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Objetivo: Avaliar as crenças que norteiam o cuidar do recém-nascido prematuro em domicílio, na perspectiva da mãe cuidadora. Método: Trata-se de um estudo descritivo com abordagem qualitativa. Foram realizadas 30 entrevistadas semiestruturadas com mães que tiveram filhos prematuros. Para a análise dos discursos apreendidos nas entrevistas foi utilizada a Teoria Fundamentada nos Dados. Resultados: As mães de recém-nascidos prematuros apresentaram baixa renda, pouco acesso ao sistema de saúde e eram moradoras de áreas consideradas geográfica e economicamente menos favorecidas. Evidenciou-se que as mães apresentaram medo e insegurança ao cuidar dos seus filhos e não receberam apoio da Estratégia Saúde da Família. Conclusão: As mães do estudo relataram grande interferência na adoção das práticas parentais no domicílio, principalmente da avó e não se sentem preparadas para cuidar do filho prematuro, em casa, por sentirem medo de realizar os cuidados. (AU)
Objective: To evaluate the beliefs that guide the care of the premature newborn at home from the perspective of the caregiving mother. Methods: This is a descriptive study with a qualitative approach. 30 semi-structured interviewees were carried out with mothers who had premature children. The Grounded Theory was used to analyze the speeches seized in the interviews. Results: It was evidenced that the mothers of premature newborns had low income, little access to the health system and lived in areas considered geographically and economically less favored. It was evident that mothers were afraid and insecure when taking care of their children and did not receive support from the Family Health Strategy. Conclusion: The mothers of the study reported great interference in the adoption of parenting practices at home, especially the grandmother and they do not feel prepared to take care of the premature child at home, because they are afraid to perform the care. (AU)
Objetivo: Evaluar las creencias que guían el cuidado del recién nacido prematuro en el hogar desde la perspectiva de la madre que cuida. Métodos: Este es un estudio transversal con un enfoque cualitativo. Se realizaron 30 entrevistados semiestructurados con madres que tuvieron hijos prematuros. The Grounded Theory se utilizó para analizar los discursos incautados en las entrevistas. Resultados: Se evidenció que las madres de recién nacidos prematuros tenían bajos ingresos, poco acceso al sistema de salud y vivían en áreas consideradas geográficamente y económicamente menos favorecidas. Era evidente que las madres tenían miedo e inseguridad al cuidar a sus hijos y no recibían apoyo de la Estrategia Salud Familiar. Conclusión: Las madres del estudio informaron una gran interferencia en la adopción de prácticas parentales en el hogar, especialmente la abuela, y no se sienten preparadas para cuidar al niño prematuro en casa, porque tienen miedo de realizar el cuidado. (AU)
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Parto , Recien Nacido Prematuro , Conducta Materna , MadresRESUMEN
Abstract Objective The present study aimed to evaluate the relationship between UGT1A1*28 gene polymorphism and the prevalence of neutropenia in patients with colorectal cancer treated with irinotecan. Method Thirteen studies were included. These papers were selected from the Virtual Health Library, Scientific Electronic Library Online, International Health Sciences Literature and PubMed, and their data were collected and evaluated using the BioEstat 5.3 software (BioEstat, Belém, PA, Brazil). Results Three genotypes were analyzed, namely 6/6 (wild type), 6/7, and 7/7. In total, 2,146 patients were included in the present study; of these, 55.6% (n=1,193) had 6/6 genotype, 37.3% (n=801) were heterozygous (6/7), and 7.1% (n=152) had the 7/7 genotype. A total of 1,672 (77.9%) patients displayed mild neutropenia, whereas 474 (22.1%) had severe neutropenia. When contrasting the 6/7 and 7/7 genotypes with the 6/6 genotype using statistical tests for meta-analysis, patients with the 7 allele, either Conclusion The analysis of the UGT1A1*28 gene polymorphism can aid the choice of treatment for patients with colorectal cancer in personalized medicine, increasing the chances of therapeutic success.
Resumo Objetivo Avaliar a relação do polimorfismo do gene UGT1A1*28 com a prevalência de neutropenia em pacientes com câncer colorretal submetidos a tratamento com o irinotecano. Método Foram incluídos 13 estudos sobre o tema proposto, selecionados nas bases de dados da Biblioteca Virtual de Saúde, Scientific Electronic Library Online, International Health Sciences Literature e PubMed.Os dados foramcoletados dos artigos científicos selecionados e avaliados com o auxílio do software BioEstat 5.3 (BioEstat, Belém, PA, Brasil). Resultados Osgenótipos analisados foram6/6 (tipo selvagem), 6/7 e 7/7. Foramincluídos 2.146 pacientes. Destes, 55,6% (n=1.193) apresentaram genótipo 6/6, 37,3% (n=801) eramheterozigotos (6/7) e 7,1%(n=152) tinhamo genótipo 7/7.Umtotal de 1.672 (77,9%) pacientes apresentou neutropenia leve e 474 (22,1%) neutropenia severa. Ao contrastar os genótipos 6/7 e 7/7 como 6/6, percebeu-se, coma execução dos testes estatísticos demetaanálise, que os pacientes como alelo 7, emhomozigose ou heterozigose, tinhammaior risco de desenvolver neutropenia severa que pacientes com o genótipo 6/6 (razão de chances =1,559; intervalo de confiança de 95%=1,163-2,090; p=0,003). Conclusão A análise do polimorfismo do gene UGT1A1*28 pode auxiliar na escolha do tratamento do paciente comcâncer colorretal, no contexto da medicina personalizada, ampliando, assim, as chances de sucesso terapêutico.
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Humanos , Polimorfismo Genético , Neoplasias Colorrectales/tratamiento farmacológico , Neutropenia/epidemiología , Prevalencia , Irinotecán/efectos adversos , Irinotecán/uso terapéuticoRESUMEN
Abstract Objective This metanalysis aimed to evaluate the sensitivity and specificity of computed tomography colonography in colorectal polyp detection. Methods A literature search was performed in the PubMed and Web of Science databases. Results A total of 1,872 patients (males 57.2%, females 42.8%) aged 49 to 82 years old (mean age 59.7 ± 5.3 years) were included in this metanalysis. The estimated sensitivity of computed tomography colonography was 88.4% (46.3-95.7%, coefficient of variation [CV]=28.5%) and the estimated specificity was 73.6% (47.4-100.0%, CV=37.5%). For lesions up to 9mm, the sensitivity was 82.5% (62.0-99.9%, CV =25.1%) and the specificity was 79.2% (32.0-98.0%, CV=22.9%). For lesions>9mm, the sensitivity was 90.2% (64.0-100.0%, CV=7.4%) and the specificity was 94.7% (80.0-100.0%, CV=6.2%). No statistically significant differences in sensitivity according to the size of the lesion were found (p=0.0958); however, the specificity was higher for lesions>9mm (p<0.0001). Conclusions Most of the studies analyzed in the present work were conducted before 2010, which is about a decade after computed tomography colonography started being indicated as a screening method by European and American guidelines. Therefore, more studies aimed at analyzing the technique after further technological advancements are necessary, which could lead to the development of more modern devices.
Resumo Objetivo Esta meta-análise teve como objetivo avaliar a sensibilidade e especificidade da colonografia por tomografia computadorizada na detecção de pólipos colorretais. Métodos Foi realizada uma pesquisa bibliográfica nas bases de dados da PubMed e da Web of Science. Resultados Um total de 1.872 pacientes, 57,2% homens e 42,8% mulheres, com idades entre 49 a 82 anos de idade (média de 59,7 ± 5,3 anos) foram incluídos nesta meta análise. A sensibilidade da colonografia por tomografia computadorizada foi estimada em 88,4% (46,3-95,7%; coeficiente de variância [CV]=28,5%) e a especificidade em 73,6% (47,4%-100,0%; CV=37,5%). Para lesões de até 9mm, a sensibilidade foi de 82,5% (62,0-99,9%; CV=25,1%) e a especificidade de 79,2% (32,0-98,0%; CV=22,9%). Para lesõesmaiores que 9mm, a sensibilidade foi de 90,2% (64,0-100,0%; CV=7,4%) e a especificidade de 94,7% (80,0-100,0%; CV=6,2%). Não houve diferença estatisticamente significante entre as sensibilidades por tamanho da lesão (p=0,0958), porém a especificidade foi maior em lesões acima de 9mm (p<0,0001). Conclusão A maioria dos estudos analisados no presente trabalho foi realizada antes de 2010, cerca de uma década depois que a colonografia por tomografia computadorizada passou a ser indicada como método de triagem pelas diretrizes europeias e americanas. Portanto, são necessários mais estudos com o objetivo de analisar a técnica apósmaiores avanços tecnológicos, o que poderia levar ao desenvolvimento de dispositivos mais modernos.
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Humanos , Masculino , Femenino , Persona de Mediana Edad , Anciano , Anciano de 80 o más Años , Neoplasias Colorrectales/diagnóstico , Adenocarcinoma/diagnóstico , Colonografía Tomográfica Computarizada/estadística & datos numéricosRESUMEN
There is a concern about stablishing the clinical risk of drugs used for cancer treatment. In this study, the cytotoxic, clastogenic and genotoxic properties of cis-tetraammine(oxalato)ruthenium(III) dithionite - cis-[Ru(C2O4)(NH3)4]2(S2O6), were evaluated in vitro in human lymphocytes. The mitotic index (MI), chromosomal aberrations (CA) and DNA damage by comet assay were also analyzed. The MTT test revealed that the ruthenium compound showed a slight cytotoxic effect at the highest concentration tested. The IC50 value for the compound after 24 hours of exposure was 185.4 µM. The MI values of human peripheral blood lymphocytes treated with 0.015, 0.15, 1.5 and 150 µM of cis-[Ru(C2O4)(NH3)4]2(S2O6) were 6.1, 3.9, 3.2 and 0.2%, respectively. The lowest concentration, 0.015 µM, did not show any cytotoxic activity. The CA values for the 0.015, 0.15 and 1.5 µM concentrations presented low frequency (1.5, 1.6 and 2.3%, respectively), and did not express clastogenic activity when compared to the negative control, although it was observed clastogenic activity in the highest concentration tested (150 µM). The results obtained by the comet assay suggest that this compound does not present genotoxic activity at lower concentrations. The results show that cis-[Ru(C2O4)(NH3)4]2(S2O6) has no cytotoxic, clastogenic or genotoxic in vitro effects at concentrations less than or equal to 0.015 µM. This information proves as promising in the treatment of cancer and is crucial for future trials.
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Humanos , Citotoxinas/análisis , Compuestos de Rutenio , Linfocitos/citología , Linfocitos/química , Oxalatos , Daño del ADNRESUMEN
Abstract Invasive aspergillosis is a common fungal infection in immunocompromised individuals. Some studies have shown that toll-like receptor and dectin-1 genetic polymorphisms may alter signaling pathways, thus increasing an individual's susceptibility to invasive aspergillosis. We investigated the pertinent literature to determine whether polymorphisms in the genes encoding toll-like receptors and dectin-1 increase the susceptibility to invasive aspergillosis. This study systematically reviewed the literature using the databases PubMed/PMC, Scopus, and Web of Science using the keywords invasive aspergillosis, polymorphism, Toll-like, and Dectin-1. From the initial search, 415 studies were found and according to our inclusion and exclusion criteria, eight studies were selected. Several studies described single-nucleotide polymorphisms (SNPs) that are associated with a greater susceptibility to invasive aspergillosis. These SNPs were found in the genes that encode toll-like receptors 1, 3, 4, and 5 and the gene that encodes dectin-1; upon activation, both cellular receptors initiate a signaling cascade that can result in the production of cytokines and chemokines. Thus, our literature review uncovered a significant association between polymorphisms in the genes that encode toll-like receptors and dectin-1 and invasive aspergillosis. More studies should be performed to better understand the relationship between toll-like receptor and dectin-1 genetic polymorphisms and invasive aspergillosis susceptibility.
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Humanos , Aspergilosis/genética , Predisposición Genética a la Enfermedad/genética , Polimorfismo de Nucleótido Simple/genética , Lectinas Tipo C/genética , Receptores Toll-Like/genéticaRESUMEN
Introduction: The circadian cycle plays several roles at the organism functions and are important to the maintenance of health, when synchronized. Nowadays, one of the main risk factors for the change of the sleep-wake cycle in the population is the high exposure to light at night, consequently deregulating the circadian cycle, inhibiting the release of melatonin and favoring oncogenesis. Objectives: The aim of this study was to identify the possible associations between circadian rhythm's desynchronization and breast cancer. Methods: This is a descriptive cross-sectional study and two collection instruments were used in it: sociodemographic questionnaire and the Horne and Ostberg matutinal-vespertine questionnaire. They were applied in a group of 74 women in a highly complex oncology service. Results: To evaluate whether the discriminant factors such as night work and chronotype exerted some influence on the discriminated factor that is breast cancer, χ2 test was applied showing that the characteristics among the groups were similar and so it was not possible to confirm that there is a relationship between them. Conclusions: More studies about the subject is needed
Introdução: O ciclo circadiano desempenha vários papéis nas funções do organismo e é importante para a manutenção da saúde, quando sincronizado. Atualmente, um dos principais fatores de risco para a mudança do ciclo vigília-sono na população é a alta exposição à luz noturna, desregulando consequentemente o ciclo circadiano, inibindo a liberação de melatonina e favorecendo a oncogênese. Objetivo: O objetivo deste estudo foi identificar as possíveis associações entre dessincronização do ritmo circadiano e o câncer de mama. Métodos: Trata-se de um estudo descritivo de corte transversal em que foram utilizados dois instrumentos de coleta: um questionário sociodemográfico e o questionário matutino-vespertino de Horne e Ostberg. Os questionários foram aplicados a um grupo de 74 mulheres em um serviço de oncologia. Resultados: Para avaliar se os fatores discriminantes como o trabalho noturno e o cronotipo exerceram alguma influência sobre o fator discriminado, câncer de mama, foi aplicado o teste do χ2, que revelou semelhança entre as características dos grupos estudados. Conclusões: Mais estudos sobre o assunto são necessários de forma a se compreender melhor a possível relação entre o ciclo circadiano e a susceptibilidade ao desenvolvimento de neoplasias, especialmente o câncer de mama
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Introdução: O câncer de mama é a segunda neoplasia mais frequente no mundo e a primeira mais comum no sexo feminino. Dados epidemiológicos apontam o efeito de agentes carcinogênicos e fatores ambientais para maior susceptibilidade em desenvolver o câncer de mama. No contexto das avaliações moleculares, o polimorfismo nulo do gene GSTM1 é comumente estudado na tentativa de associá-lo ao desenvolvimento desta neoplasia. Objetivo: Avaliar se os indivíduos que apresentam o polimorfismo nulo para o gene GSTM1 possuem susceptibilidade ao câncer de mama. Métodos: Realizou-se meta-análise com 10 estudos do tipo caso-controle, que apresentavam pacientes com confirmação histológica de câncer de mama e que faziam uso da PCR e/ou sequenciamento de DNA para determinar o polimorfismo nulo do gene GSTM1. A análise foi realizada após a coleta dos dados necessários (autor, ano de publicação, país e resultados). Os cálculos estatísticos e a representação dos dados foram obtidos com o auxílio do software BioEstat® 5.0. Resultados: O total de indivíduos, após o agrupamento dos dados dos estudos, foi de 7.607 (3.759 casos e 3.848 controles). As frequências para o polimorfismo nulo do gene GSTM1 em pacientes com câncer de mama foram, respectivamente, 51,0% no grupo casos e 50,3% no grupo controle. A análise dos dados obtidos revelou OR: 0,967 e IC95% 0,883?1,060. Conclusão: Conforme os dados obtidos na meta-análise, não foi encontrada associação significativa entre o polimorfismo nulo do gene GSTM1 e o desenvolvimento do câncer de mama. Assim, os resultados do presente estudo mostram que o polimorfismo em questão não alterou suscetibilidade ao câncer de mama, portanto, devem-se levar em consideração outros fatores com maior significância, como: tabagismo, outros marcadores genéticos, tais como BRCA1 e BRCA2, paridade, entre outros.
Introduction: Breast cancer is the second most common cancer worldwide and the first more common in females. Epidemiological data show the effect of carcinogens and environmental factors in the increased susceptibility of developing breast cancer. In the context of molecular assessments, the null polymorphism of GSTM1 gene is commonly studied in an attempt to associate with the development of this neoplasm. Objective: To evaluate whether individuals with the GSTM1-null polymorphism possess susceptibility to breast cancer. Methods: It was conducted a meta-analysis of 10 case-control studies, which had patients with histological confirmed breast cancer and used PCR and/or DNA sequencing to determine the null polymorphism of GSTM1 gene. The analysis was performed after gathering the necessary data (author, publication year, country and results). Statistical calculations and the representation of the data were obtained with the help of BioEstat® 5.0 software. Results: The total number of individuals, after grouping the data was 7,607 (3,759 cases and 3,848 controls). The frequencies for the null polymorphism of GSTM1 gene were, respectively, 51.0% in the case group and 50.3% in the control group. The analysis of the obtained data revealed OR: 0.967 and 95%CI 0.883?1.060. Conclusion: According to the data obtained by meta-analysis it was not found significant association between GSTM1-null polymorphism and the development of breast cancer. Thus, the results of this study revealed that the polymorphism in question did not change the susceptibility to breast cancer, so it should be considered other factors with greater significance, such as smoking, other genetic markers like BRCA1 and BRCA2, parity, among others.
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Ruthenium(III) complexes are increasingly attracting the interest of researchers due to their promising pharmacological properties. Recently, we reported that the cis-(dichloro)tetrammineruthenium(III) chloride compound has cytotoxic effects on murine sarcoma 180 (S-180) cells. In an effort to understand the mechanism responsible for their cytotoxicity, study we investigated the genotoxicity, cell cycle distribution and induction of apoptosis caused by cis- (dichloro)tetrammineruthenium(III) chloride in S-180 tumour cells. cis-(dichloro)tetrammineruthenium(III) chloride treatment induced signifi cant DNA damage in S-180 cells, as detected by the alkaline comet assay. In the cell cycle analysis, cis-(dichloro)tetrammineruthenium(III) chloride caused an increase in the number of cells in G1 phase, accompanied by a decrease in the S and G2 phases after 24 h of treatment. In contrast, the cell cycle distribution of S-180 cells treated with cis-(dichloro)tetrammineruthenium(III) chloride for 48 h showed a concentration-dependent increase in the sub-G1 phase (indicating apoptosis), with a corresponding decrease in cells in the G1, S and G2 phases. In addition, cis-(dichloro)tetrammineruthenium(III) chloride treatment induced apoptosis in a time-dependent manner, as observed by the increased numbers of annexin V-positive cells. Taken together, these fi ndings strongly demonstrate that DNA damage, cell cycle changes and apoptosis may correlate with the cytotoxic effects of cis-(dichloro)tetrammineruthenium( III) chloride on S-180 cells.