Exon Inclusion Is Dependent on Predictable Exonic Splicing Enhancers

doi:10.1128/MCB.25.16.7323-7332.2005

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Molecular and Cellular Biology, August 2005, p. 7323-7332, Vol. 25, No. 16
0270-7306/05/$08.00+0 doi:10.1128/MCB.25.16.7323-7332.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

Exon Inclusion Is Dependent on Predictable Exonic Splicing Enhancers

Xiang H.-F. Zhang, Thaned Kangsamaksin, Mann S. P. Chao, Joydeep K. Banerjee, and Lawrence A. Chasin^*

Department of Biological Sciences, Columbia University, New York, New York 10027

Received 1 March 2005/ Returned for modification 25 March 2005/ Accepted 16 May 2005

We have previously formulated a list of approximately 2,000RNA octamers as putative exonic splicing enhancers (PESEs) basedon a statistical comparison of human exonic and nonexonic sequences(X. H. Zhang and L. A. Chasin, Genes Dev. 18:1241-1250, 2004).When inserted into a poorly spliced test exon, all eight testedoctamers stimulated splicing, a result consistent with theiridentification as exonic splicing enhancers (ESEs). Here wepresent a much more stringent test of the validity of this listof PESEs. Twenty-two naturally occurring examples of nonoverlappingPESEs or PESE clusters were identified in six mammalian exons;five of the six exons tested are constitutively spliced. Eachof the 22 individual PESEs or PESE clusters was disrupted bysite-directed mutagenesis, usually by a single-base substitution.Eighteen of the 22 disruptions (82%) resulted in decreased splicingefficiency. In contrast, 24 control mutations had little orno effect on splicing. This high rate of success suggests thatmost PESEs function as ESEs in their natural context. Like mostexons, these exons contain several PESEs. Since knocking outany one of several could produce a severalfold decrease in splicingefficiency, we conclude that there is little redundancy amongESEs in an exon and that they must work in concert to optimizesplicing.

* Corresponding author: Department of Biological Sciences, Columbia University, 1212 Amsterdam Ave., MC 2433, New York, NY 10027. Phone: (212) 854-4645. Fax: (212) 531-0425. E-mail: lac2{at}columbia.edu.

Molecular and Cellular Biology, August 2005, p. 7323-7332, Vol. 25, No. 16
0022-538X/05/$08.00+0 doi:10.1128/MCB.25.16.7323-7332.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

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