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Gene Expression

p68 RNA Helicase Is an Essential Human Splicing Factor That Acts at the U1 snRNA-5′ Splice Site Duplex

Pages 5443-5450 | Received 21 Feb 2002, Accepted 03 May 2002, Published online: 27 Mar 2023
 

Abstract

Modulation of the interaction between U1 snRNP and the 5′ splice site (5′ss) is a key event that governs 5′ss recognition and spliceosome assembly. Using the methylene blue-mediated cross-linking method (Z. R. Liu, A. M. Wilkie, M. J. Clemens, and C. W. Smith, RNA 2: 611-621, 1996), a 65-kDa protein (p65) was shown to interact with the U1-5′ss duplex during spliceosome assembly (Z. R. Liu, B. Sargueil, and C. W. Smith, Mol. Cell. Biol. 18: 6910-6920, 1998). In this report, p65 was identified as p68 RNA helicase and shown to be essential for in vitro pre-mRNA splicing. Depletion of endogenous p68 RNA helicase does not affect the loading of the U1 snRNP to the 5′ss during early stage of splicing. However, dissociation of the U1 from the 5′ss is largely inhibited. The data suggest that p68 RNA helicase functions in destabilizing the U1-5′ss interactions. Furthermore, depletion of p68 RNA helicase arrested spliceosome assembly at the prespliceosome stage, suggesting that p68 may play a role in the transition from prespliceosome to spliceosome.

I thank Frances Fuller-Pace for providing hybridoma cells for the antibody PAb204 and Roger Bridgeman for antibody PAb204 production. I am also grateful to D. L. Peterson for the HCV-NS3 expression vector. I thank Chris W. J. Smith, Mariano A. Garcia-Blanco, Jenny Yang, and Jan Szechi for detailed critical comments on the manuscript.

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