CARLOS ALBERTO MOREIRA FILHO

(Fonte: Lattes)
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Departamento de Pediatria, Faculdade de Medicina - Docente
LIM/36 - Laboratório de Pediatria Clínica, Hospital das Clínicas, Faculdade de Medicina - Líder

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  • article 68 Citação(ões) na Scopus
    Comprehensive Analysis of BRCA1, BRCA2 and TP53 Germline Mutation and Tumor Characterization: A Portrait of Early-Onset Breast Cancer in Brazil
    (2013) CARRARO, Dirce Maria; FOLGUEIRA, Maria Aparecida Azevedo Koike; LISBOA, Bianca Cristina Garcia; OLIVIERI, Eloisa Helena Ribeiro; KREPISCHI, Ana Cristina Vitorino; CARVALHO, Alex Fiorini de; MOTA, Louise Danielle de Carvalho; PUGA, Renato David; MACIEL, Maria do Socorro; MICHELLI, Rodrigo Augusto Depieri; LYRA, Eduardo Carneiro de; GROSSO, Stana Helena Giorgi; SOARES, Fernando Augusto; ACHATZ, Maria Isabel Alves de Souza Waddington; BRENTANI, Helena; MOREIRA-FILHO, Carlos Alberto; BRENTANI, Maria Mitzi
    Germline mutations in BRCA1, BRCA2 and TP53 genes have been identified as one of the most important disease-causing issues in young breast cancer patients worldwide. The specific defective biological processes that trigger germline mutation-associated and -negative tumors remain unclear. To delineate an initial portrait of Brazilian early-onset breast cancer, we performed an investigation combining both germline and tumor analysis. Germline screening of the BRCA1, BRCA2, CHEK2 (c.1100delC) and TP53 genes was performed in 54 unrelated patients <35 y; their tumors were investigated with respect to transcriptional and genomic profiles as well as hormonal receptors and HER2 expression/amplification. Germline mutations were detected in 12 out of 54 patients (22%) [7 in BRCA1 (13%), 4 in BRCA2 (7%) and one in TP53 (2%) gene]. A cancer familial history was present in 31.4% of the unrelated patients, from them 43.7% were carriers for germline mutation (37.5% in BRCA1 and in 6.2% in the BRCA2 genes). Fifty percent of the unrelated patients with hormone receptor-negative tumors carried BRCA1 mutations, percentage increasing to 83% in cases with familial history of cancer. Over-representation of DNA damage-, cellular and cell cycle-related processes was detected in the up-regulated genes of BRCA1/2-associated tumors, whereas cell and embryo development-related processes were over-represented in the up-regulated genes of BRCA1/2-negative tumors, suggesting distinct mechanisms driving the tumorigenesis. An initial portrait of the early-onset breast cancer patients in Brazil was generated pointing out that hormone receptor-negative tumors and positive familial history are two major risk factors for detection of a BRCA1 germline mutation. Additionally, the data revealed molecular factors that potentially trigger the tumor development in young patients.
  • article 5 Citação(ões) na Scopus
    Disruption of the CREBBP gene and decreased expression of CREB, NF kappa B p65, c-JUN, c-FOS, BCL2 and c-MYC suggest immune dysregulation
    (2013) TORRES, Leuridan Cavalcante; KULIKOWSKI, Leslie Domenici; RAMOS, Patricia Locosque; SUGAYAMA, Sofia Mizuko Miura; MOREIRA-FILHO, Carlos Alberto; CARNEIRO-SAMPAIO, Magda
    Genomic aberrations in the CREBBP (CREB-binding protein - CREBBP or CBP) gene such as point mutations, small insertions or exonic copy number changes are usually associated with Rubinstein-Taybi syndrome (RTs). In this study, the disruption of the CREBBP gene on chromosome 16p13.3, as revealed by CGH-array and FISH, suggests immune dysregulation in a patient with the Rubinstein Taybi syndrome (RTs) phenotype. Further investigation with Western blot techniques demonstrated decreased expression of CREB, NP kappa B, c-Jun, c-Fos, BCL2 and cMyc in peripheral blood mononuclear cells, thus indicating that the CREBBP gene is essential for the normal expression of these proteins and the regulation of immune responses.
  • article 20 Citação(ões) na Scopus
    Complex Network Analysis of CA3 Transcriptome Reveals Pathogenic and Compensatory Pathways in Refractory Temporal Lobe Epilepsy
    (2013) BANDO, Silvia Yumi; SILVA, Filipi Nascimento; COSTA, Luciano Da Fontoura; SILVA, Alexandre V.; PIMENTEL-SILVA, Luciana R.; CASTRO, Luiz H. M.; WEN, Hung-Tzu; AMARO JR., Edson; MOREIRA-FILHO, Carlos Alberto
    We previously described - studying transcriptional signatures of hippocampal CA3 explants - that febrile (FS) and afebrile (NFS) forms of refractory mesial temporal lobe epilepsy constitute two distinct genomic phenotypes. That network analysis was based on a limited number (hundreds) of differentially expressed genes (DE networks) among a large set of valid transcripts (close to two tens of thousands). Here we developed a methodology for complex network visualization (3D) and analysis that allows the categorization of network nodes according to distinct hierarchical levels of gene-gene connections (node degree) and of interconnection between node neighbors (concentric node degree). Hubs are highly connected nodes, VIPs have low node degree but connect only with hubs, and high-hubs have VIP status and high overall number of connections. Studying the whole set of CA3 valid transcripts we: i) obtained complete transcriptional networks (CO) for FS and NFS phenotypic groups; ii) examined how CO and DE networks are related; iii) characterized genomic and molecular mechanisms underlying FS and NFS phenotypes, identifying potential novel targets for therapeutic interventions. We found that: i) DE hubs and VIPs are evenly distributed inside the CO networks; ii) most DE hubs and VIPs are related to synaptic transmission and neuronal excitability whereas most CO hubs, VIPs and high hubs are related to neuronal differentiation, homeostasis and neuroprotection, indicating compensatory mechanisms. Complex network visualization and analysis is a useful tool for systems biology approaches to multifactorial diseases. Network centrality observed for hubs, VIPs and high hubs of CO networks, is consistent with the network disease model, where a group of nodes whose perturbation leads to a disease phenotype occupies a central position in the network. Conceivably, the chance for exerting therapeutic effects through the modulation of particular genes will be higher if these genes are highly interconnected in transcriptional networks.
  • article 3 Citação(ões) na Scopus
    New CBP mutations in Brazilian patients with Rubinstein-Taybi syndrome
    (2013) SUZUKI, K. T.; TORRES, L. C.; SUGAYAMA, S. M. M.; ALVES, B. da Costa Aguiar; MOREIRA-FILHO, C. A.; CARNEIRO-SAMPAIO, M.