Unmasking the U2AF homology motif family: a bona fide protein–protein interaction motif in disguise

Loerch, Sarah; Kielkopf, Clara L.

doi:10.1261/rna.057950.116

Cited by 51 publications

(87 citation statements)

References 108 publications

(179 reference statements)

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“…The SPF45 protein contains a G-patch motif for the interactions with proteins and nucleic acids (Silverman et al, 2004;Svec et al, 2004), and C-terminal U2AF-homology motif (UHM) that binds the UHM-Ligand motifs (ULM) of its partner proteins. The binding between the UHM and the ULM plays an essential role in the splicing reactions; for instance, interaction between U2AF 65 and SF3b155 (SF3B1 as HGNC approved symbols) component of U2 snRNP (Reviewed in Loerch and Kielkopf, 2016). Remarkably, the UHM of SPF45 was shown to bind directly with ULM of both U2AF 65 and SF3b155 using the purified recombinant proteins (Corsini et al, 2007).…”

Section: Sf3b155-u2af 65 /U2af 35 Is Displaced By Sf3b155-spf45 Via Umentioning

confidence: 99%

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

Fukumura

Yoshimoto

Sperotto

et al. 2019

Preprint

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Human pre-mRNA introns vary in size from under fifty to over a million nucleotides. We searched for specific splicing factors involved in human short introns by screening siRNAs against 154 human nuclear proteins for activity on a model short 56-nucleotide intron-containing HNRNPH1 pre-mRNA. We identified a known alternative splicing regulator SPF45 (RBM17) as a general splicing factor that is essential to splice out this 56-nt intron. Whole-transcriptome sequencing of SPF45 deficient cells revealed that SPF45 is specifically required for the efficient splicing of many short introns. Our crosslinking and biochemical analyses demonstrate that SPF45 specifically replaces U2AF heterodimer on the truncated pyrimidine tracts. To initiate splicing, the U2AFhomology motif (UHM) of the replaced SPF45 interacts with the UHM-ligand motif (ULM) of the U2 snRNP protein SF3b155 (SF3b1). We propose the existence of a distinct subset of SPF45-dependently spliced short introns.

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Section: Sf3b155-u2af 65 /U2af 35 Is Displaced By Sf3b155-spf45 Via Umentioning

confidence: 99%

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

Fukumura

Yoshimoto

Sperotto

et al. 2019

Preprint

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“…U2AF2 initially binds SF1, which is the first protein to recognize a branch point sequence (BPS) of the pre-mRNA (reviewed in [39]). Subsequently at the transition to the “A-complex”, U2AF2 associates with a “U2AF Ligand Motif” region of SF3B1 (reviewed in [40]), displacing SF1. The U2 snRNA anneals with the BPS [41], which ultimately offers the nucleophile for the first step of the splicing reaction.…”

Section: Sf3b1 and U2af1 Splicing Factors Function In Spliceosome Assmentioning

confidence: 99%

“…The U2AF1 hotspots are located in two CCCH-type zinc knuckles that surround the U2AF2-heterodimerization motif (UHM, [40]), namely S34 is in the N-terminal ZnK1 and Q157 in the C-terminal ZnK2 (Figure 1A). Until recently, ZnK–RNA complexes were limited to two structures: an NMR structure of TIS11d, which comprises tandem ZnK1 and ZnK2 bound to an AU-rich mRNA regulatory element [66], and a 1.7 Å resolution crystal structure of the alternative splicing regulator MBNL1, which comprises a GCU-containing RNA bound to tandem ZnK1 and ZnK2 (formally ZnK3 and ZnK4 in the intact MBNL1 protein sequence) [67].…”

Section: Rna Contacts In Homologous Structures Support Roles For U2afmentioning

confidence: 99%

Splicing Factor Mutations in Myelodysplasias: Insights from Spliceosome Structures

Jenkins

Kielkopf

2017

Trends in Genetics

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Somatic mutations of pre-mRNA splicing factors recur among patients with myelodysplastic syndromes (MDS) and related malignancies. Although these MDS-relevant mutations alter splicing of a subset of transcripts, the mechanisms by which these single amino acid substitutions change gene expression remain controversial. New structures of spliceosome intermediates and associated protein complexes shed light on the molecular interactions mediated by “hotspots” of the SF3B1 and U2AF1 pre-mRNA splicing factors. The frequently mutated SF3B1 residues contact the pre-mRNA splice site. Based on structural-homology with other spliceosome subunits and recent findings of altered RNA binding by mutant U2AF1 proteins, we suggest that affected U2AF1 residues also contact pre-mRNA. Altered pre-mRNA recognition emerges as a molecular theme among MDS-relevant mutations of pre-mRNA splicing factors.

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“…The U2AF large subunit (U2AF 65 ) binds the polypyrimidine tract (PPT) through its tandem RNA recognition motifs (RRM) [3,[6][7][8]. U2AF 65 also possesses a C-terminal atypical RRM motif called "U2AF Homology Motif" (UHM) [9,10] ( Fig 1B). This atypical RRM has lost its RNA-binding ability, but it interacts with an N-terminal "UHM Ligand Motif" (ULM) of SF1 [11][12][13].…”

Section: Introductionmentioning

confidence: 99%

U2 AF ⁶⁵ assemblies drive sequence‐specific splice site recognition

et al. 2019

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The essential splicing factor U2AF65 is known to help anchoring U2 snRNP at the branch site. Its C‐terminal UHM domain interacts with ULM motifs of SF3b155, an U2 snRNP protein. Here, we report a cooperative binding of U2AF65 and the related protein CAPERα to the multi‐ULM domain of SF3b155. In addition, we show that the RS domain of U2AF65 drives a liquid–liquid phase separation that is amplified by intronic RNA with repeated pyrimidine tracts. In cells, knockdown of either U2AF65 or CAPERα improves the inclusion of cassette exons that are preceded by such repeated pyrimidine‐rich motifs. These results support a model in which liquid‐like assemblies of U2AF65 and CAPERα on repetitive pyrimidine‐rich RNA sequences are driven by their RS domains, and facilitate the recruitment of the multi‐ULM domain of SF3b155. We anticipate that posttranslational modifications and proteins recruited in dynamical U2AF65 and CAPERα condensates may further contribute to the complex mechanisms leading to specific splice site choice that occurs in cells.

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Unmasking the U2AF homology motif family: a bona fide protein–protein interaction motif in disguise

Cited by 51 publications

References 108 publications

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

Splicing Factor Mutations in Myelodysplasias: Insights from Spliceosome Structures

U2 AF ⁶⁵ assemblies drive sequence‐specific splice site recognition

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Unmasking the U2AF homology motif family: a bona fide protein–protein interaction motif in disguise

Cited by 51 publications

References 108 publications

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

Splicing Factor Mutations in Myelodysplasias: Insights from Spliceosome Structures

U2 AF 65 assemblies drive sequence‐specific splice site recognition

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U2 AF ⁶⁵ assemblies drive sequence‐specific splice site recognition