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14 results on '"Oliveira, Laura M. A."'

1. Cellular and circuit excitability in rodent models of neurodevelopmental disorders

Author

Simões De Oliveira, Laura M., Wyllie, David, Kind, Peter, and Booker, Sam

Subjects
Autism Spectrum Disorders, intellectual disability, CDKL5 deficiency disorder, Fragile X syndrome, neuron signalling, hippocampus
Abstract

Autism spectrum disorders and intellectual disabilities (ASD/ID) are estimated to a↵ect approximately 3-5% of the population. Genetic factors constitute a major risk factor in ASD/ID, accounting for 40 to 50% of cases, with monogenic forms of syndromic ASD representing 5% of cases. Many of the genetic causes of ASD/ID are thought to share common phenotypes at the cellular level, thus animal models of monogenic forms of ASD/ID provide a valuable tool to better understand the underlying pathophysiology of these disorders. In this thesis I examined two rodent models of monogenic forms of ASD/ID associated with developmental delay, impaired cognitive function and epilepsy, namely CDKL5 deficiency disorder (CDD) and Fragile X Syndrome (FXS). First, I examined synaptic function and intrinsic excitability in the hippocampus of a novel Cdkl5 knock-out (Cdkl5-/y) rat model of CDD. I show an increase in long-term potentiation (LTP) in the hippocampus of Cdkl5-/y rats, consistent to what has previously been reported in mouse models of this disorder. I extend this finding by using a combination of electrophysiological and histological techniques to assess the properties of pre-synaptic neurotransmitter release together with multiple post-synaptic mechanisms that may contribute to the observed Cdk-/y phenotype. Intriguingly, I demonstrated that many of the mechanisms that have been postulated to underlie enhanced LTP are not altered in Cdkl5-/y rats when tested at the single cell level, including changes in AMPAR/NMDAR ratios and increased expression of Ca2+-permeable AMPA receptors. Second, I examined the contribution of the axon initial segment (AIS) to the cellular hyperexcitability of CA1 pyramidal cells in the Fmr1-/y mouse model of FXS. I show that increased AIS length in CA1 pyramidal cells in Fmr1-/y mice is associated with cellular hyperexcitability. I show that depolarisation induced AIS plasticity is unaltered in Fmr1-/y mice is associated with cellular hyperexcitability. I show that depolarisation induced AIS plasticity is unaltered in Fmr1-/y mice, despite an observed reduction in synaptic transmission of EC inputs. In the final chapter of this thesis, I built on my findings in the hippocampus of Fmr1-/y mice, despite an observed reduction in synaptic transmission of EC inputs. In the final chapter of this thesis, I built on my findings in the hippocampus of Fmr1-/y mice. I found the AIS developmental trajectory to be a↵ected in a layer specific manner, with Fmr1-/y mice exhibiting a typical developmental profile in L2/3 and 5 but altered AIS development in L4. However, I did not observe an e↵ect of visual deprivation on AIS length or cellular excitability in either genotype. In summary, this thesis provides insights into the cellular excitability and synaptic physiology in two rodent models of monogenic ASD/ID. I further our existing understanding of rodent models of CDD by characterising hippocampal synaptic and intrinsic physiology in a novel rat model of this disorder, highlighting the need for the identification of robust cross species phenotypes that can be used as potential biomarkers and therapeutic targets in CDD. Furthermore, I put forward the notion of AIS regulation as a contributor to the underpinning of cellular excitability in rodent models of FXS. Additionally, this work contributes to the growing body of evidence showing that compensatory mechanisms have a major contribution to the phenotypes observed in rodent models of ASD/ID, and which should be taken into consideration when developing potential treatment strategies.

Published
2020
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2. Genomic and functional determinants of host spectrum in Group B Streptococcus.

Author

Crestani, Chiara, Forde, Taya L., Bell, John, Lycett, Samantha J., Oliveira, Laura M. A., Pinto, Tatiana C. A., Cobo-Ángel, Claudia G., Ceballos-Márquez, Alejandro, Phuoc, Nguyen N., Sirimanapong, Wanna, Chen, Swaine L., Jamrozy, Dorota, Bentley, Stephen D., Fontaine, Michael, and Zadoks, Ruth N.

Subjects
BIOLOGICAL evolution, STREPTOCOCCUS agalactiae, GENE clusters, BACTERIAL evolution, FOOD security
Abstract

Group B Streptococcus (GBS) is a major human and animal pathogen that threatens public health and food security. Spill-over and spill-back between host species is possible due to adaptation and amplification of GBS in new niches but the evolutionary and functional mechanisms underpinning those phenomena are poorly known. Based on analysis of 1,254 curated genomes from all major GBS host species and six continents, we found that the global GBS population comprises host-generalist, host-adapted and host-restricted sublineages, which are found across host groups, preferentially within one host group, or exclusively within one host group, respectively, and show distinct levels of recombination. Strikingly, the association of GBS genomes with the three major host groups (humans, cattle, fish) is driven by a single accessory gene cluster per host, regardless of sublineage or the breadth of host spectrum. Moreover, those gene clusters are shared with other streptococcal species occupying the same niche and are functionally relevant for host tropism. Our findings demonstrate (1) the heterogeneity of genome plasticity within a bacterial species of public health importance, enabling the identification of high-risk clones; (2) the contribution of inter-species gene transmission to the evolution of GBS; and (3) the importance of considering the role of animal hosts, and the accessory gene pool associated with their microbiota, in the evolution of multi-host bacterial pathogens. Collectively, these phenomena may explain the adaptation and clonal expansion of GBS in animal reservoirs and the risk of spill-over and spill-back between animals and humans. Author summary: Group B Streptococcus (GBS) is a bacterium that represents a health and food security threat in three major host groups: humans (in particular neonates), bovines, and fishes. However, the genomic mechanisms driving adaptation to these hosts remain unclear. Here, we use powerful statistical approaches to compare genomes of GBS from around the world. We found that GBS' ability to exchange genes is a good indicator of how well it can adapt to different hosts. Additionally, three groups of genes appear crucial for GBS to infect either humans, cows, or fishes, regardless of the bacterial strain. These gene groups are also found in other similar bacteria that live in the same hosts or environments. Where a functional role is already known for two gene groups in humans and bovines, respectively, it is shown here for the first time for the third gene group in fishes. Our findings demonstrate the importance of considering the role of animals in the evolution of multi-host bacterial pathogens like GBS. Gene exchange between bacteria infecting multiple hosts represents a high threat to human health, as high-risk types of GBS could adapt and expand in animals, which could then act as reservoirs for highly pathogenic human infections. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Group B Streptococcus Sequence Type 103 as Human and Bovine Pathogen, Brazil.

Author

Oliveira, Laura M. A., Simões, Leandro C., Crestani, Chiara, Costa, Natália S., Pantoja, José Carlos F., Rabello, Renata F., Fracalanzza, Sérgio E. L., Teixeira, Lucia M., Khan, Uzma B., Jamrozy, Dorota, Bentley, Stephen, Pinto, Tatiana C. A., and Zadoks, Ruth N.

Subjects
*STREPTOCOCCUS agalactiae, *BOVINE mastitis, *BOS, *PATHOGENIC microorganisms
Abstract

Group B Streptococcus sequence type 103 is known primarily as a bovine mastitis pathogen. In Brazil, it has circulated in cattle and humans since the 1990s. It lacks scpB and, in humans, was found only among carriage isolates. Bovine-human interspecies transmission may have contributed to its evolution and spread. [ABSTRACT FROM AUTHOR]

Published
2024
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4. Detection of Hanseniaspora opuntiae in anovaginal samples of pregnant women in Rio de Janeiro, Brazil--a case report.

Author

Pinto, Tatiane Nobre, A. Oliveira, Laura M., da Costa, Gisela L., Costa, Natalia Silva, Francisco, Elaine Cristina, Pinto, Tatiana C. A., and Oliveira, Manoel M. E.

Subjects
PREGNANT women, BACTEROIDES fragilis, STREPTOCOCCUS agalactiae, GESTATIONAL diabetes, PRENATAL care, MEDICAL screening
Abstract

In this study, we report the first isolation of Hanseniaspora opuntiae obtained from four pregnant women in Brazil. Clinical isolates were obtained from four samples taken between 35 and 37 gestational weeks, as part of the routine antenatal care for maternal colonization screening for Streptococcus agalactiae group B. The patients were immunocompetent, with two of them diagnosed with gestational diabetes mellitus. Species identification was performed by MALDI-TOF MS and rDNA sequencing. While Hanseniaspora species have not traditionally been considered a typical opportunist pathogen, our findings emphasize the importance of investigating and screening for Hanseniaspora in pregnant populations, highlighting H. opuntiae as a potential agent of human infections. [ABSTRACT FROM AUTHOR]

Published
2024
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8. Virulence-Associated Characteristics of Serotype 14 and Serogroup 9 Streptococcus pneumoniae Clones Circulating in Brazil: Association of Penicillin Non-susceptibility With Transparent Colony Phenotype Variants

Author

Pinto, Tatiana C. A., primary, Costa, Natália S., additional, Pina, Sandrine E. C. M., additional, Souza, Aline R. V., additional, Oliveira, Laura M. A., additional, Moura, Camille A. B., additional, Kegele, Fabíola C. O., additional, Merquior, Vânia L. C., additional, Botelho, Ana Caroline N., additional, Peralta, José M., additional, and Teixeira, Lúcia M., additional

Published
2020
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9. Necessidades educativas do cuidador informal da pessoa idosa dependente em contexto domiciliário

Author

Oliveira, Laura M V C C B

Subjects
cuidador informal, idoso dependente, necessidades educativas
Abstract

Este estudo pretende identificar as necessidades educativas dos cuidadores informais de modo a promover ações concertadas que se traduzem em ganhos para quem cuida e para quem é cuidado por outros. Para a sua realização enveredamos por um Estudo de Caso, selecionando dezoito cuidadores de pessoas idosas dependentes inscritas na UCSP da zona. Realizou-se um estudo qualitativo, exploratório e descritivo. Recorreu-se a uma amostra, não probabilística por escolha racional. Foi utilizado a triangulação no sentido de aumentar a fiabilidade dos resultados. Foram utilizados como instrumentos de recolha de dados uma entrevista semiestruturada que aplicamos aos cuidadores informais principais. Conjuntamente aplicamos um questionário de administração indireta ao cuidador e três escalas para avaliar a capacidade funcional da pessoa idosa dependente (Escala de Barthel, Índice de Lawton e Escala de Pfeiffer, sendo as duas primeiras aplicadas ao cuidador e a terceira aplicada à pessoa idosa dependente). Os cuidadores referiram que desenvolveram as suas capacidades para cuidar através das necessidades advindas do cuidar no dia a dia, através de tentativas e erros com construção da aprendizagem informal de forma autónoma e formal de forma pontual através dos profissionais de saúde, aquando da visita domiciliária. Os principais resultados revelaram que os cuidadores informais revelam necessidades de formação, nomeadamente em cuidados, instrumentais e expressivos. Os resultados deste estudo mostram a necessidade de os profissionais de saúde nortearem a sua ação para os cuidadores informais promovendo a capacitação das suas capacidades e habilidades, através de intervenções que visem colmatar as necessidades percecionadas, de forma promover a continuidade de prestação de cuidados adequados em cada fase da doença.

Published
2020

14. Characterization of Streptococcus pneumoniae serotype 19F-variants occurring in Brazil uncovers a predominant lineage that can lead to misinterpretation in capsular typing.

Author

Oliveira LMA, Souza ARV, Pinto TCA, and Teixeira LM

Subjects
Alleles, Asymptomatic Infections, Bacterial Capsules classification, Bacterial Capsules genetics, Brazil, Carrier Proteins genetics, Carrier State microbiology, Female, Genetic Variation, Humans, Male, Multilocus Sequence Typing, Polymerase Chain Reaction, Serogroup, Serotyping, Streptococcus pneumoniae genetics, Pneumococcal Infections microbiology, Streptococcus pneumoniae classification, Streptococcus pneumoniae isolation & purification
Abstract

Background: Streptococcus pneumoniae (S. pneumoniae) of serogroup 19 are mainly represented by serotypes 19A and 19F, which are associated with antimicrobial resistance and disease. The wzy gene, a component of the pneumococcal capsular locus, is the target to differentiate serotypes 19A and 19F by PCR-based capsular typing. In the last decade, allelic variants of the wzy 19F gene have been described, leading to misinterpretation of capsular typing results., Methods: A collection of 154 serotype 19F S. pneumoniae strains recovered from carriage and disease in Brazil was evaluated to identify and characterize wzy 19F variant isolates., Results: Eleven (7%) wzy 19F variant isolates were detected and identified as belonging to ST810 (n = 10) or ST13673 (n = 1; single-locus variant of ST810). They were mostly recovered from diseased patients, susceptible to the antimicrobial agents tested (except for one multidrug-resistant strain) and did not harbor pili genes. Sequences of the wzy 19F gene of these variants were identical to each other and to those previously described in Brazil, but slightly different from wzy 19F variants identified in other countries., Conclusion: This study indicated that wzy 19F variants present a geographically driven distribution and was the first to uncover phenotypic and genetic features of a wzy 19F variant lineage occurring in Brazil since 1989., (Copyright © 2021 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published
2021
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