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Journal of Virology, August 1999, p. 6319-6326, Vol. 73, No. 8
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Attenuated, Replication-Competent Herpes Simplex Virus Type 1 Mutant G207: Safety Evaluation of Intracerebral Injection in
Nonhuman Primates
William D.
Hunter,1,
Robert L.
Martuza,1
Frank
Feigenbaum,1
Tomoki
Todo,1
Toshihiro
Mineta,1,
Takahito
Yazaki,1,§
Masahiro
Toda,1,
Joseph T.
Newsome,3
R. Craig
Platenberg,4
Herbert J.
Manz,5 and
Samuel D.
Rabkin1,2,*
Departments of
Neurosurgery,1 Microbiology and
Immunology,2
Radiology,4 and
Pathology5 and Division of
Comparative Medicine,3 Georgetown University
Medical Center, Washington, D.C. 20007
Received 12 February 1999/Accepted 16 April 1999
This study examined the safety of intracerebral inoculation of
G207, an attenuated, replication-competent herpes simplex virus type 1 (HSV-1) recombinant, in nonhuman primates. Sixteen New World owl
monkeys (Aotus nancymae [karyotype 1, formerly believed to
be A. trivirgatus]), known for their exquisite
susceptibility to HSV-1 infection, were evaluated. Thirteen underwent
intracerebral inoculation with G207 at doses of 107 or
109 PFU, two were vehicle inoculated, and one served as an
infected wild-type control and received 103 PFU of HSV-1
strain F. HSV-1 strain F caused rapid mortality and symptoms consistent
with HSV encephalitis, including fever, hemiparesis, meningitis, and
hemorrhage in the basal ganglia. One year after G207 inoculation, seven
of the animals were alive and exhibited no evidence of clinical
complications. Three deaths resulted from nonneurologic causes
unrelated to HSV infection, and three animals were sacrificed for
histopathologic examination. Two animals were reinoculated with G207
(107 PFU) at the same stereotactic coordinates 1 year after
the initial G207 inoculation. These animals were alive and healthy 2 years after the second inoculation. Cerebral magnetic resonance imaging studies performed both before and after G207 inoculation failed to
reveal radiographic evidence of HSV-related sequelae. Despite the lack
of outwardly observable HSV pathology, measurable increases in serum
anti-HSV titers were detected. Histopathological examination of
multiple organ tissues found no evidence of HSV-induced histopathology or dissemination. We conclude that intracerebral inoculation of up to
109 PFU of G207, well above the efficacious dose in mouse
tumor studies, is safe and therefore appropriate for human clinical trials.
*
Corresponding author. Mailing address: Department of
Neurosurgery, Georgetown University Medical Center, 3970 Reservoir Rd. NW, Washington, DC 20007. Phone: (202) 687-8047. Fax: (202) 687-3046. E-mail: rabkins{at}odrge.odr.georgetown.edu.

Present address: Department of Neurosurgery, University of
Wisconsin, Madison, WI
53792.

Present address: Department of Neurosurgery, Saga Medical School,
Saga 849,
Japan.
§
Present address: Department of Physiology, Keio University School
of Medicine, Shinjuku-ku, Tokyo 160,
Japan.

Present address: Division of Cellular Signaling, Institute for
Advanced Medical Research, Keio University School of Medicine,
Shinjuku-ku, Tokyo 160,
Japan.
Journal of Virology, August 1999, p. 6319-6326, Vol. 73, No. 8
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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