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Volume 17, Number 17,
Issue of September 1, 1997
pp. 6504-6511
Copyright ©1997 Society for Neuroscience
Targeted Transduction of CNS Neurons with Adenoviral Vectors
Carrying Neurotrophic Factor Genes Confers Neuroprotection That Exceeds
the Transduced Population
Received March 5, 1997; revised May 1, 1997; accepted June 10, 1997.
Brian J. Baumgartner1 and
H. David Shine1, 2, 3
1 Department of Neurosurgery, 2 Department
of Cell Biology, and 3 Division of Neuroscience, Baylor
College of Medicine, Houston, Texas 77030
Application of neurotrophic factors (NFs) to the cut stump of motor
nerves of neonatal rats confers neuroprotection from trauma-induced neuronal death. To test whether motoneurons are capable of responding to endogenously produced NFs, facial motoneurons were genetically modified in vivo to express several NFs and then tested
for their response to peripheral nerve damage. Replication-defective
adenoviral vectors [Adv.Rous sarcoma virus
(RSV)-nf] representing three families of NFs were
constructed that carried genes for brain-derived neurotrophic factor
(BDNF), ciliary neurotrophic factor (CNTF), glial cell-derived neurotrophic factor (GDNF), and nerve growth factor. Media from cultured cells transduced with Adv.RSV-nf contained NFs
that supported the survival of cultured chick sensory neurons in the
same manner as recombinant NF standards. When Adv.RSV-nf
or an adenoviral vector containing the -galactosidase gene
(Adv.RSV- -gal) were injected into the facial muscles of neonatal
rats the vectors were retrogradely transported to the facial nucleus
where the NFs or -gal were expressed. A fraction (~10%) of the
neurons were transduced as demonstrated by reverse transcriptase-PCR, histochemistry, and immunocytochemistry. In the case of Adv.RSV-BDNF, Adv.RSV-CNTF, and Adv.RSV-GDNF, a significant portion of the facial nucleus neurons was protected, 16.5, 18.2, and 53.3%, respectively, from death after axotomy, showing that neurons are capable of transporting the Adv.RSV-nf, expressing the recombinant
NF genes, and responding to the NFs. In the case of Adv.RSV-GDNF, a
greater number of facial nucleus motoneurons survived than were
transduced, indicating that neighboring untransduced neurons were
protected by the GDNF expressed by the transduced neurons by a
paracrine mechanism.
Key words:
neurotrophic factors;
neuroprotection;
adenoviral vector;
facial nerve;
facial nucleus;
nervous system trauma;
retrograde
transport
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