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How protein misfolding may kickstart chemical evolution

February 27, 2017
Emory Health Sciences
Researchers have demonstrated a connection between abnormal protein folding and the potential to kickstart chemical evolution.

Alzheimer's disease, and other neurodegenerative conditions involving abnormal folding of proteins, may help explain the emergence of life -- and how to create it.

Researchers at Emory University and Georgia Tech demonstrated this connection in two new papers published by Nature Chemistry: "Design of multi-phase dynamic chemical networks" and "Catalytic diversity in self-propagating peptide assemblies."

"In the first paper we showed that you can create tension between a chemical and physical system to give rise to more complex systems. And in the second paper, we showed that these complex systems can have remarkable and unexpected functions," says David Lynn, a systems chemist in Emory's Department of Chemistry who led the research. "The work was inspired by our current understanding of Darwinian selection of protein misfolding in neurodegenerative diseases."

The Lynn lab is exploring ways to potentially control and direct the processes of these proteins -- known as prions -- adding to knowledge that might one day help to prevent disease, as well as open new realms of synthetic biology. For the current papers, Emory collaborated with the research group of Martha Grover, a professor in the Georgia Tech School of Chemical & Biomolecular Engineering, to develop molecular models for the processes.

"Modeling requires us to formulate our hypotheses in the language of mathematics, and then we use the models to design further experiments to test the hypotheses," Grover says.

Darwin's theory of evolution by natural selection is well-established -- organisms adapt over time in response to environmental changes. But theories about how life emerges -- the movement through a pre-Darwinian world to the Darwinian threshold -- remain murkier.

The researchers started with single peptides and engineered in the capacity to spontaneously form small proteins, or short polymers. "These protein polymers can fold into a seemingly endless array of forms, and sometimes behave like origami," Lynn explains. "They can stack into assemblies that carry new functions, like prions that move from cell-to-cell, causing disease."

This protein misfolding provided the model for how physical changes could carry information with function, a critical component for evolution. To try to kickstart that evolution, the researchers engineered a chemical system of peptides and coupled it to the physical system of protein misfolding. The combination results in a system that generates step-by-step, progressive changes, through self-driven environmental changes.

"The folding events, or phase changes, drive the chemistry and the chemistry drives the replication of the protein molecules," Lynn says. "The simple system we designed requires only the initial intervention from us to achieve progressive growth in molecular order. The challenge now becomes the discovery of positive feedback mechanisms that allow the system to continue to grow."

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Journal References:

  1. Chenrui Chen, Junjun Tan, Ming-Chien Hsieh, Ting Pan, Jay T. Goodwin, Anil K. Mehta, Martha A. Grover & David G. Lynn. Design of multi-phase dynamic chemical networks. Nature Chemistry, February 2017 DOI: 10.1038/nchem.2737
  2. Tolulope O. Omosun, Ming-Chien Hsieh, W. Seth Childers, Dibyendu Das, Anil K. Mehta, Neil R. Anthony, Ting Pan, Martha A. Grover, Keith M. Berland & David G. Lynn. Catalytic diversity in self-propagating peptide assemblies. Nature Chemistry, February 2017 DOI: 10.1038/nchem.2738

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Emory Health Sciences. "How protein misfolding may kickstart chemical evolution." ScienceDaily. ScienceDaily, 27 February 2017. <>.
Emory Health Sciences. (2017, February 27). How protein misfolding may kickstart chemical evolution. ScienceDaily. Retrieved May 27, 2017 from
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