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Kathryn J. Jones, Ph.D.
Professor
Department of Cell Biology, Neurobiology
and Anatomy
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B.S. and Certificate, Physical Therapy, 1975. University of
Wisconsin-Madison.
Ph.D., Neuroscience, 1983. Department of Anatomy, University of Illinois at
Chicago.
Postdoctoral Fellow, Neuroendocrinology, 1983-1986. Laboratories of Neurobiology
and Behavior, and Neuroendocrinology, The Rockefeller University.
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EMAIL |
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Current Interests |
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Gonadal steroid hormones as neurotherapeutics in PNS
and CNS injuries, translational studies of gonadal steroid use in facial
paralysis caused by acoustic neuromas, neuroimmunology and CD4+T-mediated
neuroprotection, ALS and motoneuron diseases |
Laboratory Focus |
- The overall goal of the research in our laboratory is to understand the basis for
successful neuronal regeneration in neurons capable of survival and full axonal regrowth
following injury and to extrapolate that information to enhance survival and regeneration
of neurons otherwise incapable of survival and/or axonal regrowth and injury.
We are currently investigating the use of steroids for the treatment of
facial nerve paralysis induced by intracranial tumors.
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- Toward that goal, we have a number of currently funded projects which are focused on
elucidating the cellular/molecular events associated with nerve regeneration. The
therapeutic role of gonadal steroids in enhancing peripheral nerve is being investigated.
Gonadal steroids are neurotrophic agents capable of affecting many neuronal properties
associated with successful regeneration. In the human neurological disorder, amyotrophic
lateral sclerosis, a steroid hormone receptor deficiency has been postulated to play an
etiological role in the development of that disease. Administration of testosterone at the
time of facial nerve injury in adult rodents accelerates functional recovery from facial
paralysis. These steroidal effects on nerve regeneration are steroid receptor-mediated and
appear to involve an augmentation of the intrinsic molecular program of regenerating
facial neurons. We are also exploring the ability of steroids to improve outcome from
spinal cord injury in rodent models. The long-term objective is to extend these studies to
the human. In collaboration with Dr. Virginia Sanders, we have recently
discovered a role for CD4+T cells in promoting motoneuron survival after
peripheral nerve injury and have advanced a model for how motoneurons
direct a pro-survival, anti-inflammatory injury response. The long term
goal of these studies is to extrapolate the results to ALS and other
motoneuron diseases.
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Publications |
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Huppenbauer, C.B., Tanzer, L., DonCarlos, L.L., and Jones, K.J. (2005)
Gonadal
steroid attenuation of developing hamster facial motoneuron loss by axotomy:
equal
efficacy of testosterone, dihydrotestosterone, and 17-beta estradiol, J.
Neurosci.,
25:4004-4013. |
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DeBoy, C.A., Byram, S.C., Serpe,
C.J., and Sanders, V.M, and Jones, K.J. (2006)
Immune-mediated
neuroprotection of axotomized mouse facial motoneurons is
dependent on the
IL-4/STAT6 signaling pathway in CD4+ T cells, Exp. Neurol.,.
201:2120224. |
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Tetzlaff, J.E., Huppenbauer, C.B.,
Tanzer, L., Alexander, T.D., and Jones, K.J.
(2006) Motoneuron injury and
repair: new perspectives on gonadal steroids as
neurotherapeutics. J.
Molec. Neurosci, 28: in press.
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Byram, S.C., Serpe,
C.J., DeBoy, C.A., Sanders, V.M. and Jones, K.J. (2006) The
neuroprotective
Th1/Th2 paradigm: a working model of motoneuron repair. Clin.
Neurosci.
Res., 6: 86-96. |
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