Polypyrimidine Tract Binding Protein Antagonizes Exon Definition

doi:10.1128/MCB.21.10.3281-3288.2001

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Molecular and Cellular Biology, May 2001, p. 3281-3288, Vol. 21, No. 10
0270-7306/01/$04.00+0 DOI: 10.1128/MCB.21.10.3281-3288.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

MINIREVIEW
Polypyrimidine Tract Binding Protein Antagonizes Exon Definition

Eric J. Wagner¹^,² and Mariano A. Garcia-Blanco¹^,³^,⁴^,^*

Departments of Genetics,¹ Microbiology,³ and Medicine,⁴ and Program in Molecular Cancer Biology,² Duke University Medical Center, Durham, North Carolina 27710

	INTRODUCTION

Top Introduction Conclusion References

The removal of introns from mRNA precursors (pre-mRNAs) involves two relatively straightforward chemical reactions. The recognitionof intron-exon boundaries, the splice sites, however, requiresthe integration of information provided by many cis-acting elementsand a complex splicing machinery (64). The cis-acting elementsthat define the borders between exons and introns are quite diverseand yet are recognized efficiently by the splicing machinery.This machinery is composed of general splicing factors (GSFs),which make up the spliceosome and its associated proteins, andof regulatory factors. The same machinery must also make cell-type-specificchoices in cases in which pre-mRNAs are alternatively spliced.This is a monumental task given that it is estimated that transcriptsfrom 30% of all genes in humans are alternatively spliced (http://devnull.lbl.gov:8888/alt).

The spliceosome, like many macromolecular machines, is not preassembled as an active enzyme but rather assembles on the substrate.The substrate, a functional pre-mRNA, is thought to first interactwith U1 snRNP, hnRNP proteins, and SR proteins (5, 34). Theinteraction is determined by RNA-RNA base pairing between the5' end of U1 snRNA and the consensus sequence at the 5' splicesite and by interactions mediated by protein factors (34). Theprotein factors U2AF and SF1 also recognize the polypyrimidinetract, the branch point, and the 3' splice site, thus bridgingthe two groups that subsequently will be involved in the firsttransesterification reaction. This leads to the formation of thecommitment complex (CC). The interaction between the protein factorsand the 3' splice site of an internal exon is enhanced by thebinding of U1 snRNP at the downstream 5' splice site (35, 59).This interaction is the basis for exon definition, an idea discussedin greater detail below. The CC and the U2 snRNP interact to yieldthe prespliceosome, and the branch point sequence is recognizedagain, albeit differently in this complex. The prespliceosomeinteracts with a preformed U5-U4-U6 tri-snRNP to form the immaturespliceosome, which then undergoes rearrangements that result inthe formation of a fully competent enzyme. This interplay of multipleprotein factors and RNA components sets the stage for numerousopportunities for and targets ofregulation.

The complexity of constitutive and alternative splice site recognition suggests multiple layers of regulation, with each layerthe result of combinatorial arrays of elements and factors (38,48, 64). The first layer is direct sequence recognition thatlikely occurs early in the formation of the spliceosome. U1 snRNAcan read the sequence at the 5' splice site, and protein factorsSF1, U2AF⁶⁵, and U2AF³⁵ recognize the branch point, the polypyrimidine tract, and the3' splice site, respectively (3, 5, 45, 61, 75). Theseand other GSFs interact with each other and can act as molecularrulers sensing the relative locations of the cis-acting elements.Positional and distance information provides a second layer ofdiscrimination that overlies the detection of individual bindingsites. This type of information is transmitted via protein-proteininteractions in the definition of exons (2). Another exampleof this type of distance detection is seen in the $alpha$ -tropomyosinpre-mRNA (63), where the close proximity of the 5' splice siteof exon 2 to the branch point upstream of exon 3 precludes theinclusion of both exons into the mRNA. Modulation of splice sitestrength by proteins of the SR family provides yet another layerof regulation (33, 66, 71). SR proteins play roles in constitutivesplicing and can be considered GSFs; however, in some instancesSR proteins have important roles in alternative splicing. Theseproteins can be recruited directly to the RNA by enhancer elementsin exons or introns or indirectly by interactions with other GSFs(36, 43, 58, 67). hnRNP proteins, some of which bind allpre-mRNAs, can also influence splice site choices, possibly bycounteracting SR proteins (6). hnRNP A1 and polypyrimidinetract binding protein (PTB), two proteins classified as hnRNPproteins, repress certain splicing events and thereby providea layer of negative regulation. Very precise regulation is providedby the existence of cell-type-specific factors; several of thesehave been described in Drosophila melanogaster (38). The integrationof the information in these regulatory layers leads to splicesitechoice.

Negative regulation of exon inclusion is emerging as a critical layer in splice site choice. Fairbrother and Chasin consideredwhy certain exons are selected, while others, which seem perfectlycompetent, are ignored (21). These authors suggest that many,and possibly all, exons are under a global repressive influencemediated by many intronic sequences (21). Thus, splice siteutilization can be described as a function of both splice sitestrength and the intensity of the repressive field within a specificregion of a pre-mRNA. This global repressive influence can alsocontribute to the outcome of regulated alternative splicing events,setting the stage for cell-type-specific derepression of exons(1, 8, 12, 46-49, 72, 73). In mammalian cells PTB hasbeen identified as a key splicing repressor. In this review wecritically evaluate the role of PTB in exon silencing and speculateon possible mechanisms of its action. We also provide a briefdiscussion of potential ways in which selective exon inclusioncould be achieved by cell-type-specificderepression.

	PTB: A REPRESSOR OF EXON DEFINITION

PTB was discovered as a protein that bound the U-rich polypyrimidine tract of several introns (22, 70). Multiple formsof PTB were observed and at least three different cDNAs, whichare the result of alternative splicing, were cloned and sequenced(24, 54, 60) (Fig. 1A). Numerous homologs have been subsequentlyidentified, suggesting highly conserved function (Fig. 1B). Sequencealignment reveals that the highest homology lies within the secondRNA recognition motif (RRM2) and a flanking region that has beensuggested to be required for PTB dimerization (53, 56). RRM4,which is required for function (P. J. Grabowski, personal communication)is also highly conserved. The binding to active polypyrimidinetracts (22) and biochemical complementation assays (54) suggesteda role in constitutive splicing; however, this view did not withstandthe test of time. Mulligan et al. (51) noted that PTB boundsequences that repressed inclusion of exon 7 in the $beta$ -tropomyosinpre-mRNA and proposed that PTB was a repressor of splicing. Thisinsightful proposal was supported by subsequent data from severallaboratories.

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FIG. 1. Functional domains and motifs of PTB. (A) Three variants of human PTB exist: PTB1 (protein accession no. CAA43973), PTB2 (protein accession no. CAA46443), and PTB4 (protein accession no. CAA46444). The PTB4 isoform was also identified as a member of the hnRNP family and named hnRNP I (23). Each of the isoforms has four RRMs (24, 54), as well as an N-terminal nuclear localization signal (56). RRM2, as well as the flanking sequence, has been demonstrated to be necessary for PTB oligomerization (53, 56). RRM3 has been shown to be required for RNA binding (53, 56). RRM4 appears to be required for function but not for RNA binding and thus may bind to an unknown corepressor (Grabowski, personal communication). (B) Alignment of PTB protein sequences from seven species using the MacVector CLUSTALW Alignment function. Dark-gray regions within the alignment represent identity, while the light-gray regions denote conserved amino acid changes. Areas of purple shading are the RRMs, and the segment shaded in light red highlights the region of presumed alternative splicing. The NCBI protein accession numbers for these proteins are as follows: Homo sapiens PTB4, CAA46444; S. scrofa PTB4, CAA63597; Mus musculis PTB1, P17225; Rattus norvegicus PTB4, Q00438; Xenopus laevis PTB4, AAF00041; D. melanogaster PTB4, AAF22979; and Caenorhabditis elegans PTB4, T20381.

PTB has also been implicated in other processes that may be unrelated to its role in pre-mRNA splicing, such as a regulationof cap-independent translation, localization of cytoplasmic RNA,and poly(A) site cleavage (see, for example, references 13,27, and 50 and references therein). These activities are notdiscussed here. We address here evidence that PTB is a key regulatorof splicing, and we argue that its major, if not only, effecton pre-mRNA splicing is exonsilencing.

There are compelling, if not definitive, data that PTB mediates exon silencing. Here we define exon silencing as the oppositeof exon definition (2). PTB binds to intronic sequences thatmediate splicing repression (intronic splicing silencers [ISS])in a long list of alternatively spliced pre-mRNAs (1, 8,10, 26, 51, 52, 65) (Fig. 2). Mutation of the PTB bindingsites within ISS sequences reverses both exon silencing in vivoand PTB binding in vitro (1, 8, 10, 12, 25, 26,55, 65). PTB has also been found to bind an exonic splicingsilencer that represses use of a suboptimal 3' splice site inbovine papillomavirus type 1 (74). Competition for PTB withexogenous RNAs (1, 10) and, more importantly, depletion ofPTB (12, 65) leads to derepression of regulated exons in vitro.Readdition of purified or recombinant PTB can reconstitute repression(1, 12, 65). Finally, in vivo overexpression of PTB enhancesthe silencing of exon IIIb in FGF-R2 pre-mRNAs (8), and thiseffect depends on the presence of a PTB binding site upstreamof exon IIIb (Fig. 2). Overexpression of PTB did not result inan overall decrease in splicing. Similar results have been observedwith an $alpha$ -actinin splicing precursor (C. Smith, personal communication).These data suggest that PTB mediates exon silencing.

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FIG. 2. Schematic representation of six pre-mRNAs that are regulated by PTB through exon definition antagonism. Blue exons represent constitutively spliced exons, while the gray exons are regulated. Dark-blue segments represent PTB binding sites; red rectangles are the branch point-associated polypyrimidine tract, while the black dots represent identified or putative branch points. (c-src) The N1 exon is repressed in nonneural cell types by intronic PTB binding sites flanking the exon (9, 10, 12). ( $alpha$ -actinin) The SM exon may be repressed in tissues other than smooth muscle through a network of PTB binding sites located on both sides of the SM exon (65). It should be noted that in vitro the intron downstream of SM is not required for PTB repression. (FGF-R2) Exon IIIb is also repressed in mesenchymal tissues through multiple PTB binding sites found on either side of IIIb (8; E. J. Wagner and M. A. Garcia-Blanco, unpublished results). (Calcitonin/CGRP) The calcitonin-CGRP fourth exon is included and subsequently polyadenylated in the majority of tissues, possibly due to PTB-mediated repression of a zero-length exon located in the downstream intron. Repression of this exon blocks a potential recursive-splicing pathway to exon 5 (14, 39-42). Splicing to exon 5 occurs in neural cell types where PTB levels may be reduced. (GABA_A $gamma$ 2) The small 24-nucleotide exon is repressed in nonneural cell types through PTB binding near the branch point sequence (1, 72, 73). ( $alpha$ -tropomyosin). Exon 3 is specifically repressed in smooth muscle tissue by PTB or a novel PTB variant (25, 26, 55) (Smith, unpublished).

PTB overexpression was also found to activate polyadenylation and concomitant inclusion of exon 4 as the 3'-terminal exonin the CT/CGRP pre-mRNA (Fig. 2) (40). Lou et al. (40) positthat PTB binding to exon 4 promotes polyadenylation by stabilizingan interaction with U1 snRNP at the intronic enhancer of polyadenylation.PTB binding to sites both within exon 4 and the intronic enhancerare believed to be required to activate polyadenylation. A potentialproblem with this model is that mutations of the PTB binding sitewithin exon 4 have no effect on polyadenylation. An alternativemodel predicts dual and competing roles for U1 snRNP bound tothe enhancer: U1 snRNP could activate polyadenylation throughenhancement of exon 4 recognition or it could be involved in arecursive splicing pathway leading to exon 5 inclusion (30)(Fig. 2). PTB would repress the use of the zero-length exon predictedin recursive splicing, thus freeing U1 snRNP to activate polyadenylation.Overexpression of PTB would therefore increase the likelihoodof this event. In this case, as in those mentioned above, PTBcan be best thought of as an antagonist of exon definition (Fig.2).

Although PTB has the ability to interfere with exon definition, it seems likely that the presence of PTB binding sites isnot sufficient to silence otherwise robust exons (25, 26,37, 55). This may be the case for exon 3 of the rat $alpha$ -tropomyosinpre-mRNA, which is silenced in smooth muscle cells but not inmany other tissues. Although silencing of exon 3 requires PTBbinding sites, it cannot be mediated by PTB alone, given thatthis protein is found in cells where exon 3 is included. Regulatedweak exons require other silencer sequences or weak splice sitesin order to achieve repression of exon inclusion. This is clearlythe case with the IIIb exon of FGF-R2 in which, in addition toelements that bind PTB, silencing requires a weak polypyrimidinetract and an exonic silencer that interacts with hnRNP A1 (8,16, 19). PTB also appears to be a component of a multiproteincomplex that assembles on regulatory elements in c-src and $beta$ -tropomyosinpre-mRNAs (10, 12, 29, 64). Together, these data suggestthat PTB acts in concert with corepressors to mediate exon silencing.Given its ubiquitous distribution in cell lines and tissues, itis likely that PTB provides global repression of weak exons. PTBmay play a dual role by not only discriminating between splicesites and pseudo-splice sites during constitutive splicing butalso setting the stage for cell-type-specific selection of regulatedexons during alternativesplicing.

	MECHANISMS OF PTB REPRESSION

PTB binding sites sometimes overlap binding sites for U2AF⁶⁵, and simple competition could account for the inhibitory actionof PTB (37, 62). A well-characterized example of a potentialcompetition model is the repression of the 24-nucleotide exonof the GABA_A $gamma$ 2 pre-mRNA. In this case, there are four silencersequences that bind PTB and act in concert to inhibit the recognitionof this exon. Three of these PTB binding sites surround the branchpoint, with one sitting within the associated polypyrimidine tract(Fig. 2). In this particular example, PTB may be acting in a mannersimilar to the D. melanogaster female-specific splicing factorSXL on TRA pre-mRNA (28, 68). SXL has but one site on theTRA pre-mRNA and excludes access to U2AF⁶⁵ when bound, thus repressing the use of the non-sex-type-specificexon. In most other instances, PTB binding sites do not directlyoverlap the binding sites of GSFs (9, 10, 12, 25, 26,55, 65). In fact, it has recently been demonstrated for theSM exon in $alpha$ -actinin that the critical sites do not overlap withthe branch point and polypyrimidine tract of intron 3 (J. Southbyand C. Smith, personal communication). Therefore, in this caseand many others, PTB-mediated exon silencing is clearly not causedby direct competition with GSFs (see discussion about SXL below).Although these observations suggest that PTB may act by two distinctmechanisms, we argue below for a more parsimoniousexplanation.

The majority of exons silenced by PTB are flanked by PTB binding sites on both adjacent introns (Fig. 2). Given that PTB canmultimerize, it has been postulated that PTB proteins can interactacross the exon (12, 53, 56) (Fig. 3). Chou et al. (12)have shown evidence for such an interaction in vitro, demonstratingthat mutations in the upstream binding site affected binding ofPTB to the downstream site and vice versa. A very similar interactionwas proposed for hnRNP A1 proteins binding on either side of aregulated exon of the hnRNP A1 pre-mRNA (4). In that case theeffect was postulated to be activation of the downstream exonby approximation. The idea that PTB can interact across exonsfits well with the evidence that PTB is an antagonist of exondefinition. The PTB sites flanking silenced exons could definea repressive zone within a pre-mRNA. Binding on both flanks ismost reminiscent of the postulated mechanism for SXL autoregulation(31, 32). The SXL protein binds in numerous positions flankingthe male-specific exon 3 in its own pre-mRNA and prevents itsinclusion. SXL interacts with the Drosophila U1A/U2B" homolog,a component of both U1 and U2 snRNPs, and is likely to interferewith both splice sites (20, 38). It is not known, however,whether SXL multimerizes to promote an exon sequestration eventor if it instead inhibits the recognition of the 5' and 3' splicesites independently. The data of Chou et al. (12) make it unlikelythat PTB is independently inhibiting recognition of the 3' and5' splice sites. We favor exon sequestration mediated in one oftwo ways: PTB-PTB interactions at a distance or PTB multimerization(Fig. 3). The zone of repression formed by PTB may or may notinvolve direct competition with U2AF.

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FIG. 3. Two potential mechanisms to define a zone of silencing. The left model predicts that PTB-PTB interactions between binding sites flanking an exon sequesters an exon, thus precluding the definition of this exon. The model on the right suggests that PTB can oligomerize across an exon, resulting in the coating of the exon, which will also antagonize its definition. The model on the right could also explain the silencing of exons that have a PTB site only on one flank; PTB could multimerize, covering a region of the RNA determined by interactions with other factors.

	CELL TYPE-DEPENDENT DEREPRESSION OF EXONS

PTB is one of the mediators of global silencing of weak or otherwise highly regulated exons. It is interesting to examinehow this layer of negative regulation is specifically derepressedin some cells and tissues. The question of how PTB action is counteractedprobably separates PTB from SXL in terms of mechanistic similarities.In Drosophila, counteracting SXL is simple; its absence in malesresults in the inclusion of exons repressed by SXL in females.PTB, however, is expressed in most cell types, albeit at differentlevels (54).

There are several examples of exons included only in neural cells; silencing in nonneural cells is attributed to PTB action(1, 10, 73). How do neural tissues overcome the repressiveeffect of PTB? Lower levels of PTB in neural tissues and the presenceof a neural type of PTB (nPTB) or brPTB (for brain PTB) have beenproposed as explanations (10, 73). Indeed nPTB can competewith PTB for binding of the RNA but has a weaker repressive effect(44). Overexpression of nPTB, however, can inhibit neuron-specificexon activation by the Nova protein (57), suggesting that nPTBmay act both as an activator and as a repressor depending on thecontext. Levels of PTB per se may not be the whole answer, buta combination of lower levels of PTB and antagonizing factorscould result in neuron-specific exon inclusion (11, 46, 47).Recently, in splicing extracts from cells that include the c-srcN1 exon, but not in extracts that exclude it, PTB binding wasshown to be inhibited in the presence of ATP (Fig. 4) (12).It is clear that PTB is not displaced by the ATP-dependent bindingof U2 snRNP, and the identity of the process that mediates PTBdissociation is unknown.

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FIG. 4. Two possible mechanisms of PTB derepression. (c-src N1 Derepression) In neural cell types it has been suggested that an activity that requires ATP is capable of displacing PTB from the intronic binding sites. This could allow the formation of a neuron-specific complex on the downstream control sequence enhancer resulting in the further activation of the exon (11, 44, 46-49). (FGF-R2 IIIb Derepression) In epithelial cells, exon IIIb is included. The repressive effect of PTB is overcome at least in part through the counteracting activity of yet-to-be-identified proteins, which could potentially stabilize a secondary structure between the two cis elements ISAR and IAS2 (7, 8, 15, 17; Wagner and Garcia-Blanco, unpublished).

In the case of the FGF-R2 pre-mRNA, exon IIIb is silenced in cells of mesenchymal origin, and this silencing is mediated inpart by PTB (7, 8). In epithelial cells, exon IIIb is includedefficiently even though PTB is plentiful (69). The activationof exon IIIb is mediated by at least two cell-type-specific ciselements and others that appear to be activated in all cells (18).Two of the cell-type-specific elements can form a predicted RNAsecondary structure in which one stem would be located betweenseven consensus PTB binding sites in a downstream intronic silencersequence (17) (Fig. 4). Formation of this structure might beexpected to interfere with PTB binding and exonsilencing.

	SUMMARY

Top Introduction Conclusion References

PTB appears to be a global repressor of weak or regulated exons. We propose here that PTB multimerization sequesters theseexons to prevent exon definition. This is likely critical notonly to prevent inclusion of pseudo-exons but also to set up cell-type-specificexon definition. What remains unclear about PTB can probably bebroken down into two basic questions. First, what is the precisemechanism of repression? Second, how is this mechanism circumvented?Most of the research to resolve the first question has focusedprimarily on identifying instances of PTB repression but has donelittle to understand how that repression is achieved. Recently,both in vivo and in vitro assays for PTB repression have beendeveloped (8, 65); thus, a detailed structure-function analysiscan be done. Information from this approach may address mechanisticquestions such as if PTB multimerization is required for repressionor if there are PTB cofactors. Understanding how this repressionis lifted will probably be a more complicated issue. OverwhelmingPTB may occur by numerous mechanisms, such as strengthening weaksplice sites via activators such as TIA-1 (18), causing theenhancement of inclusion via a tissue-specific expression of antagonizingRNA-binding proteins, or simply by modulating the expression ofa PTBcofactor.

	ACKNOWLEDGMENTS

We thank B. Cullen, A. Goldstrohm, P. Grabowski, J. Keene, and C. Smith for critically reading the manuscript and for insightfulsuggestions. We thank members of the Garcia-Blanco laboratory,most especially R. Carstens, for helpfuldiscussions.

This work was supported by a grant from the American Cancer Society. E.J.W. acknowledges the support of a predoctoral fellowshipfrom the D.O.D. M.A.G.-B. acknowledges the support of the Raymondand Beverly SacklerFoundation.

	FOOTNOTES

^* Corresponding author. Mailing address: Department of Genetics, Box 3053, Duke University Medical Center, Durham, NC 27710.Phone: (919) 613-8632. Fax: (919) 613-8646. E-mail: garci001{at}mc.duke.edu.

REFERENCES

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Conclusion
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MINIREVIEW Polypyrimidine Tract Binding Protein Antagonizes Exon Definition

MINIREVIEW
Polypyrimidine Tract Binding Protein Antagonizes Exon Definition