Efeito pró-oxidante do hidroperóxido de urato sobre proteínas sensíveis às alterações redox: implicações na resposta inflamatória / Pro-oxidant effect of urate hydroperoxide on redoxsensitive proteins: implications on inflammatory reponse

Carvalho, Larissa Anastácio da Costa

19 May 2017

O hidroperóxido de urato (HOOU) é o produto da oxidação do ácido úrico por peroxidases. Sua produção é favorecida durante a inflamação e hiperuricemia, uma vez que há grande quantidade de ácido úrico, peroxidases inflamatórias e superóxido. Neste sentido, o objetivo deste estudo foi avaliar o efeito do hidroperóxido de urato sobre proteínas sensíveis à modulação redox em um ambiente inflamatório asséptico e outro que imita infecção. Assim, nesta tese comparou-se a estrutura química do HOOU obtido fotoquimicamente daquele obtido através da catálise enzimática pela mieloperoxidase. A obtenção do HOOU por foto-oxidação permitiu o melhor isolamento do composto. Este oxidante foi capaz de reagir especificamente com os aminoácidos contendo enxofre (metionina e cisteína). Neste sentido, foi investigada sua reatividade com tiol-peroxidases detoxificadoras de peróxido, a peroxiredoxina 1 e 2 (Prx1 e Prx2). O HOOU apresentou cinética rápida de reação com a Prx1, k = 4,9 × 105 M-1s-1 e Prx2, k = 2,3 × 106 M-1s-1, o que as torna um provável alvo celular, além disso, foi capaz de oxidar a Prx2 de eritrócitos humanos, mostrando ser capaz de atravessar a membrana plasmática. Além das Prxs, a albumina do soro também desempenha papel importante na homeostase redox. O HOOU foi capaz de oxidar a albumina com constante de velocidade de 0,2 × 102 M-1s- 1. Outra tiol-proteína com importante função na homeostase e sinalização redox é a tioredoxina (Trx). A Trx foi oxidada pelo HOOU com constante de reação de 2,8 × 102 M-1s-1 e foi liberada juntamente com a Prx1 e Prx2 das células de macrófagos humanos (linhagem THP-1) quando estas células foram incubadas com HOOU. A liberação dessas proteínas é reconhecidamente um sinal de estresse celular. Assim o HOOU pode estar envolvido na exacerbação do estresse oxidativo em ambiente inflamatório. Quando neutrófilos (linhagem HL- 60) e macrófagos humanos (linhagem THP-1) foram incubados na presença de ácido úrico e Pseudomonas aeruginosa houve uma diminuição na produção de ácido hipocloroso (HOCl). Isto se deveu à competição entre ácido úrico e cloreto pela mieloperoxidase e resultou em menor atividade microbicida pelas células, demonstrando que a formação do HOOU não contribui e, ao contrário, prejudica a atividade microbicida das células inflamatórias. Dessa forma, a oxidação do ácido úrico e formação do hidroperóxido de urato tanto altera a atividade microbicida das células inflamtárias, quanto leva à oxidação de tiósproteínas importantes para manutenção da homeostase redox. Assim, o HOOU pode ser o responsável pelos efeitos pró-oxidantes e pró-inflamatórios do ácido úrico solúvel, e isso indica que o papel antioxidante do ácido úrico deve ser revisto em situações de inflamação. / Urate hydroperoxide (HOOU) is the product of the oxidation of uric acid by peroxidases. The formation of HOOU is favored during inflammation and in hyperuricemia, where there is plenty amount of uric acid, inflammatory peroxidases and superoxide. Therefore, the aim of the present study was to evaluate the effect of urate hydroperoxide on redox sensitive proteins in an inflammatory environment and another that mimics infection. In this thesis the chemical structure of the HOOU produced by photo-oxidation was compared to that obtained by myeloperoxidase catalysis. The chemical production of HOOU allowed a better purification of the compound. This oxidant was able to specifically react with sulfur containing amino acids (methionine and cysteine). In this sense, its reactivity with peroxiredoxins (Prx1 and Prx2) was investigated. HOOU reacted fast with Prx1 k = 4.9 × 105 M-1s-1 and Prx2 k = 2.3 × 106 M-1s-1. In addition, HOOU was able to oxidize Prx2 from intact erythrocytes at the same extend as does hydrogen peroxide. Albumin is an important thiol-containing protein to redox homeostasis in plasma. HOOU was able to oxidize albumin with a rate constant of 0.2 × 102 M-1s-1. Another protein with important function in redox homeostasis is thioredoxin (Trx). Trx was oxidized by HOOU with a rate constant of 2.8 × 102 M-1s-1 and was released together with Prx1 and Prx2 from human macrophages cells (THP-1 cell line) that were incubated with HOOU. The release of these proteins is a signal of cellular stress. Thus, HOOU may be involved in the exacerbation of oxidative stress in inflammatory environments. When neutrophil (HL-60 cell line) and macrophages (THP-1 cell line) were incubated with uric acid and Pseudomonas aeruginosa there was a decrease in hypochlorous acid (HOCl) production because of the competition between chloride and uric acid by myeloperoxidase. It decreased HOCl and impaired the microbicidal activity of the cells, showing that HOOU does not contribute in bacteria clearance. Therefore, the oxidation of uric acid to urate hydroperoxide impairs microbicidal activity and oxidizes thiol-proteins in inflammatory cells contributing to a pro-oxidant status. In this context, the antioxidant role of uric acid in inflammatory response should be reviwed.

Acido úrico

Albumin

Albumina

Hidroperóxido de urato

Inflamação

Inflammation

Modulação redox

Oxidação

Oxidation

Peroxiredoxinas

Redox modulation

Thiol proteins peroxiredoxins

Thioredoxin

Tioredoxina

Urate hydroperoxide

Uric acid

Efeito pró-oxidante do hidroperóxido de urato sobre proteínas sensíveis às alterações redox: implicações na resposta inflamatória / Pro-oxidant effect of urate hydroperoxide on redoxsensitive proteins: implications on inflammatory reponse

Larissa Anastácio da Costa Carvalho

19 May 2017

O hidroperóxido de urato (HOOU) é o produto da oxidação do ácido úrico por peroxidases. Sua produção é favorecida durante a inflamação e hiperuricemia, uma vez que há grande quantidade de ácido úrico, peroxidases inflamatórias e superóxido. Neste sentido, o objetivo deste estudo foi avaliar o efeito do hidroperóxido de urato sobre proteínas sensíveis à modulação redox em um ambiente inflamatório asséptico e outro que imita infecção. Assim, nesta tese comparou-se a estrutura química do HOOU obtido fotoquimicamente daquele obtido através da catálise enzimática pela mieloperoxidase. A obtenção do HOOU por foto-oxidação permitiu o melhor isolamento do composto. Este oxidante foi capaz de reagir especificamente com os aminoácidos contendo enxofre (metionina e cisteína). Neste sentido, foi investigada sua reatividade com tiol-peroxidases detoxificadoras de peróxido, a peroxiredoxina 1 e 2 (Prx1 e Prx2). O HOOU apresentou cinética rápida de reação com a Prx1, k = 4,9 × 105 M-1s-1 e Prx2, k = 2,3 × 106 M-1s-1, o que as torna um provável alvo celular, além disso, foi capaz de oxidar a Prx2 de eritrócitos humanos, mostrando ser capaz de atravessar a membrana plasmática. Além das Prxs, a albumina do soro também desempenha papel importante na homeostase redox. O HOOU foi capaz de oxidar a albumina com constante de velocidade de 0,2 × 102 M-1s- 1. Outra tiol-proteína com importante função na homeostase e sinalização redox é a tioredoxina (Trx). A Trx foi oxidada pelo HOOU com constante de reação de 2,8 × 102 M-1s-1 e foi liberada juntamente com a Prx1 e Prx2 das células de macrófagos humanos (linhagem THP-1) quando estas células foram incubadas com HOOU. A liberação dessas proteínas é reconhecidamente um sinal de estresse celular. Assim o HOOU pode estar envolvido na exacerbação do estresse oxidativo em ambiente inflamatório. Quando neutrófilos (linhagem HL- 60) e macrófagos humanos (linhagem THP-1) foram incubados na presença de ácido úrico e Pseudomonas aeruginosa houve uma diminuição na produção de ácido hipocloroso (HOCl). Isto se deveu à competição entre ácido úrico e cloreto pela mieloperoxidase e resultou em menor atividade microbicida pelas células, demonstrando que a formação do HOOU não contribui e, ao contrário, prejudica a atividade microbicida das células inflamatórias. Dessa forma, a oxidação do ácido úrico e formação do hidroperóxido de urato tanto altera a atividade microbicida das células inflamtárias, quanto leva à oxidação de tiósproteínas importantes para manutenção da homeostase redox. Assim, o HOOU pode ser o responsável pelos efeitos pró-oxidantes e pró-inflamatórios do ácido úrico solúvel, e isso indica que o papel antioxidante do ácido úrico deve ser revisto em situações de inflamação. / Urate hydroperoxide (HOOU) is the product of the oxidation of uric acid by peroxidases. The formation of HOOU is favored during inflammation and in hyperuricemia, where there is plenty amount of uric acid, inflammatory peroxidases and superoxide. Therefore, the aim of the present study was to evaluate the effect of urate hydroperoxide on redox sensitive proteins in an inflammatory environment and another that mimics infection. In this thesis the chemical structure of the HOOU produced by photo-oxidation was compared to that obtained by myeloperoxidase catalysis. The chemical production of HOOU allowed a better purification of the compound. This oxidant was able to specifically react with sulfur containing amino acids (methionine and cysteine). In this sense, its reactivity with peroxiredoxins (Prx1 and Prx2) was investigated. HOOU reacted fast with Prx1 k = 4.9 × 105 M-1s-1 and Prx2 k = 2.3 × 106 M-1s-1. In addition, HOOU was able to oxidize Prx2 from intact erythrocytes at the same extend as does hydrogen peroxide. Albumin is an important thiol-containing protein to redox homeostasis in plasma. HOOU was able to oxidize albumin with a rate constant of 0.2 × 102 M-1s-1. Another protein with important function in redox homeostasis is thioredoxin (Trx). Trx was oxidized by HOOU with a rate constant of 2.8 × 102 M-1s-1 and was released together with Prx1 and Prx2 from human macrophages cells (THP-1 cell line) that were incubated with HOOU. The release of these proteins is a signal of cellular stress. Thus, HOOU may be involved in the exacerbation of oxidative stress in inflammatory environments. When neutrophil (HL-60 cell line) and macrophages (THP-1 cell line) were incubated with uric acid and Pseudomonas aeruginosa there was a decrease in hypochlorous acid (HOCl) production because of the competition between chloride and uric acid by myeloperoxidase. It decreased HOCl and impaired the microbicidal activity of the cells, showing that HOOU does not contribute in bacteria clearance. Therefore, the oxidation of uric acid to urate hydroperoxide impairs microbicidal activity and oxidizes thiol-proteins in inflammatory cells contributing to a pro-oxidant status. In this context, the antioxidant role of uric acid in inflammatory response should be reviwed.

Acido úrico

Albumina

Hidroperóxido de urato

Inflamação

Modulação redox

Oxidação

Peroxiredoxinas

Tioredoxina

Albumin

Inflammation

Oxidation

Redox modulation

Thiol proteins peroxiredoxins

Thioredoxin

Urate hydroperoxide

Uric acid

A memória hiperglicêmica no rim diabético: marcas metabólicas, moleculares e epigenéticas / The hyperglycemic memory in diabetic kidney: metabolic, molecular, and epigenetic marks

Antonio Anáx Falcão de Oliveira

10 February 2017

A nefropatia diabética (ND) é uma das complicações microvasculares do diabetes e consiste no dano ao parênquima renal por consequência de uma série de fatores hemodinâmicos e moleculares. A ocorrência de ND e de outras complicações mesmo em indivíduos sob adequado controle glicêmico tem sido associada a um fenômeno conhecido como memória metabólica. Neste trabalho foram investigadas vias bioquímicas e moleculares persistentemente alteradas no rim de animais diabéticos tratados após um período inicial de hiperglicemia, com o propósito de entender os mecanismos envolvidos na memória metabólica. Para tanto, ratos com diabetes induzida por estreptozotocina foram mantidos hiperglicêmicos durante 4 semanas (período curto) ou 12 semanas (período longo) e posteriormente tratados com insulina isoladamente ou combinada com metformina (100mg/kg/dia) durante as 4 (período curto) ou 12 (período longo) semanas seguintes. Todos os animais tratados tiveram os seus níveis glicêmicos e função renal normalizados. Os tratamentos também foram capazes de normalizar os níveis elevados de malonaldeído no rim, bem como a excreção aumentada dos adutos de DNA 8-oxo-2\'-desoxiguanosina (8-oxodG) e N2-carboxietil-2\'- desoxiguanosina (CEdG) na urina observados nos animais diabéticos. Níveis aumentados de 8-oxodG foram detectados em DNA mitocondrial (mtDNA), mas não em DNA nuclear, de animais diabéticos apenas no período curto de estudo e também foram normalizados após o controle glicêmico. Nós identificamos uma via gradualmente alterada durante o curso do diabetes que permanece persistentemente alterada após o controle glicêmico tardio. Essa via compreende um declínio precoce do clearance de ácido úrico e expressão da pAMPK, seguida pelo acúmulo de fumarato, expressão aumentada de TGF-β, expressão reduzida de PGC-1α e redução da metilação e hidroximetilação do mtDNA. A redução persistente do clearance de ácido úrico em animais diabéticos tratados pode sustentar as alterações bioquímicas renais prolongadas observadas após o controle glicêmico, e essa regulação é provavelmente mediada pela redução sustentada da expressão de pAMPK e pela indução de inflamação. Este trabalho propõe a primeira consideração do possível papel da hiperuricemia e das alterações bioquímicas subjacentes como parte da memória metabólica na nefropatia diabética. / Diabetic nephropathy is one of the diabetes microvascular complications, and it consists on the damage to the renal parenchyma due to several hemodynamic and molecular factors. The occurrence of diabetic nephropathy and other complications even in those individuals under tight glycemic control has been associated to a phenomenon known as metabolic memory. Here we investigated biochemical and molecular pathways persistently altered in the kidney of diabetic animals treated after a previous period of hyperglycemia, aiming to understand underlying mechanisms in metabolic memory. Streptozotocin-induced diabetic rats were maintained hyperglycemic during 4 (short period) or 12 weeks (long period), and then they were treated with insulin alone or combined with metformin (100 mg/kg/day) for the following 4 or 12 weeks, respectively. All the treated animals had them glycemic levels and renal function normalized. The treatments were also able to control enhanced kidney malondialdehyde levels, as well as the increased urine excretion of the DNA adducts 8-oxo-2\'- deoxyguanosine (8-oxodG) and N2-carboxyethyl-2\'-deoxyguanosine seen in diabetic animals. Increased levels of 8-oxodG were detected in mitochondrial DNA, but not in nuclear DNA of diabetic animals in the short period, and were also recovered after glycemic control. We have identified a kidney pathway that is gradually altered during the course of diabetes and remains persistently changed after late glycemic control. This pathway comprises an early decline of uric acid clearance and pAMPK expression followed by fumarate accumulation, increased TGF-β expression, reduced PGC-1α expression, and downregulation of methylation and hydroxymethylation of mitochondrial DNA. The sustained decrease of uric acid clearance in treated diabetes may support the prolonged kidney biochemical alterations observed after tight glycemic control, and this regulation is likely mediated by the sustained decrease of AMPK activity and the induction of inflammation. This work proposes the first consideration of the possible role of hyperuricemia and the underlying biochemical changes as part of metabolic memory in diabetic nephropathy.

Ácido úrico

Fumarato

Memória metabólica

Nefropatia diabética

pAMPK

TGF-β

Diabetic nephropathy

Fumarate

Metabolic memory

pAMPK

TGF-β

Uric acid

Functional characterization of urate handling by hSLC2A9 (hGLUT9) splice variants in a heterologous expression system

Witkowska, Katarzyna

Unknown Date

No description available.

GLUT9

SLC2A9

uric acid

urate

splice variants

Xenopus oocytes

heterologous expression

solute transport

simple carrier model

facilitative glucose transporters

GLUTs

gout

hyperuricemia

Cardiovascular dysfunction in black South Africans: an investigation from various perspectives / I.M. Palmer

Palmer, Iolanthe Marike

January 2010

Motivation: The prevalence of cardiovascular dysfunction, especially hypertension, in Africans has increased dramatically over the past few decades. Despite considerable in~ depth studies, cardiovascular diseases remain the leading cause of morbidity and mortality. Further escalations are predicted, especially in developing countries such as South Africa, if measures are not taken to combat the trend. Numerous cardiovascular risk factors have been investigated within African-Americans as well as Caucasians. However, it is not known to what extent African-Americans and Africans from South Africa are comparable. Therefore, it is essential to investigate risk factors and their possible contributory role in the high susceptibility of cardiovascular dysfunction in the black South African population. Aim: To investigale potential risk factors and their possible involvement and association with the high prevalence of cardiovascular dysfunction within the black South African population. Methodology: Manuscripts presented in Chapters 2, 3 and 4 made use of the data obtained from the cross-sectional SAfrEIC (The South African study regarding the influence of Sex, age and ethnicity on insulin sensitivity and Cardiovascular function) study. The study group included 756 asymptomatic, apparently healthy African men and women as well as Caucasian men and women, recruited from the North West Province, South Africa. Anthropometric and cardiovascular measurements were taken as well as their lipid profiles, fasting insulin levels, and uric acid and adiponectin levels. Independent t-tests, analyses of variance (ANOVA) and analyses of covariance (ANCOVA) were used for comparison of variables between groups to determine significant differences. Partial correlations coefficients were used to show association between variables while adjusting for confounders. Multiple analyses of covariance (MANCOVA) were performed to compare variables between the groups, whilst adjusting for relevant confounders. Stepwise multiple and single regression analyses were also used to determine and confirm the most significant associations between variables. All subjects gave informed consent in writing and the Ethics Committee of the NorthWest University approved the study, The reader is referred to the "Materials and Methods" section of Chapters 2, 3 and 4 for a more elaborate description of the subjects, study design and analytical methods used in each paper. Results and conclusions of the individual manuscripts *Results from Chapter 2 revealed significantly lower uric acid levels for African men compared to Caucasian men, Despite these lower levels. the association between uric acid and blood pressure is more pronounced within the African men. The strong positive relationship between uric acid and blood pressure might be explained by uric acid's independent relationship with vascular resistance, Uric acid also revealed a positive association with triglycerides in both the African and Caucasian men. These results suggest that uric acid per se can act as a risk factor in the development of cardiovascular dysfunction in African men, *Results from Chapter 3 showed opposing changes in insulin secretion for African men and Caucasian men with increasing age. Whereas insulin levels increased in Caucasian men with progressive age, insulin levels in African men tended to decrease with ageing. Additionally, the insulin-blood pressure relationship within African men revealed opposite results as to what was expected. While the Caucasian men revealed a more positive association between insulin and blood pressure within the younger individuals, older individuals revealed a negative association between insulin and blood pressure, This implies that the vasoconstrictory actions of insulin seem to dominate in young individuals while the vasodilatory actions of insulin take over in older individuals, The turnaround probably acts as a counter protective mechanism against age-related cardiovascular dysfunction. On the contrary, despite decreased insulin secretion in older African men, they exhibit a more positive association between insulin and blood pressure, whereas younger subjects showed a more negative association, These results might suggest dissociation between insulin and blood pressure, Insulin per se might, therefore, not act as a risk factor, but rather the lack of insulin-mediated vasodilatory effects as observed within younger Africans. *Results from Chapter 4 contradicted the notion found in the literature that age-related increase in adiponectin levels are due to impaired renal function. Although the results from this chapter confirmed a Significant association between renal function (estimated creatinine clearance) and adiponectin levels a multiple regression model revealed insulin resistance (HOMA-IR) as the major contributor to adiponectin levels. Adiponectin levels increased with progressive ageing only in the Africans. No such change was observed for the Caucasians. This might be due to development of functional adiponectin resistance or perhaps due to a decline in pancreatic cell mass with ageing. In conclusion, the cardiovascular profile of Africans seems to be more detrimentally affected compared to Caucasians. Results from this study have elucidated on the associations and potential involvement of possible risk factors including, uric acid, insulin, C-peptide, as well as adiponectin, with regards to the high prevalence of cardiovascular dysfunction within the black South African population. / Thesis (Ph.D. (Physiology))--North-West University, Potchefstroom Campus, 2010.

Africans

Cardiovascular dysfunction

Ageing

Hypertension

Uric acid

Insulin

C-peptide

Adiponectin

Swart Afrikane

Kardiovaskulêre disfunksie

Veroudering

Hipertensie

Uriensuur

Insulien

C-peptied

Adiponektien

Cardiovascular dysfunction in black South Africans: an investigation from various perspectives / I.M. Palmer

Palmer, Iolanthe Marike

January 2010

Motivation: The prevalence of cardiovascular dysfunction, especially hypertension, in Africans has increased dramatically over the past few decades. Despite considerable in~ depth studies, cardiovascular diseases remain the leading cause of morbidity and mortality. Further escalations are predicted, especially in developing countries such as South Africa, if measures are not taken to combat the trend. Numerous cardiovascular risk factors have been investigated within African-Americans as well as Caucasians. However, it is not known to what extent African-Americans and Africans from South Africa are comparable. Therefore, it is essential to investigate risk factors and their possible contributory role in the high susceptibility of cardiovascular dysfunction in the black South African population. Aim: To investigale potential risk factors and their possible involvement and association with the high prevalence of cardiovascular dysfunction within the black South African population. Methodology: Manuscripts presented in Chapters 2, 3 and 4 made use of the data obtained from the cross-sectional SAfrEIC (The South African study regarding the influence of Sex, age and ethnicity on insulin sensitivity and Cardiovascular function) study. The study group included 756 asymptomatic, apparently healthy African men and women as well as Caucasian men and women, recruited from the North West Province, South Africa. Anthropometric and cardiovascular measurements were taken as well as their lipid profiles, fasting insulin levels, and uric acid and adiponectin levels. Independent t-tests, analyses of variance (ANOVA) and analyses of covariance (ANCOVA) were used for comparison of variables between groups to determine significant differences. Partial correlations coefficients were used to show association between variables while adjusting for confounders. Multiple analyses of covariance (MANCOVA) were performed to compare variables between the groups, whilst adjusting for relevant confounders. Stepwise multiple and single regression analyses were also used to determine and confirm the most significant associations between variables. All subjects gave informed consent in writing and the Ethics Committee of the NorthWest University approved the study, The reader is referred to the "Materials and Methods" section of Chapters 2, 3 and 4 for a more elaborate description of the subjects, study design and analytical methods used in each paper. Results and conclusions of the individual manuscripts *Results from Chapter 2 revealed significantly lower uric acid levels for African men compared to Caucasian men, Despite these lower levels. the association between uric acid and blood pressure is more pronounced within the African men. The strong positive relationship between uric acid and blood pressure might be explained by uric acid's independent relationship with vascular resistance, Uric acid also revealed a positive association with triglycerides in both the African and Caucasian men. These results suggest that uric acid per se can act as a risk factor in the development of cardiovascular dysfunction in African men, *Results from Chapter 3 showed opposing changes in insulin secretion for African men and Caucasian men with increasing age. Whereas insulin levels increased in Caucasian men with progressive age, insulin levels in African men tended to decrease with ageing. Additionally, the insulin-blood pressure relationship within African men revealed opposite results as to what was expected. While the Caucasian men revealed a more positive association between insulin and blood pressure within the younger individuals, older individuals revealed a negative association between insulin and blood pressure, This implies that the vasoconstrictory actions of insulin seem to dominate in young individuals while the vasodilatory actions of insulin take over in older individuals, The turnaround probably acts as a counter protective mechanism against age-related cardiovascular dysfunction. On the contrary, despite decreased insulin secretion in older African men, they exhibit a more positive association between insulin and blood pressure, whereas younger subjects showed a more negative association, These results might suggest dissociation between insulin and blood pressure, Insulin per se might, therefore, not act as a risk factor, but rather the lack of insulin-mediated vasodilatory effects as observed within younger Africans. *Results from Chapter 4 contradicted the notion found in the literature that age-related increase in adiponectin levels are due to impaired renal function. Although the results from this chapter confirmed a Significant association between renal function (estimated creatinine clearance) and adiponectin levels a multiple regression model revealed insulin resistance (HOMA-IR) as the major contributor to adiponectin levels. Adiponectin levels increased with progressive ageing only in the Africans. No such change was observed for the Caucasians. This might be due to development of functional adiponectin resistance or perhaps due to a decline in pancreatic cell mass with ageing. In conclusion, the cardiovascular profile of Africans seems to be more detrimentally affected compared to Caucasians. Results from this study have elucidated on the associations and potential involvement of possible risk factors including, uric acid, insulin, C-peptide, as well as adiponectin, with regards to the high prevalence of cardiovascular dysfunction within the black South African population. / Thesis (Ph.D. (Physiology))--North-West University, Potchefstroom Campus, 2010.

Africans

Cardiovascular dysfunction

Ageing

Hypertension

Uric acid

Insulin

C-peptide

Adiponectin

Swart Afrikane

Kardiovaskulêre disfunksie

Veroudering

Hipertensie

Uriensuur

Insulien

C-peptied

Adiponektien

Desenvolvimento de um biossensor amperométrico baseado em uricase oxidase associado com nanopartículas de platina para detecção de ácido úrico / Development of a amperometric biosensor based on uricase oxidase associated with platinum nanoparticles for detection of uric acid

Anunciação, Eduardo Almeida

28 March 2017

Submitted by Milena Rubi (milenarubi@ufscar.br) on 2017-08-16T16:46:54Z No. of bitstreams: 1 ANUNCIACAO_Eduardo_2017.pdf: 22889091 bytes, checksum: eaec97b1dbf9de44c126b87bb16c49c5 (MD5) / Approved for entry into archive by Milena Rubi (milenarubi@ufscar.br) on 2017-08-16T16:47:02Z (GMT) No. of bitstreams: 1 ANUNCIACAO_Eduardo_2017.pdf: 22889091 bytes, checksum: eaec97b1dbf9de44c126b87bb16c49c5 (MD5) / Approved for entry into archive by Milena Rubi (milenarubi@ufscar.br) on 2017-08-16T16:47:10Z (GMT) No. of bitstreams: 1 ANUNCIACAO_Eduardo_2017.pdf: 22889091 bytes, checksum: eaec97b1dbf9de44c126b87bb16c49c5 (MD5) / Made available in DSpace on 2017-08-16T16:47:17Z (GMT). No. of bitstreams: 1 ANUNCIACAO_Eduardo_2017.pdf: 22889091 bytes, checksum: eaec97b1dbf9de44c126b87bb16c49c5 (MD5) Previous issue date: 2017-03-28 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / Uric acid is an endogenous substance produced from the metabolism of purines. The concentration of serum uric acid in the human body considered normal is between 0.24 - 0.52 mmol.L-1 . High levels of uric acid in the body lead to a condition known as hyperuricemia. Therefore, the monitoring of uric acid in the body is of great importance. In this work we present amperometric biosensors based on the association of the enzyme UOx with platinum nanoparticles to detect uric acid. The technique used to assemble the films that compose the biosensor was the Layer-by-Layer (LbL). Two techniques were used for the synthesis of nanoparticles for the construction of two different film architectures. In the first architecture, the nanoparticles were deposited in situ on a polyethyleneimine (PEI) and sodium polyvinyl sulfate (PVS) film - by reducing hexachloroplatinic acid hexahydrate with sodium borohydride. The bilayers composed of (PEI/UOx)n were deposited on a film containing platinum nanoparticles deposited in situ. In the second architecture, the nanoparticles were synthesized by mixing PEI solution with hexachloroplatinic acid solution and sodium borohydride solution. This solution was deposited alternating with enzymatic solution. The amperometric analyses were performed at +0.347 V potential, with successive additions of 2 mmol.L-1 of uric acid in an electrochemical cell containing phosphate buffered saline (PBS) pH 7.4. For the first architecture, the limit of detection found by the amperometric method was 5.17 µmol.L-1 with the linear detection range comprised in the range between 3.92 - 11.3 µmol.L-1 . For the second architecture, the limit of detection found by the amperometric method was 4.68 µmol.L-1 with a linear detection range between 14.18 - 55.56 µmol.L-1 . For the same architecture an using the differential pulse voltammetry method the values of limit of detection and linear detection range were 0.11 µmol.L-1 and particles / mL, respectively. The biosensors presented limits of detection close to the values found in the literature for other biosensor proving to be efficient for the detection of uric acid. / O ácido úrico é uma substância endógena produzida a partir do metabolismo das purinas. A concentração de ácido úrico sérico no organismo humano considerado normal é entre 0,24 - 0,52 mmol.L-1 . Altos níveis de ácido úrico no organismo levam a um quadro conhecido como hiperuricemia. Portanto, o monitoramento de ácido úrico no organismo é de grande importância. Neste trabalho apresentamos biossensores amperométricos baseados na associação da enzima UOx com nanopartículas de platina para detecção de ácido úrico. A técnica utilizada para a fabricação dos filmes que compõem o biossensor foi a Layer-by-Layer (LbL). Duas técnicas foram utilizadas para a síntese de nanopartículas para a construção de duas arquiteturas diferentes na construção dos filmes. Na primeira arquitetura, as nanopartículas foram depositadas in situ sobre um colchão de polieletrólitos – polietilenoimina (PEI) e polivinil sulfato de sódio (PVS) – pela redução do ácido hexacloroplatínico hexaidratado com boroidreto de sódio. As bicamadas compostas por (PEI/UOx)n foram depositadas sobre colchão contendo nanopartículas de platina depositadas in situ. Na segunda arquitetura, as nanopartículas foram sintetizadas misturando-se solução de PEI com solução de ácido hexacloroplatínico e solução de borohidreto de sódio. Esta solução foi depositada alternando-se com solução enzimática. As análises amperométricas foram realizadas em potencial +0,347 V, com adições sucessivas de ácido úrico de concentração 2 mmol.L-1 em uma célula eletroquímica contendo tampão fosfato salino (PBS) pH 7,4. Para a primeira arquitetura, o limite de detecção encontrado pelo método amperométrico foi de 5,17 µmol.L-1 com a faixa linear de detecção compreendido no intervalo entre 3,92 - 11,3 µmol.L-1 . Para a segunda arquitetura, o limite de detecção encontrado pelo método amperométrico foi de 4,68 µmol.L-1 com a faixa linear de detecção compreendido no intervalo entre 14,18 – 55,56 µmol.L-1 , e para o método DPV os valores de LD e faixa linear de detecção encontrados foram 0,11 µmol.L-1 e 1,8×10& ± 0,2×10& partículas/mL, respectivamente. Os biossensores apresentaram limites de detecção próximos aos valores encontrados na literatura, mostrando-se eficientes para detecção de ácido úrico.

Uric acid

Biosensors

Platinum nanoparticles

Ácido úrico

Biossensores

Técnica Layer-by-Layer

Uricase

Nanopartículas de platina

Aplicações analíticas do eletrodo híbrido modificado acetato de celulose/grafite/azul da prússia

Nectoux, Aline da Silveira

January 2015

Neste trabalho foram estudadas as potencialidades eletroanalíticas de um material híbrido condutor baseado em acetato de celulose e grafite com eletrodeposição de filme condutor de Azul da Prússia (CA/G/PB) como sensor para espécies com importância biológica. O material híbrido foi preparado pelo processo de inversão de fase e caracterizado pelas técnicas de microscopia eletrônica de varredura acoplada com espectroscopia de energia dispersiva (SEM-EDS) e voltametria cíclica. O composto Azul da Prússia (PB) foi imobilizado na superfície do material por eletropolimerização, aplicando-se um potencial fixo de 20 mV em uma janela de -0,3 V a 1,2 V. Os estudos eletroquímicos do eletrodo modificado CA/G/PB foram realizados em solução de KCl 0,1 mol.L-1, sendo obtidos dois pares redox para a espécie eletroativa imobilizada com potenciais médios (E0) em 0,204 V e 0,842 V, indicando um comportamento quase-reversível. O eletrodo demonstrou alta estabilidade após 500 ciclos redox, não sendo observada lixiviação da espécie eletroativa da superfície da matriz modificada. Os dois pares redox do material híbrido CA/G/PB permaneceram praticamente constantes entre os pH 5,0 e 8,0, indicando que as intensidades de pico não são significativamente afetadas nessa faixa de pH. A correlação linear entre as intensidades de pico e a raiz quadrada da velocidade de varredura, indicou que o sistema possui um comportamento similar aqueles em que o processo é controlado por difusão das espécies eletroativas à superfície do eletrodo. O azul da Prússia imobilizado foi aplicado na determinação de dopamina (DP), ácido úrico (AU), ácido ascórbico (AA) e Paracetamol (PCT) através da técnica de voltametria cíclica, voltametria de pulso diferencial e cronoamperometria. / In this work, we studied the electroanalytical potential of a conductive hybrid material based on cellulose acetate and graphite with electrodeposition Blue conductor film of Prussia (CA / G / PB) as a sensor for species with biological importance. The hybrid material was prepared by phase inversion process and characterized by the techniques of scanning electron microscopy coupled with energy dispersive spectroscopy (SEM-EDS) and cyclic voltammetry. The dye of Prussian blue (PB) was immobilized on the surface of the material by electropolymerization applying a fixed potential of 20 mV in a interval from -0.3 V to 1.2 V. The electrochemical behavior of the modified electrode CA / G / PB were performed in solution of 0.1 mol L-1 KCl being obtained two redox couples for the electroactive species immobilized with midpoint potentials (E0) in 0.204 V and 0.842 V, indicating a quasi-reversible behavior. The electrode showed high stability after 500 redox cycles with no observed leaching of electroactive species to the surface of the modified electrode. The two redox pair of the CA / G / PB electrode was kept practically constant within pH 5.0 and 8.0, indicating that the peak intensities are not significantly affected in this pH range. The linear correlation between peak intensities and the square root of scan rate, indicated that the system has a similar behavior those in which the process is controlled by diffusion of electroactive species to the electrode surface. The immobilized Prussian blue was applied to determine dopamine (DP), uric acid (UA), ascorbic acid (AA) and paracetamol (PCT) by analytical techniques of cyclic voltammetry, differential pulse voltammetry and chronoamperometry.

Eletroquímica

Microscopia eletrônica de varredura

Acetato de celulose

Grafite

Cellulose acetate

Graphite electrode

Prussian blue

Dopamine

Ascorbic acid

Uric acid

Paracetamol

Voltammetric techniques

Associação entre ácido úrico materno com resultados maternos e perinatais na pré-eclâmpsia / Uric uric association between mother with results and perinatal maternal in preeclampsia

Damacena, Andressa Trecenti [UNESP]

23 February 2016

Submitted by ANDRESSA TRECENTI DAMACENA null (dretrecenti@hotmail.com) on 2016-05-04T11:16:43Z No. of bitstreams: 1 Dissertacao Andressa - Repositório.pdf: 2946507 bytes, checksum: 9abbfaa6ae7910659e2f50cdfcba9757 (MD5) / Approved for entry into archive by Juliano Benedito Ferreira (julianoferreira@reitoria.unesp.br) on 2016-05-04T20:44:45Z (GMT) No. of bitstreams: 1 damacena_at_me_bot.pdf: 2946507 bytes, checksum: 9abbfaa6ae7910659e2f50cdfcba9757 (MD5) / Made available in DSpace on 2016-05-04T20:44:45Z (GMT). No. of bitstreams: 1 damacena_at_me_bot.pdf: 2946507 bytes, checksum: 9abbfaa6ae7910659e2f50cdfcba9757 (MD5) Previous issue date: 2016-02-23 / Introdução: Pré-eclâmpsia é uma síndrome sistêmica específica da gestação com etiopatogenia ainda não esclarecida, porém acredita -se ser decorrente de alterações no processo de invasão trofoblástica, com consequente inadequado suprimento sanguíneo uterino e estresse oxidativo do tecido placentário. O aumento da concentração de ácido úrico sérico materno (AU) em mulheres com pré-eclâmpsia tem sido associado com a gravidade da hipertensão, proteinúria e prognóstico materno e perinatal na gestação. Objetivos: Identificar a associação entre a concentração sérica de ácido úrico e resultados maternos e perinatais adversos e correlacionar a concentração sérica do ácido úrico materno com recémnascidos pequenos para idade gestacional e proteinúria materna. Sujeitos e Métodos: Foi realizado estudo retrospectivo, em gestantes com pré-eclâmpsia, as quais foram estratificadas de acordo com a dosagem de ácido úrico sérico em dois grupos: I (inferior a 6 mg/dL) e II (igual ou superior a 6 mg/dL) e avaliados resultados adversos maternos e perinatais. Resultados: No grupo II houve maior frequência de crise hipertensiva(25%), eclampsia(6,9%), síndrome HELPP parcial (7,8%) e síndrome HELLP(6,9%), maior número de recém-nascidos pequenos para idade gestacional(47%), menor peso do recém-nascido, maior porcentagem de óbito fetal(1,8%), de prematuridade(68%) e de índice de Apgar no 1º minuto(38%). Conclusões: Os resultados demonstram que as paciente com ácido úrico elevado apresentam piores resultados adversos tanto maternos quanto perinatais, sendo assim a dosagem de ácido úrico sérico materna associadas a outros exames clínicos e laboratoriais, pode auxiliar nos processos de decisão na prática obstétrica. / Introduction: Preeclampsia is a specific systemic disease of pregnancy with unknown etiology, but it is believed to be due to changes in the process of trophoblastic invasion, leading to an inadequate uterine blood supply and oxidative stress of the placental tissue. Increasing of maternal uric acid serum concentration (UA) in women with pre-eclampsia has been associated with the severity of hypertension, proteinuria and maternal and perinatal outcome on pregnancy. Objectives: Identify the association between serum uric acid and adverse maternal and perinatal outcomes. More specifically, the correlation of maternal UA serum concentration with newborn size for gestational age and maternal proteinuria. Subjects and Methods: Cross observational study in pregnant women with preeclampsia, which were stratified according to dose of serum uric acid into two groups, as follow: I (below 6 mg/dL) and II (greater or equal to 6 mg/dL). Maternal and perinatal adverse outcomes were examined. Results were analyzed by T - Student and chi-square tests and correlations were evaluated by Pearson test. The level of significance used was 5%. Results: In group II there were a greater frequency of hypertensive crisis, eclampsia, partial HELPP syndrome and HELLP syndrome. Also it were observed an increased number of small newborns for gestational age, lower weight of the newborn, the higher percentage of fetal death, prematurity and index Apgar at 1 minute. Conclusions: The results suggest that patients with higher uric acid have worse adverse outcomes both for maternal and perinatal. In conclusion, the dosage of maternal serum uric acid associated with other clinical and laboratory tests can help in the decision on obstetrical practice.

Ácido úrico

Complicações maternas

Complicações perinatais

Pré-eclâmpsia

Uric acid

Adverse maternal outcomes

Adverse perinatal outcomes

Preeclampsia

Small for gestational age

Desenvolvimento, otimização, validação e comparação de diferentes abordagens para a avaliação da incerteza na determinação eletroquímica de ácido úrico em soro / Development, optimization, validation and comparison of different approaches for the evaluation of uncertainty in the electrochemical determination of uric acid in human serum

Dadamos, Tony Rogério de Lima [UNESP]

24 January 2018

Submitted by Tony Rogerio de Lima Dadamos null (tonyrlrl@yahoo.com.br) on 2018-02-20T16:25:35Z No. of bitstreams: 1 Tese_AU_TRLD_2018.pdf: 2071412 bytes, checksum: ba59227c90cba94171f8548d07346f1a (MD5) / Approved for entry into archive by Elza Mitiko Sato null (elzasato@ibilce.unesp.br) on 2018-02-21T19:00:37Z (GMT) No. of bitstreams: 1 dadamos_trl_dr_sjrp.pdf: 2071412 bytes, checksum: ba59227c90cba94171f8548d07346f1a (MD5) / Made available in DSpace on 2018-02-21T19:00:37Z (GMT). No. of bitstreams: 1 dadamos_trl_dr_sjrp.pdf: 2071412 bytes, checksum: ba59227c90cba94171f8548d07346f1a (MD5) Previous issue date: 2018-01-24 / Este trabalho apresenta metodologias de desenvolvimento, otimização, e validação de procedimentos de medição eletroquímica de parâmetros bioquímicos em fluidos biológicos. As ferramentas desenvolvidas foram aplicadas à medição voltamétrica, simples e de baixo custo de ácido úrico (AU) em soro humano que se apresenta como uma alternativa confiável às medições realizadas pelo método de referência espectrofométrico. Foi estudada a medição de AU no soro visto a ser utilizada no diagnóstico de várias doenças, tais como gota, doenças cardiovasculares e neoplasias. O eletrodo de trabalho modificado desenvolvido e otimizado é composto por 25 % de lignina, 60 % de nanografite, 15 % de óleo mineral e cobre metálico eletrodepositado. As medições foram realizadas por um método de adição cumulativa de padrão (MAP-C), recorrendo a um novo tratamento estatístico dos dados de calibração, que permite a calibração da instrumentação num pequeno volume de soro. A incerteza da medição foi estimada recorrendo a diversas abordagens bottom-up desenvolvidas e usando abordagens pragmáticas top-down apresentadas na bibliografia. As componentes de incerteza foram combinadas usando a Lei de Propagação de Incertezas ou os métodos numéricos de Kragten e Monte Carlo. Procedeu-se igualmente a uma avaliação bayesiana da incerteza da medição que envolve a atualização de dados da prevalência de ácido úrico na população com o resultado da medição do soro específico analisado. Os modelos metrológicos desenvolvidos foram implementados em folhas de cálculo MSExcel de fácil utilização pelo analista. As avaliações bottom-up da incerteza da medição recorreram a estimativas da incerteza de extrapolação produzidas pelo modelo de regressão ou usando simulações de Monte Carlo aplicáveis quando os pressupostos do modelo de regressão não são cumpridos. O método de adição cumulativa de padrão foi aplicado com sucesso à análise de soro humano pela adição de 1,0, 3,0, 5,0, 7,0 e 9,0 mg dL-1 de AU a 5 mL de soro. A adequação da qualidade das medições eletroquímicas foi avaliada comparando sua incerteza com um valor alvo de 0,56 mg dL-1 (uma oitava parte das faixas de AU de indivíduos saudáveis) e avaliado a compatibilidades das medições com determinações realizadas pelo procedimento de referência. As medições realizadas revelaram-se válidas e com menor custo do que as produzidas pelo método de referência. As ferramentas desenvolvidas para a construção e otimização de eletrodos de trabalho são aplicáveis à medição de outras espécies de análise e em outras matrizes. O método de adição cumulativa de padrão desenvolvido, bem como os modelos de medição respectivos desenvolvidos, são aplicáveis a qualquer tipo de medição instrumental não destrutiva de soluções. / This work presents methodologies for the development, optimization and validation of procedures for the electrochemical measurement of biochemical parameters in biological fluids. The developed tools were applied to voltammetric, simple and low-cost measurements of uric acid (AU) in human serum, which proved to be a reliable alternative to the spectrophotometric reference method. It was studied the measurement of AU in serum since it is used in the diagnosis of various diseases, such as gout, cardiovascular diseases and neoplasms. The developed and optimized modified working electrode is composed of 25 % lignin, 60 % nanocarbon, 15 % mineral oil and electrodeposited copper. The measurements were performed using a cumulative standard addition method (MAP-C), using a new statistical treatment of the calibration data, which allows the calibration of the instrumentation in a small volume of serum. The measurement uncertainty was estimated using developed bottom-up approaches and using pragmatic top-down approaches presented in the literature. The uncertainty components were combined using the Uncertainty Propagation Law or the numerical Kragten and Monte Carlo methods. A bayesian evaluation of the measurement uncertainty was performed, involving the updating of uric acid prevalence in the population with the result of the measurement of AU in the specific serum sample. The developed metrological models were implemented in user-friendly MS-Excel spreadsheets. The bottom-up assessments of measurements uncertainty involve the estimation of the extrapolation uncertainty from the regression model or using Monte Carlo simulations applicable to when the assumptions of the regression model are not valid. The cumulative standard addition method was successfully applied to the analysis of human serum by adding 1.0, 3.0, 5.0, 7.0 and 9.0 mg dL-1 of AU to 5 mL of serum. The adequacy of the electrochemical measurements was assessed by comparing their uncertainty with a target value of 0.56 mg dL-1 (one-eighth of the range of AU in healthy individuals) and by evaluating the compatibility of measurements with determinations performed by the reference procedure. The performed measurements are valid and significantly cheaper than those produced by the reference method. The tools developed for the construction and optimization of working electrodes are applicable to the measurement of other analytes and matrices. The developed cumulative standard addition method and respective measurement models, are applicable to any kind of non-destructive chemical measurement of a solution.

Eletrodo modificado

Ácido úrico

Soro

Método de adição de padrão

Validação de procedimentos

Incerteza da medição

Modified electrode

Uric acid

Serum

Standard addition method

Validation of procedures

Measurement uncertainty