TEP1/YNL128W Summary

TEP1 BASIC INFORMATION

Standard Name	TEP1
Systematic Name	YNL128W
Feature Type	ORF, Verified
Description	Homolog of human tumor suppressor gene PTEN/MMAC1/TEP1 that has lipid phosphatase activity and is linked to the phosphatidylinositol signaling pathway; plays a role in normal sporulation (1, 2)
Name Description	TEnsin-like Phosphatase 1

GO Annotations	All TEP1 GO evidence and references
	View Computational GO annotations for TEP1
Molecular Function
Manually curated	inositol or phosphatidylinositol phosphatase activity (IDA)
Biological Process
Manually curated	ascospore wall assembly (IMP) inositol lipid-mediated signaling (IMP) phosphoinositide dephosphorylation (IDA)
Cellular Component
Manually curated	cellular_component unknown (ND)

Mutant Phenotype	All TEP1 Phenotype details and references
Large-scale survey
null	sporulation: normal viable

Interactions	TEP1 All interactions details and references
	23 total interaction(s) for 23 unique genes/features.
Physical Interactions	Affinity Capture-MS: 3
Genetic Interactions	Phenotypic Enhancement: 19 Phenotypic Suppression: 1

Sequence Information

ChrXIV:382361 to 383665 | |

Last Update

Coordinates: 2005-11-07 | Sequence: 1996-07-31

Subfeature details

	Relative Coordinates	Chromosomal Coordinates	Most Recent Updates
	Relative Coordinates	Chromosomal Coordinates	Coordinates	Sequence
CDS	1..1305	382361..383665	2005-11-07	1996-07-31

External Links	All Associated Seq \| E.C. \| Entrez Gene \| Entrez RefSeq Protein \| MIPS \| UniProtKB

Primary SGDID	S000005072

TEP1 RESOURCES

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SGD ORF map	GBrowse

Click on histogram for expression summary
Expression Summary

ADDITIONAL INFORMATION for TEP1

REFERENCES CITED ON THIS PAGE [View Complete Literature Guide for TEP1]

1)	Heymont J, et al. (2000) TEP1, the yeast homolog of the human tumor suppressor gene PTEN/MMAC1/TEP1, is linked to the phosphatidylinositol pathway and plays a role in the developmental process of sporulation. Proc Natl Acad Sci U S A 97(23):12672-7
2)	Huang J, et al. (2004) Finding new components of the target of rapamycin (TOR) signaling network through chemical genetics and proteome chips. Proc Natl Acad Sci U S A 101(47):16594-9

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