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WormBase Tree Display for Gene: WBGene00003319

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WBGene00003319	Evidence	Paper_evidence	WBPaper00005879
			WBPaper00005825
	SMap	S_parent	Sequence	C29E6
	Identity	Version	1
		Name	CGC_name	mir-124	Person_evidence	WBPerson18
			Sequence_name	C29E6.7
			Molecular_name	C29E6.7
				C29E6.7a
				C29E6.7b
			Other_name	cel-mir-124	Remark	miRBase V21 import
						MirGeneDB 2.1 import
				CELE_C29E6.7	Accession_evidence	NDB	BX284604
			Public_name	mir-124
		DB_info	Database	miRBase	acc	MI0000302
				SignaLink	mirna	cel-mir-124
				MirGeneDB	cel	Cel-Mir-124
				OMIM	disease	277700
					gene	609327
				NDB	locus_tag	CELE_C29E6.7
				NCBI	gene	3565990
				RefSeq	protein	NR_002382.2
				RNAcentral	URSid	URS000016C218
						URS0000324A65
						URS000040D400
		Species	Caenorhabditis elegans
		History	Version_change	1	07 Apr 2004 11:29:31	WBPerson1971	Event	Imported	Initial conversion from geneace
		Status	Live
	Gene_info	Biotype	SO:0001265
		Gene_class	mir
		Allele	WBVar01500079
			WBVar01498996
			WBVar01499925
			WBVar00090811
			WBVar01500245
		Strain	WBStrain00027428
			WBStrain00034639
			WBStrain00040276
		In_cluster	MIR-124
		RNASeq_FPKM (74)
		Ortholog	HGNC:31502	Homo sapiens	Accession_evidence	miRBase	MIPF0000021
			HGNC:31503	Homo sapiens	Accession_evidence	miRBase	MIPF0000021
			HGNC:31504	Homo sapiens	Accession_evidence	miRBase	MIPF0000021
		Structured_description	Concise_description	mir-124 encodes a highly conserved microRNA, a small non-protein coding RNA; based on RNA sequence, the miR-124 family of microRNAs includes C. elegans miR-228 and human miR-124A1, miR-124A2, miR-124A3 and miR-183; miR-124 is mostly expressed in the nervous system,; in C. elegans it is expressed in a subset of sensory neurons, where it may regulate the expression of target genes; mir-124 also plays a role in aging, as mutants show reduced lifespan, increased reactive oxygen species (ROS) and reduction in ATP levels.	Paper_evidence	WBPaper00005825
						WBPaper00005879
						WBPaper00035973
						WBPaper00041652
					Curator_confirmed	WBPerson324
					Date_last_updated	19 Dec 2013 00:00:00
			Automated_description	Expressed in nervous system and tail. Used to study Werner syndrome. Is an ortholog of human MIR124-1 (microRNA 124-1); MIR124-2 (microRNA 124-2); and MIR124-3 (microRNA 124-3).	Paper_evidence	WBPaper00065943
					Curator_confirmed	WBPerson324
						WBPerson37462
					Inferred_automatically	This description was generated automatically by a script based on data from the WS291 version of WormBase
					Date_last_updated	29 Nov 2023 00:00:00
	Disease_info	Experimental_model	DOID:5688	Homo sapiens	Paper_evidence	WBPaper00041652
					Accession_evidence	OMIM	277700
					Curator_confirmed	WBPerson324
					Date_last_updated	25 Oct 2018 00:00:00
		Disease_relevance	mir-124 is a highly conserved microRNA (miRNA); C. elegans has been used as a model system to study the exact function and importance of this miRNA in accelerated aging, which occurs in diseases like Werner syndrome; mutations in the human WRN gene (also called RECQL2) have been implicated in Werner syndrome; studies in elegans and mice indicate that in wrn-1/WRN mutant animals, the microRNA miR-124 is significantly reduced; mir-124 mutants in C. elegans show reduced lifespan, increased reactive oxygen species (ROS) and reduction in ATP levels; double mutants of mir-124 and wrn-1 showed further reduction in lifespan and ATP levels, and increased ROS generation.	Homo sapiens	Paper_evidence	WBPaper00035973
						WBPaper00041652
					Accession_evidence	OMIM	277700
							609327
					Curator_confirmed	WBPerson324
					Date_last_updated	18 Dec 2013 00:00:00
	Models_disease_asserted	WBDOannot00000257
		WBDOannot00000623
	Molecular_info	Corresponding_transcript	C29E6.7
			C29E6.7a
			C29E6.7b
	Experimental_info	Expr_pattern	Expr2503
			Expr8945
			Expr10944
			Expr12853
			Expr13534
		Drives_construct	WBCnstr00005987
			WBCnstr00016043
			WBCnstr00022904
		Expression_cluster (24)
		Interaction	WBInteraction000504275
			WBInteraction000504276
			WBInteraction000504277
			WBInteraction000504278
			WBInteraction000504279
			WBInteraction000504280
			WBInteraction000504281
			WBInteraction000504282
			WBInteraction000504283
			WBInteraction000504284
			WBInteraction000504285
			WBInteraction000504286
			WBInteraction000504287
			WBInteraction000504288
			WBInteraction000504289
			WBInteraction000504290
			WBInteraction000504291
			WBInteraction000504292
			WBInteraction000504293
			WBInteraction000504294
			WBInteraction000504295
			WBInteraction000504296
			WBInteraction000504297
			WBInteraction000504298
			WBInteraction000504299
			WBInteraction000504300
			WBInteraction000504301
			WBInteraction000504302
			WBInteraction000504303
			WBInteraction000504304
			WBInteraction000504305
			WBInteraction000504306
			WBInteraction000504307
			WBInteraction000504308
			WBInteraction000504309
			WBInteraction000504310
			WBInteraction000504311
			WBInteraction000504312
			WBInteraction000504313
			WBInteraction000504314
			WBInteraction000504315
			WBInteraction000504316
			WBInteraction000504317
			WBInteraction000504318
			WBInteraction000504319
			WBInteraction000504320
			WBInteraction000523949
			WBInteraction000523950
	Map_info	Map	IV	Position	5.35462	Error	0.004076
		Positive	Positive_clone	C29E6	Inferred_automatically	From CDS info
						From sequence, transcript, pseudogene data
		Mapping_data	Multi_point	5253
				5308
		Pseudo_map_position
	Reference (13)
	Remark	Map position created from combination of previous interpolated map position (based on known location of sequence) and allele information. Therefore this is not a genetic map position based on recombination frequencies or genetic experiments. This was done on advice of the CGC.	CGC_data_submission
	Method	Gene