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Fusion Protein:PARK2-PACRG

Fusion Gene and Fusion Protein Summary

Fusion gene summary

Fusion partner gene information	Fusion gene name: PARK2-PACRG
	FusionPDB ID: 62754
	FusionGDB2.0 ID: 62754
		Hgene	Tgene
	Gene symbol	PARK2	PACRG
	Gene ID	5071	135138
	Gene name	parkin RBR E3 ubiquitin protein ligase	parkin coregulated
	Synonyms	AR-JP\|LPRS2\|PARK2\|PDJ	GLUP\|HAK005771\|PACRG2.1\|PARK2CRG
	Cytomap	6q26	6q26
	Type of gene	protein-coding	protein-coding
	Description	E3 ubiquitin-protein ligase parkinParkinson disease (autosomal recessive, juvenile) 2, parkinparkinson juvenile disease protein 2parkinson protein 2 E3 ubiquitin protein ligaseparkinson protein 2, E3 ubiquitin protein ligase (parkin)	parkin coregulated gene proteinPARK2 co-regulatedPARK2 coregulatedmolecular chaperone/chaperonin-binding proteinparkin co-regulated gene protein
	Modification date	20200329	20200313
	UniProtAcc	.	PACRGL Main function of 5'-partner protein: 248
Ensembl transtripts involved in fusion gene	ENST ids	ENST00000366892, ENST00000366896, ENST00000366897, ENST00000366898, ENST00000338468, ENST00000366894,	ENST00000542669, ENST00000337019, ENST00000366888, ENST00000366889,
Fusion gene scores for assessment (based on all fusion genes of FusionGDB 2.0)	* DoF score	20 X 15 X 7=2100	13 X 11 X 13=1859
	# samples	21	19
	** MAII score	log2(21/2100*10)=-3.32192809488736 possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs). DoF>8 and MAII<0	log2(19/1859*10)=-3.29045544658853 possibly effective Gene in Pan-Cancer Fusion Genes (peGinPCFGs). DoF>8 and MAII<0
Fusion gene context	PubMed: PARK2 [Title/Abstract] AND PACRG [Title/Abstract] AND fusion [Title/Abstract]
Fusion neoantigen context	PubMed: PARK2 [Title/Abstract] AND PACRG [Title/Abstract] AND neoantigen [Title/Abstract]
Most frequent breakpoint (based on all fusion genes of FusionGDB 2.0)	PARK2(163148694)-PACRG(163235179), # samples:2
Anticipated loss of major functional domain due to fusion event.	PARK2-PACRG 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. PARK2-PACRG 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)

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	PARK2	GO:0000209	protein polyubiquitination	12150907\|16227987\|18541373\|19880420
Hgene	PARK2	GO:0000422	autophagy of mitochondrion	25621951
Hgene	PARK2	GO:0001933	negative regulation of protein phosphorylation	17512523
Hgene	PARK2	GO:0006511	ubiquitin-dependent protein catabolic process	12925569\|17097639
Hgene	PARK2	GO:0006513	protein monoubiquitination	20889974
Hgene	PARK2	GO:0010506	regulation of autophagy	20889974
Hgene	PARK2	GO:0010821	regulation of mitochondrion organization	21113145
Hgene	PARK2	GO:0016567	protein ubiquitination	10973942\|11439185\|12628165\|17314283
Hgene	PARK2	GO:0031648	protein destabilization	19591802\|29311685
Hgene	PARK2	GO:0032232	negative regulation of actin filament bundle assembly	17512523
Hgene	PARK2	GO:0033132	negative regulation of glucokinase activity	24187134
Hgene	PARK2	GO:0043123	positive regulation of I-kappaB kinase/NF-kappaB signaling	17314283\|19880420
Hgene	PARK2	GO:0043161	proteasome-mediated ubiquitin-dependent protein catabolic process	11439185\|21376232
Hgene	PARK2	GO:0043388	positive regulation of DNA binding	17314283
Hgene	PARK2	GO:0043524	negative regulation of neuron apoptotic process	12628165\|22511790\|23985028
Hgene	PARK2	GO:0044828	negative regulation by host of viral genome replication	25244949
Hgene	PARK2	GO:0045944	positive regulation of transcription by RNA polymerase II	23453807
Hgene	PARK2	GO:0046676	negative regulation of insulin secretion	24187134
Hgene	PARK2	GO:0051865	protein autoubiquitination	12628165\|15728840\|16352719\|17512523
Hgene	PARK2	GO:0060548	negative regulation of cell death	15603737
Hgene	PARK2	GO:0061734	parkin-mediated stimulation of mitophagy in response to mitochondrial depolarization	19029340
Hgene	PARK2	GO:0070534	protein K63-linked ubiquitination	15728840\|17314283\|19880420\|25621951
Hgene	PARK2	GO:0070936	protein K48-linked ubiquitination	21376232\|23858059
Hgene	PARK2	GO:0070979	protein K11-linked ubiquitination	25621951
Hgene	PARK2	GO:0085020	protein K6-linked ubiquitination	25621951
Hgene	PARK2	GO:0090090	negative regulation of canonical Wnt signaling pathway	19591802
Hgene	PARK2	GO:0090201	negative regulation of release of cytochrome c from mitochondria	19880420\|23453807
Hgene	PARK2	GO:0098779	positive regulation of mitophagy in response to mitochondrial depolarization	20457763
Hgene	PARK2	GO:0099074	mitochondrion to lysosome transport	24446486
Hgene	PARK2	GO:1900407	regulation of cellular response to oxidative stress	24446486
Hgene	PARK2	GO:1902236	negative regulation of endoplasmic reticulum stress-induced intrinsic apoptotic signaling pathway	11439185\|12150907\|23453807
Hgene	PARK2	GO:1903265	positive regulation of tumor necrosis factor-mediated signaling pathway	23453807
Hgene	PARK2	GO:1903377	negative regulation of oxidative stress-induced neuron intrinsic apoptotic signaling pathway	17314283
Hgene	PARK2	GO:1903599	positive regulation of autophagy of mitochondrion	26310625

Four levels of functional features of fusion genes
Go to FGviewer search page for the most frequent breakpoint (https://ccsmweb.uth.edu/FGviewer/chr6:163148694/chr6:163235179)
- 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.

Retention 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.

Fusion gene breakpoints across PARK2 (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 PACRG (3'-gene)
* Click on the image to open the UCSC genome browser with custom track showing this image in a new window.

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Fusion Amino Acid Sequences

Fusion information from ORFfinder translation from full-length transcript sequence from FusionPDB.

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)
ENST00000366898	PARK2	chr6	162864342	-	ENST00000337019	PACRG	chr6	163483182	+	1378	274	1	873	290
ENST00000366898	PARK2	chr6	162864342	-	ENST00000366889	PACRG	chr6	163483182	+	1262	274	1	756	251
ENST00000366898	PARK2	chr6	162864342	-	ENST00000366888	PACRG	chr6	163483182	+	1081	274	1	756	251
ENST00000366897	PARK2	chr6	162864342	-	ENST00000337019	PACRG	chr6	163483182	+	1378	274	1	873	290
ENST00000366897	PARK2	chr6	162864342	-	ENST00000366889	PACRG	chr6	163483182	+	1262	274	1	756	251
ENST00000366897	PARK2	chr6	162864342	-	ENST00000366888	PACRG	chr6	163483182	+	1081	274	1	756	251
ENST00000366896	PARK2	chr6	162864342	-	ENST00000337019	PACRG	chr6	163483182	+	1378	274	1	873	290
ENST00000366896	PARK2	chr6	162864342	-	ENST00000366889	PACRG	chr6	163483182	+	1262	274	1	756	251
ENST00000366896	PARK2	chr6	162864342	-	ENST00000366888	PACRG	chr6	163483182	+	1081	274	1	756	251
ENST00000366892	PARK2	chr6	162864342	-	ENST00000337019	PACRG	chr6	163483182	+	1371	267	36	866	276
ENST00000366892	PARK2	chr6	162864342	-	ENST00000366889	PACRG	chr6	163483182	+	1255	267	36	749	237
ENST00000366892	PARK2	chr6	162864342	-	ENST00000366888	PACRG	chr6	163483182	+	1074	267	36	749	237

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
ENST00000366898	ENST00000337019	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.003166073	0.996834
ENST00000366898	ENST00000366889	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.001930866	0.9980691
ENST00000366898	ENST00000366888	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.002748479	0.9972516
ENST00000366897	ENST00000337019	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.003166073	0.996834
ENST00000366897	ENST00000366889	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.001930866	0.9980691
ENST00000366897	ENST00000366888	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.002748479	0.9972516
ENST00000366896	ENST00000337019	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.003166073	0.996834
ENST00000366896	ENST00000366889	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.001930866	0.9980691
ENST00000366896	ENST00000366888	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.002748479	0.9972516
ENST00000366892	ENST00000337019	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.002938156	0.9970618
ENST00000366892	ENST00000366889	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.001570534	0.9984295
ENST00000366892	ENST00000366888	PARK2	chr6	162864342	-	PACRG	chr6	163483182	+	0.002225912	0.99777406

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 PARK2-PACRG

+/-13 AA sequence from the breakpoints of the fusion protein sequences.

Hgene	Hchr	Hbp	Tgene	Tchr	Tbp	Length(fusion protein)	BP in fusion protein	Peptide
PARK2	chr6	162864342	PACRG	chr6	163483182	267	76	IFAGKELRNDWTVQVEIEKLDYHHYL
PARK2	chr6	162864342	PACRG	chr6	163483182	274	90	IFAGKELRNDWTVQVEIEKLDYHHYL

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Potential FusionNeoAntigen Information of PARK2-PACRG in HLA I

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.

PARK2-PACRG_162864342_163483182.msa

Potential FusionNeoAntigen Information
* We used NetMHCpan v4.1 (%rank<0.5) and deepHLApan v1.1 (immunogenic score>0.5)

Fusion gene	Hchr	Hbp	Tgene	Tchr	Tbp	HLA I	FusionNeoAntigen peptide	Binding score	Immunogenic score	Neoantigen start (at BP 13)	Neoantigen end (at BP 13)
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B52:01	VQVEIEKL	0.9397	0.8567	12	20
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:13	VQVEIEKL	0.7981	0.8063	12	20
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:02	LRNDWTVQV	0.9989	0.5067	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:04	LRNDWTVQV	0.9988	0.6414	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:05	LRNDWTVQV	0.9987	0.7499	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:06	LRNDWTVQV	0.9974	0.9714	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B14:01	LRNDWTVQV	0.9965	0.9743	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B14:02	LRNDWTVQV	0.9965	0.9743	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:24	LRNDWTVQV	0.9959	0.8422	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:01	VQVEIEKLDY	0.9996	0.793	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:25	VQVEIEKLDY	0.9511	0.842	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-A02:19	ELRNDWTVQV	0.4493	0.7835	5	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:14	LRNDWTVQV	0.9989	0.7615	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B73:01	LRNDWTVQV	0.9957	0.9695	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:12	LRNDWTVQV	0.9955	0.9772	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:05	LRNDWTVQV	0.9808	0.9766	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:95	LRNDWTVQV	0.9555	0.9017	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:27	LRNDWTVQV	0.9549	0.9765	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:03	LRNDWTVQV	0.9399	0.7689	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:29	LRNDWTVQV	0.9249	0.9672	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:13	LRNDWTVQV	0.8677	0.9553	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B51:07	NDWTVQVEI	0.854	0.9534	8	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:46	LRNDWTVQV	0.8298	0.959	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:10	LRNDWTVQV	0.8293	0.9848	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:80	LRNDWTVQV	0.8207	0.9822	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:67	LRNDWTVQV	0.8207	0.9822	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:19	LRNDWTVQV	0.8082	0.9056	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C06:03	LRNDWTVQV	0.156	0.998	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C12:16	LRNDWTVQV	0.0126	0.9826	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:07	VQVEIEKLDY	0.9985	0.5841	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:05	VQVEIEKLDY	0.9298	0.7985	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:02	VQVEIEKL	0.9022	0.7999	12	20
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:09	LRNDWTVQV	0.999	0.7505	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:06	LRNDWTVQV	0.999	0.6987	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:08	LRNDWTVQV	0.9988	0.6423	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:10	LRNDWTVQV	0.9987	0.7771	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B39:31	LRNDWTVQV	0.9957	0.977	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:01	LRNDWTVQV	0.9613	0.8396	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C18:01	LRNDWTVQV	0.9213	0.9447	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:17	LRNDWTVQV	0.8999	0.9866	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C06:08	LRNDWTVQV	0.887	0.9965	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:02	LRNDWTVQV	0.8207	0.9822	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:04	LRNDWTVQV	0.7414	0.9548	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C06:06	LRNDWTVQV	0.7366	0.9926	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C07:22	LRNDWTVQV	0.7106	0.8926	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C06:02	LRNDWTVQV	0.0895	0.9976	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-C06:17	LRNDWTVQV	0.0895	0.9976	6	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:34	VQVEIEKLDY	0.9996	0.793	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:27	VQVEIEKLDY	0.9996	0.8157	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:125	VQVEIEKLDY	0.9996	0.793	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:33	VQVEIEKLDY	0.9996	0.793	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:135	VQVEIEKLDY	0.9995	0.7937	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:50	VQVEIEKLDY	0.9993	0.7026	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:24	VQVEIEKLDY	0.9984	0.7754	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:35	VQVEIEKLDY	0.9978	0.7762	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:53	VQVEIEKLDY	0.9978	0.7369	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:12	VQVEIEKLDY	0.9967	0.7499	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:54	VQVEIEKLDY	0.9883	0.713	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:39	VQVEIEKLDY	0.9557	0.7172	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B15:20	VQVEIEKLDY	0.9286	0.8677	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B35:28	VQVEIEKLDY	0.9044	0.8698	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-A69:01	ELRNDWTVQV	0.8728	0.9289	5	15
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B48:02	VQVEIEKLDY	0.7502	0.8534	12	22
PARK2-PACRG	chr6	162864342	chr6	163483182	267	HLA-B27:09	KELRNDWTVQV	0.9933	0.9089	4	15

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Potential FusionNeoAntigen Information of PARK2-PACRG in HLA II

PARK2-PACRG_162864342_163483182.msa

Potential FusionNeoAntigen Information
* We used NetMHCIIpan v4.1 (%rank<0.5).

Fusion gene	Hchr	Hbp	Tgene	Tchr	Tbp	HLA II	FusionNeoAntigen peptide	Neoantigen start (at BP 13)	Neoantigen end (at BP 13)
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0310	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0326	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0338	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0342	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0342	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0422	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-0422	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1201	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1203	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1205	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1206	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1207	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1208	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1210	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1211	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1212	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1214	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1217	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1476	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1479	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1525	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB1-1525	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0101	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0101	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0101	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0104	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0104	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0104	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0105	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0105	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0105	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0108	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0108	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0108	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0109	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0111	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0111	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0111	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0112	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0112	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0112	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0113	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0113	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0113	FAGKELRNDWTVQVE	1	16
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0114	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0114	AGKELRNDWTVQVEI	2	17
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0204	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0301	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB3-0303	GKELRNDWTVQVEIE	3	18
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0101	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0101	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0101	DWTVQVEIEKLDYHH	9	24
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0103	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0103	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0103	DWTVQVEIEKLDYHH	9	24
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0104	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0104	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0104	DWTVQVEIEKLDYHH	9	24
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0106	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0106	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0106	DWTVQVEIEKLDYHH	9	24
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0107	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0107	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0107	DWTVQVEIEKLDYHH	9	24
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0108	WTVQVEIEKLDYHHY	10	25
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0108	TVQVEIEKLDYHHYL	11	26
PARK2-PACRG	chr6	162864342	chr6	163483182	267	DRB4-0108	DWTVQVEIEKLDYHH	9	24

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Fusion breakpoint peptide structures of PARK2-PACRG

3D 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 name	BPseq	Hgene	Tgene	Hchr	Hbp	Tchr	Tbp	AAlen
5538	LRNDWTVQVEIEKL	PARK2	PACRG	chr6	162864342	chr6	163483182	267

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Filtering FusionNeoAntigens Through Checking the Interaction with HLAs in 3D of PARK2-PACRG

Virtual screening between 25 HLAs (from PDB) and FusionNeoAntigens
* We used Glide to predict the interaction between HLAs and neoantigens.

HLA allele	PDB ID	File name	BPseq	Docking score	Glide score
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-9.4281	-9.6469
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-7.76688	-7.98568
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-6.2022	-8.3012
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-6.14062	-8.23962
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-5.65086	-6.42956
HLA-B14:02	3BVN	5538	LRNDWTVQVEIEKL	-5.35296	-6.13166
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-7.00686	-7.22566
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-6.52655	-6.74535
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-6.50505	-7.28375
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-5.74553	-7.84453
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-4.97091	-5.74961
HLA-B52:01	3W39	5538	LRNDWTVQVEIEKL	-4.90249	-7.00149
HLA-A11:01	4UQ2	5538	LRNDWTVQVEIEKL	-9.64906	-9.86786
HLA-A11:01	4UQ2	5538	LRNDWTVQVEIEKL	-6.30103	-6.51983
HLA-A11:01	4UQ2	5538	LRNDWTVQVEIEKL	-4.36837	-5.14707
HLA-A11:01	4UQ2	5538	LRNDWTVQVEIEKL	-2.41335	-4.51235
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-7.58503	-7.80383
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-6.61296	-6.83176
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-6.17421	-8.27321
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-6.07857	-6.85727
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-4.9658	-5.7445
HLA-A24:02	5HGA	5538	LRNDWTVQVEIEKL	-4.01973	-6.11873
HLA-B27:05	6PYJ	5538	LRNDWTVQVEIEKL	-3.16581	-3.38461
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-10.1677	-10.3865
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-7.6956	-9.7946
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-7.2116	-7.9903
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-5.76025	-6.53895
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-5.46695	-5.68575
HLA-B44:05	3DX8	5538	LRNDWTVQVEIEKL	-4.06081	-6.15981
HLA-A02:01	6TDR	5538	LRNDWTVQVEIEKL	-3.36956	-3.58836

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Vaccine Design for the FusionNeoAntigens of PARK2-PACRG

mRNA and peptide sequences of FusionNeoAntigens that have potential interaction with HLA-Is.

Fusion gene	Hchr	Hbp	Tchr	Tbp	Start in +/-13AA	End in +/-13AA	FusionNeoAntigen peptide sequence	FusionNeoAntigen RNA sequence
PARK2-PACRG	chr6	162864342	chr6	163483182	12	20	VQVEIEKL	CAGGTAGAAATTGAGAAGCTGGAT
PARK2-PACRG	chr6	162864342	chr6	163483182	12	22	VQVEIEKLDY	CAGGTAGAAATTGAGAAGCTGGATTACCAT
PARK2-PACRG	chr6	162864342	chr6	163483182	4	15	KELRNDWTVQV	GAGCTGAGGAATGACTGGACTGTGCAGGTAGAA
PARK2-PACRG	chr6	162864342	chr6	163483182	5	15	ELRNDWTVQV	CTGAGGAATGACTGGACTGTGCAGGTAGAA
PARK2-PACRG	chr6	162864342	chr6	163483182	6	15	LRNDWTVQV	AGGAATGACTGGACTGTGCAGGTAGAA
PARK2-PACRG	chr6	162864342	chr6	163483182	8	17	NDWTVQVEI	GACTGGACTGTGCAGGTAGAAATTGAG

mRNA and peptide sequences of FusionNeoAntigens that have potential interaction with HLA-IIs.

Fusion gene	Hchr	Hbp	Tchr	Tbp	Start in +/-13AA	End in +/-13AA	FusionNeoAntigen peptide	FusionNEoAntigen RNA sequence
PARK2-PACRG	chr6	162864342	chr6	163483182	1	16	FAGKELRNDWTVQVE	GCAGGGAAGGAGCTGAGGAATGACTGGACTGTGCAGGTAGAAATT
PARK2-PACRG	chr6	162864342	chr6	163483182	10	25	WTVQVEIEKLDYHHY	ACTGTGCAGGTAGAAATTGAGAAGCTGGATTACCATCATTATCTG
PARK2-PACRG	chr6	162864342	chr6	163483182	11	26	TVQVEIEKLDYHHYL	GTGCAGGTAGAAATTGAGAAGCTGGATTACCATCATTATCTGCCT
PARK2-PACRG	chr6	162864342	chr6	163483182	2	17	AGKELRNDWTVQVEI	GGGAAGGAGCTGAGGAATGACTGGACTGTGCAGGTAGAAATTGAG
PARK2-PACRG	chr6	162864342	chr6	163483182	3	18	GKELRNDWTVQVEIE	AAGGAGCTGAGGAATGACTGGACTGTGCAGGTAGAAATTGAGAAG
PARK2-PACRG	chr6	162864342	chr6	163483182	9	24	DWTVQVEIEKLDYHH	TGGACTGTGCAGGTAGAAATTGAGAAGCTGGATTACCATCATTAT

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Information of the samples that have these potential fusion neoantigens of PARK2-PACRG

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 type	Fusion gene	Hchr	Hbp	Henst	Tchr	Tbp	Tenst	Sample
GBM	PARK2-PACRG	chr6	162864342	ENST00000366892	chr6	163483182	ENST00000337019	TCGA-27-1832-01A

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Potential target of CAR-T therapy development for PARK2-PACRG

Predicted 3D structure. We used RoseTTAFold.

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, 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'.

Partner

Gene

Hbp

Tbp

ENST

Strand

BPexon

TotalExon

Protein feature loci

*BPloci

TotalLen

Protein feature

Protein feature note

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.

Hgene

Hchr

Hbp

Henst

Tgene

Tchr

Tbp

Tenst

DeepLoc result

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Related Drugs to PARK2-PACRG

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

Hgene

Tgene

Drug

Source

PMID

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Related Diseases to PARK2-PACRG

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

Hgene

Tgene

Disease

Source

PMID

Diseases associated with fusion partners.
(DisGeNet 4.0)

Partner

Gene

Disease ID

Disease name

# pubmeds

Source

	Fusion Gene and Fusion Protein Summary
	Fusion Amino Acid Sequences (multiple BPs and multiple gene isoforms)
	Fusion Protein Breakpoint Sequences - (for the Screening of the FusionNeoAntigens)
	Potential FusionNeoAntigens in HLA I - (netMHCpan v4.1 + deepHLApan v1.1)
	Potential FusionNeoAntigens in HLA II - (netMHCIIpan v4.1)
	Fusion Breakpoint 14 AA Peptide Structure - (RoseTTAFold)
	Filtering FusionNeoAntigens Through Checking the Interaction with HLAs in 3D - (Glide)
	Vaccine Design for the FusionNeoAntigens (RNA/protein sequences)
	Potential target of CAR-T therapy development
	Information on the samples that have these potential fusion neoantigens
	Fusion Protein Targeting Drugs - (Manual Curation)
	Fusion Protein Related diseases - (Manual Curation)