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      Peripheral Facial Nerve Axotomy in Mice Causes Sprouting of Motor Axons Into Perineuronal Central White Matter: Time Course and Molecular Characterization

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          Abstract

          Generation of new axonal sprouts plays an important role in neural repair. In the current study, we examined the appearance, composition and effects of gene deletions on intrabrainstem sprouts following peripheral facial nerve axotomy. Axotomy was followed by the appearance of galanin + and calcitonin gene-related peptide (CGRP) + sprouts peaking at day 14, matching both large, neuropeptide + subpopulations of axotomized facial motoneurons, but with CGRP + sprouts considerably rarer. Strong immunoreactivity for vesicular acetylcholine transporter (VAChT) and retrogradely transported MiniRuby following its application on freshly cut proximal facial nerve stump confirmed their axotomized motoneuron origin; the sprouts expressed CD44 and alpha7beta1 integrin adhesion molecules and grew apparently unhindered along neighboring central white matter tracts. Quantification of the galanin + sprouts revealed a stronger response following cut compared with crush (day 7–14) as well as enhanced sprouting after recut (day 8 + 6 vs. 14; 14 + 8 vs. 22), arguing against delayed appearance of sprouting being the result of the initial phase of reinnervation. Sprouting was strongly diminished in brain Jun-deficient mice but enhanced in alpha7 null animals that showed apparently compensatory up-regulation in beta1, suggesting important regulatory roles for transcription factors and the sprout-associated adhesion molecules. Analysis of inflammatory stimuli revealed a 50% reduction 12–48 hours following systemic endotoxin associated with neural inflammation and a tendency toward more sprouts in TNFR1/2 null mutants ( P = 10%) with a reduced inflammatory response, indicating detrimental effects of excessive inflammation. Moreover, the study points to the usefulness of the facial axotomy model in exploring physiological and molecular stimuli regulating central sprouting. J. Comp. Neurol. 518:699–721, 2010. © 2009 Wiley-Liss, Inc.

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          Disruption of the glucocorticoid receptor gene in the nervous system results in reduced anxiety.

          F Tronche, C Kellendonk, O Kretz (1999)
          The glucocorticoid receptor (Gr, encoded by the gene Grl1) controls transcription of target genes both directly by interaction with DNA regulatory elements and indirectly by cross-talk with other transcription factors. In response to various stimuli, including stress, glucocorticoids coordinate metabolic, endocrine, immune and nervous system responses and ensure an adequate profile of transcription. In the brain, Gr has been proposed to modulate emotional behaviour, cognitive functions and addictive states. Previously, these aspects were not studied in the absence of functional Gr because inactivation of Grl1 in mice causes lethality at birth (F.T., C.K. and G.S., unpublished data). Therefore, we generated tissue-specific mutations of this gene using the Cre/loxP -recombination system. This allowed us to generate viable adult mice with loss of Gr function in selected tissues. Loss of Gr function in the nervous system impairs hypothalamus-pituitary-adrenal (HPA)-axis regulation, resulting in increased glucocorticoid (GC) levels that lead to symptoms reminiscent of those observed in Cushing syndrome. Conditional mutagenesis of Gr in the nervous system provides genetic evidence for the importance of Gr signalling in emotional behaviour because mutant animals show an impaired behavioural response to stress and display reduced anxiety.
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            The Universal Protein Resource (UniProt) 2009

            Amos Bairoch, Claire O'Donovan (2009)
            The mission of UniProt is to provide the scientific community with a comprehensive, high-quality and freely accessible resource of protein sequence and functional information that is essential for modern biological research. UniProt is produced by the UniProt Consortium which consists of groups from the European Bioinformatics Institute, the Protein Information Resource and the Swiss Institute of Bioinformatics. The core activities include manual curation of protein sequences assisted by computational analysis, sequence archiving, a user-friendly UniProt website and the provision of additional value-added information through cross-references to other databases. UniProt is comprised of four major components, each optimized for different uses: the UniProt Archive, the UniProt Knowledgebase, the UniProt Reference Clusters and the UniProt Metagenomic and Environmental Sequence Database. One of the key achievements of the UniProt consortium in 2008 is the completion of the first draft of the complete human proteome in UniProtKB/Swiss-Prot. This manually annotated representation of all currently known human protein-coding genes was made available in UniProt release 14.0 with 20 325 entries. UniProt is updated and distributed every three weeks and can be accessed online for searches or downloaded at www.uniprot.org.
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              Activating transcription factor 3 (ATF3) induction by axotomy in sensory and motoneurons: A novel neuronal marker of nerve injury.

              H Tsujino, E Kondo, T Fukuoka (2000)
              Activating transcription factor 3 (ATF3), a member of ATF/CREB family of transcription factors, is induced in a variety of stressed tissue. ATF3 regulates transcription by binding to DNA sites as a homodimer or heterodimer with Jun proteins. The purpose of this study was to examine the expression and regulation of ATF3 after axonal injury in neurons in dorsal root ganglia (DRG) and spinal cord. In naive rats, ATF3 was not expressed in the DRG and spinal cord. Following the cut of peripheral nerve, ATF3 was immediately induced in virtually all DRG neurons and motoneurons that were axotomized, and the time course of induction was dependent on the distance between the injury site and the cell body. Double labeling using immunohistochemistry revealed that the population of DRG neurons expressing ATF3 included those expressing c-jun, and in motoneurons ATF3 and c-jun were concurrently expressed after axotomy. In contrast to c-jun, ATF3 was not induced transsynaptically in spinal dorsal horn neurons. We conclude that ATF3 is specifically induced in sensory and motoneurons in the spinal cord following nerve injury and should be regarded as an unique neuronal marker of nerve injury in the nervous system. Copyright 2000 Academic Press.
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                Author and article information

                Journal
                Journal ID (nlm-ta): J Comp Neurol
                Journal ID (iso-abbrev): J. Comp. Neurol
                Journal ID (publisher-id): cne
                Title: The Journal of Comparative Neurology
                Publisher: Wiley Subscription Services, Inc., A Wiley Company (Hoboken )
                ISSN (Print): 0021-9967
                ISSN (Electronic): 1096-9861
                Publication date (Print): 01 March 2010
                Publication date (Electronic): 13 October 2009
                Volume: 518
                Issue: 5
                Pages: 699-721
                Affiliations
                [1 ]Perinatal Brain Repair Group, Department of Obstetrics and Gynaecology, EGA Institute for Women's Health, University College London London WC1E 6HX, United Kingdom
                [2 ]Department of Neuromorphology, Max-Planck Institute for Neurobiology 82152 Martinsried, Germany
                [3 ]Aurigon Co. D-82327 Tutzing, Germany
                [4 ]Molecular Immunology Unit, Institute of Child Health, University College London London WC1E 6HX, United Kingdom
                [5 ]Department of Anatomy and Developmental Biology, University College London London WC1E 6HX, United Kingdom
                [6 ]Biomedical Research Centre, University of East Anglia Norwich NR4 7, United Kingdom
                [7 ]Cancer Research UK, London Research Institute London WC2A 3PX, United Kingdom
                Author notes
                *CORRESPONDENCE TO: Gennadij Raivich, MD, PhD, Perinatal Brain Repair Group, Department of Obstetrics and Gynaecology and Department of Anatomy and Developmental Biology, University College London, 86-96 Chenies Mews, London WC1E 6HX, United Kingdom. E-mail: g.raivich@ 123456ucl.ac.uk

                The first three authors contributed equally to this work.

                Grant sponsor: International Spinal Research Trust Natalie-Rose-Barr Fellowship (to M.M., G.R.); Grant sponsor: Motor Neuron Disease (MND) Association; Grant number: 06/6220 (to A.A.-S., G.R.); Grant sponsor: Biotechnology and Biological Sciences Research Council; Grant number: 31/S20299 (to G.R.); Grant number: BB/D009537/1 (to G.R.).

                Article
                DOI: 10.1002/cne.22240
                PMC ID: 4491910
                PubMed ID: 20034058
                SO-VID: 4e1bcd99-5ac7-4d81-9884-5808fe966084
                Copyright © Copyright © 2009 Wiley-Liss, Inc.
                History
                Date received : 02 June 2008
                Date revision received : 18 June 2009
                Date accepted : 02 October 2009
                Categories
                Subject: Research Articles

                ScienceOpen disciplines: Neurology
                Keywords: growth cones,regeneration,central sprouting,adhesion molecules,transcription factors,inflammation
                Data availability:
                ScienceOpen disciplines: Neurology
                Keywords: growth cones, regeneration, central sprouting, adhesion molecules, transcription factors, inflammation

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