Literature DB >> 27699230

A cord blood monocyte-derived cell therapy product accelerates brain remyelination.

Arjun Saha1, Susan Buntz1, Paula Scotland1, Li Xu1, Pamela Noeldner1, Sachit Patel1, Amy Wollish1, Aruni Gunaratne1, Tracy Gentry1, Jesse Troy1, Glenn K Matsushima2, Joanne Kurtzberg1, Andrew E Balber1.   

Abstract

Microglia and monocytes play important roles in regulating brain remyelination. We developed DUOC-01, a cell therapy product intended for treatment of demyelinating diseases, from banked human umbilical cord blood (CB) mononuclear cells. Immunodepletion and selection studies demonstrated that DUOC-01 cells are derived from CB CD14+ monocytes. We compared the ability of freshly isolated CB CD14+ monocytes and DUOC-01 cells to accelerate remyelination of the brains of NOD/SCID/IL2Rγnull mice following cuprizone feeding-mediated demyelination. The corpus callosum of mice intracranially injected with DUOC-01 showed enhanced myelination, a higher proportion of fully myelinated axons, decreased gliosis and cellular infiltration, and more proliferating oligodendrocyte lineage cells than those of mice receiving excipient. Uncultured CB CD14+ monocytes also accelerated remyelination, but to a significantly lesser extent than DUOC-01 cells. Microarray analysis, quantitative PCR studies, Western blotting, and flow cytometry demonstrated that expression of factors that promote remyelination including PDGF-AA, stem cell factor, IGF1, MMP9, MMP12, and triggering receptor expressed on myeloid cells 2 were upregulated in DUOC-01 compared to CB CD14+ monocytes. Collectively, our results show that DUOC-01 accelerates brain remyelination by multiple mechanisms and could be beneficial in treating demyelinating conditions.

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Year:  2016        PMID: 27699230      PMCID: PMC5033827          DOI: 10.1172/jci.insight.86667

Source DB:  PubMed          Journal:  JCI Insight        ISSN: 2379-3708


  75 in total

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4.  Preclinical characterization of DUOC-01, a cell therapy product derived from banked umbilical cord blood for use as an adjuvant to umbilical cord blood transplantation for treatment of inherited metabolic diseases.

Authors:  Joanne Kurtzberg; Susan Buntz; Tracy Gentry; Pamela Noeldner; April Ozamiz; Benjamin Rusche; Robert W Storms; Amy Wollish; David A Wenger; Andrew E Balber
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7.  Abbreviated exposure to cuprizone is sufficient to induce demyelination and oligodendrocyte loss.

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Journal:  J Neurosci Res       Date:  2012-12-26       Impact factor: 4.164

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Review 9.  Cuprizone-induced demyelination as a tool to study remyelination and axonal protection.

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10.  Astrogliosis during acute and chronic cuprizone demyelination and implications for remyelination.

Authors:  Norah Hibbits; Jun Yoshino; Tuan Q Le; Regina C Armstrong
Journal:  ASN Neuro       Date:  2012-10-30       Impact factor: 4.146

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8.  High Integrity and Fidelity of Long-Term Cryopreserved Umbilical Cord Blood for Transplantation.

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