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The Journal of Neuroscience, March 15, 2000, 20(6):2218-2228
Proliferation and Differentiation of Progenitor Cells Throughout
the Intact Adult Rat Spinal Cord
Philip J.
Horner1,
Ann
E.
Power2,
Gerd
Kempermann1, 3,
H. Georg
Kuhn3,
Theo D.
Palmer1,
Jürgen
Winkler2, 3,
Leon
J.
Thal2, and
Fred H.
Gage1
1 The Salk Institute for Biological Studies, Laboratory
of Genetics, La Jolla, California 92037, 2 Department of
Neurosciences, University of California, San Diego, California
92093-0608, and 3 Department of Neurology, University of
Regensburg, 93053 Regensburg, Germany
The existence of multipotent progenitor populations in the adult
forebrain has been widely studied. To extend this knowledge to the
adult spinal cord we have examined the proliferation, distribution, and
phenotypic fate of dividing cells in the adult rat spinal cord.
Bromodeoxyuridine (BrdU) was used to label dividing cells in 13- to
14-week-old, intact Fischer rats. Single daily injections of BrdU were
administered over a 12 d period. Animals were killed either
1 d or 4 weeks after the last injection of BrdU. We observed frequent cell division throughout the adult rodent spinal cord, particularly in white matter tracts (5-7% of all nuclei). The majority of BrdU-labeled cells colocalized with markers of immature glial cells. At 4 weeks, 10% of dividing cells expressed mature astrocyte and oligodendroglial markers. These data predict that 0.75%
of all astrocytes and 0.82% of all oligodendrocytes are derived from a
dividing population over a 4 week period. To determine the migratory
nature of dividing cells, a single BrdU injection was given to animals
that were killed 1 hr after the injection. In these tissues, the
distribution and incidence of BrdU labeling matched those of the 4 week
post injection (pi) groups, suggesting that proliferating cells divide
in situ rather than migrate from the ependymal zone.
These data suggest a higher level of cellular plasticity for the intact
spinal cord than has previously been observed and that glial
progenitors exist in the outer circumference of the spinal cord that
can give rise to both astrocytes and oligodendrocytes.
Key words:
spinal cord; progenitor; proliferation; rat; neurogenesis; stem cell; adult; gliogenesis
Copyright © 2000 Society for Neuroscience 0270-6474/00/2062218-11$05.00/0
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