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Detection of Strand Cleavage And Oxidation Damage Using Model DNA Molecules Captured in a Nanoscale PoreWe use a biological nano-scale pore to distinguish among individual DNA hairpins that differ by a single site of oxidation or a nick in the sugar-phosphate backbone. In earlier work we showed that the protein ion channel alpha-hemolysin can be used as a detector to distinguish single-stranded from double-stranded DNA, single base pair and single nucleotide differences. This resolution is in part a result of sensitivity to structural changes that influence the molecular dynamics of nucleotides within DNA. The strand cleavage products we examined here included a 5-base-pair (5-bp) hairpin with a 5-prime five-nucleotide overhang, and a complementary five-nucleotide oligomer. These produced predictable shoulder-spike and rapid near-full blockade signatures, respectively. When combined, strand annealing was monitored in real time. The residual current level dropped to a lower discrete level in the shoulder-spike blockade signatures, and the duration lengthened. However, these blockade signatures had a shorter duration than the unmodified l0bp hairpin. To test the pore sensitivity to nucleotide oxidation, we examined a 9-bp hairpin with a terminal 8-oxo-deoxyguanosine (8-oxo-dG), or a penultimate 8-oxo-dG. Each produced blockade signatures that differed from the otherwise identical control 9bp hairpins. This study showed that DNA structure is modified sufficiently by strand cleavage or oxidation damage at a single site to alter in a predictable manner the ionic current blockade signatures produced. This technique improves the ability to assess damage to DNA, and can provide a simple means to help characterize the risks of radiation exposure. It may also provide a method to test radiation protection.
Document ID
20040008882
Acquisition Source
Ames Research Center
Document Type
Conference Paper
Authors
Vercoutere, W.
(NASA Ames Research Center Moffett Field, CA, United States)
Solbrig, A.
(California Univ. Santa Cruz, CA, United States)
DeGuzman, V.
(California Univ. Santa Cruz, CA, United States)
Deamer, D.
(California Univ. Santa Cruz, CA, United States)
Akeson, M.
(California Univ. Santa Cruz, CA, United States)
Date Acquired
August 21, 2013
Publication Date
January 1, 2003
Subject Category
Inorganic, Organic And Physical Chemistry
Meeting Information
Meeting: Biophysical Society Meeting
Location: Baltimore, MD
Country: United States
Start Date: February 14, 2004
End Date: February 18, 2004
Sponsors: Biophysical Society
Distribution Limits
Public
Copyright
Work of the US Gov. Public Use Permitted.

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