Title of article
Selecting optimal antisense reagents
Author/Authors
Sohail، نويسنده , , M and Southern، نويسنده , , E.M، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2000
Pages
12
From page
23
To page
34
Abstract
Selection of the appropriate target site is crucial to the success of an antisense experiment. The selection is difficult because RNAs fold to form secondary structures, rendering most of the molecule inaccessible to intermolecular base pairing with complementary nucleic acids. Conventional approaches, such as selection by ‘sequence-walking’ or computer-assisted design, have not brought significant success. Several empirical selection methods have been reported, a number of which are summarised in this review. Of notable significance are the ‘global’ methods based on mapping of transcripts with the endoribonuclease H (RNase H) and oligonucleotide scanning arrays.
Keywords
Oligonucleotide scanning arrays , RNase H mapping , RNase T1 , Antisense oligonucleotides , secondary structure , Target Selection , Deoxyribozymes , ribozymes
Journal title
Advanced Drug Delivery Reviews
Serial Year
2000
Journal title
Advanced Drug Delivery Reviews
Record number
1760795
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