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Articles, Development/Plasticity/Repair

Anti-Muscarinic Adjunct Therapy Accelerates Functional Human Oligodendrocyte Repair

Kavitha Abiraman, Suyog U. Pol, Melanie A. O'Bara, Guang-Di Chen, Zainab M. Khaku, Jing Wang, David Thorn, Bansi H. Vedia, Ezinne C. Ekwegbalu, Jun-Xu Li, Richard J. Salvi and Fraser J. Sim
Journal of Neuroscience 25 February 2015, 35 (8) 3676-3688; DOI: https://doi.org/10.1523/JNEUROSCI.3510-14.2015
Kavitha Abiraman
1Neuroscience Program,
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Suyog U. Pol
2Department of Pharmacology and Toxicology, and
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Melanie A. O'Bara
2Department of Pharmacology and Toxicology, and
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Guang-Di Chen
3School of Medicine and Biomedical Sciences, Center for Hearing and Deafness, University at Buffalo, Buffalo, New York 14214
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Zainab M. Khaku
2Department of Pharmacology and Toxicology, and
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Jing Wang
2Department of Pharmacology and Toxicology, and
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David Thorn
2Department of Pharmacology and Toxicology, and
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Bansi H. Vedia
2Department of Pharmacology and Toxicology, and
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Ezinne C. Ekwegbalu
2Department of Pharmacology and Toxicology, and
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Jun-Xu Li
2Department of Pharmacology and Toxicology, and
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Richard J. Salvi
3School of Medicine and Biomedical Sciences, Center for Hearing and Deafness, University at Buffalo, Buffalo, New York 14214
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Fraser J. Sim
1Neuroscience Program,
2Department of Pharmacology and Toxicology, and
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Abstract

Therapeutic repair of myelin disorders may be limited by the relatively slow rate of human oligodendrocyte differentiation. To identify appropriate pharmacological targets with which to accelerate differentiation of human oligodendrocyte progenitors (hOPCs) directly, we used CD140a/O4-based FACS of human forebrain and microarray to hOPC-specific receptors. Among these, we identified CHRM3, a M3R muscarinic acetylcholine receptor, as being restricted to oligodendrocyte-biased CD140a+O4+ cells. Muscarinic agonist treatment of hOPCs resulted in a specific and dose-dependent blockade of oligodendrocyte commitment. Conversely, when hOPCs were cocultured with human neurons, M3R antagonist treatment stimulated oligodendrocytic differentiation. Systemic treatment with solifenacin, an FDA-approved muscarinic receptor antagonist, increased oligodendrocyte differentiation of transplanted hOPCs in hypomyelinated shiverer/rag2 brain. Importantly, solifenacin treatment of engrafted animals reduced auditory brainstem response interpeak latency, indicative of increased conduction velocity and thereby enhanced functional repair. Therefore, solifenacin and other selective muscarinic antagonists represent new adjunct approaches to accelerate repair by engrafted human progenitors.

  • glia
  • human
  • microarray
  • oligodendrocyte
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The Journal of Neuroscience: 35 (8)
Journal of Neuroscience
Vol. 35, Issue 8
25 Feb 2015
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Anti-Muscarinic Adjunct Therapy Accelerates Functional Human Oligodendrocyte Repair
Kavitha Abiraman, Suyog U. Pol, Melanie A. O'Bara, Guang-Di Chen, Zainab M. Khaku, Jing Wang, David Thorn, Bansi H. Vedia, Ezinne C. Ekwegbalu, Jun-Xu Li, Richard J. Salvi, Fraser J. Sim
Journal of Neuroscience 25 February 2015, 35 (8) 3676-3688; DOI: 10.1523/JNEUROSCI.3510-14.2015

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Anti-Muscarinic Adjunct Therapy Accelerates Functional Human Oligodendrocyte Repair
Kavitha Abiraman, Suyog U. Pol, Melanie A. O'Bara, Guang-Di Chen, Zainab M. Khaku, Jing Wang, David Thorn, Bansi H. Vedia, Ezinne C. Ekwegbalu, Jun-Xu Li, Richard J. Salvi, Fraser J. Sim
Journal of Neuroscience 25 February 2015, 35 (8) 3676-3688; DOI: 10.1523/JNEUROSCI.3510-14.2015
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Keywords

  • glia
  • human
  • microarray
  • oligodendrocyte

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