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The engineered counters may be used to monitor toxins in the environment or keep track of the number of times a cell divides. The system can even be programmed to destroy the cell that holds it after a certain number of events.
“This is the first example of a synthetic counter in the field,” says Christina Smolke, a bioengineer at Stanford University and the author of a commentary published in the same issue of Science. Although these new counters are simple, “the first step is building the framework. The next step is, how do we start tailoring these to respond to something relevant? There are a lot of places to take this.”
The new research adds a tool to the burgeoning field of synthetic biology, in which scientists engineer biological systems such as DNA to create new capabilities. DNA molecules are designed to direct certain activities in a cell, and so can respond to specific signals and start and terminate protein production. Since the field emerged in the late 1970s, scientists have been creating artificial cellular “parts” that could be used to modify a living organism or even build a synthetic simple one from scratch. Assembling the right parts in the right order could, for example, allow engineered bacteria to produce biofuels or eat toxins in polluted areas in the environment.
A strong motivator for developing a system that can count, says study coauthor James Collins, was worry over the presence of genetically modified organisms in the environment.
“This came from growing concern that programmed cells could pose a danger to the environment or human bodies. You’d be worried about how long these things were going to stick around,” says Collins, of Boston University. Organisms endowed with counting abilities could be programmed to commit suicide after a certain number of cell divisions or day-and-night cycles, he says. This built-in kill switch may offer a greater level of control over the spread of introduced genes into wild organisms.
These counters rely on the novel assembly of simpler genetic tools. Collins and his team created “multiple numbers of switches cascaded behind one another to create more complex circuits,” says Kaustubh Bhalerao, a biological engineer at the University of Illinois at Urbana-Champaign.
Collins and his colleagues built two systems that count in different ways but are both based on the same basic idea. “Each of the counters is what you call daisy chain cascades: You have to do the first event before you do the next event,” Collins says. This is what endows the systems with the counting ability.
One of the team’s systems counts by starting and stopping the production of certain proteins. In the experiments, the first bit of a strip of modified DNA acts as a detector. When it detects a pulse of the sugar arabinose, it responds by triggering the production of a specific protein. When the DNA detects a second pulse of the sugar, the first protein helps produce a second protein. After a final pulse of the sugar, the second protein helps make green fluorescent protein as an output. When the cells glow green under ultraviolet light, the researchers know that the cells have counted exactly three pulses of sugar. The team could easily make the counting region of the modified DNA longer, allowing for higher counting.
The second counting system relies on enzymes that chop out and invert specific pieces of DNA. When the DNA strip detects the first signal, it causes one of these enzymes to be made. The enzyme then chops its own DNA sequence out of the modified strand of DNA, flips it and reinserts it backward, rendering it unreadable and useless. A second signal leads to the production of another enzyme, which chops another bit of DNA further along on the strand. At the end of the process, an output protein is produced.
The second system can be programmed to respond to different signals at each step of the process. By putting outputs between counts, researchers could track exactly when each step in a series happens.
The first system is better for counting relatively quick events, those that happen every 30 minutes or so. The second system is more useful for counting longer events that unfold over days, because the enzymes need more time to do their cutting and flipping.
Tinkering with the detector and the output, and leaving the basic process intact, may make for innumerable functions, Bhalerao says. Already, some bacteria have DNA that respond to light, arsenic, temperature, nutrients and some metals. In the new counting system, swapping out the signal, such as sugar, to be detected is trivial, says Bhalerao. “It’s like switching brands of mouse on your computer” but leaving the processor alone.
At the other end of the process, the proteins produced after counting can accomplish a wide variety of functions, Collins says. Proteins could “explode the cell, make the cell long, short, fat.” Researchers could even tailor the artificial network to produce different signals — like fluorescent proteins — at different counts. Cells could glow yellow after the first event, red after the second, green after the third and so on. This would allow researchers to monitor every step of complex processes, such as the development and growth of a cell.
The mix-and-match capabilities offer many possibilities, Bhalerao says, but “there is still a long way to go. These things don’t work all the time, and that’s because you’re making the cells do things they don’t want to do.”
Found in: Genes & Cells
- Friedland, A.E., et al. In press. Synthetic gene networks that count. Science. Doi:10.1126/science.1172005
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Recapitulation of some earlier notes on the
Scientific Comprehension Of The Origin, Drive, Nature And Purpose Of Life
A. Uniqueness Of science among human artifacts
ALL aspects of our culture are, of course, anthropoartifacts, including science. Yet among those artifacts science has a distinct uniqueness for us.
During the recent several centuries in the course of human history humans have been developing science at an accelerating rate as a provider of convincing, ever closer approaching, approximate models of the real world.
B. Origin and nature of life
Astronomically there are two "physics", a "classical physics" system of and between galactic clusters, and a "quantum physics" system WITHIN the galactic clusters.
The onset of big-bang's inflation started gravity, followed by formation of galactic clusters that behave as Newtonian bodies while continuously reconverting their shares of pre-inflation masses back to energy, and of endless intertwined evolutions WITHIN the clusters in attempts to resist this reconversion.
As mass is just another face of energy it is commonsensible to regard not only life, but mass in general, as a format of temporarily constrained energy.
It therefore ensues that whereas the in-space expanding cosmic constructs, the galaxies clusters, are - overall - continuously converting their original pre-inflation mass back to energy, the overall evolution WITHIN them, within the clusters, is in the opposite direction, temporarily constrained energy packages such as black holes and biospheres and other energy-storing mass-formats are precariuosly forming and "doing best" to survive as long as "possible"...
C. The drive and nature of Earth life
Earth life Genesis, formation of the first genes, was a phenomenon of serendipitous occurrence, in a supportive environment, of 'favourably-coursed' energy potential between in-coming sun's radiation and polymerizing-precipitating RNA-related oligomeric configuration.
The drive of Earth life and of its evolution is to enhance the functionality and survivability of Earth's genes, in order to maintain and enhance Earth-biosphere's temporary constrained energy storage and to maintain the biosphere BIO as long as possible.
It is the genes, life's prime strata organisms, that evolve, and the evolution of genomes, the 2nd stratum of life, and of the 3rd life stratum cellular organisms, is an interenhancing consequence of their genes' evolution.
D. The formation of Earth life
Earth Life: 1. a format of temporarily constrained energy, retained in temporary constrained genetic energy packages in forms of genes, genomes and organisms 2. a real virtual affair that pops in and out of existence in its matrix, which is the energy constrained in Earth's biosphere.
Earth organism: a temporary self-replicable constrained-energy genetic system that supports and maintains Earth's biosphere by proliferating and maintenance of genes.
Gene: the primal Earth's organism. (1st stratum organism)
Genome: a multigenes organism consisting of a cooperative commune of its member genes. (2nd stratum organism)
Cellular organisms: mono- or multi-celled Earth organisms. (3rd stratum organism)
E. Update of underlying life sciences conception is thus feasible
- First were independent individual genes, Earth's primal organisms.
- Genes aggregated cooperatively into genomes, multigenes organisms, with genomes' organs.
- Simultaneously or consequently genomes evolved protective-functional membranes, organs.
- Then followed cellular organisms, with a variety of outer-cell membrane shapes and
functionalities.
This conception is a scientific, NOT TECHNICAL, life-science innovation.
It is tomorrow's comprehension of life and of its evolution.
IT IS FRAUGHT WITH INTRIGUING DARWINIAN EVOLUTION IMPLICATIONS.
IT IS FRAUGHT WITH INTRIGUING TECHNOLOGICAL DEVELOPMENTS POTENTIALS.
F. The purpose of OUR, human, life
The purpose of OUR life and of its promotion is ours to formulate and set. It derives solely from our cognition.
Suggesting,
Dov Henis
(Comments from 22nd century)
http://blog.360.yahoo.com/blog-P81pQcU1dLBbHgtjQjxG_Q--?cq=1
On Energy, Mass, Gravity, Galaxies Clusters, AND Life
A Commonsensible Recapitulation
http://www.the-scientist.com/community/posts/list/184.page#2125
EVOLUTION Beyond Darwin 200
http://www.physforum.com/index.php?showtopic=14988&st=405entry396201
http://www.the-scientist.com/community/posts/list/100/122.page#1407
http://www.amazon.com/gp/product/1424337445
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