Modeling RNA folding paths with pseudoknots: Application to hepatitis delta virus ribozyme
AUTOR(ES)
Isambert, Hervé
FONTE
National Academy of Sciences
RESUMO
A quantitative understanding of nucleic acid hybridization is essential to many aspects of biotechnology, such as DNA microarrays, as well as to the structure and folding kinetics of RNA. However, predictions of nucleic acid secondary structures have long been impeded by the presence of helices interior to loops, so-called pseudoknots, which impose complex three-dimensional conformational constraints. In this paper we compute the pseudoknot free energies analytically in terms of known standard parameters, and we show how the results can be included in a kinetic Monte Carlo code to follow the succession of secondary structures during quenched or sequential folding. For the hepatitis delta virus ribozyme, we predict several nonnative stems on the folding path, characterize a kinetically trapped state, interpret several experimentally characterized mutations in terms of the folding path, and suggest how hybridization with other parts of the genome inactivates the newly formed ribozyme.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=18642Documentos Relacionados
- Hepatitis delta antigens enhance the ribozyme activities of hepatitis delta virus RNA in vivo.
- A circular trans-acting hepatitis delta virus ribozyme.
- Characterization of hepatitis delta antigen: specific binding to hepatitis delta virus RNA.
- Mutagenesis analysis of a hepatitis delta virus genomic ribozyme.
- Self-cleavage of a 71 nucleotide-long ribozyme derived from hepatitis delta virus genomic RNA.
