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Dive into the research topics where Ernesto Farina is active.

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Featured researches published by Ernesto Farina.


Biomaterials | 2004

Zirconium oxide: analysis of MG63 osteoblast-like cell response by means of a microarray technology.

Francesco Carinci; Furio Pezzetti; Stefano Volinia; Francesca Francioso; Diego Arcelli; Ernesto Farina; Adriano Piattelli

Zirconium oxide ceramics have outstanding mechanical properties, a high biocompatibility and a high resistance to scratching. Expression profiling by DNA microarray is a molecular technology that allows the analysis of gene expression in a cell system. By using DNA microarrays containing 19,200 genes, we identified in osteoblast-like cells line (MG-63) cultured on zirconium oxide discs (Cercon, Degussa Dental, Hanau, Germany) several genes whose expression was significantly up or down-regulated. The differentially expressed genes cover a broad range of functional activities: (a) immunity, (b) vesicular transport and (c) cell cycle regulation. It was also possible to detect some genes whose function is unknown. The data reported are, to our knowledge, the first genetic portrait of a zirconium oxide surface. They can be relevant to better understand the molecular mechanism of biocompatibility and as a model for comparing other materials.


Peptides | 2008

Bombesin: A possible role in wound repair

Adone Baroni; B. Perfetto; N. Canozo; A. Braca; Ernesto Farina; A. Melito; S. De Maria; Maria Cartenì

During tissue regeneration and wound healing of the skin, migration, proliferation and differentiation of keratinocytes are important processes. Here we assessed the effect of a neuropeptide, bombesin, on keratinocytes during regeneration from scratch wounding. Bombesin purified from amphibian skin, is homologous of mammalian gastrin-releasing peptide and is active in mammals. Its pharmacological effects mediate various physiological activities: hypertensive action, stimulating action on gastric secretion, hyperglycemic effect or increased insulin secretion. In vitro it shows a hyperproliferative effect on different experimental models and is involved in skin repair. The aim of this study was to elucidate the effect of Bombesin in an in vitro experimental model on a mechanically injured human keratinocyte monolayer. We evaluated different mediators involved in wound repair such as IL-8, TGFbeta, IL-1, COX-2, VEGF and Toll-like receptors 2 and 4 (TLR2 and TLR4). We also studied the effects of bombesin on cell proliferation and motility and its direct effect on wound repair by observing the wound closure after mechanical injury. The involvement of the bombesin receptors neuromedin receptor (NMBR) and gastrin-releasing peptide receptor (GRP-R) was also evaluated. Our data suggest that bombesin may have an important role in skin repair by regulating the expression of healing markers. It enhanced the expression of IL-8, TGFbeta, COX-2 and VEGF. It also enhanced the expression of TLR2, while TLR4 was not expressed. Bombesin also increased cell growth and migration. In addition, we showed that NMBR was more involved in our experimental model compared to GRP-R.


Journal of Craniofacial Surgery | 2005

An in vitro model for dissecting distraction osteogenesis.

Francesco Carinci; Furio Pezzetti; Anna Spina; Annalisa Palmieri; Friedrick Carls; Gregorio Laino; A. De Rosa; Ernesto Farina; Fausto Illiano; Giordano Stabellini; L. Lomuzio; Vittoria Perrotti; Adriano Piattelli

Distraction osteogenesis (DO) is a mechanotransduction process capable of generating viable osseous tissue by the gradual separation of osteotomized bone edges. Several variables are implicated in DO: magnitude of mechanical strain, distraction rate, and type of distracted bone. The combination of these factors acts on different types of cells inducing apoptosis, cell proliferation, and differentiation. The elucidation of the molecular mechanisms has important clinical implications because it may facilitate the use of recombinant proteins or gene therapy to accelerate bone regeneration. Previous reports have analyzed several molecules such as extracellular matrix proteins, cytokines, bone morphogenetic proteins, hormones, and angiogenic factors. Moreover, a single protein can have multifunctional roles. With such a huge number of mechanical, histologic, cellular, and molecular variables, there is the need to have a cell culture model that enables the selection of the effect of a specific strength to a single cell type at different time points and with or without cytokines. The analysis of the genetic profiling of a cell line cultured on an equibiaxial stretch device has such characteristic. Because there is a recruitment and commitment of preosteoblastic cells during bone lengthening and no previous report has focus on them, the authors used a preosteoblast MC3T3-E1 cell line to detect the early molecular effects of distraction on mesenchymal cells. By using DNA microarrays containing 15,000 clones, the authors identified several genes the expression of which was significantly upor down-regulated. The differentially expressed genes cover a broad range of biological processes: cell growth, metabolism, morphogenesis, cell communication, response to stress, and cell death. The data reported are the first genetic portrait of stretched preosteoblasts. They can be relevant in the better understanding of the molecular mechanism of DO and as a model for comparing the effect of distraction on different cell lines and primary cultures, rate and strength of distraction, and with or without cytokines.


Process Biochemistry | 2002

Degradation of dental plaque glucans and prevention of glucan formation using commercial enzymes

M Marotta; Angela Martino; A De Rosa; Ernesto Farina; Maria Cartenı̀; M. De Rosa


Journal of Cancer Research and Clinical Oncology | 2009

Survivin gene-expression and splicing isoforms in oral squamous cell carcinoma

Salvatore De Maria; Giuseppe Pannone; Pantaleo Bufo; Angela Santoro; Rosario Serpico; Salvatore Metafora; Corrado Rubini; Daniela Pasquali; Silvana Papagerakis; Stefania Staibano; Gaetano De Rosa; Ernesto Farina; Monica Emanuelli; Andrea Santarelli; Maria A. Mariggiò; Lucio Lo Russo; Lorenzo Lo Muzio


Archives of Oral Biology | 2005

Effect of Vitamin C on pre-osteoblast gene expression.

Francesco Carinci; Furio Pezzetti; Anna Spina; Annalisa Palmieri; Gregorio Laino; Alfredo De Rosa; Ernesto Farina; Fausto Illiano; Giordano Stabellini; Vittoria Perrotti; Adriano Piattelli


Journal of Biomedical Materials Research Part A | 2003

Quantitative evaluation of bacteria adherent to polyelectrolyte HEMA-based hydrogels.

Francesca Berlutti; Franco Rosso; Pietro Bosso; Francesco Giansanti; Maria Ajello; Alfredo De Rosa; Ernesto Farina; Giovanni Antonini; Piera Valenti


International Journal of Oncology | 2007

Prognostic value of human telomerase reverse transcriptase gene expression in oral carcinogenesis

Giuseppe Pannone; S. De Maria; Rosanna Zamparese; Salvatore Metafora; Rosario Serpico; Franco Morelli; Corrado Rubini; Ernesto Farina; Maria Cartenì; S. Staibano; G. De Rosa; Lorenzo Lo Muzio; Pantaleo Bufo


Journal of Cellular Biochemistry | 2008

A case report: bone marrow mesenchymal stem cells from a Rett syndrome patient are prone to senescence and show a lower degree of apoptosis.

Tiziana Squillaro; Giuseppe Hayek; Ernesto Farina; Marilena Cipollaro; Alessandra Renieri; Umberto Galderisi


Oncology Letters | 2011

Survivin promoter -31G/C polymorphism in oral cancer cell lines

Salvatore De Maria; Lorenzo Lo Muzio; Alessandra Braca; Paolo Rega; Amalia Cassano; Angela Vinella; Ruggiero Fumarulo; Rosario Serpico; Ernesto Farina; Vittoria Metafora; Giuseppe Pannone; Gian Pietro Ravagnan; Salvatore Metafora; Corrado Rubini; Maria Cartenì; Maria Addolorata Mariggiò

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Rosario Serpico

Seconda Università degli Studi di Napoli

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Adriano Piattelli

University of Chieti-Pescara

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Corrado Rubini

Marche Polytechnic University

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Maria Cartenì

Seconda Università degli Studi di Napoli

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S. De Maria

Seconda Università degli Studi di Napoli

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