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	Fusion Gene Summary
	Fusion Gene ORF analysis
	Fusion Genomic Features
	Fusion Protein Features
	Fusion Gene Sequence
	Fusion Gene PPI analysis
	Related Drugs
	Related Diseases

Fusion gene:SPARC-DTL (FusionGDB2 ID:85489)

Fusion Gene Summary for SPARC-DTL

Fusion gene summary

Fusion gene information	Fusion gene name: SPARC-DTL
	Fusion gene ID: 85489
		Hgene	Tgene
	Gene symbol	SPARC	DTL
	Gene ID	6678	51514
	Gene name	secreted protein acidic and cysteine rich	denticleless E3 ubiquitin protein ligase homolog
	Synonyms	BM-40\|OI17\|ON\|ONT	CDT2\|DCAF2\|L2DTL\|RAMP
	Cytomap	5q33.1	1q32.3
	Type of gene	protein-coding	protein-coding
	Description	SPARCbasement-membrane protein 40secreted protein, acidic, cysteine-rich (osteonectin)	denticleless protein homologDDB1- and CUL4-associated factor 2RA-regulated nuclear matrix-associated proteinlethal(2) denticleless protein homologretinoic acid-regulated nuclear matrix-associated protein
	Modification date	20200329	20200320
	UniProtAcc	SPARC	Q9NZJ0
	Ensembl transtripts involved in fusion gene	ENST00000231061, ENST00000537849,	ENST00000366991, ENST00000475419, ENST00000542077,
Fusion gene scores	* DoF score	39 X 30 X 11=12870	5 X 6 X 4=120
	# samples	47	6
	** MAII score	log2(47/12870*10)=-4.77520748654306 possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs). DoF>8 and MAII<0	log2(6/120*10)=-1 possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs). DoF>8 and MAII<0
Context	PubMed: SPARC [Title/Abstract] AND DTL [Title/Abstract] AND fusion [Title/Abstract]
Most frequent breakpoint	SPARC(151042005)-DTL(212252520), # samples:2
Anticipated loss of major functional domain due to fusion event.

* DoF score (Degree of Frequency) = # partners X # break points X # cancer types
** MAII score (Major Active Isofusion Index) = log2(# samples/DoF score*10)

Gene ontology of each fusion partner gene with evidence of Inferred from Direct Assay (IDA) from Entrez

Partner	Gene	GO ID	GO term	PubMed ID
Hgene	SPARC	GO:0001937	negative regulation of endothelial cell proliferation	12867428
Hgene	SPARC	GO:0010595	positive regulation of endothelial cell migration	12867428
Hgene	SPARC	GO:0016525	negative regulation of angiogenesis	12867428
Hgene	SPARC	GO:0022604	regulation of cell morphogenesis	15389586
Tgene	DTL	GO:0000209	protein polyubiquitination	18794347
Tgene	DTL	GO:0006511	ubiquitin-dependent protein catabolic process	18794347
Tgene	DTL	GO:0006513	protein monoubiquitination	20129063
Tgene	DTL	GO:0006974	cellular response to DNA damage stimulus	20129063
Tgene	DTL	GO:0009411	response to UV	18794347
Tgene	DTL	GO:0019985	translesion synthesis	20129063

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

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

Fusion gene information from two resources (ChiTars 5.0 and ChimerDB 4.0)
* All genome coordinats were lifted-over on hg19.
* Click on the break point to see the gene structure around the break point region using the UCSC Genome Browser.

Source	Disease	Sample	Hgene	Hchr	Hbp	Hstrand	Tgene	Tchr	Tbp	Tstrand
ChiTaRS5.0	N/A	AW022643	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
ChiTaRS5.0	N/A	DL127885	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
ChiTaRS5.0	N/A	DM112996	SPARC	chr5	151042005	-	DTL	chr1	212252520	-

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Fusion Gene ORF analysis for SPARC-DTL

Open reading frame (ORF) analsis of fusion genes based on Ensembl gene isoform structure.
* Click on the break point to see the gene structure around the break point region using the UCSC Genome Browser.

ORF	Henst	Tenst	Hgene	Hchr	Hbp	Hstrand	Tgene	Tchr	Tbp	Tstrand
intron-intron	ENST00000231061	ENST00000366991	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000231061	ENST00000366991	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
intron-intron	ENST00000231061	ENST00000475419	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000231061	ENST00000475419	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
intron-intron	ENST00000231061	ENST00000542077	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000231061	ENST00000542077	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000366991	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000366991	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000475419	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000475419	SPARC	chr5	151042005	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000542077	SPARC	chr5	151042001	-	DTL	chr1	212252520	-
intron-intron	ENST00000537849	ENST00000542077	SPARC	chr5	151042005	-	DTL	chr1	212252520	-

ORFfinder result based on the fusion transcript sequence of in-frame fusion genes.

Henst

Tenst

Hgene

Hchr

Hbp

Hstrand

Tgene

Tchr

Tbp

Tstrand

Seq length
(transcript)

BP loci
(transcript)

Predicted start
(transcript)

Predicted stop
(transcript)

Seq length
(amino acids)

DeepORF 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.

Henst

Tenst

Hgene

Hchr

Hbp

Hstrand

Tgene

Tchr

Tbp

Tstrand

No-coding score

Coding score

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Fusion Genomic Features for SPARC-DTL

FusionAI prediction of the potential fusion gene breakpoint based on the pre-mature RNA sequence context (+/- 5kb of individual partner genes, total 20kb length sequence). FusionAI is a fusion gene breakpoint classifier based on convolutional neural network by comparing the fusion positive and negative sequence context of ~ 20K fusion gene data. From here, we can have the relative potentency of the 20K genomic sequence how individual sequnce will be likely used as the gene fusion breakpoints.

Hgene

Hchr

Hbp

Hstrand

Tgene

Tchr

Tbp

Tstrand

1-p

p (fusion gene breakpoint)

Distribution of 44 human genomic features loci across 20kb length fusion breakpoint regions. We integrated a total of 44 different types of human genomic feature loci information across five big categories including virus integration sites, repeats, structural variants, chromatin states, and gene expression regulation. More details are in help page.

Distribution of 44 human genomic features loci across 20kb length fusion breakpoint regions that are ovelapped with the top 1% feature importance score regions. More details are in help page.

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Fusion Protein Features for SPARC-DTL

Four levels of functional features of fusion genes
Go to FGviewer search page for the most frequent breakpoint (https://ccsmweb.uth.edu/FGviewer/:151042005/:212252520)
- 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.

Main function of each fusion partner protein. (from UniProt)

Hgene	Tgene
SPARC SPARC	DTL Q9NZJ0
664	FUNCTION: Substrate-specific adapter of a DCX (DDB1-CUL4-X-box) E3 ubiquitin-protein ligase complex required for cell cycle control, DNA damage response and translesion DNA synthesis. The DCX(DTL) complex, also named CRL4(CDT2) complex, mediates the polyubiquitination and subsequent degradation of CDT1, CDKN1A/p21(CIP1), FBH1, KMT5A and SDE2 (PubMed:16861906, PubMed:16949367, PubMed:16964240, PubMed:17085480, PubMed:18703516, PubMed:18794347, PubMed:18794348, PubMed:19332548, PubMed:20129063, PubMed:23478441, PubMed:23478445, PubMed:23677613, PubMed:27906959). CDT1 degradation in response to DNA damage is necessary to ensure proper cell cycle regulation of DNA replication (PubMed:16861906, PubMed:16949367, PubMed:17085480). CDKN1A/p21(CIP1) degradation during S phase or following UV irradiation is essential to control replication licensing (PubMed:18794348, PubMed:19332548). KMT5A degradation is also important for a proper regulation of mechanisms such as TGF-beta signaling, cell cycle progression, DNA repair and cell migration (PubMed:23478445). Most substrates require their interaction with PCNA for their polyubiquitination: substrates interact with PCNA via their PIP-box, and those containing the 'K+4' motif in the PIP box, recruit the DCX(DTL) complex, leading to their degradation. In undamaged proliferating cells, the DCX(DTL) complex also promotes the 'Lys-164' monoubiquitination of PCNA, thereby being involved in PCNA-dependent translesion DNA synthesis (PubMed:20129063, PubMed:23478441, PubMed:23478445, PubMed:23677613). The DDB1-CUL4A-DTL E3 ligase complex regulates the circadian clock function by mediating the ubiquitination and degradation of CRY1 (PubMed:26431207). {ECO:0000269\|PubMed:16861906, ECO:0000269\|PubMed:16949367, ECO:0000269\|PubMed:16964240, ECO:0000269\|PubMed:17085480, ECO:0000269\|PubMed:18703516, ECO:0000269\|PubMed:18794347, ECO:0000269\|PubMed:18794348, ECO:0000269\|PubMed:19332548, ECO:0000269\|PubMed:20129063, ECO:0000269\|PubMed:23478441, ECO:0000269\|PubMed:23478445, ECO:0000269\|PubMed:23677613, ECO:0000269\|PubMed:26431207, ECO:0000269\|PubMed:27906959}.

Retention 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, because of limited space for viewing, we only show the protein feature retention information belong to the 13 regional features. All retention annotation result can be downloaded at
download page

* Minus value of BPloci means that the break pointn is located before the CDS.

- In-frame and retained protein feature among the 13 regional features.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Protein feature

Protein feature note

- In-frame and not-retained protein feature among the 13 regional features.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Protein feature

Protein feature note

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Fusion Gene Sequence for SPARC-DTL

For in-frame fusion transcripts, we provide the fusion transcript sequences and fusion amino acid sequences. To have fusion amino acid sequence, we ran ORFfinder and chose the longest ORF among the all predicted ones.

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Fusion Gene PPI Analysis for SPARC-DTL

Go to ChiPPI (Chimeric Protein-Protein interactions) to see the chimeric PPI interaction in
ChiPPI page.

Protein-protein interactors with each fusion partner protein in wild-type (BIOGRID-3.4.160)

Hgene

Hgene's interactors

Tgene

Tgene's interactors

- Retained PPIs in in-frame fusion.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Still interaction with

- Lost PPIs in in-frame fusion.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Interaction lost with

- Retained PPIs, but lost function due to frame-shift fusion.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Interaction lost with

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Related Drugs for SPARC-DTL

Drugs targeting genes involved in this fusion gene.
(DrugBank Version 5.1.8 2021-05-08)

Partner

Gene

UniProtAcc

DrugBank ID

Drug name

Drug activity

Drug type

Drug status

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Related Diseases for SPARC-DTL

Diseases associated with fusion partners.
(DisGeNet 4.0)

Partner

Gene

Disease ID

Disease name

# pubmeds

Source