Alternative splice acceptor utilization during human immunodeficiency virus type 1 infection of cultured cells.

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J Virol. 1990 September; 64(9): 4093-4098

Alternative splice acceptor utilization during human immunodeficiency virus type 1 infection of cultured cells.

J C Guatelli, T R Gingeras and D D Richman

Department of Medicine, University of California, San Diego.

ABSTRACT

The utilization of alternative splice acceptors for excisionof the 5' major intron of human immunodeficiency virus type1 RNA was observed after infection in vitro. Specific spliceevents were monitored by a cDNA-polymerase chain reaction. Thesesplice events shared a common splice donor but utilized severalalternative splice acceptors. In addition to identifying thepreviously documented splice acceptors for tat and nef (S. K.Arya, C. Guo, S. F. Josephs, and F. Wong-Staal, Science 229:69-73,1985), nucleotide sequence analysis of cDNA-polymerase chainreaction fragments also revealed the following: (i) two spliceacceptors 15 and 9 nucleotides upstream from the rev start codon,which are utilized to create transcripts suitable for specificrev expression; and (ii) use of the splice acceptor previouslyattributed to nef to generate a singly spliced, env-encodingtranscript. Hybridization signals representing the nef/env,tat, and rev splice events increased in intensity between 6and 12 h after infection of CEM cells with the LAV-1BRU strainof human immunodeficiency virus type 1. In contrast, the signalfor utilization of the nef/env splice acceptor for the singlyspliced env transcript appeared first at 12 h and increasedto maximum intensity by 24 h. The nef/env splice acceptor wasdominant at all time points examined. We propose that this dominanceensures efficient downstream splicing proximal to the env initiationcodon in singly spliced transcripts. However, early after infection,the dominance of the nef/env splice acceptor appears to divertprimary transcripts away from tat- and rev-specific processingpaths. The relative proportions of hybridization signals representingthese alternative splice events remained constant throughoutthe viral replicative cycle. This result suggests that trans-actingfactors that might influence splice choices are not inducedduring infection, but rather that cis-acting, sequence-specificsplice preferences determine the relative efficiency of alternativeacceptor utilization.

J Virol. 1990 September; 64(9): 4093-4098

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