It seems like every week thereās some amazing new development involving ālab on a chipā devices: in the May 9th issue of PNAS, Blazej et al. reported a nanoliter-scale microfabricated bioprocessor that was able to perform all three Sanger sequencing steps.
The device āāhttp://www.pnas.org/cgi/reprint/0602476103v1">incorporates a range of advanced lab-on-a-chip technologies, including miniaturized temperature sensing, nanoliter-scale Sanger extension reactions, microvalves/pumps, DNA affinity-capture, and high-performance CE." Like many other lab-on-a-chip devices, itās remarkably small (100 mm diameter) and the authors were able to sequence 556 continuous bases from 1 femtomole of a DNA template (with 99% accuracy).
Only 10e-15 moles of template? Thatās amazing! (And the raw sequencing data in Figure 4 looks fantasticā¦)
Since a āāhttp://www.pnas.org/cgi/reprint/0602476103v1">reaction containing 1 fmol of template generates [approximately] 26 times more product than is needed for detection,ā the authors believe that they could run the reaction with only 100 attomoles of the DNA template. If this was done, āa sequencing reaction performed at standard concentrations in an easily fabricated 25-nl reactor [would represent] a 400-fold reduction in current sequencing reagent consumption.ā
This is bound to make the NIH happy: āāhttp://www.genome.gov/15015208">it still costs about $10 million to sequence 3 billion base pairs" and āāhttp://www.genome.gov/15015208">NHGRIās near-term goal is to lower the cost of sequencing a mammalian-sized genome to $100,000, which would enable researchers to sequence the genomes of hundreds or even thousands of people as part of studies to identify genes that contribute to common, complex diseases." One of their long-term goals is to find a way to sequence a human-sized genome for $1,000 or less.
But the $1,000 genome would come with potential ethical concerns ā I donāt know about you, but I donāt think Iād want my genome sequencedā¦ I guess it would be good to know if I was genetically predisposed to get cancer or heart disease so I could take steps to prevent it, but part of me thinks that Iāll enjoy life a bit more being blissfully ignorantā¦ And what if the markers they discover are only right 90% of the time? Then Iād worry away my adulthood only to die of something elseā¦
If you could get your genome sequenced during your next check-up, would you do it?
Joshua
Joshua Finkelstein (Associate Editor, Nature)
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