News Release

When proteins get stuck at solid: unlocking the secrets to brain diseases

Nanoscale view of proteins opens window to treat neurodegenerative illness

Peer-Reviewed Publication

University of Sydney

Nanoscale 3D scan of protein condensate

video: 3D confocal microscopy scan of a FUS protein condensate incubated for 24 hours showing the characteristic core-shell structure unveiled by this research. view more 

Credit: The University of Sydney

Many diseases affecting the brain and nervous system are linked to the formation of protein aggregates, or solid condensates, in cells from their liquid form condensate, but little is known about this process.

This liquid-to-solid transition can trigger the formation of what are called amyloid fibrils. These can further form plaques in neurons causing neurodegenerative diseases such as Alzheimer's.

Biomedical engineers at the University of Sydney, in collaboration with scientists at the University of Cambridge and Harvard University, have now developed sophisticated optical techniques to monitor at close range the process by which these protein aggregates form.

By testing a protein associated with Amyotrophic Lateral Sclerosis – ALS disease, which affected astrophysicist Professor Stephen Hawking – the Sydney engineers closely monitored the transition of this protein from its liquid to solid phase.

“This is a huge step forward to understanding how neurogenerative diseases develop from a fundamental perspective,” said Dr Yi Shen, lead author of the research published in the Proceedings of the National Academy of Sciences (PNAS) in the United States.

“We can now directly observe the transition of these critical proteins from liquid to solid at the nanoscale – a millionth of a metre in scale,” said Dr Daniele Vigolo, a senior lecturer in the School of Biomedical Engineering and a member of the University of Sydney Nano Institute.

Proteins regularly form condensates during liquid-to-liquid phase separation in a wide range of critical and healthy biological functions, such as the formation of human embryos. This process assists biochemical reactions where protein concentrations are critical and also promotes healthy protein–protein interactions.

“However, this process also increases the risk of dysfunctional aggregation, where unhealthy aggregates of solid proteins form in human cells,” said Dr Shen, who is an ARC DECRA Fellow in the School of Chemical and Biomolecular Engineering and also a member of Sydney Nano.

“This can lead to aberrant structures associated with neurodegenerative diseases because the proteins no longer exhibit rapid reversibility back to liquid form. It is therefore crucial to monitor condensate dynamics, as they directly affect pathological states,” she said.

The world-first nanoscale optical observation of this process has allowed the team to determine that the transition from liquid to solid protein starts at the interface of the protein condensates. This window onto the phase transition also revealed that the internal structures of these protein agglomerates are heterogenous, where previously they were thought to be homogeneous.

Dr Vigolo said: “Our findings promise to greatly improve our understanding of neurogenerative diseases from a fundamental perspective.

“This means a promising new area of research to better understand how Alzheimer’s disease and ALS develops in the brain, affecting millions of people worldwide.”

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DOWNLOAD photos and a short video of the condensate process at this link.

YouTube: short clip of condensate interaction at this link.

INTERVIEWS

Dr Daniele Vigolo                                          Dr Yi Shen

School of Biomedical Engineering                 School of Chemical and Biomolecular Engineering

Faculty of Engineering                                    Faculty of Engineering

The University of Sydney                               The University of Sydney

daniele.vigolo@sydney.edu.au                      yi.shen@sydney.edu.au

 

MEDIA ENQUIRIES

Marcus Strom | +61 423 982 485 | marcus.strom@sydney.edu.au

DECLARATION

The authors declare no competing interests.

This work is supported by the Newman Foundation, the Wellcome Trust, ERC, US Alzheimer Association Zenith, ALS Canada–Brain Canada, Canadian Institutes of Health Research and the Cambridge Centre for Misfolding Diseases. Canadian Institutes of Health Research, Alzheimer Society of Ontario Chair in Alzheimer’s Disease Research; US National Institute of Aging. Researchers acknowledge the Cambridge Advanced Imaging Centre and K.H. Muller for help with flash-freezing and SEM imaging.


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