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      Commitment to splice site pairing coincides with A complex formation.

      Molecular Cell
      Animals, Humans, Kinetics, RNA Splicing, genetics, physiology, RNA, Messenger, biosynthesis, Spliceosomes

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          Abstract

          Differential recognition of exons by the spliceosome regulates gene expression and exponentially increases the complexity of metazoan proteomes. After definition of the exons, the spliceosome is activated by a series of sequential structural rearrangements. Formation of the first ATP-independent spliceosomal complex commits the pre-mRNA to the general splicing pathway. However, the time at which a commitment to a specific splice site choice and pairing is made is unknown. Here, we demonstrate that alternative splicing patterns are irreversibly chosen at a kinetic step different from the ATP-independent commitment to splicing. Splice sites become committed at the first ATP-dependent spliceosomal complex when rearrangements lock U2 snRNP onto the pre-mRNA. Thus, commitment to the splicing pathway and commitment to splice site pairing are separate steps during spliceosomal assembly, and ATP hydrolysis drives the irreversible juxtaposition of exons within the spliceosome.

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          Author and article information

          Journal
          15304226
          10.1016/j.molcel.2004.06.025

          Chemistry
          Animals,Humans,Kinetics,RNA Splicing,genetics,physiology,RNA, Messenger,biosynthesis,Spliceosomes
          Chemistry
          Animals, Humans, Kinetics, RNA Splicing, genetics, physiology, RNA, Messenger, biosynthesis, Spliceosomes

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