Title of article
Transformation of Aminoacyl tRNAs for the In Vitro Selection of “Drug-like” Molecules Original Research Article
Author/Authors
Chuck Merryman، نويسنده , , Rachel Green، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2004
Pages
8
From page
575
To page
582
Abstract
Evolutionary approaches are regularly used to isolate single molecules with desired activities from large populations of nucleic acids (∼1015). Several methods have also been developed to generate libraries of mRNA-encoded peptides and proteins for the in vitro selection of functional polypeptides. In principal, such mRNA encoding systems could be used with libraries of nonbiological polymers if the ribosome can be directed to polymerize tRNAs carrying unnatural amino acids. The fundamental problem is that current chemical aminoacylation systems cannot easily produce sufficient amounts of the numerous misacylated tRNAs required to synthesize a complex library of encoded polymers. Here, we show that bulk-aminoacylated tRNA can be transformed into N-monomethylated aminoacyl tRNA and translated. Because poly-N-methyl peptide backbones are refractory to proteases and are membrane permeable, our method provides an uncomplicated means of evolving novel drug candidates.
Journal title
Chemistry and Biology
Serial Year
2004
Journal title
Chemistry and Biology
Record number
1158823
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