteria

Human Malaria

Immunology (Research)

Malaria (Clinical study)-Brazil

Plasmodium vivax

Recombinant Proteins (Review)

Estudo clínico, histológico e molecular na miopatia congênita nemalínica e na miopatia congênita com alterações mínimas / A clinical, histological and molecular study of nemaline congenital myopathy and congenital myopathy with minimal changes

Cristiane de Araujo Martins Moreno

21 November 2016

Introdução: As miopatias congênitas são doenças musculares genéticas caracterizadas por hipotonia e fraqueza muscular de início precoce na infância. Histologicamente são caracterizadas por alterações estruturais no músculo esquelético (corpos nemalínicos, cores ou centralização nuclear), no entanto, existem casos com alterações leves e inespecíficas, alterações mínimas, tais como, desproporção no tamanho das fibras e desarranjo na arquitetura interna das fibras (falhas focais na atividade oxidativa). Quanto ao aspecto molecular, vários genes já foram identificados em associação com os diversos subtipos, porém com grande sobreposição de achados histológicos e clínicos. Objetivo: Caracterização clínica, histológica e molecular de pacientes Brasileiros com miopatia nemalínica e com miopatia congênita com achados histológicos mínimos. Métodos: Avaliação clínica e histológica (revisão dos achados das biopsias musculares) de pacientes com diagnóstico de miopatia congênita nemalínica e com alterações mínimas, provenientes de dois centros de investigação em doenças neuromusculares da cidade de São Paulo (HC-FMUSP e UNIFESP). O estudo molecular foi realizado através de sequenciamento Sanger para os genes ACTA1, TPM3, MYH7 e SEPN1 e/ou sequenciamento de nova geração para painel de genes musculares e/ou exoma. Resultados: Foram avaliados 23 pacientes com miopatia nemalínica (20 famílias) e 22 pacientes com alterações mínimas (20 famílias). O diagnóstico molecular foi concluído em sete famílias com miopatia nemalínica, sendo quatro com variantes missense, em heterozigose, no gene ACTA1 já associadas previamente a miopatia nemalínica, e três famílias, com variantes não conhecidas, em heterozigose, no gene NEB com alta predição de patogenicidade. Na coorte de miopatias congênitas com alterações mínimas o diagnóstico molecular foi concluído em nove famílias, sendo uma com variante conhecida no gene CHRNE, descrita em miastenia congênita; duas famílias com variantes no gene TPM3, sendo uma inédita, em homozigose, e outra, em heterozigose, já conhecida; duas famílias com variantes novas, em heterozigose, no RYR1, uma no gene TTN e três famílias com variantes já conhecidas no gene no MYH7 com fenótipo de miopatia distal de Laing. A despeito da realização de sequenciamento de exoma, sete famílias ainda permanecem sem gene candidato. Conclusões: Os achados clínicos, histológicos e moleculares dos pacientes da coorte de miopatia nemalínica seguem aos padrões descritos da literatura. O estudo dos pacientes com miopatia congênita com alterações mínimas se revelou complexo e variável, tanto no fenótipo quanto no genótipo. As mutações novas no gene NEB, RYR1, TTN, TPM3 e MYH7 confirmam a importância e patogenicidade destes genes nas miopatias congênitas e ampliam o seu espectro de alterações. Diante da quantidade de genes candidatos e do tamanho de alguns genes envolvidos com essas miopatias, técnicas de sequenciamento de nova geração são de grande valor / Introduction: Congenital myopathy are a group of genetic muscle diseases characterized by hypotonia and weakness in early childhood. They are characterized by structural abnormalities in muscle biopsy (nemaline bodies, central-cores or nuclear centralization). However, it can present within mild and unspecific findings like fiber type disproportion and abnormalities on oxidative staining (minimal changes). Regarding the molecular aspects, there are many genes associated with the congenital myopathies with an important overlapping between the histological and phenotypical findings. Objectives: Clinical, histological and molecular characterization of Brazilian patients with nemaline myopathy and congenital myopathy with minimal changes. Methods: Clinical and histological evaluation (review of muscle biopsy) of patients with nemaline myopathy and congenital myopathy with minimal changes from two centers of neuromuscular diseases (HC-FMUSP e UNIFESP). The molecular study was performed using Sanger sequencing for ACTA1, TPM3, SEPN1 and MYH7 genes and/or neuromuscular panel and/or exome. Results: Twenty-three patients with nemaline myopathy (20 families) and 22 patients with congenital myopathy with minimal changes (20 families) were evaluated. The molecular diagnose were concluded in seven families with nemaline myopathy, with four families having missense, heterozygous and pathogenic ACTA1 variants and three families having unknown heterozygous and pathogenic variants in NEB gene. In the congenital myopathy with minimal findings group, the diagnose was concluded in 9 families. One presenting with a pathogenic variant in CHRNE gene previously described in congenital myasthenia, two families with pathogenic variants in TPM3, one novel homozygous and one heterozygous previously reported. Two families presented with novel and pathogenic RYR1 variants, one with novel and pathogenic TTN variants and 3 families presented with heterozygous variants in MYH7 myopathy with Laing distal myopathy phenotype. Despite the NGS realization, 7 families remain without a gene candidate. Conclusions: The clinical, histological and molecular findings of nemaline myopathy cohort follow the literature pattern. In contrast, the study for minimal change patients appear complex and variable, either on phenotype or on genotype. The new gene mutations for NEB, RYR1, TTN, TPM3 and MYH7 reinforce relevance and pathogenicity of these genes in the congenital myopathies and expand the mutation spectrum. In light of diversity of candidate genes and the size of some genes involved with these myopathies, next generation sequencing techniques have been proved essential

Doenças musculares

Estudo clínico

Miopatias congênitas estruturais

Miopatias da nemalina

Músculos/biópsia

Clinical study

Muscles/biopsy

Muscular diseases

Myopathies nemaline

Myopathies structural congenital

Tributirina reduz a expressão de bcl-xLno cólon médio-distal quando administrada a ratos durante a etapa de pós-iniciação de modelo de carcinogênese de cólon / Tributyrin reduces bcl- XL expression on distal colon when offered to rats during post-initiation phase of colon carcinogenesis

Giulianna Paola Cruzetta

24 October 2008

O butirato é um importante ácido graxo de cadeia curta proveniente da fermentação bacteriana de vários tipos de fibras no cólon. Diversos estudos têm demonstrado que o butirato desempenha um papel importante na prevenção do câncer e na manutenção da homeostase colônica, por meio da regulação da proliferação celular, diferenciação e apoptose. A acetilação das histonas tem sido proposta como um dos possíveis mecanismos de ação responsável pelo efeito quimiopreventivo do butirato. O objetivo desse trabalho foi avaliar o papel da tributirina (TB), um pró-fármaco do ácido butírico, na fase de pós-iniciação da carcinogênese de cólon induzida por dimetilhidrazina (DMH), enfatizando a expressão das histonas acetiladas (H3K9 e H4K16) e das proteínas pró e anti-apoptóticas da família Bcl-2 (Bak, Bcl-xL). Durante 5 semanas consecutivas, ratos Wistar receberam diariamente TB (200 mg/100 g peso corpóreo; grupo TB) ou maltodextrina (MD; 300 mg/100 g peso corpóreo; grupo MD; controle isocalórico). Focos de Criptas Aberrantes (FCAs) são lesões pré-neoplásicas e biomarcadores da carcinogênese de cólon. Esses foram analisados nos cólons corados com azul de metileno a 0,02%, porém, nenhuma diferença estatística foi encontrada entre os grupos, TB e MD (p>0,05). A mucosa colônica foi utilizada para analisar a expressão de H3K9 e H4K16 por western blot, contudo, não houve diferença significativa entre os grupos TB e MD. A expressão da proteína pró-apoptotica Bak também foi semelhante nos grupos TB e MD; todavia, a expressão da proteína anti-apoptótica Bcl-XL foi menor no cólon distai dos ratos tratados com TB sugerindo participação dessa na indução de apoptose. Portanto, apesar de trabalhos apontarem para os resultados benéficos do butirato, são necessários mais estudos in vivo para o melhor entendimento dos efeitos mediados pelo butirato na carcinogênese de cólon. / Butyrate is an important short-chain fatty acid, product of intestinal bacterial fermentation of mainly dietary fiber. Several studies have shown that butyrate has an important role in the maintenance of colonic homeostasis as regulator of colonocyte proliferation, differentiation and apoptosis. Thus may play a role in cancer prevention. Histone deacetylation has been proposed to be one of the possible mechanisms of action of butyrate mediated effects on colon carcinogenesis. The aim of this study was to evaluate the role of tributyrin (TB), a butyric acid pro-drug, on post-initiation phase of colon carcinogenesis induced by dimethylhydrazine (DMH), emphasizing the expression of acetylated histones (H3K9, H4K16) and BeI-2 family proteins (Bak, Bcl-XL) mediated apoptosis. During 5 consecutive weeks, Wistar rats received daily TB (200 mg/100 9 body weight; TB group) or maltodextrin (MD; 300 mg/100 9 body weight; MD group; isocaloric control). Aberrant Crypt Focus (ACFs) are considered pre-neoplastic cells and biomarker of colon carcinogenesis. ACFs were counted on colons stained with 0,02% methylene blue, under a light microscope. No statistic differences were found for ACF when compared both groups receiving TB or MD (p>0,05). Colonic mucosa scraping was used for analysis of H3K9 and H4K16 by Western Blot. No significant differences were demonstrated between TB and MD groups. Bak expression were similar between TB and MD groups, but Bcl-XL expression seems to be reduced only on distal colon of the TB group, suggesting that TB may induce apoptosis Although most studies point towards beneficial results of butyrate, more in vivo studies are needed to contribute to our current understanding of butyrate-mediated effects on colon carcinogenesis.

Apoptose

Carcinogênese

Histona

Neoplasias colorretais (Estudo clínico)

Nutrição experimental

Proliferação celular

Quimioprevenção

Tributirina

Activity)

Apoptosis

Carcinogenesis

Cell Proliferation

Chemoprevention

Chemotherapy (Prevention and control

Colorectal Neoplasms (Clinical study)

Experimental Nutrition

Histone

Tributyrin

Efeitos da suplementação com zinco na redução do estresse oxidativo em indivíduos com diabetes mellitus do tipo 2 / Effects of zinc supplementation on the reduction of oxidative stress in subjects with type 2 diabetes mellitus

Vanuska Lima da Silva

09 May 2006

O zinco é um elemento-traço essencial que está envolvido em diferentes processos metabólicos. Possui função antioxidante, uma vez que faz parte da estrutura da enzima superóxido dismutase (CuZn-SOD), atua na restrição da produção endógena de radicais livres e, na estabilização da estrutura de membranas. Diabéticos geralmente apresentam deficiência de zinco, além de possuírem um grau aumentado de estresse oxidativo, que é gerado pela própria doença. Portanto o presente estudo teve como objetivo verificar se a suplementação com zinco em pacientes com diabetes mellitus do tipo 2 poderia melhorar as características indicativas de dano oxidativo. O estudo realizado foi duplo cego, sendo administrado zinco aminoquelado (20mg/dia) e placebo, durante 6 meses, sendo os parâmetros do estudo avaliados antes e depois da suplementação, para que fosse possível se observar as mudanças nos parâmetros indicativos do estresse oxidativo. Na avaliação antropométrica, se verificou peso, estatura, medidas da cintura e bioimpedância elétrica. Foi feita a avaliação dos parâmetros glicêmicos e lipídicos, do mineral zinco, bem como dos indicadores de estresse oxidativo, incluindo os óxidos de colesterol e os autoanticorpos anti-LDL eletronegativa. A avaliação alimentar foi realizada por meio do registro de consumo alimentar. Como resultados, podemos ressaltar alta prevalência de sobrepeso/obesidade. Após a suplementação, as concentrações do zinco no plasma e eritrócito tiveram um leve aumento, passando de 68±10 para 72,9±13µg/dL, e de 40,7±6,2 para 43±6,8µgZn/gHb, respectivamente, entretanto, este aumento não foi estatisticamente significativo. Também não foram encontradas diferenças significativas nas concentrações dos autoanticorpos anti-LDL eletronegativa e do total dos óxidos de colesterol, apesar de existir tendência de melhora destes parâmetros. / Zinc is an essential trace element that is involved with a variety of metabolic processes. It has an antioxidant function as it is part of the superoxidedismutase (CuZn-SOD) enzyme. It works in the restriction of the free-radicals endogenous production and in the membrane structure stabilization. Diabetic people often present zinc deficiency, besides of having an augmented degree of oxidative stress, which is generated by the own disease. Therefore, the present study had as objective to verify if the zinc supplementation would better the indicating characteristics of oxidative damage to type 2 diabetes mellitus patients. The study done was double-blind, with the administration of zinc chelate (20mg/day) and placebo, during 6 months. The study parameters were assessed both before and after the supplementation, in order to be possible for one to observe changes in the indicating oxidative stress parameters. In the antropometric evaluation, it was verified the weight, height, the measure of the waistline and the electric bioimpedance. It was evaluated the glicemic and fat parameters, zinc, as well as the oxidative stress indicators, which included the oxysterols and the electronegative anti-LDL autoantibody. The alimentary evaluation was done by means of the feed consumption registration. As a result, it could be highlighted the predomination of overweigh/obesity. After supplementation, the zinc concentrations in the plasma and erythrocyte showed a slight increase, from 68±10 to 72,9±13mg/dL, and from 40,7±6,2 to 43±6,8mgZn/gHb, respectively. However, this increase was not statically significative. Besides that, it was not found significative differences in the concentration of the electronegative anti-LDL autoantibody and of the oxysterols totals, despite of a trend in improvement of those parameters.

Avaliação nutricional

Diabetes mellitus (Estudo clínico)

Diabetes mellitus tipo 2

Estresse oxidativo

Nutrição experimental

Zinco (Aplicações terapêuticas)

Diabetes mellitus (Clinical study)

Dietary supplements

Experimental nutrition

Nutrition assessment

Oxidative stress

Type 2 Diabetes mellitus

Zinc (Therapeutic applications)

Estudo de variantes da leptina do receptor de leptina: impacto sobre as características relacionadas com a obesidade / Study of the leptin and the leptin receptor gene variants: impact on characteristics related with obesity

Raquel de Oliveira

17 June 2008

Neste estudo, foi avaliada a relação entre polimorfismos dos genes da leptina (LEP) e receptores da leptina (LEPR) e parâmetros antropométricos, leptinemia glicemia e lipídeos séricos, em indivíduos da população brasileira. Foram incluídos 238 indivíduos com idade entre 30 e 80 anos. Foram medidos o índice de massa corporal (IMC), a cintura abdominal (CA) e a razão cintura quadril (RCQ). Amostras de sangue periférico foram obtidas para análise do perfil bioquímico e extração de DNA. Os polimorfismos de nuleotideo único (SNPs) LEP G-2548A e LEPR Lys109Arg, Gln223Arg e Lys656Asn foram detectados por PCR-RFLP. Os SNPs LEPR Lys109Arg e Gln223Arg foram associados com obesidade e com IMC e CA aumentados (p<0.05). Estes polimorfismos também foram associados com leptina e glicose elevada (p<0,05). O perfil lipídico sérico foi influenciado pelo polimorfismo LEPR Lys109Arg (p<0.05). A relação entre os SNPs LEPR Lys109Arg e Gln223Arg e o perfil lipídico foi modificada pelo gênero. Os haplótipos LEP G-2548/ LEPR Lys109Arg foram relacionados com diferenças no IMC de obesos. Os haplotipos LEPR Lys109Arg/Gln223Arg foram associados com diferenças na CA e glicemia e lipídeos séricos. Em conclusão, os polimorfismos LEPR Lys109Arg e Gln223Arg estão associados com obesidade e alterações de leptina, glicose e lipídeos circulantes de forma dependente do gênero. / We have assessed the relationship between polymorphisms of the leptin (LEP) and the leptin receptor (LEPR) genes and anthropometric parameters, plasma leptin and glucose and serum lipids in individuals of the Brazilian population. We included 238 individuais with 30 to 80 years. Body mass index (BMI), abdominal circumference (AC) and waist-to-hip ratio (WHR) were measured. Peripheral blood samples were collected for analysis of the biochemical profile and DNA extraction. The single nucleotide polymorphisms (SNP) LEP G-2548A and LEPR Lys109Arg, Gln223Arg and Lys656Asn were detected by PCR-RFLP. The SNPs LEPR Lys109Arg and Gln223Arg were associated with obesity and with increased BMI and AC (p <0.05). These polymorphisms were also associated with increase leptin and glucose (p<0,05). The serum lipid profile was influenced by the LEPR Lys 1 09Arg (p<0.05). The relationship between the SNPs LEPR Lys 1 09Arg and Gln223Arg and the lipid profile was modified by gender. The haplotypes LEP G-2548A1 LEPR Lys109Arg were related with differences on BMI in obese group. The haplotypes LEPR Lys109Arg/Gln223Arg were associated with differences on AC, glucose and serum lipids. In conclusion, the LEPR Lys109Arg and Gln223Arg polymorphisms are associated with obesity and alterations in blood leptin, glucose and lipids in a gender-dependent manner.

Antropometria (Medidas; Determinação)

Dislipidemia

DNA (Análise)

Genética

Hiperglicemia

Índice de massa corporal

Polimorfismos genéticos

Receptor de leptina

Body mass index

DNA (Analysis)

Dyslipidemia

Genetic polymorphisms

Genetics

Hyperglycemia

Leptin receptor

Perceived stress and high fat intake: A study in a sample of undergraduate students

Vidal, E. Jair, Alvarez, Daily, Martinez-Velarde, Dalia, Vidal-Damas, Lorena, Yuncar-Rojas, Kelly A., Julca-Malca, Alesia, Bernabe-Ortiz, Antonio

09 March 2018

Objectives Different studies have reported the association between perceived stress and unhealthy diet choices. We aimed to determine whether there is a relationship between perceived stress and fat intake among undergraduate medical students. Methods/Principal findings A cross-sectional study was performed including first-year medical students. The outcome of interest was the self-report of fat intake assessed using the Block Screening Questionnaire for Fat Intake (high vs. low intake), whereas the exposure was perceived stress (low/ normal vs. high levels). The prevalence of high fat intake was estimated and the association of interest was determined using prevalence ratios (PR) and 95% confidence intervals (95% CI). Models were created utilizing Poisson regression with robust standard errors. Data from 523 students were analyzed, 52.0% female, mean age 19.0 (SD 1.7) years. The prevalence of high fat intake was 42.4% (CI: 38.2%–46.7%). In multivariate model and compared with those with lowest levels of stress, those in the middle (PR = 1.59; 95%CI: 1.20–2.12) and highest (PR = 1.92; 95%CI: 1.46–2.53) categories of perceived stress had greater prevalence of fat intake. Gender was an effect modifier of this association (p = 0.008). Conclusions Greater levels of perceived stress were associated with higher fat intake, and this association was stronger among males. More than 40% of students reported having high fat consumption. Our results suggest the need to implement strategies that promote decreased fat intake.

Adult

Cross-sectional study

Error

Fat intake

Female

Gender

Human

Major clinical study

Male

Medical student

Outcome assessment

Perceived Stress Scale

Prevalence

Questionnaires

Self report

Stress

undergraduate student

young adult

The impact of material surface characteristics on the clinical wetting properties of silicone hydrogel contact lenses

Read, Michael Leonard

January 2011

This PhD project investigated the ramifications of air-cured and nitrogen-cured manufacturing processes during silicone hydrogel contact lens manufacture in terms of lens surface characterisation and clinical performance. A one-hour contralateral clinical study was conducted for ten subjects to compare the clinical performance of the two study lenses. The main clinical findings were reduced levels of subjective performance, reduced surface wettability and increased deposition. Contact angle analysis showed the air-cured lenses had consistently higher advancing and receding contact angle measurements, in comparison with the nitrogen-cured lens. Chemical analysis of the study lens surfaces in the dehydrated state, by x-ray photoelectron spectroscopy (XPS) and time-of-flight mass spectrometry (ToF-SIMS), showed no difference due to surface segregation of the silicone components. Analysis of frozen lenses limited surface segregation and showed a higher concentration of silicone polymer components and lower concentration of hydrophilic polymer components at the surface of the air-cured lens, in comparison with the nitrogen-cured lens. Scanning electron microscope (SEM) imaging showed the nitrogen-cured lens to have a surface typical of a hydrogel material, whereas the air-cured lens had regions of apparent phase separation. In addition, atomic force microscopy (AFM) showed the air-cured lens to have a rougher surface associated with greater adherence of contaminants (often observed in materials with reduced polymer cross-linking). In conclusion, clinical assessment of the study lenses confirmed the inferior performance of the air-cured lens. Surface analysis suggested that the non-wetting regions on the air-cured lenses were associated with elevated level of silicone components, reduced polymer cross-linking and polymer phase separation.

617.7