After several years of serving the research community, our ActiveDriverDB database will be retired on May 1st 2026. Please make sure to download any data you need and update your links or workflows before that date.
We want to sincerely thank all our users for their support, feedback, and collaboration over the years — your contributions have been invaluable to this project. A special thank you to Dr. Michal Krassowski for leading the development of our open-source software and database.
For any questions or assistance, please contact Jüri Reimand (juri.reimand@utoronto.ca).
CHD4 (NM_001273) - chromodomain helicase DNA binding protein 4
Chromodomain-Helicase-Dna-Binding Protein 4 Isoform 1
Legend
                Mutation impacts
                
  
    
    
  
              
                
                Sites
                
  
    
    
  
              
                  -    C-linked
 -    N-linked
 -    O-linked
 -    S-linked
 
-    SARS-CoV-2
 
Others
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              Mutations Visualisation
              
  
    
    
  
            
          
        Protein summary
        
  
    
    
  
      
    The product of this gene belongs to the SNF2/RAD54 helicase family. It represents the main component of the nucleosome remodeling and deacetylase complex and plays an important role in epigenetic transcriptional repression. Patients with dermatomyositis develop antibodies against this protein. Somatic mutations in this gene are associated with serous endometrial tumors. Alternative splicing results in multiple transcript variants encoding different isoforms. [provided by RefSeq, Jul 2014].
Publication Note:
  This RefSeq record includes a subset of the publications that are available for this gene. Please see the Gene record to access additional publications.  
Evidence data:
 Transcript exon combination :: SRR1803615.127809.1, SRR1803615.262254.1 [ECO:0000332] RNAseq introns              :: mixed/partial sample support SAMEA1965299, SAMEA1966682 [ECO:0000350] 
- Strand
 - -
 - Chromosome
 - 12
 
- Protein
 - 1912 residues
 - All mutations
 - 276
 
- PTM sites
 - 118
 - CDS
 - 6,679,841 - 6,715,539
 - Transcription
 - 6,679,247 - 6,716,599