Your search keyword '"Navone F"' showing total 9 results

1. The kinesin superfamily motor protein KIF4 is associated with immune cell activation in idiopathic inflammatory myopathies.

Author

Bernasconi P, Cappelletti C, Navone F, Nessi V, Baggi F, Vernos I, Romaggi S, Confalonieri P, Mora M, Morandi L, and Mantegazza R

Subjects

Adult, Blotting, Western, Female, Humans, Immunohistochemistry, Male, Microscopy, Confocal, Muscle, Skeletal immunology, Muscle, Skeletal metabolism, RNA, Messenger analysis, Reverse Transcriptase Polymerase Chain Reaction, Transcription, Genetic, Kinesins biosynthesis, Lymphocyte Activation immunology, Myositis immunology, Myositis metabolism, T-Lymphocytes immunology

Abstract

The idiopathic inflammatory myopathies (IIMs) dermatomyositis, polymyositis, and inclusion body myositis are characterized by myofiber degeneration and inflammation. The triggering factors of muscle autoaggression in these disorders are unknown, but infiltrating T cells may be activated locally and proliferate in situ. T-cell polarization involving reorientation of cytoskeleton and microtubule-organizing centers mediated by motor proteins may occur within inflammatory cells in the muscle. We therefore analyzed ubiquitous and neuronal kinesin superfamily (KIF) members KIF-5, dynein, and KIF4 in IIM muscle biopsies and in activated peripheral blood lymphocytes from healthy donors. Only KIF-4 was altered. Transcript levels were significantly higher in IIM muscle than in controls, and KIF4 inflammatory cells were found in IIM muscles. In polymyositis and inclusion body myositis, KIF4 cells were mainly located around individual muscle fibers, whereas in dermatomyositis, they were also near blood vessels. KIF4 cells were not specific to any immune lineage, and some were Ki67. In peripheral blood lymphocytes stimulated with mitogens, interleukin 2 or anti-CD3/CD28 antibodies, KIF4 expression was upregulated, and the protein was localized in the cytoplasm in association with lysosome-associated membrane protein 1 and perforin lysosomal vesicles. These results imply that KIF4 is associated with activated T cells, irrespective of their functional phenotype, and that it is likely involved in cytoskeletal modifications associated with in situ T-cell activation in IIM.

Published

2008

2. Expression of KIF3C kinesin during neural development and in vitro neuronal differentiation.

Author

Navone F, Consalez GG, Sardella M, Caspani E, Pozzoli O, Frassoni C, Morlacchi E, Sitia R, Sprocati T, and Cabibbo A

Subjects

Animals, Blotting, Northern, Brain Chemistry, Gestational Age, Humans, Immunoblotting, Immunoenzyme Techniques, Immunohistochemistry, In Situ Hybridization, Kinesins analysis, Kinetics, Mice, Neuroblastoma metabolism, Neuroblastoma pathology, Neuroglia chemistry, Neurons chemistry, RNA, Messenger analysis, Tretinoin pharmacology, Tumor Cells, Cultured, Brain embryology, Cell Differentiation, Gene Expression drug effects, Kinesins genetics, Neurons cytology

Abstract

KIF3A, KIF3B and KIF3C are kinesin-related motor subunits of the KIF3 family that associate to form the kinesin-II motor complex in which KIF3C and KIF3B are alternative partners of KIF3A. We have analysed the expression of Kif3 mRNAs during prenatal murine development. Kif3c transcripts are detectable from embryonic day 12.5 and persist throughout development both in the CNS and in some peripheral ganglia. Comparison of the expression patterns of the Kif3 genes revealed that Kif3c and Kif3a mRNAs colocalize in the CNS, while only Kif3a is also present outside the CNS. In contrast, Kif3b is detectable in several non-neural tissues. We have also performed immunocytochemical analyses of the developing rat brain and have found the presence of the KIF3C protein in selected brain regions and in several fibre systems. Using neuroblastoma cells as an in vitro model for neuronal differentiation, we found that retinoic acid stimulated the expression of the three Kif3 and the kinesin-associated protein genes, although with different time courses. The selective expression of Kif3c in the nervous system during embryonic development and its up-regulation during neuroblastoma differentiation suggest a role for this motor during maturation of neuronal cells.

Published

2001

3. KIF3C, a novel member of the kinesin superfamily: sequence, expression, and mapping to human chromosome 2 at 2p23.

Author

Sardella M, Navone F, Rocchi M, Rubartelli A, Viggiano L, Vignali G, Consalez GG, Sitia R, and Cabibbo A

Subjects

Amino Acid Sequence, Animals, Chromosome Mapping, Cloning, Molecular, Humans, Mice, Mice, Inbred C57BL, Molecular Sequence Data, Rats, Sequence Homology, Amino Acid, Chromosomes, Human, Pair 2 genetics, Gene Expression, Kinesins biosynthesis, Kinesins genetics

Abstract

Kinesins are microtubule-dependent molecular motors involved in intracellular transport and mitosis. Here, we report the cloning, sequencing, mapping, and expression of a novel member of the kinesin superfamily. The sequence of this newly identified human cDNA reveals an open reading frame encoding a putative protein of 792 residues. Based on its high sequence similarity to the kinesin-like molecule KIF3B, we named this protein KIF3C. KIF3C is encoded by transcripts that are distinct from the KIF3B mRNA in human, rat, and mouse and is preferentially expressed in the brain. Fluorescence in situ hybridization reveals that, in the human genome, the KIF3C gene maps to chromosome 2 at 2p23. The sequence of KIF3C predicts an unusually long insertion in the proximity of L11, a region thought to mediate microtubule binding. Taken together, these findings suggest that KIF3C is a novel kinesin-like protein that might be specifically involved in microtubule-based transport in neuronal cells., (Copyright 1998 Academic Press.)

Published

1998

4. Expression of neuronal kinesin heavy chain is developmentally regulated in the central nervous system of the rat.

Author

Vignali G, Lizier C, Sprocati MT, Sirtori C, Battaglia G, and Navone F

Subjects

Aging metabolism, Animals, Animals, Newborn, Brain embryology, Brain growth & development, Immunohistochemistry, Kinesins analysis, Macromolecular Substances, Neurons cytology, Organ Specificity, Rats, Rats, Sprague-Dawley, Brain metabolism, Gene Expression Regulation, Developmental, Kinesins biosynthesis, Neurons metabolism

Abstract

The kinesin family of motor proteins comprises at least two isoforms of conventional kinesin encoded by different genes: ubiquitous kinesin, expressed in all cells and tissues, and neuronal kinesin, expressed exclusively in neuronal cells. In the present study, we have analyzed the expression of the two kinesin isoforms by immunochemistry at different stages of development of the rat CNS. We have found that the level of expression of neuronal kinesin is five to eight times higher in developing than in adult rat brains, whereas that of ubiquitous kinesin is only approximately 2.5 times higher in maturing versus adult brains. Moreover, we have studied the distribution of neuronal kinesin by light microscopic immunocytochemistry in the rat brain at different postnatal ages and have found this protein not only to be more highly expressed in juvenile than in adult rat brains but also to show a different pattern of distribution. In particular, tracts of axonal fibers were clearly stained at early postnatal stages of development but were markedly unlabeled in adult rat brains. Our results indicate that the expression of at least one isoform of conventional neuron-specific kinesin is up-regulated in the developing rat CNS and suggest that this protein might play an important role in microtubule-based transport during the maturation of neuronal cells in vivo.

Published

1997

5. Differential expression of ubiquitous and neuronal kinesin heavy chains during differentiation of human neuroblastoma and PC12 cells.

Author

Vignali G, Niclas J, Sprocati MT, Vale RD, Sirtori C, and Navone F

Subjects

Animals, Cells, Cultured, Humans, PC12 Cells, Rats, Cell Differentiation, Gene Expression genetics, Kinesins metabolism, Neuroblastoma metabolism

Abstract

Kinesin is a microtubule-based motor protein involved in intracellular organelle transport. Neurons are characterized by the presence of at least two isoforms of conventional kinesin: ubiquitous kinesin, expressed in all cells and tissues, and neuronal kinesin, whose pattern of expression is confined to neuronal cells. In order to investigate whether the two kinesin motors, which are encoded by different genes, may play distinct biological roles in neurons, we studied their expression during neuronal differentiation. Human neuroblastoma SH-SY5Y and IMR32 cells and rat phaeochromocytoma PC12 cells were used as an in vitro system for neuronal differentiation and were induced to differentiate in the presence of retinoic acid, a combination of dibutyryl cAMP and 5-bromodeoxyuridine, and nerve growth factor respectively. The expression level of each kinesin isoform was evaluated by quantitative immunoblot before and after pharmacological treatment. We found that in all cell types the expression level of neuronal kinesin, but not of ubiquitous kinesin, is stimulated during differentiation. In particular, SH-SY5Y cells show a 4.5-fold, IMR32 cells a 3-fold and PC12 cells a 7-fold increase in the level of expression of neuronal kinesin. By Northern blot analysis we found that the selective increase in the expression of neuronal kinesin is paralleled by an increase in its mRNA, indicating that there is a transcriptional control of the expression of this kinesin isoform during differentiation of neuroblastoma and PC12 cells. Our results suggest that these cells represent an adequate model to study the function of conventional kinesin and its isoforms.

Published

1996

6. Cloning and localization of a conventional kinesin motor expressed exclusively in neurons.

Author

Niclas J, Navone F, Hom-Booher N, and Vale RD

Subjects

Aging metabolism, Amino Acid Sequence, Animals, Animals, Newborn, Blotting, Northern, Brain growth & development, Cells, Cultured, Cloning, Molecular, Drosophila metabolism, Fluorescent Antibody Technique, HeLa Cells, Humans, Macromolecular Substances, Molecular Sequence Data, Poly A biosynthesis, Poly A isolation & purification, RNA biosynthesis, RNA isolation & purification, RNA, Messenger, Rats, Recombinant Fusion Proteins biosynthesis, Recombinant Fusion Proteins isolation & purification, Sciatic Nerve metabolism, Sequence Homology, Amino Acid, Brain metabolism, Gene Expression, Hippocampus metabolism, Kinesins biosynthesis, Neurons metabolism, Organelles metabolism

Abstract

Kinesin is a microtubule-based motor protein involved in organelle transport in neuronal and nonneuronal cells. Although a single kinesin motor has been thought to serve all cell types, we document here that neurons express a second conventional kinesin heavy chain (nKHC) that is 65% identical in amino acid sequence to the ubiquitously expressed kinesin heavy chain (uKHC). By preparing antibodies which distinguish between the two KHCs, we demonstrate that nKHC is a nucleotide-dependent microtubule-binding protein which partially cofractionates with membrane organelles. Immunolocalization experiments show that nKHC is distributed throughout the CNS but is highly enriched in subsets of neurons. In hippocampal neurons in culture, uKHC is distributed uniformly throughout the neuron, whereas nKHC is selectively concentrated in the cell body. These results demonstrate that mammalian neuronal tissue contains two conventional kinesin motors which may serve distinct functions in microtubule-based transport.

Published

1994

7. Cloning and expression of a human kinesin heavy chain gene: interaction of the COOH-terminal domain with cytoplasmic microtubules in transfected CV-1 cells.

Author

Navone F, Niclas J, Hom-Booher N, Sparks L, Bernstein HD, McCaffrey G, and Vale RD

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cell Line, Cloning, Molecular, Cytoplasm metabolism, DNA, Fluorescent Antibody Technique, Humans, Kinesins metabolism, Molecular Sequence Data, Sequence Alignment, Transfection, Kinesins genetics, Microtubules metabolism

Abstract

To understand the interactions between the microtubule-based motor protein kinesin and intracellular components, we have expressed the kinesin heavy chain and its different domains in CV-1 monkey kidney epithelial cells and examined their distributions by immunofluorescence microscopy. For this study, we cloned and sequenced cDNAs encoding a kinesin heavy chain from a human placental library. The human kinesin heavy chain exhibits a high level of sequence identity to the previously cloned invertebrate kinesin heavy chains; homologies between the COOH-terminal domain of human and invertebrate kinesins and the nonmotor domain of the Aspergillus kinesin-like protein bimC were also found. The gene encoding the human kinesin heavy chain also contains a small upstream open reading frame in a G-C rich 5' untranslated region, features that are associated with translational regulation in certain mRNAs. After transient expression in CV-1 cells, the kinesin heavy chain showed both a diffuse distribution and a filamentous staining pattern that coaligned with microtubules but not vimentin intermediate filaments. Altering the number and distribution of microtubules with taxol or nocodazole produced corresponding changes in the localization of the expressed kinesin heavy chain. The expressed NH2-terminal motor and the COOH-terminal tail domains, but not the alpha-helical coiled coil rod domain, also colocalized with microtubules. The finding that both the kinesin motor and tail domains can interact with cytoplasmic microtubules raises the possibility that kinesin could crossbridge and induce sliding between microtubules under certain circumstances.

Published

1992

8. Expression of KIF3C kinesin during neural development and in vitro neuronal differentiation

Author

F, Navone, G G, Consalez, M, Sardella, E, Caspani, O, Pozzoli, C, Frassoni, E, Morlacchi, R, Sitia, T, Sprocati, A, Cabibbo, Navone, F, Consalez, GIAN GIACOMO, Sardella, M, Caspani, E, Pozzoli, O, Frassoni, C, Morlacchi, E, Sitia, Roberto, Sprocati, T, and Cabibbo, A.

Subjects

Brain Chemistry, Neurons, Immunoblotting, Brain, Gene Expression, Kinesins, Cell Differentiation, Gestational Age, Tretinoin, Blotting, Northern, Immunohistochemistry, Immunoenzyme Techniques, Kinetics, Mice, Neuroblastoma, Tumor Cells, Cultured, Animals, Humans, RNA, Messenger, Neuroglia, In Situ Hybridization

Abstract

KIF3A, KIF3B and KIF3C are kinesin-related motor subunits of the KIF3 family that associate to form the kinesin-II motor complex in which KIF3C and KIF3B are alternative partners of KIF3A. We have analysed the expression of Kif3 mRNAs during prenatal murine development. Kif3c transcripts are detectable from embryonic day 12.5 and persist throughout development both in the CNS and in some peripheral ganglia. Comparison of the expression patterns of the Kif3 genes revealed that Kif3c and Kif3a mRNAs colocalize in the CNS, while only Kif3a is also present outside the CNS. In contrast, Kif3b is detectable in several non-neural tissues. We have also performed immunocytochemical analyses of the developing rat brain and have found the presence of the KIF3C protein in selected brain regions and in several fibre systems. Using neuroblastoma cells as an in vitro model for neuronal differentiation, we found that retinoic acid stimulated the expression of the three Kif3 and the kinesin-associated protein genes, although with different time courses. The selective expression of Kif3c in the nervous system during embryonic development and its up-regulation during neuroblastoma differentiation suggest a role for this motor during maturation of neuronal cells.

Published

2001

9. KIF3C, a novel member of the kinesin superfamily: sequence, expression, and mapping to human chromosome 2 at 2p23

Author

Roberto Sitia, Luigi Viggiano, Mariano Rocchi, Anna Rubartelli, Francesca Navone, Giovanna Vignali, Milena Sardella, Andrea Cabibbo, G. Giacomo Consalez, Sardella, M, Navone, F, Rocchi, M, Rubartelli, A, Viggiano, L, Vignali, G, Consalez, GIAN GIACOMO, Sitia, Roberto, and Cabibbo, A.

Subjects

Genetics, Gene map, Sequence Homology, Amino Acid, Molecular Sequence Data, Nucleic acid sequence, Chromosome Mapping, Gene Expression, Kinesins, Biology, Cell biology, Rats, Mice, Inbred C57BL, Open reading frame, Mice, Gene mapping, Complementary DNA, Chromosomes, Human, Pair 2, Kinesin, Animals, Humans, Human genome, Amino Acid Sequence, Cloning, Molecular, Gene

Abstract

Kinesins are microtubule-dependent molecular motors involved in intracellular transport and mitosis. Here, we report the cloning, sequencing, mapping, and expression of a novel member of the kinesin superfamily. The sequence of this newly identified human cDNA reveals an open reading frame encoding a putative protein of 792 residues. Based on its high sequence similarity to the kinesin-like molecule KIF3B, we named this protein KIF3C. KIF3C is encoded by transcripts that are distinct from the KIF3B mRNA in human, rat, and mouse and is preferentially expressed in the brain. Fluorescence in situ hybridization reveals that, in the human genome, the KIF3C gene maps to chromosome 2 at 2p23. The sequence of KIF3C predicts an unusually long insertion in the proximity of L11, a region thought to mediate microtubule binding. Taken together, these findings suggest that KIF3C is a novel kinesin-like protein that might be specifically involved in microtubule-based transport in neuronal cells.

Published

1998