Publications by authors named "Eduardo M Reis"

Article Synopsis
  • Developing new painkillers is tough because many potential drugs have serious side effects due to their impact on various biological pathways beyond just pain relief.
  • Researchers are focusing on targeting protein-protein interactions (PPIs) involved in pain signaling to create more effective and safer analgesics, using rodent models to evaluate their pain-reducing abilities.
  • By analyzing data from sensory nerve tissues, they identified key PPIs for exploring new drug designs, suggesting that blocking specific interactions in relevant proteins may improve pain treatment while minimizing unwanted effects.
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The search for prognostic markers in breast cancer has bumped into a typical feature of these tumors, intra and intertumoral heterogeneity. Changes in the expression profile, localization of these proteins or shedding to the surrounding stroma can be useful in the search for new markers. In this context, classification by molecular subtypes can bring perspectives for both diagnosis and screening for appropriate treatments.

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Background: Neural progenitor cells (NPCs) can be cultivated from developing brains, reproducing many of the processes that occur during neural development. They can be isolated from a variety of animal models, such as transgenic mice carrying mutations in amyloid precursor protein (APP) and presenilin 1 and 2 (PSEN 1 and 2), characteristic of familial Alzheimer's disease (fAD). Modulating the development of these cells with inflammation-related peptides, such as bradykinin (BK) and its antagonist HOE-140, enables the understanding of the impact of such molecules in a relevant AD model.

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Proteins involved in the Alzheimer's disease (AD), such as amyloid precursor protein (APP) and presenilin-1 (PS1), play critical roles in early development of the central nervous system (CNS), as well as in innate immune and glial cell responses. Familial AD is associated with the presence of APP and PS1 mutations. However, it is still unknown whether these mutations cause deficits in CNS development of carriers.

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5-aminolevulinic acid (5-ALA) is the first precursor of the heme biosynthesis pathway, accumulated in acute intermittent porphyria (AIP), an inherited metabolic disease characterized by porphobilinogen deaminase deficiency. An increased incidence of hepatocellular carcinoma (HCC) has been reported as a long-term manifestation in symptomatic AIP patients. 5-ALA is an α-aminoketone prone to oxidation, yielding reactive oxygen species and 4,5-dioxovaleric acid.

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Protein kinase M zeta, PKMζ, is a brain enriched kinase with a well characterized role in Long-Term Potentiation (LTP), the activity-dependent strengthening of synapses involved in long-term memory formation. However, little is known about the molecular mechanisms that maintain the tissue specificity of this kinase. Here, we characterized the epigenetic factors, mainly DNA methylation, regulating PKMζ expression in the human brain.

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Pancreatic ductal adenocarcinomas (PDAC) are the fourth leading cause of death due to neoplasms. In view of the urgent need of effective treatments for PDAC, photodynamic therapy (PDT) appears as a promising alternative. However, its efficacy against PDAC and the mechanisms involved in cell death induction remain unclear.

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Article Synopsis
  • The study investigates the epigenetic changes in melanoma progression using a four-stage cell line model, examining how CpG methylation varies across different stages: from non-tumorigenic melanocytes to metastatic melanoma cells.
  • Researchers identified specific gene promoters that are hypo- and hypermethylated, which characterize distinct malignancy and metastasis signatures, totaling 540 hypo- and 37 hypermethylated promoters for malignancy, and 646 hypo- and 520 hypermethylated promoters for metastasis.
  • The findings suggest that specific CpGs could serve as potential markers for predicting poor survival in melanoma patients, as they showed a correlation between DNA methylation and transcriptional levels in key genes linked to melanoma prognosis.
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Invasion of surrounding stroma is an early event in breast cancer metastatic progression, and involves loss of cell polarity, loss of myoepithelial layer, epithelial-mesenchymal transition (EMT) and remodeling of the extracellular matrix (ECM). Integrins are transmembrane receptors responsible for cell-ECM binding, which triggers signals that regulate many aspects of cell behavior and fate. Changes in the expression, localization and pairing of integrins contribute for abnormal responses found in transformed epithelia.

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  • Epigenetic changes, such as DNA methylation, play a crucial role in the development and progression of melanoma, alongside genetic mutations.* -
  • The study aimed to discover how methylation of promoter and gene body regions affects gene expression, linking these changes to various stages of melanoma progression using a linear mouse model.* -
  • Key genes related to tumor growth (Adcy3) and metastasis (Inpp4b) were identified, and the findings showed a correlation between the mouse model's results and clinical data from melanoma patient cohorts, suggesting possible prognostic markers.*
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  • Despite improvements in treatment, melanoma still often leads to poor patient outcomes, and there is a lack of effective biological models to study its progression.
  • Researchers analyzed the gene expression profiles of various melanoma cell lines representing different stages of the disease, finding distinct gene expression patterns linked to cell differentiation and mesenchymal transitions.
  • The study identified several genes that could serve as prognostic markers for melanoma progression, enhancing our understanding of the disease and suggesting potential new drug targets.
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Article Synopsis
  • - The study developed a murine cellular system to model the transition from melanocytes to metastatic melanoma cells, analyzing four distinct cell lines to understand the progression of melanoma through gene co-expression and histone modification profiling.
  • - Researchers identified 18 gene modules related to melanoma progression and metastasis, which were linked to biological processes like cell migration and DNA repair, and some showed potential as prognostic biomarkers based on patient survival data from melanoma cohorts.
  • - Analysis revealed specific patterns of histone modifications connected to melanoma stages, with certain marks being reduced or increased in metastatic cells, suggesting these modifications may play a role in the disease's progression.
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Purpose: Oncogenic KRAS mutations are found in over 90% of pancreatic ductal adenocarcinomas (PDACs). As yet, however, no effective therapies are available for KRAS-induced malignancies. Therefore, research aimed at the identification of KRAS targets with therapeutic potential is warranted.

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Among the clinical manifestations observed in septic patients, sepsis-associated encephalopathy (SAE) is probably the most obscure and poorly explored. It is well established, however, that SAE is more prevalent in aged individuals and related to a worse outcome. In this context, we decided to investigate the acute effects of sepsis, induced by cecal ligation and puncture (CLP), on the cerebral transcriptional profile of young and old rats.

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Cell signaling events triggered by androgen hormone in prostate cells is dependent on activation of the androgen receptor (AR) transcription factor. Androgen hormone binding to AR promotes its displacement from the cytoplasm to the nucleus and AR binding to DNA motifs, thus inducing activatory and inhibitory transcriptional programs through a complex regulatory mechanism not yet fully understood. In this work, we performed RNA-seq deep-sequencing of LNCaP prostate cancer cells and found over 7000 expressed long intergenic non-coding RNAs (lincRNAs), of which ∼4000 are novel lincRNAs, and 258 lincRNAs have their expression activated by androgen.

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Sepsis is a major cause of death and its incidence and mortality increase exponentially with age. Most gene expression studies in sepsis have focused in protein-coding genes and the expression patterns, and potential roles of long noncoding RNAs (lncRNAs) have not been investigated yet. In this study, we performed co-expression network analysis of protein-coding and lncRNAs measured in neutrophil granulocytes from adult and elderly septic patients, along with age-matched healthy controls.

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Changes in RNA stability have an important impact in the gene expression regulation. Different methods based on the transcription blockage with RNA polymerase inhibitors or metabolic labeling of newly synthesized RNAs have been developed to evaluate RNA decay rates in cultured cell. Combined with techniques to measure transcript abundance genome-wide, these methods have been used to reveal novel features of the eukaryotic transcriptome.

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Breast carcinoma (BC) corresponds to 23 % of all cancers in women, with 1.38 million new cases and 460,000 deaths worldwide annually. Despite the significant advances in the identification of molecular markers and different modalities of treatment for primary BC, the ability to predict its metastatic behavior is still limited.

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Article Synopsis
  • Long noncoding RNAs (lncRNAs) are often overlooked in research due to the assumption they are just byproducts of other RNA processes, but this study investigates thousands of these RNAs for their characteristics and significance.
  • The research found that a high percentage of intronic and antisense lncRNAs displayed features typical of actively transcribed RNA and were more stable than typical mRNAs, with some even being expressed independently of their related protein-coding genes.
  • These lncRNAs showed evolutionary conservation and were found in the cytoplasm, indicating they could have important roles in regulating cellular functions, particularly related to cell division and DNA replication.
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Sepsis is one of the highest causes of mortality in hospitalized people and a common complication in both surgical and clinical patients admitted to hospital for non-infectious reasons. Sepsis is especially common in older people and its incidence is likely to increase substantially as a population ages. Despite its increased prevalence and mortality in older people, immune responses in the elderly during septic shock appear similar to that in younger patients.

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Signaling via epidermal growth factor receptor (EGFR) and Src kinase pathways promote triple-negative breast cancer (TNBC) cell invasion and tumor metastasis. Here, we address the role of Cdc42-interacting protein-4 (CIP4) in TNBC metastasis in vivo, and profile CIP4 expression in human breast cancer patients. In human TNBC cells, CIP4 knock-down (KD) led to less sustained activation of Erk kinase and impaired cell motility compared to control cells.

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BCL-X mRNA alternative splicing generates pro-apoptotic BCL-XS or anti-apoptotic BCL-XL gene products and the mechanism that regulates splice shifting is incompletely understood. We identified and characterized a long non-coding RNA (lncRNA) named INXS, transcribed from the opposite genomic strand of BCL-X, that was 5- to 9-fold less abundant in tumor cell lines from kidney, liver, breast and prostate and in kidney tumor tissues compared with non-tumors. INXS is an unspliced 1903 nt-long RNA, is transcribed by RNA polymerase II, 5'-capped, nuclear enriched and binds Sam68 splicing-modulator.

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Background: Intronic and intergenic long noncoding RNAs (lncRNAs) are emerging gene expression regulators. The molecular pathogenesis of renal cell carcinoma (RCC) is still poorly understood, and in particular, limited studies are available for intronic lncRNAs expressed in RCC.

Methods: Microarray experiments were performed with custom-designed arrays enriched with probes for lncRNAs mapping to intronic genomic regions.

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