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WormBase Tree Display for Gene: WBGene00001808

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Name Class

WBGene00001808EvidencePerson_evidenceWBPerson1846
SMapS_parentSequenceT10G3
IdentityVersion1
NameCGC_namegut-2Person_evidenceWBPerson579
Sequence_nameT10G3.6
Molecular_nameT10G3.6a
T10G3.6a.1
CE37990
T10G3.6b
CE45330
T10G3.6b.1
Other_namelsm-2CGC_data_submission
CELE_T10G3.6Accession_evidenceNDBBX284605
Public_namegut-2
DB_infoDatabaseAceViewgene5N979
WormQTLgeneWBGene00001808
WormFluxgeneWBGene00001808
NDBlocus_tagCELE_T10G3.6
PanthergeneCAEEL|WormBase=WBGene00001808|UniProtKB=P92022
familyPTHR13829
NCBIgene179833
RefSeqproteinNM_001269582.2
NM_001269583.3
TREEFAMTREEFAM_IDTF314960
TrEMBLUniProtAccP92022
E1B6V1
UniProt_GCRPUniProtAccP92022
SpeciesCaenorhabditis elegans
HistoryVersion_change107 Apr 2004 11:29:25WBPerson1971EventImportedInitial conversion from geneace
StatusLive
Gene_infoBiotypeSO:0001217
Gene_classgut
Allele (31)
Legacy_information[C.elegansII] lw6 : E cells fail to gastrulate, division rate does not slow; mutant EMS not responsive to WT P2 induction. lw6/Df similar. OA>10: it92, lw63 (Gro, sterile). Cloned: cosmid rescue (T10G8). [EH; CB]
[Shaw JE] lw6 and it92 are not null alleles. lw6 and it92 are recessive, strict maternal effect lethal. Dead embryos arrest development with approximately normal cell number but no morphogenesis. Dead embryos are highly penetrant for lack of both differentiated gut cells and pharyngeal muscle. Other tissues (hypodermal, neuronal, body-wall muscle) are present. Early defects in E lineage,i.e. early 2E to 4E division and failure to gastrulate, highly penetrant. Null phenotype likely recessive slow-growing, sterile adult.
StrainWBStrain00036163
WBStrain00036228
RNASeq_FPKM (74)
GO_annotation (19)
Ortholog (33)
Structured_descriptionConcise_descriptiongut-2 encodes a member of the Sm protein family with highest similarity to human U6 snRNA-associated Sm-like protein, LSm2, that affects embryonic viability.Paper_evidenceWBPaper00012624
WBPaper00023072
Curator_confirmedWBPerson48
Date_last_updated17 Jun 2004 00:00:00
Automated_descriptionPredicted to contribute to RNA binding activity. Predicted to be involved in mRNA splicing, via spliceosome. Predicted to be located in P-body. Predicted to be part of Lsm1-7-Pat1 complex and ribonucleoprotein complex. Is an ortholog of human LSM2 (LSM2 homolog, U6 small nuclear RNA and mRNA degradation associated).Paper_evidenceWBPaper00065943
Curator_confirmedWBPerson324
WBPerson37462
Inferred_automaticallyThis description was generated automatically by a script based on data from the WS291 version of WormBase
Date_last_updated29 Nov 2023 00:00:00
Molecular_infoCorresponding_CDST10G3.6a
T10G3.6b
Corresponding_CDS_historyT10G3.6:wp138
Corresponding_transcriptT10G3.6a.1
T10G3.6b.1
Other_sequence (54)
Associated_featureWBsf647462
WBsf662028
WBsf232784
Experimental_infoRNAi_result (28)
Expr_patternExpr1016964
Expr1031059
Expr1156677
Expr2012349
Expr2030585
Microarray_results (20)
Expression_cluster (131)
Interaction (330)
Map_infoMapVPosition5.35258Error0.004597
Well_ordered
PositivePositive_cloneK10B8
T10G3Inferred_automaticallyFrom sequence, transcript, pseudogene data
NegativeNegative_cloneR11G10
Mapping_data2_point7109
Multi_point3848
ReferenceWBPaper00012624
WBPaper00014687
WBPaper00015015
WBPaper00021955
WBPaper00022720
WBPaper00023072
WBPaper00038491
WBPaper00046572
WBPaper00055090
WBPaper00059527
RemarkThe gut-2 gene was merged with lsm-2 following advice from the CGC. gut-2 is the main name for this gene.CGC_data_submission
MethodGene