Project Details
Abstract
Neuroinflammation is a hallmark of all major CNS neurodegenerative disorders such as Alzheimer's
disease (AD) and Parkinson’s disease (PD). There is strong evidence that oxidative stresses are considered to
play an important role in the induction of inflammatory proteins implicated in brain inflammatory processes.
In our previous studies, we have demonstrated the involvement of redox signals (ROS production) in the
development of neuroinflammation and neuronal death. Many of the well-known inflammatory target
proteins, such as MMP-9, COX-2, and cPLA2, can be up-regulated by various proinflammatory factors,
including IL-1, BK, thrombin, LPS, LTA or viral infection, via a ROS signal-dependent manner in
neuroglial cells. The induction of these proteins might be mediated through NADPH oxidase/ROS, various
intracellular signaling pathways, and transcription factors in these cells. Given the important role of oxidative
stress in neurodegeneration, therapeutic strategies which are directed at early interventions targeted at
oxidative stress may be effective in delaying the development of neurodegeneration. Despite the intensive
investigations, there is no effectively therapeutic strategy available to prevent the progression of
neurodegeneration. Therefore, development of anti-oxidative and anti-inflammatory effects of drugs may be
beneficial to block the pathological progression of these diseases. Although statins and peroxisome
proliferation-activated receptors (PPARs) agonists are widely used in clinics, recent studies suggest that these
drugs could modulate neurodegeneration-related signaling processes and may be beneficial for
neuroinflammation. Therefore, this project will continue to approach which simultaneously induces various
host defense mechanisms against oxidative injury may be more effective in combating neurodegeneration.
Moreover, heme oxygenase (HO)-1 is the inducible isoform of the first and rate-limiting enzyme of heme
degradation. Induction of HO-1 has been shown to protect against the cytotoxicity of oxidative stress and
apoptotic cell death. Therefore, there is an excellent rationale for the development of neuroprotective drugs
based on the induction of HO-1 expression. Statins and PPAR agonists have attracted considerable attention
in treating various neurodegenerative diseases. They could attenuate the proinflammatory signalings such as
cytokine and oxygen radical formation, mediated through the induction of antioxidant defense protein HO-1
in various cell types. Despite the intense level of interest, there is a deficiency in information on how statins
and PPAR agonists exert neuroprotective effects in the brain diseases. Therefore, the purpose of this
proposal will dissect the molecular mechanisms and signaling pathways that are involved in HO-1 gene
expression induced by statins, PPAR agonists, CoPPIX, and CORM-2. In particular, we make an
attempt to approach how redox-dependently transcriptional activators such as NF-E2 related factor 2
(Nrf2), Sp1, and AP-1 control the inducible HO-1 gene expression. The role of central pro- and
anti-inflammatory cellular signaling cascades including Rho/ROCK, NADPH oxidase/ROS, MAPKs,
transactivation of growth factor receptors and PI3K/Akt in HO-1 regulation is engaged. Finally,
up-regulation of HO-1 protected against pro-inflammatory mediator-induced expression of inflammatory
proteins will be investigated in brain cells and animal model. These results will provide new insights into the
mechanisms of HO-1 expression, supporting the hypothesis that HO-1/CO may contribute to protect against
oxidative stress-mediated brain inflammation. Although the protective function by HO-1 has been
investigated in various cell types, the regulatory roles of major transcription factors (TFs) and signaling
pathways that govern the inducible HO-1 gene expression induced by various chemicals and drugs are not
completely understood in astrocytes and neurons. Our proposal is to connect what is known and the gaps
in our knowledge on the mechanisms underlying statins, PPAR agonists, CoPPIX, and CORM-2 exert
their potentials in the induction of anti-oxidant enzymes such as HO-1 and anti-inflammatory effects
which may be beneficial for treatment of neurodegenerative diseases. Understanding the molecular
mechanisms of these chemicals induced expression of HO-1 in the brain would provide insight into specific
drug targets and also provide the rationale for development of novel drugs for the treatment of
neurodegenerative diseases.
Project IDs
Project ID:PC10507-1229
External Project ID:MOST105-2320-B182-005-MY3
External Project ID:MOST105-2320-B182-005-MY3
Status | Finished |
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Effective start/end date | 01/08/16 → 31/07/17 |
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