Description
We introduced a novel concept of the functional role of CRP as a ‘pro-inflammatory agent'. This concept is based on our findings that pentameric (p)CRP can undergo a conformational change to monomeric (m)CRP, which is highly pro-inflammatory and pro-coagulant, and induces a localised inflammatory reaction that aggravates many diseases. We have shown that pCRP to mCRP dissociation occurs on the surface of ‘stressed cells', such as activated necrotic or apoptotic cells, and on microparticles (MPs) circulating in blood. For example, the surface of activated platelets causes a rapid dissociation of pCR to mCRP. We have also described mCRP formation induced by misfolded proteins, such as Alzheimer's plaques, as a clearance mechanism that can ‘overshoot' in pathological situations.
We are now developing inhibitors of CRP dissociation that can form the basis of a novel therapeutic approach for a range of inflammatory diseases including atherosclerotic plaque instability and autoimmune diseases.
Technologies/models to learn/apply: Drug design and development, medicinal chemistry, biotechnology, various animal models of inflammation, myocardial infarction, atherosclerosis, stroke, Alzheimer's disease.
Essential criteria:
Minimum entry requirements can be found here: https://www.monash.edu/admissions/entry-requirements/minimum
Keywords
Atherosclerosis, Atherothrombosis, Cardiovascular
Available options
PhD/Doctorate
Masters by research
Masters by coursework
Honours
Time commitment
Full-time
Top-up scholarship funding available
Yes
Year 1:
$6000
Physical location
Baker Heart & Diabetes Instititute, Prahran (Next to Alfred Hospital)
Research webpage
Co-supervisors
Dr
James McFadyen