Your search keyword '"Valéria Pereira Ferrer"' showing total 2 results

1. Glioma infiltration and extracellular matrix: key players and modulators

Author

Vivaldo Moura Neto, Valéria Pereira Ferrer, and Rolf Mentlein

Subjects

0301 basic medicine, Chemokine, Angiogenesis, Integrin, Extracellular matrix, 03 medical and health sciences, Cellular and Molecular Neuroscience, Cell Movement, Glioma, medicine, Extracellular, Animals, Humans, Neoplasm Invasiveness, biology, Brain Neoplasms, CD44, medicine.disease, Extracellular Matrix, Cell biology, 030104 developmental biology, Neurology, biology.protein, Neuroglia, Infiltration (medical)

Abstract

An outstanding characteristic of gliomas is their infiltration into brain parenchyma, a property that impairs complete surgical resection; consequently, these tumors might recur, resulting in a high mortality rate. Gliomas invade along preferential routes, such as those along white matter tracts and in the perineuronal and perivascular spaces. Brain extracellular components and their partners and modulators play a crucial role in glioma cell invasion. This review presents an extensive survey of the literature, showing how the brain extracellular matrix (ECM) is modulated during the glioma infiltration process. We explore aspects of ECM interaction with glioma cells, reviewing the main glycosaminoglycans, glycoproteins and proteoglycans. We discuss the roles of ECM-binding proteins, including CD44, RHAMM, integrins and axonal guidance molecules, and highlight the role of proteases and glycosidases in glioma infiltration; in binding and release chemokines, cytokines and growth factors; and in generating new bioactive ECM fragments. We also consider the roles of cytoskeletal signaling, angiogenesis, miRNAs and the glial-to-mesenchymal transition linked to glioma invasion. We closely discuss therapeutic approaches based on the modulation of the extracellular matrix, targeting the control of glioma infiltration, its relative failure in clinical trials, and potential means to overcome this difficulty.

Published

2018

2. Brown spider phospholipase-D containing a conservative mutation (D233E) in the catalytic site: Identification and functional characterization

Author

Matheus Regis Belisário-Ferrari, Silvio Sanches Veiga, Luiza Helena Gremski, Andrea Senff-Ribeiro, Olga Meiri Chaim, Larissa Vuitika, Valéria Pereira Ferrer, and Daniele Chaves-Moreira

Subjects

Phospholipase D, Toxin, Venom, Cell Biology, Biology, medicine.disease, medicine.disease_cause, Biochemistry, Molecular biology, Hemolysis, Loxoscelism, law.invention, law, Complementary DNA, medicine, Recombinant DNA, Heterologous expression, Molecular Biology

Abstract

Brown spider (Loxosceles genus) bites have been reported worldwide. The venom contains a complex composition of several toxins, including phospholipases-D. Native or recombinant phospholipase-D toxins induce cutaneous and systemic loxoscelism, particularly necrotic lesions, inflammatory response, renal failure, and hematological disturbances. Herein, we describe the cloning, heterologous expression and purification of a novel phospholipase-D toxin, LiRecDT7 in reference to six other previously described in phospholipase-D toxin family. The complete cDNA sequence of this novel brown spider phospholipase-D isoform was obtained and the calculated molecular mass of the predicted mature protein is 34.4 kDa. Similarity analyses revealed that LiRecDT7 is homologous to the other dermonecrotic toxin family members particularly to LiRecDT6, sharing 71% sequence identity. LiRecDT7 possesses the conserved amino acid residues involved in catalysis except for a conservative mutation (D233E) in the catalytic site. Purified LiRecDT7 was detected as a soluble 36 kDa protein using anti-whole venom and anti-LiRecDT1 sera, indicating immunological cross-reactivity and evidencing sequence-epitopes identities similar to those of other phospholipase-D family members. Also, LiRecDT7 exhibits sphingomyelinase activity in a concentration dependent-manner and induces experimental skin lesions with swelling, erythema and dermonecrosis. In addition, LiRecDT7 induced a massive inflammatory response in rabbit skin dermis, which is a hallmark of brown spider venom phospholipase-D toxins. Moreover, LiRecDT7 induced in vitro hemolysis in human erythrocytes and increased blood vessel permeability. These features suggest that this novel member of the brown spider venom phospholipase-D family, which naturally contains a mutation (D233E) in the catalytic site, could be useful for future structural and functional studies concerning loxoscelism and lipid biochemistry. Highlights: 1- Novel brown spider phospholipase-D recombinant toxin contains a conservative mutation (D233E) on the catalytic site. 2-LiRecDT7 shares high identity level with isoforms of Loxosceles genus. 3-LiRecDT7 is a recombinant protein immunodetected by specific antibodies to native and recombinant phospholipase-D toxins. 4-LiRecDT7 shows sphingomyelinase-D activity in a concentration-dependent manner, but less intense than other isoforms. 5-LiRecDT7 induces dermonecrosis and inflammatory response in rabbit skin. 6-LiRecDT7 increases vascular permeability in mice. 7-LiRecDT7 triggers direct complement-independent hemolysis in erythrocytes. J. Cell. Biochem. 114: 2479–2492, 2013. © 2013 Wiley Periodicals, Inc.

Published

2013