Abstract

The external cues that guide the migration of developing neurons and outgrowth of neurons upon differentiation have been intensely studied for decades. CXCR4, a chemokine receptor, has been implicated in the regulation of chemotaxis, neuronal migration, and axonal guidance. Neuroblastoma cells, which are of neural crest origin, are capable of differentiating into more mature sympathetic neurons in culture, and insulin-like growth factor I (IGF-1), has been shown to promote both migration and neurite outgrowth in these cells. In addition, neuroblastoma cells often express high levels of CXCR4, are responsive to CXCLI 2 and, depending upon the level of differentiation, are capable of producing fully extended axons. The mediator of the cytoskeletal changes seen in during process extension is actin polymerization. We have shown that in the neuroblastoma cell line, SHSY-5Y, both CXCR4 and IGF I receptors are involved in neuronal outgrowth, however, treatment with ligands for these receptors results in different cellular morphologies. CXCR4 stimulation stimulated the cells to take on a more differentiated neuronal form and directly involved actin, while IGF-IR stimulation resulted in a very immature neuronal morphology with shorter, broader processes. Based on these results, our overall hypothesis is that CXCR4 promotes neuronal migration and neurite extension through direct regulation of actin dynamics. Our preliminary data suggest that activation of CXCR4 by CXCL12 in cultured neuroblastoma cells promotes the elongation of neurites, and we have found CXCR4 along these projections. In this work we will be testing three specific hypotheses: 1) Cellular context, including the extracellular matrix present and the concentration of CXCL12 ligand to which the cells are exposed play a large role in determining the signaling pathways that are activated, and thereby the ability of the cells to migrate; 2) CXCR4 activation by CXCL12 promotes an increase in neurite length in neuroblastoma cells; 3) CXCR4 regulates elongation of neuronal processes through interaction with actin using the actinbinding protein Dbn; We will use immunocytochemistry/confocal microscopy, neurite analysis, and immunoprecipitation with cultured neuroblastoma and sympathetic neurons to test these hypotheses. Posttranslational modification of CXCR4 will be analyzed using Mass Spectroscopy.

Public Health Relevance

Neuronal migration during development is critical for the proper formation of nervous system structures and proper synaptic connections. Elucidating the mechanisms underlying CXCR4 mediated neuronal migration is mportant for both understanding normal development and determining strategies for correcting defects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Exploratory Grants (P20)
Project #
4P20GM103653-05
Application #
9132807
Study Section
Special Emphasis Panel (ZRR1-RI-4)
Project Start
Project End
Budget Start
2016-09-01
Budget End
2017-08-31
Support Year
5
Fiscal Year
2016
Total Cost
$161,849
Indirect Cost
$48,667

  Institution

Name
Delaware State University
Department
Type
DUNS #
114337629
City
Dover
State
DE
Country
United States
Zip Code
19901

  Publications

Lombardo, Joseph; Sun, Jianli; Harrington, Melissa A (2018) Rapid activity-dependent modulation of the intrinsic excitability through up-regulation of KCNQ/Kv7 channel function in neonatal spinal motoneurons. PLoS One 13:e0193948
Davis, Stephani A; Itaman, Sheed; Khalid-Janney, Christopher M et al. (2018) TDP-43 interacts with mitochondrial proteins critical for mitophagy and mitochondrial dynamics. Neurosci Lett 678:8-15
Ruggiero, M J; Boschen, K E; Roth, T L et al. (2018) Sex Differences in Early Postnatal Microglial Colonization of the Developing Rat Hippocampus Following a Single-Day Alcohol Exposure. J Neuroimmune Pharmacol 13:189-203
Gawrysiak, Michael J; Grassetti, Stevie N; Greeson, Jeffrey M et al. (2018) The many facets of mindfulness and the prediction of change following mindfulness-based stress reduction (MBSR). J Clin Psychol 74:523-535
Sanchez, Karla R; Mersha, Mahlet D; Dhillon, Harbinder S et al. (2018) Assessment of the Effects of Endocrine Disrupting Compounds on the Development of Vertebrate Neural Network Function Using Multi-electrode Arrays. J Vis Exp :
Staib, Jennifer M; Della Valle, Rebecca; Knox, Dayan K (2018) Disruption of medial septum and diagonal bands of Broca cholinergic projections to the ventral hippocampus disrupt auditory fear memory. Neurobiol Learn Mem 152:71-79
Sadeh, Naomi; Spielberg, Jeffrey M; Logue, Mark W et al. (2018) Linking genes, circuits, and behavior: network connectivity as a novel endophenotype of externalizing. Psychol Med :1-9
Knox, Dayan; Stanfield, Briana R; Staib, Jennifer M et al. (2018) Using c-Jun to identify fear extinction learning-specific patterns of neural activity that are affected by single prolonged stress. Behav Brain Res 341:189-197
Boschen, K E; Keller, S M; Roth, T L et al. (2018) Epigenetic mechanisms in alcohol- and adversity-induced developmental origins of neurobehavioral functioning. Neurotoxicol Teratol 66:63-79
Boppana, Sridhar; Lawal, Hakeem O (2017) Data on the specificity of an antibody to Drosophila vesicular acetylcholine transporter. Data Brief 15:257-261

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