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(processing or calculation part; of course, you have to have created the reference database
first), and finally there is a nice output list (list of hits and statistical parameters).
Question 1.6
Answer A, C, D
Example 1.7
Answer B.
The BLAST algorithm can perform a number of searches, e.g. blastn for a nucleotide
sequence and blastp for a protein sequence. But it can do much more, e.g. blastx translates
a nucleotide sequence into a protein sequence and then searches against the protein data
base, tblastn searches with a protein sequence against a translated nucleotide database, and
tblastx searches with a translated nucleotide sequence against a translated nucleotide
database.
Example 1.8
Answer A, D.
The sequence comparison with BLAST first tells what the function of the sequence is
(which piece of which virus is here as a sequence). In the example, the blastp search
should have found the pol protein and protease of HIV-1. Another important output is the
E-value (expected value). This indicates that my output alignment will be found again in
the database with a similar or better score, so it depends on the size of the database (unlike
the p-value). If you are looking for the highest possible similarity, the selected BLAST hit
should have the smallest possible e-value and a high identity.
20.1
Question 1.9 and Example 1.10
A dotplot allows you to compare two sequences on a graph (x−/y-axis) to find similar
areas (represented as a dot). In both cases (by hand and software), your dotplot should find
similar areas between the two exercise sequences.
20.2
Magic RNA
Example 2.1
1. Answer C, E
20.2 Magic RNA