Bioretrosynthesis

Bioretrosynthesis is a technique for synthesizing organic chemicals from inexpensive precursors and evolved enzymes.^[1] The technique builds on the retro-evolution hypothesis proposed in 1945 by geneticist Norman Horowitz.^[2]

Technique

The technique works backwards from the target to identify a precursor molecule and an enzyme that converts it into the target, and then a second precursor that can produce the first and so on until a simple, inexpensive molecule becomes the beginning of the series.^[1] For each precursor, the enzyme is evolved using induced mutations and natural selection to produce a more productive version. The evolutionary process can be repeated over multiple generations until acceptable productivity is achieved.^[1] The process does not require high temperature, high pressure, the use of exotic catalysts or other elements that can increase costs.^[1] The enzyme "optimizations" that increase the production of one precursor from another are cumulative in that the same precursor productivity improvements can potentially be leveraged across multiple target molecules.^[1]

Didanosine

In 2014 the technique was used to produce the HIV drug didanosine:^[2] a simpler molecule was identified that can be converted into didanosine when subjected to a specific chemical transformation in the presence of a specific enzyme.^[2] The gene that creates the enzyme was then "copied", adding random mutations to each copy using ribokinase engineering.^[2] The mutant genes were inserted into Escherichia coli bacteria and used to produce (now-mutant) enzymes. The enzymes were then mixed with the precursor and the mutant enzymes that produced the greatest amount of didanosine were retained and replicated. One mutant stimulated a 50x increase in didanosine production.^[2] The first step was repeated, using the first precursor in place of didanosine, finding a yet simpler precursor and an enzyme to produce it. One mutated enzyme produced a 9,500x increase in nucleoside production.^[2] A third retrogression allowed them to start with the simple and inexpensive sugar named dideoxyribose and produce didanosine in a three-step sequence.^[2]

References

^ ^a ^b ^c ^d ^e "The bioretrosynthesis solution: shifting evolution into reverse to make cheaper drugs". KurzweilAI. 2014-04-09. doi:10.1038/nchembio.1494. Retrieved 2014-04-09.
Birmingham, W. R.; Starbird, C. A.; Panosian, T. D.; Nannemann, D. P.; Iverson, T. M.; Bachmann, B. O. (2014). "Bioretrosynthetic construction of a didanosine biosynthetic pathway". Nature Chemical Biology. 10: 392–399. doi:10.1038/nchembio.1494. PMC 4017637. PMID 24657930.
^ ^a ^b ^c ^d ^e ^f ^g "Shifting evolution into reverse promises cheaper, greener way to make new drugs". ScienceDaily. doi:10.1038/nchembio.1494. Retrieved 2014-04-09.

External links

"Bio-RetroSynthesis Team — Institute of Systems & Synthetic Biology". Issb.genopole.fr. Retrieved 2014-04-09.

[k1404-1] "The bioretrosynthesis solution: shifting evolution into reverse to make cheaper drugs". KurzweilAI. 2014-04-09. doi:10.1038/nchembio.1494. Retrieved 2014-04-09.
Birmingham, W. R.; Starbird, C. A.; Panosian, T. D.; Nannemann, D. P.; Iverson, T. M.; Bachmann, B. O. (2014). "Bioretrosynthetic construction of a didanosine biosynthetic pathway". Nature Chemical Biology. 10: 392–399. doi:10.1038/nchembio.1494. PMC 4017637. PMID 24657930.

[sci14-2] ^ ^a ^b ^c ^d ^e ^f ^g "Shifting evolution into reverse promises cheaper, greener way to make new drugs". ScienceDaily. doi:10.1038/nchembio.1494. Retrieved 2014-04-09.

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