SMARCA4 (SWI/SNF related, matrix associated, actin dependent regulator of chromatin, subfamily a, member 4)

2008-04-01   Pedro P Medina  , Montse Sanchez-Cespedes, PhD 

Identity

HGNC
LOCATION
19p13.2
LOCUSID
ALIAS
BAF190,BAF190A,BRG1,CSS4,MRD16,RTPS2,SNF2,SNF2-beta,SNF2L4,SNF2LB,SWI2,hSNF2b
FUSION GENES

DNA/RNA

Atlas Image
Relative size of the 33 coding exons of SMARCA4. The entire exon 1 is UTR (untranslated region). Exon numeration corresponds to the prevalent transcript (matching the EST EU430759).

Description

The SMARCA4 is also known as BRG1 (hSWI/SNF brahma-related gene). It spans a total genomic size of 101347 bp and it is composed of 33 coding exons of varying lengths and 1 non-coding exon (exon 1).

Transcription

The human SMARCA4 transcript has approximately 5500 bp and contains an open reading frame of 4845 bp, predicting a protein of 1614 amino acid residues. There are different transcripts arising from two alternative splicing sites within intron 28 and exon 30, which predict the translation of four different BRG1 protein isoforms. In addition, between exon 26 and 27 and exon 29 and 30 there are two additional exons that may constitute tissue specific transcripts.

Proteins

Atlas Image
SMARCA4 conserved domains. Proline rich region, containing more than 25% of proline residues in the aminoacid sequence. HSA and BRK domains, containing motifs that may predict binding to DNA. ATPase/helicase domain, contains motifs present in the DEAD helicases superfamily, a diverse family of proteins involved in ATP-dependent RNA or DNA unwinding. Bromodomain, 110 aminoacid domain, found in many chromatin associated proteins. Bromodomains can interact specifically with acetylated lysine.

Description

SMARCA4 has a molecular mass of 181349 Da. SMARCA4 is the catalytic subunit of the chromatin-remodelling complex SWI-SNF and influences transcriptional regulation by disrupting histone-DNA contacts in an ATP-dependent manner. In addition to an ATPase, the SWI/SNF complex is composed of a variety of accessory proteins, termed BAFs (BRG-1-associated factors).

Expression

Widely expressed.

Localisation

SMARCA4 localizes in the nucleus.

Function

The SMARCA4 harbours the ATPase activity required for the chromatin remodelling activity of the SWI/SNF complex. This complex uses the energy of ATP hydrolysis to modify the interactions among histones leading to modifications of the chromatin structure and to the regulation of gene expression. The SWI/SNF complex plays a role in differentiation, development and cell cycle control. SMARCA4 binds to or it is related to important tumor suppressor proteins, including BRCA2, LKB1, RB and FANCA. Moreover, the SWI/SNF complex has been shown to modulate the transcriptional activity of steroid receptors (e.g. glucocorticoids receptors, retinoic acid receptors, androgen and estrogen receptors), CMYC and RB. SMARCA4 acts as a tumor suppressor because:
  • i) it induces cell-growth arrest after ectopic expression in deficient tumor cells;
  • ii) SMARCA4-heterozygous mice have an increased predisposition to tumor development and
  • iii) it is biallelically inactivated by homozygous deletions or combinations of deletions and mutations in several types of tumors, specially in lung cancer.
  • Homology

    The mammalian SWI/SNF complex contains either SMARCA4 or SMARCA2 as its central ATPase subunit. Both ATPases share 80% homology in their aminoacid sequence. However, differences in expression patterns and in the phenotypes of Brm and Brg1 knockout mice suggest specific biological roles between both ATPases.
    SMARCA2 and SMARCA4 are orthologous to the snf2/swi2 gene from S. cerevisiae and to the "brahma" (brm) gene from Drosophila. These encode proteins that are highly conserved along evolution, especially in the ATPase/helicase domain. Actually, SMARCA2 is 56% identical and 72% homologous to the Drosophila brm.

    Implicated in

    Entity name
    Various cancers
    Note
    SMARCA4 somatic mutations have been identified in some cancer cell lines including those from the lung, prostate, breast, pancreas and colon. While somatic mutations have been detected in a small subset of lung primary tumors, about one third of the lung cancer cell lines of the non-small cell lung cancer type harbour inactivating SMARCA4 somatic mutations. All mutations are homozygous and most of them predict truncated proteins. The type of mutations commonly observed include nonsense, indels and large deletions. Although less frequently, missense mutations have also been reported. Four of the aminoacid substitutions found in human lung and colorectal cancer, the p.W764R, p.G1160R, p.L1163P and p.S1176C represent changes in highly conserved residues within the ATPase/helicase domain. In vitro generated mutations of some highly conserved aminoacid within this motif lead to a seriously diminished catalytic activity of SMARCA4.
    SMARCA4 germ-line mutations have not been reported so far.
    Prognosis
    The lost of either SMARCA4 or SMARCA2, detected by immunostaining, predicts decreased survival in some cancer patients.

    Article Bibliography

    Pubmed IDLast YearTitleAuthors

    Other Information

    Locus ID:

    NCBI: 6597
    MIM: 603254
    HGNC: 11100
    Ensembl: ENSG00000127616

    Variants:

    dbSNP: 6597
    ClinVar: 6597
    TCGA: ENSG00000127616
    COSMIC: SMARCA4

    RNA/Proteins

    Gene IDTranscript IDUniprot
    ENSG00000127616ENST00000344626P51532
    ENSG00000127616ENST00000344626A7E2E1
    ENSG00000127616ENST00000413806A0A0A0MT49
    ENSG00000127616ENST00000429416P51532
    ENSG00000127616ENST00000429416A7E2E1
    ENSG00000127616ENST00000444061P51532
    ENSG00000127616ENST00000450717Q9HBD4
    ENSG00000127616ENST00000538456A0A2R8YFK5
    ENSG00000127616ENST00000541122P51532
    ENSG00000127616ENST00000586985K7EQF0
    ENSG00000127616ENST00000589677P51532
    ENSG00000127616ENST00000590574P51532
    ENSG00000127616ENST00000591545A0A2R8YGP5
    ENSG00000127616ENST00000592158K7EP28
    ENSG00000127616ENST00000642350A0A2R8Y6N0
    ENSG00000127616ENST00000642508A0A2R8Y523
    ENSG00000127616ENST00000642628A0A2R8Y7S2
    ENSG00000127616ENST00000642726A0A2R8Y7S2
    ENSG00000127616ENST00000643208A0A2R8Y7F3
    ENSG00000127616ENST00000643296P51532
    ENSG00000127616ENST00000643534A0A2R8Y6V2
    ENSG00000127616ENST00000643549A0A2R8Y4P4
    ENSG00000127616ENST00000643857A0A2R8Y526
    ENSG00000127616ENST00000643995A0A2R8YGG3
    ENSG00000127616ENST00000644065A0A2R8Y440
    ENSG00000127616ENST00000644290A0A2R8Y7R0
    ENSG00000127616ENST00000644327A0A2R8Y4C5
    ENSG00000127616ENST00000644737P51532
    ENSG00000127616ENST00000644760A0A2R8Y866
    ENSG00000127616ENST00000644963A0A2R8YG32
    ENSG00000127616ENST00000645061A0A2R8YDA1
    ENSG00000127616ENST00000645236A0A2R8Y5K3
    ENSG00000127616ENST00000645387A0A2R8YF38
    ENSG00000127616ENST00000645460P51532
    ENSG00000127616ENST00000645648A0A2R8YCY3
    ENSG00000127616ENST00000646183A0A2R8YF80
    ENSG00000127616ENST00000646236A0A2R8Y4R6
    ENSG00000127616ENST00000646484P51532
    ENSG00000127616ENST00000646510P51532
    ENSG00000127616ENST00000646513A0A2R8YFV8
    ENSG00000127616ENST00000646593A0A2R8Y583
    ENSG00000127616ENST00000646693Q9HBD4
    ENSG00000127616ENST00000646746A0A2R8Y7Y7
    ENSG00000127616ENST00000647230P51532
    ENSG00000127616ENST00000647268A0A2R8YF58

    Expression (GTEx)

    0
    10
    20
    30
    40
    50
    60
    70
    80
    90

    Pathways

    PathwaySourceExternal ID
    Immune SystemREACTOMER-HSA-168256
    Cytokine Signaling in Immune systemREACTOMER-HSA-1280215
    Signaling by InterleukinsREACTOMER-HSA-449147
    Interleukin-7 signalingREACTOMER-HSA-1266695
    Signal TransductionREACTOMER-HSA-162582
    Signaling by WntREACTOMER-HSA-195721
    TCF dependent signaling in response to WNTREACTOMER-HSA-201681
    Formation of the beta-catenin:TCF transactivating complexREACTOMER-HSA-201722
    Chromatin organizationREACTOMER-HSA-4839726
    Chromatin modifying enzymesREACTOMER-HSA-3247509
    RMTs methylate histone argininesREACTOMER-HSA-3214858

    Protein levels (Protein atlas)

    Not detected
    Low
    Medium
    High

    References

    Pubmed IDYearTitleCitations
    381179552024Thoracic SMARCA4-deficient undifferentiated tumor: current knowledge and future perspectives.0
    381802452024Molecular and Pathologic Characterization of YAP1-Expressing Small Cell Lung Cancer Cell Lines Leads to Reclassification as SMARCA4-Deficient Malignancies.2
    382526632024Brg1/PRMT5 nuclear complex epigenetically regulates FOXO1 in IPF mesenchymal progenitor cells.0
    383068862024Thoracic SMARCA4-deficient undifferentiated tumor: A clinicopathological and prognostic analysis of 35 cases and immunotherapy efficacy.1
    383112592024BRG1 accelerates mesothelial cell senescence and peritoneal fibrosis by inhibiting mitophagy through repression of OXR1.0
    383486872024BRG1 mediates epigenetic regulation of TNFα-induced CCL2 expression in oral tongue squamous cell carcinoma cells.0
    384132512024SMARCA4 deficiency and mutations are frequent in large cell lung carcinoma and are prognostically significant.0
    384277252024BRG1 establishes the neuroectodermal chromatin landscape to restrict dorsal cell fates.0
    384581882024SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions.1
    385528922024Deciphering the role of SMARCA4 in cardiac disorders: Insights from single-cell studies on dilated cardiomyopathy and coronary heart disease.0
    386428452024SMARCA4 (BRG1) activates ABCC3 transcription to promote hepatocellular carcinogenesis.0
    386886022024ARID1 and BRG1 Expression in Endometrial Cancer.0
    387631022024Rare SMARCA4-deficient thoracic tumor: Insights into molecular characterization and optimal therapeutics methods.0
    388403872024ATP-dependent chromatin remodeller brahma related gene 1 promotes keratinocyte migration and modulates cell Signalling during wound healing in human skin.0
    388774732024Gastric SMARCA4-deficient undifferentiated tumor (SMARCA4-UT): a clinicopathological analysis of four rare cases.0

    Citation

    Pedro P Medina ; Montse Sanchez-Cespedes

    SMARCA4 (SWI/SNF related, matrix associated, actin dependent regulator of chromatin, subfamily a, member 4)

    Atlas Genet Cytogenet Oncol Haematol. 2008-04-01

    Online version: http://atlasgeneticsoncology.org/gene/42333/case-report-explorer/gene-fusions-explorer/js/lib/popper.js