Description
Chronic infectious diseases have a devastating effect on global health. HIV and Plasmodium falciparum both cause chronic disease and have evaded effective vaccine design. Production and function of memory is altered in chronic infectious diseases, with recent work segregating memory B cells generated in chronic infection into classical memory and ‘atypical' memory B cell populations. However, the role of the latter is unclear, and whether atypical memory has a positive or negative impact on classical memory responses is controversial. It is clear that revealing the origin and function of these cells, and how their formation is regulated at the molecular level, will be important for development of new antibody-based vaccines for these diseases. This project will use multiomic single-cell sequencing to investigate the requirements for formation and regulation of atypical memory B cells.
See Pupovac and Good-Jacobson Current Opinion in Immunology 2017 for a recent review of this field.
Essential criteria:
Minimum entry requirements can be found here: https://www.monash.edu/admissions/entry-requirements/minimum
Keywords
HIV, immunity, B cells, antibody, chronic infectious disease, department of biochemistry and molecular biology
School
Biomedicine Discovery Institute (School of Biomedical Sciences) » Biochemistry and Molecular Biology
Available options
PhD/Doctorate
Masters by research
Honours
Short projects
Time commitment
Full-time
Part-time
Top-up scholarship funding available
No
Physical location
Biomedicine Discovery Institute
Research webpage
Co-supervisors
Dr
TBD