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Base-calling of automated sequencer traces using phred. I. Accuracy Assessment-英文文献
RESEARCH
Base-Calling of Automated Sequencer Traces
Using Phred. I. Accuracy Assessment
Brent Ewing,1 LaDeana Hillier,2 Michael C. Wendl,2 and Phil Green1,3
1Department of Molecular Biotechnology, University of Washington, Seattle, Washington 98195-7730 USA;
2Genome Sequencing Center, Washington University School of Medicine, Saint Louis, Missouri 63108 USA
The availability of massive amounts of DNA sequence information has begun to revolutionize the practice of
biology. As a result, current large-scale sequencing output, while impressive, is not adequate to keep pace with
growing demand and, in particular, is far short of what will be required to obtain the 3-billion-base human
genome sequence by the target date of 2005. To reach this goal, improved automation will be essential, and it
is particularly important that human involvement in sequence data processing be significantly reduced or
eliminated. Progress in this respect will require both improved accuracy of the data processing software and
reliable accuracy measures to reduce the need for human involvement in error correction and make human
review more efficient. Here, we describe one step toward that goal: a base-calling program for automated
sequencer traces, phred, with improved accuracy. phred appears to be the first base-calling program to achieve a
lower error rate than the ABI software, averaging 40%–50% fewer errors in the data sets examined
independent of position in read, machine running conditions, or sequencing chemistry.
Overview of Sequence Data Processing lane (in the case of dye–terminator chemistry, this
also allows all four reactions to be carried out in a
At present, nearly all DNA sequencing is done using
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