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WormBase Tree Display for Gene: WBGene00014202

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WBGene00014202	SMap	S_parent	Sequence	ZK1058
	Identity	Version	2
		Name	CGC_name	mmcm-1	Person_evidence	WBPerson4388
						WBPerson4387
			Sequence_name	ZK1058.1
			Molecular_name	ZK1058.1
				ZK1058.1.1
				CE30404
			Other_name	CELE_ZK1058.1	Accession_evidence	NDB	BX284603
			Public_name	mmcm-1
		DB_info	Database (13)
		Species	Caenorhabditis elegans
		History	Version_change	1	26 May 2004 16:54:55	WBPerson1971	Event	Imported	Initial conversion from CDS class of WS125
				2	16 Jan 2006 17:57:11	WBPerson2970	Name_change	CGC_name	mmcm-1
		Status	Live
	Gene_info	Biotype	SO:0001217
		Gene_class	mmcm
		Allele (60)
		Strain	WBStrain00032132
		RNASeq_FPKM (74)
		GO_annotation (23)
		Contained_in_operon	CEOP3864
		Ortholog (36)
		Paralog	WBGene00020169	Caenorhabditis elegans	From_analysis	WormBase-Compara
		Structured_description	Concise_description	mmcm-1 encodes an ortholog of human methylmalonyl-CoA mutase (MUT); MMCM-1 enzyme, in vitro, kinetically resembles its human ortholog; mmcm-1 deletion mutants incorporate abnormally low levels of 1-[(14)C]-propionate into proteins; mmcm-1(RNAi) and mmcm-1 deletion mutant animals excrete abnormally high levels of methylmalonic acid into their culture medium when challenged with propionic acid; mmcm-1, in a lentiviral transgene, can partially rescue the mutant phenotype of human mut(o) fibroblasts; these data are consistent with the hypothesis that MMCM-1 participates in the conversion of propionyl-CoA to succinyl-CoA.	Paper_evidence	WBPaper00004588
						WBPaper00004637
						WBPaper00027754
					Curator_confirmed	WBPerson567
					Date_last_updated	02 Oct 2006 00:00:00
			Automated_description	Enables methylmalonyl-CoA mutase activity. Involved in amino acid metabolic process and fatty acid metabolic process. Located in mitochondrion. Used to study methylmalonic acidemia. Human ortholog(s) of this gene implicated in methylmalonic aciduria due to methylmalonyl-CoA mutase deficiency. Is an ortholog of human MMUT (methylmalonyl-CoA mutase).	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:14749	Homo sapiens	Paper_evidence	WBPaper00027754
					Accession_evidence	OMIM	251000
							251100
					Curator_confirmed	WBPerson324
					Date_last_updated	09 Oct 2018 00:00:00
		Potential_model	DOID:0060740	Homo sapiens	Inferred_automatically	Inferred by orthology to human genes with DO annotation (HGNC:7526)
		Disease_relevance	Methylmalonic aciduria is a genetically heterogeneous disorder of methylmalonate and cobalamin (vitamin B12) metabolism; the metabolism of propionyl-CoA to succinyl-CoA via the formation and isomerization of methylmalonyl-CoA is a critical metabolic pathway in humans; the defective conversion of L-methylmalonyl-CoA to succinyl-CoA in the mitochondrial matrix causes hereditary methylmalonic acidemias, characterized by the accumulation of methylmalonic acid in tissues and secondary metabolic perturbations such as hyperglycinemia and hyperammonemia; affected individuals may suffer from developmental delay, renal disease, pancreatitis and metabolic infarction of the basal ganglia; C.elegans expresses the full complement of mammalian homologues for the conversion of propionyl-CoA to succinyl-CoA, including propionyl-CoA carboxylase subunits A and B (pcca-1,pccb-1), methylmalonic acidemia cobalamin A complementation group (mmaa-1), co(I)balaminadenosyltransferase (mmab-1), MMACHC (cblc-1), methylmalonyl-CoA epimerase (mce-1) and methylmalonyl-CoA mutase (mmcm-1); deletion mutants of mmcm-1(ok1637), mmab-1(ok1484 and ok1493) and mce-1(ok243) displayed reduced 1-[14C]-propionate incorporation into macromolecules and produced increased amounts of methylmalonic acid in the culture medium, proving that a functional block in the pathway caused metabolite accumulation; lentiviral delivery of the C. elegans mmcm-1 into fibroblasts derived from a patient with mut class methylmalonic acidemia could partially restore propionate flux; the C. elegans mce-1 deletion mutant demonstrates for the first time that a lesion at the epimerase step of methylmalonyl-CoA metabolism can functionally impair flux through the methylmalonyl-CoA mutase pathway and suggests that malfunction of MCEE may cause methylmalonic acidemia in humans.	Homo sapiens	Paper_evidence	WBPaper00027754
					Accession_evidence	OMIM	251000
							251100
							609058
					Curator_confirmed	WBPerson324
					Date_last_updated	29 May 2014 00:00:00
	Models_disease_asserted	WBDOannot00000284
	Molecular_info	Corresponding_CDS	ZK1058.1
		Corresponding_transcript	ZK1058.1.1
		Other_sequence	Tcir_isotig01975
			Tcir_isotig30227
			ASC17363_1
			HC09013
			JK315817.1
			HC02458
			FC543339.1
			SSC03218_1
			BI772821.1
			OOC00380_3
			Tcol_isotig13017
			FK807616.1
			SS00250
			Dviv_isotig22871
			FC547248.1
			HC00784
			EX558746.1
			EX545131.1
			HCC01132_1
			AS10975
			HCC04517_2
			EX910020.1
			Tcir_isotig01974
			Acan_isotig07560
			EX008283.1
			Name_isotig01253
			ACC00520_1
			CR02984
			HC06998
			EX553022.1
			Tcol_isotig18357
			CRC04493_1
			SRC05460_1
			PPC04703_1
			CBC00550_1
			JO472435.1
			AE03276
			HCC01131_2
			FC540980.1
			ASC32826_1
			HC00734
			CJC11484_1
			EX561150.1
			SRC06971_1
			EX912666.1
			CBC07487_1
			Tcol_isotig18324
			ASC26095_1
			JO468692.1
			HC06270
			TM03069
			EX543888.1
			HCC01132_2
			OOC01945_1
			TSC00892_1
			HC05904
			JI178982.1
			HBC17505_1
			Tcol_isotig02723
			JI166959.1
			FE909515.1
			AS15400
			EX535086.1
			FE914568.1
			TDC02209_1
			OOC00380_2
			EX549493.1
			ACC15355_1
			EX538478.1
			EX546749.1
			HCC01131_1
			ASC01402_1
			OOC00380_1
			AS01049
			EX538130.1
			AE03667
			HCC04517_1
			EX566061.1
			HCC04379_1
			FC819601.1
			Oden_isotig17450
			FK803495.1
			HC02389
			EX536264.1
			SSC03830_1
			HC06250
			FC547869.1
			PP01026
			EX544004.1
			HCC11090_1
			AYC02434_1
			JI166182.1
			JI213844.1
			Tcol_isotig15931
			EX556099.1
			HCC11599_1
			TS02616
			Tcol_isotig12621
			BM052069.1
			SR04489
			HC06765
			HC05903
			HCC03689_1
			AE00942
			BM174788.1
			FC813721.1
			EX008717.1
			FE913710.1
			HC02042
			JI174756.1
			BG577541.1
			SS02820
			Oden_isotig17449
			HCC04476_1
			AS04699
			Hbac_isotig01620
			EX547752.1
			CB013625.1
			CRC10415_1
			ACC00905_1
			HC02313
			EY460917.1
			HC02474
			EX548548.1
			TMC00555_1
			HBC04165_1
			AE03874
			Tcol_isotig02722
			HCC04308_1
			JO472287.1
			AE04667
			AE00012
			HC02473
			CJC01468_1
		Associated_feature	WBsf666451
			WBsf666715
			WBsf666716
			WBsf226427
			WBsf226428
			WBsf226429
	Experimental_info	RNAi_result	WBRNAi00059082	Inferred_automatically	RNAi_primary
			WBRNAi00078223	Inferred_automatically	RNAi_primary
			WBRNAi00006035	Inferred_automatically	RNAi_primary
			WBRNAi00038132	Inferred_automatically	RNAi_primary
			WBRNAi00007126	Inferred_automatically	RNAi_primary
			WBRNAi00059081	Inferred_automatically	RNAi_primary
			WBRNAi00106988	Inferred_automatically	RNAi_primary
		Expr_pattern	Expr1017573
			Expr1036359
			Expr1162512
			Expr2013626
			Expr2031860
		Drives_construct	WBCnstr00029229
		Construct_product	WBCnstr00029229
		Microarray_results (20)
		Expression_cluster (134)
		Interaction (30)
	Map_info	Map	III	Position	-4.23496
		Positive	Positive_clone	ZK1058	Inferred_automatically	From sequence, transcript, pseudogene data
		Mapping_data	Multi_point	5662
				4791
		Pseudo_map_position
	Reference (15)
	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