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Center for Computational Systems Medicine
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Fusion Gene and Fusion Protein Summary

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Fusion Amino Acid Sequences (multiple BPs and multiple gene isoforms)

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Fusion Protein Breakpoint Sequences - (for the Screening of the FusionNeoAntigens)

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Potential FusionNeoAntigens in HLA I - (netMHCpan v4.1 + deepHLApan v1.1)

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Potential FusionNeoAntigens in HLA II - (netMHCIIpan v4.1)

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Fusion Breakpoint 14 AA Peptide Structure - (RoseTTAFold)

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Filtering FusionNeoAntigens Through Checking the Interaction with HLAs in 3D - (Glide)

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Vaccine Design for the FusionNeoAntigens (RNA/protein sequences)

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Potential target of CAR-T therapy development

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Information on the samples that have these potential fusion neoantigens

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Fusion Protein Targeting Drugs - (Manual Curation)

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Fusion Protein Related diseases - (Manual Curation)

Fusion Protein:FRMD3-BRD4

Fusion Gene and Fusion Protein Summary

check button Fusion gene summary
Fusion partner gene informationFusion gene name: FRMD3-BRD4
FusionPDB ID: 31316
FusionGDB2.0 ID: 31316
HgeneTgene
Gene symbol

FRMD3

BRD4

Gene ID

257019

23476

Gene nameFERM domain containing 3bromodomain containing 4
Synonyms4.1O|EPB41L4O|EPB41LO|P410CAP|HUNK1|HUNKI|MCAP
Cytomap

9q21.32

19p13.12

Type of geneprotein-codingprotein-coding
DescriptionFERM domain-containing protein 3band 4.1-like protein 4band 4.1-like protein 4Oovary type protein 4.1protein 4.1Obromodomain-containing protein 4chromosome-associated proteinmitotic chromosome-associated protein
Modification date2020031320200329
UniProtAcc

A2A2Y4

Main function of 5'-partner protein: FUNCTION: Putative tumor suppressor gene that may be implicated in the origin and progression of lung cancer. {ECO:0000269|PubMed:17260017}.

O60885

Main function of 5'-partner protein: FUNCTION: Chromatin reader protein that recognizes and binds acetylated histones and plays a key role in transmission of epigenetic memory across cell divisions and transcription regulation. Remains associated with acetylated chromatin throughout the entire cell cycle and provides epigenetic memory for postmitotic G1 gene transcription by preserving acetylated chromatin status and maintaining high-order chromatin structure (PubMed:23589332, PubMed:23317504, PubMed:22334664). During interphase, plays a key role in regulating the transcription of signal-inducible genes by associating with the P-TEFb complex and recruiting it to promoters. Also recruits P-TEFb complex to distal enhancers, so called anti-pause enhancers in collaboration with JMJD6. BRD4 and JMJD6 are required to form the transcriptionally active P-TEFb complex by displacing negative regulators such as HEXIM1 and 7SKsnRNA complex from P-TEFb, thereby transforming it into an active form that can then phosphorylate the C-terminal domain (CTD) of RNA polymerase II (PubMed:23589332, PubMed:19596240, PubMed:16109377, PubMed:16109376, PubMed:24360279). Promotes phosphorylation of 'Ser-2' of the C-terminal domain (CTD) of RNA polymerase II (PubMed:23086925). According to a report, directly acts as an atypical protein kinase and mediates phosphorylation of 'Ser-2' of the C-terminal domain (CTD) of RNA polymerase II; these data however need additional evidences in vivo (PubMed:22509028). In addition to acetylated histones, also recognizes and binds acetylated RELA, leading to further recruitment of the P-TEFb complex and subsequent activation of NF-kappa-B (PubMed:19103749). Also acts as a regulator of p53/TP53-mediated transcription: following phosphorylation by CK2, recruited to p53/TP53 specific target promoters (PubMed:23317504). {ECO:0000269|PubMed:16109376, ECO:0000269|PubMed:16109377, ECO:0000269|PubMed:19103749, ECO:0000269|PubMed:19596240, ECO:0000269|PubMed:22334664, ECO:0000269|PubMed:22509028, ECO:0000269|PubMed:23086925, ECO:0000269|PubMed:23317504, ECO:0000269|PubMed:23589332, ECO:0000269|PubMed:24360279}.; FUNCTION: [Isoform B]: Acts as a chromatin insulator in the DNA damage response pathway. Inhibits DNA damage response signaling by recruiting the condensin-2 complex to acetylated histones, leading to chromatin structure remodeling, insulating the region from DNA damage response by limiting spreading of histone H2AX/H2A.x phosphorylation. {ECO:0000269|PubMed:23728299}.
Ensembl transtripts involved in fusion geneENST idsENST00000304195, ENST00000376438, 
ENST00000328788, ENST00000376434, 
ENST00000465485, 		ENST00000602230, 
ENST00000263377, ENST00000360016, 
ENST00000371835, 
Fusion gene scores for assessment (based on all fusion genes of FusionGDB 2.0)* DoF score5 X 5 X 5=12515 X 19 X 13=3705
# samples 528
** MAII scorelog2(5/125*10)=-1.32192809488736
possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs).
DoF>8 and MAII<0		log2(28/3705*10)=-3.72597481024823
possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs).
DoF>8 and MAII<0
Fusion gene context

PubMed: FRMD3 [Title/Abstract] AND BRD4 [Title/Abstract] AND fusion [Title/Abstract]

Fusion neoantigen context

PubMed: FRMD3 [Title/Abstract] AND BRD4 [Title/Abstract] AND neoantigen [Title/Abstract]

Most frequent breakpoint (based on all fusion genes of FusionGDB 2.0)FRMD3(85987828)-BRD4(15365073), # samples:2
Anticipated loss of major functional domain due to fusion event.FRMD3-BRD4 seems lost the major protein functional domain in Hgene partner, which is a CGC by not retaining the major functional domain in the partially deleted in-frame ORF.
FRMD3-BRD4 seems lost the major protein functional domain in Hgene partner, which is a CGC by not retaining the major functional domain in the partially deleted in-frame ORF.
FRMD3-BRD4 seems lost the major protein functional domain in Hgene partner, which is a essential gene by not retaining the major functional domain in the partially deleted in-frame ORF.
FRMD3-BRD4 seems lost the major protein functional domain in Hgene partner, which is a essential gene by not retaining the major functional domain in the partially deleted in-frame ORF.
* DoF score (Degree of Frequency) = # partners X # break points X # cancer types
** MAII score (Major Active Isofusion Index) = log2(# samples/DoF score*10)

check button Gene ontology of each fusion partner gene with evidence of Inferred from Direct Assay (IDA) from Entrez
PartnerGeneGO IDGO termPubMed ID
TgeneBRD4

GO:0032968

positive regulation of transcription elongation from RNA polymerase II promoter

19103749|23086925

TgeneBRD4

GO:0043123

positive regulation of I-kappaB kinase/NF-kappaB signaling

19103749

TgeneBRD4

GO:0045944

positive regulation of transcription by RNA polymerase II

23086925|23317504|24360279

TgeneBRD4

GO:0050727

regulation of inflammatory response

19103749

TgeneBRD4

GO:1901407

regulation of phosphorylation of RNA polymerase II C-terminal domain

23086925



check button Four levels of functional features of fusion genes
Go to FGviewer search page for the most frequent breakpoint (https://ccsmweb.uth.edu/FGviewer/chr9:85987828/chr19:15365073)
- FGviewer provides the online visualization of the retention search of the protein functional features across DNA, RNA, protein, and pathological levels.
- How to search
1. Put your fusion gene symbol.
2. Press the tab key until there will be shown the breakpoint information filled.
4. Go down and press 'Search' tab twice.
4. Go down to have the hyperlink of the search result.
5. Click the hyperlink.
6. See the FGviewer result for your fusion gene.
FGviewer

check buttonRetention analysis results of each fusion partner protein across 39 protein features of UniProt such as six molecule processing features, 13 region features, four site features, six amino acid modification features, two natural variation features, five experimental info features, and 3 secondary structure features, are available here.

check buttonFusion gene breakpoints across FRMD3 (5'-gene)
* Click on the image to open the UCSC genome browser with custom track showing this image in a new window.
all structure

check buttonFusion gene breakpoints across BRD4 (3'-gene)
* Click on the image to open the UCSC genome browser with custom track showing this image in a new window.
all structure


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Fusion Amino Acid Sequences


check buttonFusion information from ORFfinder translation from full-length transcript sequence from FusionPDB.
HenstTenstHgeneHchrHbpHstrandTgeneTchrTbpTstrandSeq length
(transcript)		BP loci
(transcript)		Predicted start
(transcript)		Predicted stop
(transcript)		Seq length
(amino acids)
ENST00000376438FRMD3chr985987828-ENST00000263377BRD4chr1915365073-41936102072651814
ENST00000376438FRMD3chr985987828-ENST00000371835BRD4chr1915365073-29556106020201
ENST00000376438FRMD3chr985987828-ENST00000360016BRD4chr1915365073-1513610207947246
ENST00000304195FRMD3chr985987828-ENST00000263377BRD4chr1915365073-4085502992543814
ENST00000304195FRMD3chr985987828-ENST00000371835BRD4chr1915365073-284750299623174
ENST00000304195FRMD3chr985987828-ENST00000360016BRD4chr1915365073-140550299839246

check buttonDeepORF prediction of the coding potential based on the fusion transcript sequence of in-frame fusion genes. DeepORF is a coding potential classifier based on convolutional neural network by comparing the real Ribo-seq data. If the no-coding score < 0.5 and coding score > 0.5, then the in-frame fusion transcript is predicted as being likely translated.
HenstTenstHgeneHchrHbpHstrandTgeneTchrTbpTstrandNo-coding scoreCoding score
ENST00000376438ENST00000263377FRMD3chr985987828-BRD4chr1915365073-0.025797810.9742022
ENST00000376438ENST00000371835FRMD3chr985987828-BRD4chr1915365073-0.089503210.9104968
ENST00000376438ENST00000360016FRMD3chr985987828-BRD4chr1915365073-0.0624647030.9375353
ENST00000304195ENST00000263377FRMD3chr985987828-BRD4chr1915365073-0.0262924470.9737075
ENST00000304195ENST00000371835FRMD3chr985987828-BRD4chr1915365073-0.13784940.8621506
ENST00000304195ENST00000360016FRMD3chr985987828-BRD4chr1915365073-0.085097160.91490287

check button Predicted full-length fusion amino acid sequences. For individual full-length fusion transcript sequence from FusionPDB, we ran ORFfinder and chose the longest ORF among all the predicted ones.

Get the fusion protein sequences from here.

Fusion protein sequence information is available in the fasta format.
>FusionGDB ID_FusionGDB isoform ID_FGname_Hgene_Hchr_Hbp_Henst_Tgene_Tchr_Tbp_Tenst_length(fusion AA) seq_BP

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Fusion Protein Breakpoint Sequences for FRMD3-BRD4

check button +/-13 AA sequence from the breakpoints of the fusion protein sequences.
HgeneHchrHbpTgeneTchrTbpLength(fusion protein)BP in fusion proteinPeptide
FRMD3chr985987828BRD4chr1915365073502135LEPNKSIFKQMKTEKVDVIAGSSKMK
FRMD3chr985987828BRD4chr1915365073502424PPPHPSVQQQLQQQPPPPPPPQPQPP
FRMD3chr985987828BRD4chr1915365073610135LEPNKSIFKQMKTEKVDVIAGSSKMK
FRMD3chr985987828BRD4chr1915365073610424PPPHPSVQQQLQQQPPPPPPPQPQPP

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Potential FusionNeoAntigen Information of FRMD3-BRD4 in HLA I

check button Multiple sequence alignments of the potential FusionNeoAntigens per fusion breakpoints. If the MSA is empty, then it means that there were predicted fusion neoantigens in this fusion breakpoint, but those predicted fusion neoantigens were not across the breakpoint, which is not fusion-specific.

check button Potential FusionNeoAntigen Information
* We used NetMHCpan v4.1 (%rank<0.5) and deepHLApan v1.1 (immunogenic score>0.5)
Fusion geneHchrHbpTgeneTchrTbpHLA IFusionNeoAntigen peptideBinding scoreImmunogenic scoreNeoantigen start (at BP 13)Neoantigen end (at BP 13)

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Potential FusionNeoAntigen Information of FRMD3-BRD4 in HLA II

check button Multiple sequence alignments of the potential FusionNeoAntigens per fusion breakpoints. If the MSA is empty, then it means that there were predicted fusion neoantigens in this fusion breakpoint, but those predicted fusion neoantigens were not across the breakpoint, which is not fusion-specific.

check button Potential FusionNeoAntigen Information
* We used NetMHCIIpan v4.1 (%rank<0.5).
Fusion geneHchrHbpTgeneTchrTbpHLA IIFusionNeoAntigen peptideNeoantigen start (at BP 13)Neoantigen end (at BP 13)

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Fusion breakpoint peptide structures of FRMD3-BRD4

check button3D structures of the fusion breakpoint peptide of 14AA sequence that have potential fusion neoantigens
* The minimum length of the amino acid sequence in RoseTTAFold is 14AA. Here, we predicted the 14AA fusion protein breakpoint sequence not the fusion neoantigen peptide, which is shorter than 14 AA.

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Filtering FusionNeoAntigens Through Checking the Interaction with HLAs in 3D of FRMD3-BRD4

check buttonVirtual screening between 25 HLAs (from PDB) and FusionNeoAntigens
* We used Glide to predict the interaction between HLAs and neoantigens.
HLA allelePDB IDFile nameBPseqDocking scoreGlide score

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Vaccine Design for the FusionNeoAntigens of FRMD3-BRD4

check button mRNA and peptide sequences of FusionNeoAntigens that have potential interaction with HLA-Is.
Fusion geneHchrHbpTchrTbpStart in +/-13AAEnd in +/-13AAFusionNeoAntigen peptide sequenceFusionNeoAntigen RNA sequence

check button mRNA and peptide sequences of FusionNeoAntigens that have potential interaction with HLA-IIs.
Fusion geneHchrHbpTchrTbpStart in +/-13AAEnd in +/-13AAFusionNeoAntigen peptideFusionNEoAntigen RNA sequence

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Information of the samples that have these potential fusion neoantigens of FRMD3-BRD4

check button These samples were reported as having these fusion breakpoints. For individual breakpoints, we checked the open reading frames considering multiple gene isoforms and chose the in-frame fusion genes only. Then, we made fusion protein sequences and predicted the fusion neoantigens. These fusion-positive samples may have these potential fusion neoantigens.
Cancer typeFusion geneHchrHbpHenstTchrTbpTenstSample

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Potential target of CAR-T therapy development for FRMD3-BRD4

check button Predicted 3D structure. We used RoseTTAFold.

check buttonRetention analysis result of each fusion partner protein across 39 protein features of UniProt such as six molecule processing features, 13 region features, four site features, six amino acid modification features, two natural variation features, five experimental info features, and 3 secondary structure features. Here, to provide the retention of the transmembrane domain, we only show the protein feature retention information of those transmembrane features


* Minus value of BPloci means that the break point is located before the CDS.
- In-frame and retained 'Transmembrane'.
PartnerGeneHbpTbpENSTStrandBPexonTotalExonProtein feature loci*BPlociTotalLenProtein featureProtein feature note

check button Subcellular localization prediction of the transmembrane domain retained fusion proteins
* We used DeepLoc 1.0. The order of the X-axis of the barplot is as follows: Entry_ID, Localization, Type, Nucleus, Cytoplasm, Extracellular, Mitochondrion, Cell_membrane, Endoplasmic_reticulum, Plastid, Golgi.apparatus, Lysosome.Vacuole, Peroxisome. Y-axis is the output score of DeepLoc. Clicking the image will open a new tab with a large image.
HgeneHchrHbpHenstTgeneTchrTbpTenstDeepLoc result

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Related Drugs to FRMD3-BRD4

check button Drugs used for this fusion-positive patient.
(Manual curation of PubMed, 04-30-2022 + MyCancerGenome)
HgeneTgeneDrugSourcePMID

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Related Diseases to FRMD3-BRD4

check button Diseases that have this fusion gene.
(Manual curation of PubMed, 04-30-2022 + MyCancerGenome)
HgeneTgeneDiseaseSourcePMID

check button Diseases associated with fusion partners.
(DisGeNet 4.0)
PartnerGeneDisease IDDisease name# pubmedsSource
TgeneBRD4C0017636Glioblastoma2CTD_human
TgeneBRD4C0334588Giant Cell Glioblastoma2CTD_human
TgeneBRD4C1621958Glioblastoma Multiforme2CTD_human
TgeneBRD4C0002170Alopecia1CTD_human
TgeneBRD4C0007102Malignant tumor of colon1CTD_human
TgeneBRD4C0009375Colonic Neoplasms1CTD_human
TgeneBRD4C0018798Congenital Heart Defects1GENOMICS_ENGLAND
TgeneBRD4C0019193Hepatitis, Toxic1CTD_human
TgeneBRD4C0020507Hyperplasia1CTD_human
TgeneBRD4C0020542Pulmonary Hypertension1CTD_human
TgeneBRD4C0025149Medulloblastoma1CTD_human
TgeneBRD4C0025958Microcephaly1GENOMICS_ENGLAND
TgeneBRD4C0029463Osteosarcoma1CTD_human
TgeneBRD4C0033578Prostatic Neoplasms1CTD_human
TgeneBRD4C0040136Thyroid Neoplasm1CTD_human
TgeneBRD4C0085413Polycystic Kidney, Autosomal Dominant1CTD_human
TgeneBRD4C0086873Pseudopelade1CTD_human
TgeneBRD4C0151468Thyroid Gland Follicular Adenoma1CTD_human
TgeneBRD4C0162311Androgenetic Alopecia1CTD_human
TgeneBRD4C0205833Medullomyoblastoma1CTD_human
TgeneBRD4C0263477Female pattern alopecia (disorder)1CTD_human
TgeneBRD4C0270972Cornelia De Lange Syndrome1CTD_human
TgeneBRD4C0278510Childhood Medulloblastoma1CTD_human
TgeneBRD4C0278876Adult Medulloblastoma1CTD_human
TgeneBRD4C0376358Malignant neoplasm of prostate1CTD_human
TgeneBRD4C0549473Thyroid carcinoma1CTD_human
TgeneBRD4C0751291Desmoplastic Medulloblastoma1CTD_human
TgeneBRD4C0860207Drug-Induced Liver Disease1CTD_human
TgeneBRD4C0887850Polycystic Kidney, Type 1 Autosomal Dominant Disease1CTD_human
TgeneBRD4C1262760Hepatitis, Drug-Induced1CTD_human
TgeneBRD4C1275668Melanotic medulloblastoma1CTD_human
TgeneBRD4C1707291NUT midline carcinoma1ORPHANET
TgeneBRD4C1802395Congenital muscular hypertrophy-cerebral syndrome1CTD_human
TgeneBRD4C1853099Cornelia de Lange Syndrome 31CTD_human
TgeneBRD4C2751306Polycystic kidney disease, type 21CTD_human
TgeneBRD4C3658290Drug-Induced Acute Liver Injury1CTD_human
TgeneBRD4C3714756Intellectual Disability1GENOMICS_ENGLAND
TgeneBRD4C4025871Abnormality of the face1GENOMICS_ENGLAND
TgeneBRD4C4083212Alopecia, Male Pattern1CTD_human
TgeneBRD4C4277682Chemical and Drug Induced Liver Injury1CTD_human
TgeneBRD4C4279912Chemically-Induced Liver Toxicity1CTD_human
TgeneBRD4C4551851Cornelia de Lange Syndrome 11CTD_human