BAIT

PRP38

L000001510, YGR075C

Unique component of the U4/U6.U5 tri-snRNP particle; tri-snRNP is required for conformational changes which result in the catalytic activation of the spliceosome; dispensable for spliceosome assembly

GO Process (1)

GO Function (0)

GO Component (1)

Gene Ontology Biological Process

spliceosome conformational change to release U4 (or U4atac) and U1 (or U11) [IMP]

Gene Ontology Cellular Component

U4/U6 x U5 tri-snRNP complex [IDA, IMP]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

PREY

SPP382

CCF8, NTR1, YLR424W

Essential protein that forms a dimer with Ntr2p; also forms a trimer, with Ntr2p and Prp43p, that is involved in spliceosome disassembly; found also in a multisubunit complex with the splicing factor Clf1p; suppressor of prp38-1 mutation

GO Process (3)

GO Function (2)

GO Component (5)

Gene Ontology Biological Process

generation of catalytic spliceosome for first transesterification step [IMP]

mRNA splicing, via spliceosome [IPI]

spliceosomal complex disassembly [IDA, IGI, IMP]

Gene Ontology Molecular Function

ATP-dependent RNA helicase activity [IDA]
RNA binding [ISS]

Gene Ontology Cellular Component

U2-type post-mRNA release spliceosomal complex [IDA, IMP]

cytoplasm [IDA]

mitochondrion [IDA]

nucleus [IDA]

spliceosomal complex [IDA]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

Synthetic Lethality

A genetic interaction is inferred when mutations or deletions in separate genes, each of which alone causes a minimal phenotype, result in lethality when combined in the same cell under a given condition.

Publication

Inhibition of a spliceosome turnover pathway suppresses splicing defects.

Pandit S, Lynn B, Rymond BC

Defects in assembly are suggested to signal the dissociation of faulty splicing complexes. A yeast genetic screen was performed to identify components of the putative discard pathway. Weak mutant alleles of SPP382 (also called NTR1) were found to suppress defects in two proteins required for spliceosome activation, Prp38p and Prp8p. Spp382p is shown necessary for cellular splicing, with premRNA and, ... [more]

Proc. Natl. Acad. Sci. U.S.A. Sep. 12, 2006; 103(37);13700-5 [Pubmed: 16945917]

Throughput

Low Throughput

Ontology Terms

phenotype: inviable (APO:0000112)

Related interactions

Interaction	Experimental Evidence Code	Dataset	Throughput	Score	Curated By	Notes
SPP382 PRP38	Dosage Lethality Dosage Lethality A genetic interaction is inferred when over expression or increased dosage of one gene causes lethality in a strain that is mutated or deleted for another gene.	Pandit S (2009)	Low	-	BioGRID	351802
PRP38 SPP382	Synthetic Rescue Synthetic Rescue A genetic interaction is inferred when mutations or deletions of one gene rescues the lethality or growth defect of a strain mutated or deleted for another gene.	Pandit S (2006)	Low	-	BioGRID	205091
PRP38 SPP382	Synthetic Rescue Synthetic Rescue A genetic interaction is inferred when mutations or deletions of one gene rescues the lethality or growth defect of a strain mutated or deleted for another gene.	Pandit S (2009)	Low	-	BioGRID	351797

Curated By

BioGRID

Interaction Summary

PRP38

Gene Ontology Biological Process

Gene Ontology Cellular Component

SPP382

Gene Ontology Biological Process

Gene Ontology Molecular Function

ATP-dependent RNA helicase activity [IDA]RNA binding [ISS]

Gene Ontology Cellular Component

Synthetic Lethality

Publication

Inhibition of a spliceosome turnover pathway suppresses splicing defects.

Throughput

Ontology Terms

Related interactions

Curated By

ATP-dependent RNA helicase activity [IDA]
RNA binding [ISS]