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Publication
Modulating Molecular Chaperones Improves Mitochondrial Bioenergetics and
Decreases the Inflammatory Transcriptome in Diabetic Sensory Neurons.
Authors
Ma J, Pan P, Anyika M, Blagg BS, Dobrowsky RT
Submitted By
Rick Dobrowsky on 8/4/2015
Status
Published
Journal
ACS chemical neuroscience
Year
2015
Date Published
7/22/2015
Volume : Pages
Not Specified
:
Not Specified
PubMed Reference
26161583
Abstract
We have previously demonstrated that modulating molecular chaperones with KU-32,
a novobiocin derivative, ameliorates physiologic and bioenergetic deficits of
diabetic peripheral neuropathy (DPN). Replacing the coumarin core of KU-32 with
a meta-fluorinated biphenyl ring system created KU-596, a novobiocin analogue
(novologue) that showed neuroprotective activity in a cell-based assay. The
current study sought to determine whether KU-596 offers similar therapeutic
potential for treating DPN. Administration of 2-20 mg/kg of KU-596 improved
diabetes induced hypoalgesia and sensory neuron bioenergetic deficits in a
dose-dependent manner. However, the drug could not improve these neuropathic
deficits in diabetic heat shock protein 70 knockout (Hsp70 KO) mice. To gain
further insight into the mechanisms by which KU-596 improved DPN, we performed
transcriptomic analysis of sensory neuron RNA obtained from diabetic wild-type
and Hsp70 KO mice using RNA sequencing. Bioinformatic analysis of the
differentially expressed genes indicated that diabetes strongly increased
inflammatory pathways and that KU-596 therapy effectively reversed these
increases independent of Hsp70. In contrast, the effects of KU-596 on decreasing
the expression of genes regulating the production of reactive oxygen species
were more Hsp70-dependent. These data indicate that modulation of molecular
chaperones by novologue therapy offers an effective approach toward correcting
nerve dysfunction in DPN but that normalization of inflammatory pathways alone
by novologue therapy seems to be insufficient to reverse sensory deficits
associated with insensate DPN.
Investigators with authorship
Name
Institution
Rick Dobrowsky
University of Kansas Medical Center
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Please acknowledge all posters, manuscripts or scientific materials that were generated in part or whole using funds from the Diabetic Complications Consortium(DiaComp) using the following text:
Financial support for this work provided by the NIDDK Diabetic Complications Consortium (RRID:SCR_001415, www.diacomp.org), grants DK076169 and DK115255
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