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Showing papers on "Small hairpin RNA published in 1989"


Patent
17 Aug 1989
TL;DR: In this article, RNA vectors comprising Sindbis virus DI RNA having inserted therein heterologous RNA are presented for the cloning and expression of heterology in eucaryotic cells as well as the packaging of heteralogous RNA into viral particles in the presence of helper virus.
Abstract: The present invention relates to RNA vectors comprising Sindbis virus DI RNA having inserted therein heterologous RNA. The vectors of the present invention provide for the cloning and expression of heterologous RNA in eucaryotic cells as well as the packaging of heterologous RNA into viral particles in the presence of helper virus. Transformed cells and genetically altered alphavirus particles comprising alphavirus DI RNA having inserted therein heterologous RNA are also provided.

165 citations


Journal ArticleDOI
TL;DR: It is shown here that base pairing between the histone stem-loop structure and the U7 RNA is not relevant for processing, and that a processing factor other than the U 7 RNA makes contact with the highly conserved hairpin structure of the hist one precursor.
Abstract: The hairpin loop structure and the downstream spacer element of histone mRNA precursors are both needed for efficient 3' end formation in vivo and in vitro Though generally considered as a single processing signal, these two motifs are involved in different types of interaction with the processing machinery Whereas RNA duplex formation between the downstream spacer element and the U7 small nuclear RNA is essential for processing, we show here that base pairing between the histone stem-loop structure and the U7 RNA is not relevant Our experiments demonstrate that a processing factor other than the U7 RNA makes contact with the highly conserved hairpin structure of the histone precursor The recognition of the target site by the processing factor is structure and sequence specific Prevention of this interaction results in an 80% decrease of 3' cleavage efficiency in vitro The hairpin binding factor is Sm-precipitable and can be partially separated from the U7 small nuclear ribonucleoprotein particle on a Mono Q column

61 citations


Journal ArticleDOI
TL;DR: It is shown that RNA polymerase II recognizes the SV40 sequence that leads to a block of transcription elongation, even when it is under the control of the MLP of adenovirus 2.

42 citations