Your search keyword '"Ciotti, Maria Teresa"' showing total 6 results

1. Che-1 enhances cyclin-dependent kinase 5 expression and interacts with the active kinase-complex.

Author

Buontempo S, Barbato C, Bruno T, Corbi N, Ciotti MT, Floridi A, Fanciulli M, and Passananti C

Subjects

Animals, Animals, Newborn, Cells, Cultured, Cerebellum cytology, Cyclin-Dependent Kinase 5 genetics, Humans, Immunoprecipitation methods, Mice, Nuclear Proteins, Rats, Rats, Wistar, Transcription Factors genetics, Transfection methods, Cyclin-Dependent Kinase 5 metabolism, Gene Expression physiology, Gene Expression Regulation genetics, Neurons physiology, Transcription Factors physiology

Abstract

Che-1 is a nuclear protein involved in the regulation of gene transcription and cell proliferation. It has also been shown to localize to the cytoplasm of postmitotic neuronal cells, where it is able to interact with the microtubule-associated protein tau. Cyclin-dependent kinase 5 (Cdk5) is a postmitotic proline-directed serine/threonine kinase that hyperphosphorylates tau under pathological conditions. We observed that Che-1 overexpression induces Cdk5 expression both at the mRNA and protein levels. Furthermore, we show that Che-1 directly interacts with Cdk5 protein in vivo. Cdk5/Che-1 complex formation does not compete with Cdk5/p35 interaction, thus Che-1 is able to bind the active kinase complex. Finally, we demonstrated that Che-1 is itself a Cdk5 substrate.

Published

2008

2. The trophic effect of nerve growth factor in primary cultures of rat hippocampal neurons is associated to an anti‐inflammatory and immunosuppressive transcriptional program.

Author

Maino, Barbara, Spampinato, Antonio G., Severini, Cinzia, Petrella, Carla, Ciotti, Maria Teresa, D'Agata, Velia, Calissano, Pietro, and Cavallaro, Sebastiano

Subjects

NEURODEGENERATION, NEUROTROPHINS, NEURONS, LABORATORY rats, INTRACELLULAR membranes, GENE expression

Abstract

Nerve growth factor, the prototype of a family of neurotrophins, elicits differentiation and survival of peripheral and central neuronal cells. Although its neural mechanisms have been studied extensively, relatively little is known about the transcriptional regulation governing its effects. We have previously observed that in primary cultures of rat hippocampal neurons treatment with nerve growth factor for 72 hr increases neurite outgrowth and cell survival. To obtain a comprehensive view of the underlying transcriptional program, we performed whole‐genome expression analysis by microarray technology. We identified 541 differentially expressed genes and characterized dysregulated pathways related to innate immunity: the complement system and neuro‐inflammatory signaling. The exploitation of such genes and pathways may help interfering with the intracellular mechanisms involved in neuronal survival and guide novel therapeutic strategies for neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2018

3. Transcriptional Analysis of Apoptotic Cerebellar Granule Neurons Following Rescue by Gastric Inhibitory Polypeptide.

Author

Maino, Barbara, Ciotti, Maria Teresa, Calissano, Pietro, and Cavallaro, Sebastiano

Subjects

*GENETIC transcription, *APOPTOSIS, *CYTOPLASMIC granules, *NEURONS, *GASTRIC inhibitory polypeptide, *GENE expression

Abstract

Apoptosis triggered by exogenous or endogenous stimuli is a crucial phenomenon to determine the fate of neurons, both in physiological and in pathological conditions. Our previous study established that gastric inhibitory polypeptide (Gip) is a neurotrophic factor capable of preventing apoptosis of cerebellar granule neurons (CGNs), during its pre-commitment phase. In the present study, we conducted whole-genome expression profiling to obtain a comprehensive view of the transcriptional program underlying the rescue effect of Gip in CGNs. By using DNA microarray technology, we identified 65 genes, we named survival related genes, whose expression is significantly de-regulated following Gip treatment. The expression levels of six transcripts were confirmed by real-time quantitative polymerase chain reaction. The proteins encoded by the survival related genes are functionally grouped in the following categories: signal transduction, transcription, cell cycle, chromatin remodeling, cell death, antioxidant activity, ubiquitination, metabolism and cytoskeletal organization. Our data outline that Gip supports CGNs rescue via a molecular framework, orchestrated by a wide spectrum of gene actors, which propagate survival signals and support neuronal viability. [ABSTRACT FROM AUTHOR]

Published

2014

4. MicroRNA-92 modulates K(+) Cl(−) co-transporter KCC2 expression in cerebellar granule neurons.

Author

Barbato, Christian, Ruberti, Francesca, Pieri, Massimo, Vilardo, Elisa, Costanzo, Manuela, Ciotti, Maria Teresa, Zona, Cristina, and Cogoni, Carlo

Subjects

GENOTYPE-environment interaction, NEUROTRANSMITTER receptors, GENETIC regulation, GENE expression, CELL receptors

Abstract

J. Neurochem. (2010) 113, 591–600. MicroRNAs have been associated to fine-tuning spatial and temporal control of gene expression during neuronal development. The neuronal Cl(−) extruding, K(+)Cl(−) co-transporter 2 (KCC2) is known to play an important role in neuronal Cl(−) homeostasis and in determining the physiological response to activation of anion selective GABA receptors. Here we show that microRNA-92 is developmentally down-regulated during maturation of rat cerebellar granule neurons (CGNs) in vitro. Computational predictions suggest several high-ranking targets for microRNA-92 including the KCC2 gene. Consistently, the KCC2 protein levels were up-regulated in mature CGN in vitro and a functional association between microRNA-92 and KCC2 3′ untranslated region was established using luciferase assays. The generation of an inward directed Cl(−) electrochemical gradient, necessary for the hyperpolarizing effect of GABA, requires robust KCC2 expression in several neuronal types. Here we show that lentiviral-mediated microRNA-92 over-expression reduced KCC2 protein levels and positively shifted reversal potential of GABA induced Cl(−) currents in CGNs. In addition KCC2 re-expression reversed microRNA-92 electrophysiological phenotype. Consistently microRNA-92 inhibition induced both an increase of the level of KCC2 and a negative shift in GABA reversal potential. These findings introduce a new player in the developmental change of GABA from depolarization to hyperpolarization. [ABSTRACT FROM AUTHOR]

Published

2010

5. Dicer expression and localization in post-mitotic neurons

Author

Barbato, Christian, Ciotti, Maria Teresa, Serafino, Annalucia, Calissano, Pietro, and Cogoni, Carlo

Subjects

*NEURONS, *GENE silencing, *GENE expression, *ORIGIN of life

Abstract

Abstract: RNA-mediated gene silencing is recently emerged as a fundamental mechanism of regulation of gene expression in many organisms and tissues, with special emphasis with respect to the nervous system. With the aim to study the components of RNA silencing machinery, we have investigated the expression profile and localization of dicer protein RNase III endonuclease in cultures of post-mitotic neurons. Dicer catalyzes the processing of double-stranded RNAs (dsRNAs) into ≈21–25 nucleotide-long small interfering (si)RNAs and micro (mi)RNAs, and it represents an essential step in the biogenesis of these small non-coding RNA molecules. We show that in rat primary neurons dicer is localized in the somatodendritic compartment, at the Golgi-reticulum area network level. This peculiar distribution was altered by brefeldin A treatment. Moreover the Golgi-reticulum dicer signal was observed also in primary astroglial cells. In addiction dicer was observed to be regulated during the embryogenesis and development in several tissues. In fact its expression is developmentally regulated in cultured cerebellar granule neurons. This is the first study in which dicer is shown preferentially distributed in the Golgi-reticulum area in post-mitotic terminally differentiated neuronal and glial cells and that its profile is modulated during maturation and development of in vitro cultured cerebellar granule neurons. [Copyright &y& Elsevier]

Published

2007

6. Gene expression profiles of apoptotic neurons

Author

Cavallaro, Sebastiano, D'Agata, Velia, Alessi, Enrico, Coffa, Salvatore, Alkon, Daniel L., Manickam, Pachiappan, Ciotti, Maria Teresa, Possenti, Roberta, Bonini, Paolo, Marlier, Lionel, and Calissano, Pietro

Subjects

*GENE expression, *APOPTOSIS, *NEURONS, *GENETIC research

Abstract

The multigenic program underlying neuronal apoptosis is mostly unknown. To study the program, we used genome-scale screening by oligonucleotide microarrays during serum and potassium deprivation-induced apoptosis of cerebellar granule neurons. From the 8740 genes interrogated by the arrays, 423 genes were found to be regulated at both the transcriptional and the posttranscriptional level and segregated into distinct clusters. Semantic clustering based on gene ontologies showed coordinated expression of genes with common biological functions and metabolic pathways. Among the genes implicated in apoptotic cerebellar granule neurons, 70 were in common with those differentially expressed in cortical neurons exposed to amyloid β-protein, indicating the existence of common mechanisms responsible for neuronal cell death. Our results offer a genomic view of the changes that accompany neuronal apoptosis and yield new insights into the underlying molecular basis. [Copyright &y& Elsevier]

Published

2004