Grafts of EGF-responsive neural stem cells derived from GFAP-hNGF transgenic mice: Trophic and tropic effects in a rodent model of huntington's disease

Authors

Jeffrey H. Kordower, Rush University Medical Center
Er Yun Chen, Rush University Medical Center
Christian Winkler, Wallenberg Neuroscience Center
Rose Fricker, Wallenberg Neuroscience Center
Vinod Charles, Rush University Medical Center
Albee Messing, University of Wisconsin School of Veterinary Medicine
Elliott J. Mufson, Rush University Medical Center
Shou C. Wong, CytoTherapeutics, Inc.
Jeffrey M. Rosenstein, The George Washington University
Anders Björklund, Wallenberg Neuroscience Center
Dwaine F. Emerich, CytoTherapeutics, Inc.
Joseph Hammang, CytoTherapeutics, Inc.
Melissa K. Carpenter, CytoTherapeutics, Inc.

Document Type

Article

Abstract

The present study examined whether implants of epidermal growth factor (EGF)responsive stems cells derived from transgenic mice in which the glial fibrillary acid protein (GFAP) promoter directs the expression of human nerve growth factor (hNGF) could prevent the degeneration of striatal neurons in a rodent model of Huntington's disease (HD). Rats received intrastriatal transplants of GFAP-hNGF stem cells or control stem cells followed 9 days later by an intrastriatal injection of quinolinic acid (QA). Nissl stains revealed large striatal lesions in rats receiving control grafts, which, on average, encompassed 12.78 mm3. The size of the lesion was significantly reduced (1.92 mm3) in rats receiving lesions and GFAP-hNGF transplants. Rats receiving QA lesions and GFAP-hNGF-secreting grafts stem cell grafts displayed a sparing of striatal neurons immunoreactive (ir) for glutamic acid decarboxylase, choline acetyltransferase, and neurons histochemically positive for nicotinamide adenosine diphosphate. Intrastriatal GFAP-hNGF- secreting implants also induced a robust sprouting of cholinergic fibers from subjacent basal forebrain neurons. The lesioned striatum in control-grafted animals displayed numerous p75 neurotrophin-ir (p75(NTR)) astrocytes, which enveloped host vasculature. In rats receiving GFAP-hNGF-secreting stem cell grafts, the astroglial staining pattern was absent. By using a mouse-specific probe, stem cells were identified in all animals. These data indicate that cellular delivery of hNGF by genetic modification of stem cells can prevent the degeneration of vulnerable striatal neural populations, including those destined to die in a rodent model of HD, and supports the emerging concept that this technology may be a valuable therapeutic strategy for patients suffering from this disease.

Keywords

Choline acetyltransferase, GABA, Immunohistochemistry, NADPH- diaphorase, Striatum

Publication Date

10-13-1997

Publication Title

Journal of Comparative Neurology

ISSN

00219967

Volume

387

Issue

1

First Page

96

Last Page

113

PubMed ID

9331174

Digital Object Identifier (DOI)

10.1002/(SICI)1096-9861(19971013)387:1<96::AID-CNE8>3.0.CO;2-I

Recommended Citation

Kordower, Jeffrey H.; Chen, Er Yun; Winkler, Christian; Fricker, Rose; Charles, Vinod; Messing, Albee; Mufson, Elliott J.; Wong, Shou C.; Rosenstein, Jeffrey M.; Björklund, Anders; Emerich, Dwaine F.; Hammang, Joseph; and Carpenter, Melissa K., "Grafts of EGF-responsive neural stem cells derived from GFAP-hNGF transgenic mice: Trophic and tropic effects in a rodent model of huntington's disease" (1997). Translational Neuroscience. 1832.
https://scholar.barrowneuro.org/neurobiology/1832