Study of Perkinsus olseni infection mechanisms: identification and regulation of parasite genes differentially expressed in response to host and environmental stress

Tese dout., Biologia, Universidade do Algarve, 2008

Técnicas biomoleculares no diagnòstico e tipificação em virologia vegetal

Tese de dout., Ciências Agrárias (Protecção de Plantas), Unidade de Ciências e Tecnologias Agrárias, Univ. do Algarve, 1994

Exploring an uncommon host-parasite interaction to unveil the uniqueness of Perkinsus sp as a model organism

We report the exploration of some unique metabolic pathways in Perkinsus olseni a marine protist parasite, responsible to significant mortalities in mollusks, especially in bivalves all around the world. In Algarve, south of Portugal carpet shell clam Ruditapes decussatus mortalities can reach up to 70%, causing social and economic losses. The objective of studying those unique pathways, is finding new therapeutic strategies capable of controlling/eliminating P. olseni proliferation in clams. In that sense metabolic pathways, were explored, and drugs affecting these cycles were tested for activity. The first step involved the identification of the genes behind those pathways, the reconstitution of the main steps, and molecular characterization of those genes and later on, the identification of possible targets within the genes studied. Metabolic cycles were screened due to the fact of not being present in host or differ in a critical way, such as the following pathways: shikimate, MEP-­‐ isoprenoids, Leloir cycle for chitin production, purine biosynthesis (unique among protists), the de novo synthesis of folates (absent in metazoa) and some unique genes like, the alternative oxidase (a branch of respiratory chain) and the hypoxia sensor HPH. All those pathways were covered and possible chemical inhibition using therapeutic drugs was tested with positive results. The relation between the common host Ruditapes decussatus and P. olseni was also explored in a dimension not possible some years ago. With the accessibility to second generation sequencers and microarray analysis platforms, genes involved in host defense or parasite virulence and resistance to the host were deciphered, allowing aiming to new targets (mechanisms and pathways), offering new possibilities for the control of Perkinsus in close environments. The thousands of genes, generated by this work, sequenced and analyzed from this commercial valuable clam and for Perkinsus olseni will be an important and value tool for the scientific community, allowing a better understanding of host-­‐parasite interactions, promoting the usage of P. olseni as an emerging model for alveolata parasites.

Filodinâmica do vírus da tristeza dos citrinos: epidemiologia molecular e biologia evolutiva

O Citrus tristeza virus (CTV), responsável por várias doenças em citrinos, é um dos maiores condicionantes da citricultura a nível mundial. Existem diversos isolados de CTV com diferentes características biológicas e moleculares, sendo que os sintomas causados pelo vírus dependem essencialmente do isolado viral e da combinação variedade/porta-enxerto. A implementação de medidas de controlo da doença depende, em grande parte, do tipo de isolados presentes numa dada região. No Capítulo 2, efetuou-se uma análise comparativa entre dois métodos de tipificação de isolados de CTV e verificou-se que a caracterização por PCR assimétrico-ELISA, que considera a existência de sete grupos, é mais adequada à descrição da estrutura genética de CTV. Estes resultados foram complementados com o estudo da dinâmica de colonização de cada grupo filogenético através de um imuno-ensaio in situ (Capítulo 3). Os resultados obtidos sugerem que os isolados de CTV diferem na quantidade de células infetadas e que essa diferença parece estar relacionada com a severidade do isolado. No Capítulo 4, o estudo da variabilidade genómica da região 3’ terminal permitiu verificar que a estrutura de grupos obtida para o gene da proteína da cápside (CP) é extensível a toda a região 3’ terminal que contém os genes mais fortemente implicados na interação com o hospedeiro. A estabilidade da estrutura genética nesta região foi também inferida a partir da pesquisa de eventos de recombinação. Os resultados sugerem uma baixa frequência de recombinação entre isolados de CTV, mesmo em isolados contendo mistura de haplótipos e mantidos há mais de 12 anos no mesmo hospedeiro. Adicionalmente, foi estimada a taxa de evolução de CTV através de um método estatístico Bayesiano (Capítulo 5). Para tal, foram usadas sequências do gene da CP de isolados de diversas regiões do mundo, pertencentes a diferentes grupos filogenéticos e obtidas entre 1990 e 2010. A taxa média de evolução estimada foi de 1,58 X 10-4 substituições nucleotídicas / ano. No geral, os resultados destes dois capítulos mostram que os isolados de CTV mantêm uma elevada estabilidade genética ao longo do tempo. Finalmente, no Capítulo 6, foi estudada a situação epidemiológica de CTV em Portugal continental a partir de isolados de CTV recolhidos no campo, onde se verificou que a maioria das árvores infetadas era composta por isolados de CTV pertencentes ao grupo M, ou seja isolados considerados suaves e que não provocam sintomas severos.

Synthesis and evaluation of polymer nanoparticles for delivery in RPE cells

Ocular pathologies are among the most debilitating medical conditions affecting all segments of the population. Traditional treatment options are often ineffective, and gene therapy has the potential to become an alternative approach for the treatment of several pathologies. Methacrylate polymers have been described as highly biocompatible and are successfully used in medical applications. Due to their cationic nature, these polymers can be used to form polyplexes with DNA for its delivery. This work aims to study the potential of PDMAEMA (poly(2-(N,N’-dimethylamino)ethyl methacrylate)) as a non viral gene delivery system to the retina. The first part of this work aimed to study the potential for gene delivery of a previously synthesized PDMAEMA polymer of high molecular weight (354kDa). In the second part, we synthesized by RAFT a PDMAEMA with a lower molecular weight (103.3kDa) and similarly, evaluated its ability to act as a gene delivery vehicle. PDMAEMA/DNA polyplexes were prepared at 5, 7.5, 10, 12.5 and 20 nitrogen/phosphorous (N/P) ratio for the 354kDa PDMAEMA and at 5 and 7.5 for the 103.3kDa PDMAEMA. Dynamic light scattering and zeta potential measurements confirmed the nanosize and positive charge of polyplexes for all ratios and for both polymers. Both high and low Mw PDMAEMA were able to efficiently complex and protect DNA from DNase I degradation. Their cytotoxicity was evaluated using a non-retinal cell line (HEK293) and a retinal pigment epithelium (RPE) cell line (D407). We have found that cytotoxicity of the free polymer is concentration and time dependent, as expected, and negligible for all the concentrations of the PDMAEMA-DNA polyplexes. Furthermore, for the concentrations to be used in vivo, the 354kDa PDMAEMA showed no signs of inflammation upon injection in the intravitreal space of C57BL/6 mice. The transfection efficiency, as evaluated by fluorescence microscopy and flow cytometry, showed that the D407 retinal cells were transfected by polyplexes of both high and low Mw PDMAEMA, but with varied efficiency, which was dependent on the N/P ratio. Althogether, these results suggest that PDMAEMA is a feasible candidate for non-viral gene delivery to the retina, and this work constitutes the basis of further studies to elucidate the bottleneck in transfection and further optimization of the material.

Síntese de trioxolanos e avaliação da sua atividade antiparasitária em Leishmania donovani e Toxoplasma gondii

Dissertação de mestrado, Ciências Farmacêuticas, Faculdade de Ciências e Tecnologia, Universidade do Algarve, 2015

Differentiation of human pluripotent stem cells to the neuronal dopaminergic fate

Dissertação de Mestrado, Ciências Biomédicas, Departamento de Ciências Biomédicas e Medicina, Universidade do Algarve, 2013