WASHINGTON — A recent study by the North Carolina State University researchers showed how a single mechanism can trigger different behaviors from the same gene — and has applications in the biotechnology sector.
The findings of the study were published in the journal “Cell Systems.”
“The fundamental idea here is that you can encode information in the dynamics of a signal that a gene is receiving,” said Albert Keung, corresponding author of a paper and an assistant professor of chemical and biomolecular engineering at NC State.
“So, rather than a signal simply being present or absent, the way in which the signal is being presented matters.”
For this study, researchers modified a yeast cell so that it has a gene that produces fluorescent proteins when the cell is exposed to blue light.
“Systematically exploring information transmission at the promoter level and how >100 chromatin regulators can reshape this transmission. Beautifully executed Albert Keungand co!” tweeted Lucasz Bugaj, Assistant Professor, Penn Bioengineering
A region of the gene called the promoter is responsible for controlling the gene’s activity.
In the modified yeast cells, a specific protein binds to the promoter region of the gene.
When researchers shine blue light on that protein, it becomes receptive to a second protein. When the second protein binds to the first protein, the gene becomes active.
And that’s easy to detect since the activated gene produces proteins that glow in the dark.
The researchers then exposed these yeast cells to 119 different light patterns.
Each light pattern differed in terms of the intensity of the light, how long each pulse of light was, and how frequently the pulses occurred.
The researchers then mapped out the amount of fluorescent protein that the cells produced in response to each light pattern.
People talk about genes being turned on or off, but it’s less like a light switch and more like a dimmer switch — a gene can be activated a little, a lot, or anywhere in between.
If a given light pattern led to the production of a lot of fluorescent protein, that means the light pattern made the gene very active.
If the light pattern led to the production of just a little fluorescent protein, that means the pattern only triggered mild activity of the gene.
“We found that different light patterns can produce very different outcomes in terms of gene activity,” said Jessica Lee, first author of the paper and a recent Ph.D. graduate from NC State.
“The big surprise, to us, was that the output was not directly correlated to the input. Our expectation was that the stronger the signal, the more active the gene would be. But that wasn’t necessarily the case. One light pattern might make the gene significantly more active than another light pattern, even if both patterns were exposing the gene to the same amount of light.”
The researchers found that all three light pattern variables — the intensity of the light, frequency of the light pulses, and how long each pulse lasted — could influence gene activity but found that controlling the frequency of light pulses gave them the most precise control over gene activity.
“We also used the experimental data here to develop a computational model that helped us better understand why different patterns produce different levels of gene activity,” said Leandra Caywood, co-author of the paper and a Ph.D. student at NC State.
“For example, we found that when you bunch rapid pulses of light very closely together, you get more gene activity than you would expect from the amount of light being applied.”
“Using the model, we were able to determine that this is happening because the proteins can’t separate and come back together quickly enough to respond to every pulse,” Caywood said.
“Basically, the proteins don’t have time to fully separate from each other between pulses, so are spending more time connected — meaning that the gene is spending more time activated. Understanding these sorts of dynamics is very useful for helping us figure out how to better control gene activity using these signals.”
“Our finding is relevant for cells that respond to light, such as those found in leaves. But it also tells us that genes are responsive to signal patterns, which could be delivered by mechanisms other than light.” Keung said.
In a separate set of experiments, the researchers found that genes were also able to filter out some signals. The mechanics of this are both straightforward and mysterious.
The researchers could tell that when a second protein was attached to the gene’s promoter region, some frequencies of light pulses did not trigger the production of fluorescent proteins.
In short, the researchers know the second protein ensures that a gene responds only to a specific suite of signals — but the researchers don’t know exactly how the second protein accomplishes that.
The researchers also found that they could control the number of distinct signals a gene could respond to by manipulating the number and type of proteins attached to the promoter region of the gene.
“One additional contribution of this work is that we’ve determined we can communicate about 1.71 bits worth of information through the promoter region of a gene with just one protein attachment,” Lee said.
“In practical terms, that means that the gene, without a complex network of protein attachments, is able to distinguish between more than three signals without error. Previous work had set that baseline at 1.55 bits, so this study advances our understanding of what’s possible here. It’s a foundation we can build on.”
The researchers said this work enables future studies that advance our understanding of cell behavior and gene expression dynamics.
In the nearer term, the researchers said there are practical applications for the work in the pharmaceutical and biotech sectors.
“In bio-manufacturing, you often want to manage both the growth of cells and the rate at which those cells are producing specific proteins,” Lee said.
“Our work here can help manufacturers fine-tune and control both of those variables.”
(With inputs from ANI)
Edited by Saptak Datta and Praveen Pramod Tewari
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