Published December 4, 2017
| Version v1
Journal article
Open
Electrostatic confinement and manipulation of DNA molecules for genome analysis
Creators
- 1. University of Nebraska–Kearney
- 2. Universidad Nacional de Colombia
- 3. University of Wisconsin-Madison
- 4. Sogang University
- 5. University of Leiden
- 6. University of Chicago
Description
Very large DNA molecules enable comprehensive analysis of complex genomes, such as human, cancer, and plants because they span across sequence repeats and complex somatic events. When physically manipulated, or analyzed as single molecules, long polyelectrolytes are problematic because of mechanical considerations that include shear-mediated breakage, dealing with the massive size of these coils, or the length of stretched DNAs using common experimental techniques and fluidic devices. Accordingly, we harness analyte "issues" as exploitable advantages by our invention and characterization of the "molecular gate," which controls and synchronizes formation of stretched DNA molecules as DNA dumbbells within nanoslit geometries. Molecular gate geometries comprise micro- and nanoscale features designed to synergize very low ionic strength conditions in ways we show effectively create an "electrostatic bottle." This effect greatly enhances molecular confinement within large slit geometries and supports facile, synchronized electrokinetic loading of nanoslits, even without dumbbell formation. Device geometries were considered at the molecular and continuum scales through computer simulations, which also guided our efforts to optimize design and functionalities. In addition, we show that the molecular gate may govern DNA separations because DNA molecules can be electrokinetically triggered, by varying applied voltage, to enter slits in a size-dependent manner. Lastly, mapping the Mesoplasma florum genome, via synchronized dumbbell formation, validates our nascent approach as a viable starting point for advanced development that will build an integrated system capable of large-scale genome analysis.
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Additional details
Identifiers
- DOI
- 10.1073/pnas.1711069114
- Other
- oai:uchicago.tind.io:9763
Funding
- National Institutes of Health
- R01-HG-000225
- National Cancer Institute
- CA182360
- National Human Genome Research Institute
- T32 HG002760
- Department of Energy, Basic Energy Sciences, Materials Science and Engineering
- Midwest Integrated Center for Computational Materials
- National Institute of Standards and Technology
- Center for Hierarchical Materials Design