Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse

Martha S. Windrem; Steven J. Schanz; Min Guo; Guo Feng Tian; Vaughn Washco; Nancy Stanwood; Matthew Rasband; Neeta S. Roy; Maiken Nedergaard; Leif A. Havton; Su Wang; Steven A. Goldman

doi:10.1016/j.stem.2008.03.020

Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse

Martha S. Windrem
, Steven J. Schanz
, Min Guo
, Guo Feng Tian
, Vaughn Washco
, Nancy Stanwood
, Matthew Rasband
, Neeta S. Roy
, Maiken Nedergaard
, Leif A. Havton
, Su Wang
, Steven A. Goldman

Research output: Contribution to journal › Article › peer-review

278 Scopus citations

Abstract

Congenitally hypomyelinated shiverer mice fail to generate compact myelin and die by 18-21 weeks of age. Using multifocal anterior and posterior fossa delivery of sorted fetal human glial progenitor cells into neonatal shiverer × rag2^-/- mice, we achieved whole neuraxis myelination of the engrafted hosts, which in a significant fraction of cases rescued this otherwise lethal phenotype. The transplanted mice exhibited greatly prolonged survival with progressive resolution of their neurological deficits. Substantial myelination in multiple regions was accompanied by the acquisition of normal nodes of Ranvier and transcallosal conduction velocities, ultrastructurally normal and complete myelination of most axons, and a restoration of a substantially normal neurological phenotype. Notably, the resultant mice were cerebral chimeras, with murine gray matter but a predominantly human white matter glial composition. These data demonstrate that the neonatal transplantation of human glial progenitor cells can effectively treat disorders of congenital and perinatal hypomyelination.

Original language	English
Pages (from-to)	553-565
Number of pages	13
Journal	Cell Stem Cell
Volume	2
Issue number	6
DOIs	https://doi.org/10.1016/j.stem.2008.03.020
State	Published - 5 Jun 2008
Externally published	Yes

Keywords

MOLNEURO
STEMCELL

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10.1016/j.stem.2008.03.020

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Windrem, M. S., Schanz, S. J., Guo, M., Tian, G. F., Washco, V., Stanwood, N., Rasband, M., Roy, N. S., Nedergaard, M., Havton, L. A., Wang, S., & Goldman, S. A. (2008). Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse. Cell Stem Cell, 2(6), 553-565. https://doi.org/10.1016/j.stem.2008.03.020

@article{a31ab6925444421894e58a1fb18258e5,

title = "Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse",

abstract = "Congenitally hypomyelinated shiverer mice fail to generate compact myelin and die by 18-21 weeks of age. Using multifocal anterior and posterior fossa delivery of sorted fetal human glial progenitor cells into neonatal shiverer × rag2-/- mice, we achieved whole neuraxis myelination of the engrafted hosts, which in a significant fraction of cases rescued this otherwise lethal phenotype. The transplanted mice exhibited greatly prolonged survival with progressive resolution of their neurological deficits. Substantial myelination in multiple regions was accompanied by the acquisition of normal nodes of Ranvier and transcallosal conduction velocities, ultrastructurally normal and complete myelination of most axons, and a restoration of a substantially normal neurological phenotype. Notably, the resultant mice were cerebral chimeras, with murine gray matter but a predominantly human white matter glial composition. These data demonstrate that the neonatal transplantation of human glial progenitor cells can effectively treat disorders of congenital and perinatal hypomyelination.",

keywords = "MOLNEURO, STEMCELL",

author = "Windrem, \{Martha S.\} and Schanz, \{Steven J.\} and Min Guo and Tian, \{Guo Feng\} and Vaughn Washco and Nancy Stanwood and Matthew Rasband and Roy, \{Neeta S.\} and Maiken Nedergaard and Havton, \{Leif A.\} and Su Wang and Goldman, \{Steven A.\}",

note = "Funding Information: This work was supported by the Miriam and Sheldon Adelson Medical Research Foundation, the G. Harold and Leila Y. Mathers Charitable Foundation, the CNS Foundation and Ataxia-Telangiectasia Children's Project, the National Multiple Sclerosis Society, and NINDS R01NS039559. We thank Devin Chandler-Militello for advice and assistance in cell preparation, and Carolyn Moyle for technical assistance. We are grateful to Brad Poulis of the Fetal Human Tissue Repository of the Albert Einstein College of Medicine for some of the fetal tissue samples used in this study. S.A.G. is a cofounder and shareholder in Q Therapeutics (Salt Lake City, UT), which has licensed relevant patents from the Cornell Research Foundation. ",

year = "2008",

month = jun,

day = "5",

doi = "10.1016/j.stem.2008.03.020",

language = "English",

volume = "2",

pages = "553--565",

journal = "Cell Stem Cell",

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publisher = "Cell Press",

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}

Windrem, MS, Schanz, SJ, Guo, M, Tian, GF, Washco, V, Stanwood, N, Rasband, M, Roy, NS, Nedergaard, M, Havton, LA, Wang, S & Goldman, SA 2008, 'Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse', Cell Stem Cell, vol. 2, no. 6, pp. 553-565. https://doi.org/10.1016/j.stem.2008.03.020

TY - JOUR

T1 - Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse

AU - Windrem, Martha S.

AU - Schanz, Steven J.

AU - Guo, Min

AU - Tian, Guo Feng

AU - Washco, Vaughn

AU - Stanwood, Nancy

AU - Rasband, Matthew

AU - Roy, Neeta S.

AU - Nedergaard, Maiken

AU - Havton, Leif A.

AU - Wang, Su

AU - Goldman, Steven A.

N1 - Funding Information: This work was supported by the Miriam and Sheldon Adelson Medical Research Foundation, the G. Harold and Leila Y. Mathers Charitable Foundation, the CNS Foundation and Ataxia-Telangiectasia Children's Project, the National Multiple Sclerosis Society, and NINDS R01NS039559. We thank Devin Chandler-Militello for advice and assistance in cell preparation, and Carolyn Moyle for technical assistance. We are grateful to Brad Poulis of the Fetal Human Tissue Repository of the Albert Einstein College of Medicine for some of the fetal tissue samples used in this study. S.A.G. is a cofounder and shareholder in Q Therapeutics (Salt Lake City, UT), which has licensed relevant patents from the Cornell Research Foundation.

PY - 2008/6/5

Y1 - 2008/6/5

N2 - Congenitally hypomyelinated shiverer mice fail to generate compact myelin and die by 18-21 weeks of age. Using multifocal anterior and posterior fossa delivery of sorted fetal human glial progenitor cells into neonatal shiverer × rag2-/- mice, we achieved whole neuraxis myelination of the engrafted hosts, which in a significant fraction of cases rescued this otherwise lethal phenotype. The transplanted mice exhibited greatly prolonged survival with progressive resolution of their neurological deficits. Substantial myelination in multiple regions was accompanied by the acquisition of normal nodes of Ranvier and transcallosal conduction velocities, ultrastructurally normal and complete myelination of most axons, and a restoration of a substantially normal neurological phenotype. Notably, the resultant mice were cerebral chimeras, with murine gray matter but a predominantly human white matter glial composition. These data demonstrate that the neonatal transplantation of human glial progenitor cells can effectively treat disorders of congenital and perinatal hypomyelination.

AB - Congenitally hypomyelinated shiverer mice fail to generate compact myelin and die by 18-21 weeks of age. Using multifocal anterior and posterior fossa delivery of sorted fetal human glial progenitor cells into neonatal shiverer × rag2-/- mice, we achieved whole neuraxis myelination of the engrafted hosts, which in a significant fraction of cases rescued this otherwise lethal phenotype. The transplanted mice exhibited greatly prolonged survival with progressive resolution of their neurological deficits. Substantial myelination in multiple regions was accompanied by the acquisition of normal nodes of Ranvier and transcallosal conduction velocities, ultrastructurally normal and complete myelination of most axons, and a restoration of a substantially normal neurological phenotype. Notably, the resultant mice were cerebral chimeras, with murine gray matter but a predominantly human white matter glial composition. These data demonstrate that the neonatal transplantation of human glial progenitor cells can effectively treat disorders of congenital and perinatal hypomyelination.

KW - MOLNEURO

KW - STEMCELL

UR - https://www.scopus.com/pages/publications/44349086935

U2 - 10.1016/j.stem.2008.03.020

DO - 10.1016/j.stem.2008.03.020

M3 - Article

C2 - 18522848

AN - SCOPUS:44349086935

SN - 1934-5909

VL - 2

SP - 553

EP - 565

JO - Cell Stem Cell

JF - Cell Stem Cell

IS - 6

ER -

Neonatal Chimerization with Human Glial Progenitor Cells Can Both Remyelinate and Rescue the Otherwise Lethally Hypomyelinated Shiverer Mouse

Abstract

Keywords

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