WormBase Tree Display for Gene: WBGene00001131

WBGene00001131 SMap: S_parent: Sequence: CHROMOSOME_I
  Identity: Version: 1
    Name: CGC_name: dys-1 Person_evidence: WBPerson571
      Sequence_name: F15D3.1
      Molecular_name (30)
      Other_name: CELE_F15D3.1 Accession_evidence: NDB BX284601
      Public_name: dys-1
    DB_info: Database (12)
    Species: Caenorhabditis elegans
    History: Version_change: 1 07 Apr 2004 11:29:23 WBPerson1971 Event: Imported: Initial conversion from geneace
    Status: Live
  Gene_info (9)
  Disease_info: Experimental_model: DOID:11723 Homo sapiens Paper_evidence: WBPaper00003867
            WBPaper00003395
            WBPaper00044415
            WBPaper00035094
          Accession_evidence: OMIM 300376
              310200
          Curator_confirmed: WBPerson324
          Date_last_updated: 22 May 2017 00:00:00
    Potential_model: DOID:11723 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:0081164 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:1561 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:2394 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:12635)
      DOID:0110461 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:12930 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:1059 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
      DOID:9883 Homo sapiens Inferred_automatically: Inferred by orthology to human genes with DO annotation (HGNC:2928)
    Disease_relevance: Mutations in human dystrophin are associated with the Duchenne and Becker types of muscular dystrophy, that affect skeletal muscles used for movement, and heart (cardiac) muscle; in C. elegans, loss-of-function mutants in dys-1 (cx18,cx26,cx35,cx40), the ortholog of human dystrophin/utrophin, display locomotion defects like hyperactivity and hypercontraction, and are hypersensitive to acetylcholine and to the acetylcholinesterase inhibitor, aldicarb, suggesting that dys-1 plays a role in the muscle response to acetylcholine; a chimeric transgene in which the C-terminal end of the elegans DYS-1 protein is replaced by the human dystrophin sequence is able to partly suppress the phenotype of the dys-1 mutants; however, the genetic model for progressive myopathy in C. elegans consists of the dys-1 mutation combined with a mutation in hlh-1, the MyoD ortholog (dys-1(cx18);hlh-1(cc561ts), these animals display time-dependent muscle degeneration; use of this model has identified several genes, that play a role in muscle degeneration, eg., dyc-1/nitric oxide synthase (nNOS)-binding protein CAPON. Homo sapiens Paper_evidence: WBPaper00003867
          Accession_evidence: OMIM 300377
          Curator_confirmed: WBPerson324
          Date_last_updated: 17 May 2017 00:00:00
  Models_disease_asserted (21)
  Molecular_info: Corresponding_CDS: F15D3.1a
      F15D3.1b
      F15D3.1c
      F15D3.1d
      F15D3.1e
      F15D3.1f
      F15D3.1g
      F15D3.1h
      F15D3.1i
      F15D3.1j
    Corresponding_CDS_history: F15D3.1a:wp47
    Corresponding_transcript: F15D3.1a.1
      F15D3.1b.1
      F15D3.1c.1
      F15D3.1d.1
      F15D3.1e.1
      F15D3.1f.1
      F15D3.1g.1
      F15D3.1h.1
      F15D3.1i.1
      F15D3.1j.1
    Other_sequence: MJ03409
      MH04342
      MH03690
      MJ01899
      Hbac_isotig03084
      ES565875.1
      CJC01335_1
      JI164799.1
      FF680099.1
      CJC18192_1
      EX536039.1
      ES672468.1
      CR01042
      ACC25872_1
      Tcol_isotig17085
      TSC09910_1
      Acan_isotig17743
      JI166323.1
      Dviv_isotig30723
      EX013948.1
      CBC02914_1
      GW412597.1
      Dviv_isotig15952
      PSC02561_1
      ACC05027_1
      EV850095.1
      HBC08168_1
      Dviv_isotig15954
      HG09533
      Oden_isotig23488
      JI163880.1
      SC00679
      DVC02336_1
      CRC00866_1
      Oden_isotig19634
      CJC15698_1
      Acan_isotig14755
      HGC05595_1
      CJC17793_1
      Dviv_isotig15953
      Hbac_isotig06761
      GR978447.1
      MAC01335_1
      CR11791
    Associated_feature (19)
  Experimental_info: RNAi_result (13)
    Expr_pattern (12)
    Drives_construct: WBCnstr00003169
      WBCnstr00010181
    Construct_product: WBCnstr00007078
      WBCnstr00008412
      WBCnstr00010181
      WBCnstr00011497
    Regulate_expr_cluster: WBPaper00028474:dys-1_downregulated
      WBPaper00028474:dys-1_upregulated
    Antibody: WBAntibody00003001
    Microarray_results (34)
    Expression_cluster (142)
    Interaction (61)
  Map_info: Map: I Position: 9.11232
    Positive: Positive_clone: F15D3 Inferred_automatically: From sequence, transcript, pseudogene data
    Mapping_data: Multi_point: 4272
        5386
    Pseudo_map_position
  Reference (86)
  Remark: Sequence connection from [Segalat L]
    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
    [210510 skd] Modified Map position as it was a reverse physical that could not be fixed by automated methods. (9.05343)
  Method: Gene