WormBase Tree Display for Gene: WBGene00014202

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: WBVar02015198
      WBVar00394988
      WBVar00394989
      WBVar00394990
      WBVar00394991
      WBVar00394992
      WBVar00394993
      WBVar00394994
      WBVar00394995
      WBVar00394996
      WBVar00394997
      WBVar00394998
      WBVar00394999
      WBVar00598586
      WBVar00395000
      WBVar01396673
      WBVar00092845
      WBVar01498832
      WBVar01643997
      WBVar02034108
      WBVar00818690
      WBVar00818691
      WBVar00818692
      WBVar00818693
      WBVar00818694
      WBVar00818695
      WBVar01903700
      WBVar01962641
      WBVar00818696
      WBVar01499768
      WBVar00818697
      WBVar01499769
      WBVar00818698
      WBVar00058006
      WBVar00818699
      WBVar00818700
      WBVar00818701
      WBVar00818702
      WBVar00058011
      WBVar00818703
      WBVar00818704
      WBVar00818705
      WBVar00818706
      WBVar00818707
      WBVar00818708
      WBVar01445120
      WBVar00818709
      WBVar01445121
      WBVar00818710
      WBVar01445122
      WBVar01445123
      WBVar00269698
      WBVar01656377
      WBVar01656378
      WBVar01474256
      WBVar01474257
      WBVar01474258
      WBVar01262557
      WBVar01709942
      WBVar00394987
    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 (134)
    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