Sialic acid accelerates the electrophoretic velocity of injured dorsal root ganglion neurons

Autor:	Ying Liu, Guo-ying Ma, Chen-xu Li, Min-fang Guo
Rok vydání:	2015
Předmět:	rabbits Wnt/β-catenin signaling pathway diagnosis middle cerebral artery occlusion hippocampus Cell intracerebral injection hydrogen sulfide calcitonin gene-related peptide Dorsal root ganglion telomere shortening NSFC grants transcranial magnetic stimulation neurotoxicity paired-pulse facilitation Schwann cells NSFC grant synaptosome viscoelasticity axon reactive oxygen species neuroimaging enhanced susceptibility-weighted angiography image traumatic brain injury brain-derived neurotrophic factor stress relaxation glutamic acid decarboxylase cellular therapy sciatic nerve injury Eg5 Cell biology cerebral ischemia/reperfusion injury cortex heat-hyperalgesia behavior nanocarrier spinal cord injuries neuroprotection tumor suppression neural regeneration dual diagnosis microtubule malondialdehyde neurite outgrowth complications glutamate rehabilitation peptide library superparamagnetic iron oxide particles post-concussion syndrome pain sense model cognitive function delayed neuronal death hyperalgesia rapamycin animal model organ index hydrogen-rich saline Sialic acid TGF-β/BMP-7/Smad signaling chemistry nervous system Polylysine regeneration Ca 2+ cell therapy Neuraminidase Neuroscience non-invasive brain stimulation caspase-3 modified neurological severity scores brain concussion 5-triphenyl-2H-tetrazolium chloride staining neurons MSCs blood brain barrier neuraminidase sodium hydrosulfide myogenic differentiation multiple sclerosis Trf3 cerebral ischemia lcsh:RC346-429 excitatory postsynaptic potential chemistry.chemical_compound electrophoresis velocity HIV-associated neurocognitive disorders tail vein injection CA1 region magnetic resonance imaging oxidative stress curcumin Basso neurotrophic factor nerve regeneration physiological saline pyramidal neurons neuromuscular junction (NMJ) biology autologous nerve repair weaning apoptosis glycosylated membrane protein protection superoxide dismutase medicine.anatomical_structure molecular motor protein Prussian blue staining p53 tumor suppressor gene family sialic acid neurodegenerative disorders glial fibrillary acidic protein Hyperalgesia Peripheral nerve injury immunohistochemistry medicine.symptom phage display γ-aminobutyric acid Research Article dorsal root ganglion polylactic glycolic acid conduit cell electrophoresis neuroplasticity extracellular matrix gel monastrol histomorphology output/input curve primary sensory neuron creep cerebral ischemia/reperfusion loss of neurons Developmental Neuroscience kinesin-5 ferumoxytol medicine peripheral nerve injury immunofluorescence targeting long-term potentiation lcsh:Neurology. Diseases of the nervous system western blotting business.industry aging cerebrum Beattie and Bresnahan score bone marrow mesenchymal stem cells brain injury electrophysiology grafting spinal cord injury rats HIV-1 gp120 V3 loop Membrane protein human adipose-derived stem cells plasticity biology.protein P2X 7 receptor business
Zdroj:	Neural Regeneration Research Neural Regeneration Research, Vol 10, Iss 6, Pp 972-975 (2015)
ISSN:	1673-5374
Popis:	Peripheral nerve injury has been shown to result in ectopic spontaneous discharges on soma and injured sites of sensory neurons, thereby inducing neuropathic pain. With the increase of membrane proteins on soma and injured site neurons, the negatively charged sialic acids bind to the external domains of membrane proteins, resulting in an increase of this charge. We therefore speculate that the electrophoretic velocity of injured neurons may be faster than non-injured neurons. The present study established rat models of neuropathic pain via chronic constriction injury. Results of the cell electrophoresis test revealed that the electrophoretic velocity of injured neuronal cells was faster than that of non-injured (control) cells. We then treated cells with divalent cations of Ca(2+) and organic compounds with positive charges, polylysine to counteract the negatively charged sialic acids, or neuraminidase to specifically remove sialic acids from the membrane surface of injured neurons. All three treatments significantly reduced the electrophoretic velocity of injured neuronal cells. These findings suggest that enhanced sialic acids on injured neurons may accelerate the electrophoretic velocity of injured neurons.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::fd72a3b42b2d89be698e3ebaf3e8736a https://pubmed.ncbi.nlm.nih.gov/26199616 Zobrazit plný text záznamu