Description
Mitochondria are critical to cellular function, producing cellular bioenergy, but they also have important roles in ion homeostasis, programmed cell death, and in ROS production and consumption. Protein interactions within the mitochondrial membrane are critical to maintaining homeostasis and regulation of cellular functions. Mitochondrial protein overexpression, de-modification and disruption or upregulation of key interactions leads to mitochondrial dysfunction and human disease such as cancer, diabetes, and a host of neurological disorders. Unfortunately, many mitochondrial protein interactions that lead to dysregulation and disease and not understood. Leveraging our recent mitochondrial import findings and our established endogenous protein tagging and in vivo tracking technology, this project aims to decipher key mitochondrial interactions using protein tagging and proteomics, in the goal to further human disease research and identify new potential drug targets.
Essential criteria:
Minimum entry requirements can be found here: https://www.monash.edu/admissions/entry-requirements/minimum
Keywords
Mitochondria, Biogenesis, Protein Biochemistry, Proteomics, CRISPR, Mass spectrometry,
School
School of Clinical Sciences at Monash Health / Hudson Institute of Medical Research
Available options
PhD/Doctorate
Masters by research
BMedSc(Hons)
Time commitment
Full-time
Top-up scholarship funding available
No
Physical location
Monash Medical Centre Clayton