Charles Dean Stiles

Charles Dean Stiles, PhD

Professor of Neurobiology, Emeritus

We are currently focused on a pair of CNS-specific bHLH transcription factors known as Olig1 and Olig2. The two Olig genes map to within 40 kb of each other on human chromosome 21 within the Down syndrome critical region. During embryonic development and also in the postnatal brain, the two Olig genes are expressed in progenitor cells that give rise to oligodendrocytes and certain types of neurons (notably motor neurons). Beyond merely marking these cell types, targeted disruption of Olig1/2 in developing embryos disrupts patterning of the ventral spinal cord, ablates formation of oligodendrocytes throughout the CNS and prevents formation of motor neurons. The two Olig proteins are similar to each other within the DNA-targeting bHLH motif. Outside the bHLH domain however, Olig1 and Olig2 are very different proteins and this is reflected in non-overlapping biological functions. Olig1 function has been shown to be essential for the repair of demyelinating lesions in murine models of multiple sclerosis. Olig2 is expressed in the stem-like cells that are found in high-grade human gliomas and is essential for tumor formation in “genetically relevant” murine models of human glioma. Current activities in the Stiles lab are aimed at defining 1) structural features of the two Olig proteins that underlie their separate biological functions, 2) genetic targets of Olig genes and 3) key co-regulator proteins. A variety of methods are used towards these ends including mass spectroscopy, ChIP/Seq and high throughput RNAi screens.

"The two Olig genes map to within 40 kb of each other on human chromosome 21 within the Down syndrome critical region. During embryonic development and also in the postnatal brain, the two Olig genes are expressed in progenitor cells that give rise to oligodendrocytes and certain types of neurons (notably motor neurons)."

Publications View
Platelet-derived growth factor stimulation of monocyte chemoattractant protein-1 gene expression is mediated by transient activation of the phosphoinositide 3-kinase signal transduction pathway.
Authors: Authors: Alberta JA, Auger KR, Batt D, Iannarelli P, Hwang G, Elliott HL, Duke R, Roberts TM, Stiles CD.
J Biol Chem
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TrkA glycosylation regulates receptor localization and activity.
Authors: Authors: Watson FL, Porcionatto MA, Bhattacharyya A, Stiles CD, Segal RA.
J Neurobiol
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Activation of neurotrophin-3 receptor TrkC induces apoptosis in medulloblastomas.
Authors: Authors: Kim JY, Sutton ME, Lu DJ, Cho TA, Goumnerova LC, Goritchenko L, Kaufman JR, Lam KK, Billet AL, Tarbell NJ, Wu J, Allen JC, Stiles CD, Segal RA, Pomeroy SL.
Cancer Res
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PTEN is inversely correlated with the cell survival factor Akt/PKB and is inactivated via multiple mechanismsin haematological malignancies.
Authors: Authors: Dahia PL, Aguiar RC, Alberta J, Kum JB, Caron S, Sill H, Marsh DJ, Ritz J, Freedman A, Stiles C, Eng C.
Hum Mol Genet
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Cancer of the central nervous system. Review of an AACR special conference in cancer research with the joint section on tumors of the AANS/CNS (San Diego, CA, June 7-11, 1997).
Authors: Authors: Stiles CD.
Biochim Biophys Acta
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Activation of ErbB2 during wallerian degeneration of sciatic nerve.
Authors: Authors: Kwon YK, Bhattacharyya A, Alberta JA, Giannobile WV, Cheon K, Stiles CD, Pomeroy SL.
J Neurosci
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Detection of activated platelet-derived growth factor receptors in human meningioma.
Authors: Authors: Shamah SM, Alberta JA, Giannobile WV, Guha A, Kwon YK, Carroll RS, Black PM, Stiles CD.
Cancer Res
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Trk receptors function as rapid retrograde signal carriers in the adult nervous system.
Authors: Authors: Bhattacharyya A, Watson FL, Bradlee TA, Pomeroy SL, Stiles CD, Segal RA.
J Neurosci
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Phosphorylation-directed antibodies in high-flux screens for compounds that modulate signal transduction.
Authors: Authors: Alberta JA, Stiles CD.
Biotechniques
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A PDGF-regulated immediate early gene response initiates neuronal differentiation in ventricular zone progenitor cells.
Authors: Authors: Williams BP, Park JK, Alberta JA, Muhlebach SG, Hwang GY, Roberts TM, Stiles CD.
Neuron
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