FusionNeoAntigen Logo

Home

Download

Statistics

Examples

Help

Contact

Terms of Use

Center for Computational Systems Medicine
leaf

Fusion Gene and Fusion Protein Summary

leaf

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

leaf

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

leaf

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

leaf

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

leaf

Fusion Breakpoint 14 AA Peptide Structure - (RoseTTAFold)

leaf

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

leaf

Vaccine Design for the FusionNeoAntigens (RNA/protein sequences)

leaf

Potential target of CAR-T therapy development

leaf

Information on the samples that have these potential fusion neoantigens

leaf

Fusion Protein Targeting Drugs - (Manual Curation)

leaf

Fusion Protein Related diseases - (Manual Curation)

Fusion Protein:PDCD4-CHD1L

Fusion Gene and Fusion Protein Summary

check button Fusion gene summary
Fusion partner gene informationFusion gene name: PDCD4-CHD1L
FusionPDB ID: 63596
FusionGDB2.0 ID: 63596
HgeneTgene
Gene symbol

PDCD4

CHD1L

Gene ID

27250

9557

Gene nameprogrammed cell death 4chromodomain helicase DNA binding protein 1 like
SynonymsH731ALC1|CHDL
Cytomap

10q25.2

1q21.1

Type of geneprotein-codingprotein-coding
Descriptionprogrammed cell death protein 4neoplastic transformation inhibitor proteinnuclear antigen H731programmed cell death 4 (neoplastic transformation inhibitor)protein 197/15achromodomain-helicase-DNA-binding protein 1-likeamplified in liver cancer 1amplified in liver cancer protein 1
Modification date2020032920200313
UniProtAcc.

Q86WJ1

Main function of 5'-partner protein: FUNCTION: DNA helicase which plays a role in chromatin-remodeling following DNA damage (PubMed:19661379, PubMed:29220653). Targeted to sites of DNA damage through interaction with poly(ADP-ribose) and functions to regulate chromatin during DNA repair (PubMed:19661379). Able to catalyze nucleosome sliding in an ATP-dependent manner (PubMed:19661379). Helicase activity is strongly stimulated upon poly(ADP-ribose)-binding (PubMed:19661379, PubMed:29220653). {ECO:0000269|PubMed:19661379, ECO:0000269|PubMed:29220653}.
Ensembl transtripts involved in fusion geneENST idsENST00000280154, ENST00000393104, 
ENST00000481353, 
ENST00000361293, 
ENST00000467213, ENST00000369258, 
ENST00000369259, ENST00000431239, 
Fusion gene scores for assessment (based on all fusion genes of FusionGDB 2.0)* DoF score9 X 10 X 1=9010 X 11 X 5=550
# samples 1014
** MAII scorelog2(10/90*10)=0.15200309344505
effective Gene in Pan-Cancer Fusion Genes (eGinPCFGs).
DoF>8 and MAII>0
log2(14/550*10)=-1.97400479146706
possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs).
DoF>8 and MAII<0
Fusion gene context

PubMed: PDCD4 [Title/Abstract] AND CHD1L [Title/Abstract] AND fusion [Title/Abstract]

Fusion neoantigen context

PubMed: PDCD4 [Title/Abstract] AND CHD1L [Title/Abstract] AND neoantigen [Title/Abstract]

Most frequent breakpoint (based on all fusion genes of FusionGDB 2.0)PDCD4(112635830)-CHD1L(146747014), # samples:1
Anticipated loss of major functional domain due to fusion event.PDCD4-CHD1L 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.
PDCD4-CHD1L 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.
PDCD4-CHD1L 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.
PDCD4-CHD1L 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
HgenePDCD4

GO:0007569

cell aging

12054647

HgenePDCD4

GO:0030509

BMP signaling pathway

18548003

HgenePDCD4

GO:0045892

negative regulation of transcription, DNA-templated

16357133

HgenePDCD4

GO:1905064

negative regulation of vascular smooth muscle cell differentiation

18548003

TgeneCHD1L

GO:0006338

chromatin remodeling

19661379

TgeneCHD1L

GO:0006974

cellular response to DNA damage stimulus

19661379



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/chr10:112635830/chr1:146747014)
- 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 PDCD4 (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 CHD1L (3'-gene)
* Click on the image to open the UCSC genome browser with custom track showing this image in a new window.
all structure


Top

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)
ENST00000280154PDCD4chr10112635830+ENST00000431239CHD1Lchr1146747014+19923172741740488
ENST00000280154PDCD4chr10112635830+ENST00000369259CHD1Lchr1146747014+19923172741740488
ENST00000280154PDCD4chr10112635830+ENST00000369258CHD1Lchr1146747014+19943172741740488

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
ENST00000280154ENST00000431239PDCD4chr10112635830+CHD1Lchr1146747014+0.0013509430.99864906
ENST00000280154ENST00000369259PDCD4chr10112635830+CHD1Lchr1146747014+0.0013509430.99864906
ENST00000280154ENST00000369258PDCD4chr10112635830+CHD1Lchr1146747014+0.0013355910.9986644

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

Top

Fusion Protein Breakpoint Sequences for PDCD4-CHD1L

check button +/-13 AA sequence from the breakpoints of the fusion protein sequences.
HgeneHchrHbpTgeneTchrTbpLength(fusion protein)BP in fusion proteinPeptide
PDCD4chr10112635830CHD1Lchr114674701431714DVENEQILNVNPAGGVGMNLTAADTV

Top

Potential FusionNeoAntigen Information of PDCD4-CHD1L 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.
PDCD4-CHD1L_112635830_146747014.msa

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)
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B35:03NPAGGVGMNL0.90240.79931020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B35:02NPAGGVGMNL0.8010.85951020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B35:04NPAGGVGMNL0.8010.85951020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B81:01NPAGGVGMNL0.70070.50121020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B82:01NPAGGVGMNL0.53570.51611020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B35:12NPAGGVGMNL0.8010.85951020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B39:10NPAGGVGMNL0.77890.92411020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B42:01NPAGGVGMNL0.70990.79741020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B35:09NPAGGVGMNL0.8010.85951020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B67:01NPAGGVGMNL0.76530.91341020
PDCD4-CHD1Lchr10112635830chr1146747014317HLA-B82:02NPAGGVGMNL0.53570.51611020

Top

Potential FusionNeoAntigen Information of PDCD4-CHD1L 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.
PDCD4-CHD1L_112635830_146747014.msa

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)
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0338EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0415ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0415NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0436ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0436NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0458NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-0458ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB1-1448EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0201EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0201NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0201ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0201QILNVNPAGGVGMNL520
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0202EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0202NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0202ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0204EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0204NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0204ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0205EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0209EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0209NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0209ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0209QILNVNPAGGVGMNL520
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0210EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0210NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0210ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0211EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0211NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0212EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0212NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0212ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0213EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0214EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0214NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0214ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0215EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0215NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0215ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0216EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0216NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0216ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0217EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0217NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0217ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0218EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0218NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0218ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0219EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0219NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0220EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0220NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0220ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0221EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0221NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0221ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0221QILNVNPAGGVGMNL520
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0222EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0222NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0223EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0223NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0223ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0224EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0224NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0224ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0224QILNVNPAGGVGMNL520
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0225EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0225NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0225ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0301EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0301NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0301ENEQILNVNPAGGVG217
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0301QILNVNPAGGVGMNL520
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0303EQILNVNPAGGVGMN419
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0303NEQILNVNPAGGVGM318
PDCD4-CHD1Lchr10112635830chr1146747014317DRB3-0303ENEQILNVNPAGGVG217

Top

Fusion breakpoint peptide structures of PDCD4-CHD1L

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.
File nameBPseqHgeneTgeneHchrHbpTchrTbpAAlen
3806ILNVNPAGGVGMNLPDCD4CHD1Lchr10112635830chr1146747014317

Top

Filtering FusionNeoAntigens Through Checking the Interaction with HLAs in 3D of PDCD4-CHD1L

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
HLA-B14:023BVN3806ILNVNPAGGVGMNL-7.9962-8.1096
HLA-B14:023BVN3806ILNVNPAGGVGMNL-5.70842-6.74372
HLA-B52:013W393806ILNVNPAGGVGMNL-6.83737-6.95077
HLA-B52:013W393806ILNVNPAGGVGMNL-4.4836-5.5189
HLA-A11:014UQ23806ILNVNPAGGVGMNL-10.0067-10.1201
HLA-A11:014UQ23806ILNVNPAGGVGMNL-9.03915-10.0745
HLA-A24:025HGA3806ILNVNPAGGVGMNL-6.56204-6.67544
HLA-A24:025HGA3806ILNVNPAGGVGMNL-5.42271-6.45801
HLA-B44:053DX83806ILNVNPAGGVGMNL-7.85648-8.89178
HLA-B44:053DX83806ILNVNPAGGVGMNL-5.3978-5.5112
HLA-A02:016TDR3806ILNVNPAGGVGMNL-3.37154-4.40684

Top

Vaccine Design for the FusionNeoAntigens of PDCD4-CHD1L

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
PDCD4-CHD1Lchr10112635830chr11467470141020NPAGGVGMNLACCCTGCAGGTGGAGTTGGCATGAACTTAA

check button mRNA and peptide sequences of FusionNeoAntigens that have potential interaction with HLA-IIs.
Fusion geneHchrHbpTchrTbpStart in +/-13AAEnd in +/-13AAFusionNeoAntigen peptideFusionNEoAntigen RNA sequence
PDCD4-CHD1Lchr10112635830chr1146747014217ENEQILNVNPAGGVGAAAATGAGCAGATACTGAATGTAAACCCTGCAGGTGGAGTTGGCA
PDCD4-CHD1Lchr10112635830chr1146747014318NEQILNVNPAGGVGMATGAGCAGATACTGAATGTAAACCCTGCAGGTGGAGTTGGCATGA
PDCD4-CHD1Lchr10112635830chr1146747014419EQILNVNPAGGVGMNAGCAGATACTGAATGTAAACCCTGCAGGTGGAGTTGGCATGAACT
PDCD4-CHD1Lchr10112635830chr1146747014520QILNVNPAGGVGMNLAGATACTGAATGTAAACCCTGCAGGTGGAGTTGGCATGAACTTAA

Top

Information of the samples that have these potential fusion neoantigens of PDCD4-CHD1L

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
N/APDCD4-CHD1Lchr10112635830ENST00000280154chr1146747014ENST00000369258DA689020

Top

Potential target of CAR-T therapy development for PDCD4-CHD1L

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

Top

Related Drugs to PDCD4-CHD1L

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

Top

Related Diseases to PDCD4-CHD1L

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