ASpdb: an integrative knowledgebase of human protein isoforms from experimental and AI-predicted structures

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	Protein Summary
	AS Summary
	Protein Functional Features
	Gene Isoform Structures and Expression Levels
	Protein Structures
	pLDDT Score Distribution
	Ramachandran Plot of Protein Structures
	Potential Active Site Information
	Protein Structure and Feature Comparision
	Protein-Protein Interaction
	Related Drugs
	Related Diseases
	Clinically Important Variants

Protein:HNRNPD

Protein Summary

Gene summary

Gene name: HNRNPD
ASpdb.0 ID: 3184
	Gene
Gene symbol	HNRNPD
Gene ID	3184
Gene name	heterogeneous nuclear ribonucleoprotein D
Synonyms	AUF1\|AUF1A\|HNRPD\|P37\|hnRNPD0
Cytomap	4q21.22
Type of gene	protein-coding
Description	heterogeneous nuclear ribonucleoprotein D0ARE-binding protein AUFI, type AAU-rich RNA-binding factor 1AU-rich element RNA binding protein 1, 37kDahnRNP D0
Modification date	20240416
UniProtAcc	Q14103

Gene ontology of this gene with evidence of Inferred from Direct Assay (IDA) from Entrez

Partner	Gene	GO ID	GO term	PubMed ID
Gene	HNRNPD	GO:0003723	RNA binding	8321232
Gene	HNRNPD	GO:0005654	nucleoplasm	-
Gene	HNRNPD	GO:0005829	cytosol	11051545
Gene	HNRNPD	GO:0042162	telomeric DNA binding	8321232
Gene	HNRNPD	GO:0070934	CRD-mediated mRNA stabilization	11051545
Gene	HNRNPD	GO:1900152	negative regulation of nuclear-transcribed mRNA catabolic process, deadenylation-dependent decay	11051545
Gene	HNRNPD	GO:1990904	ribonucleoprotein complex	17289661
Gene	HNRNPD	GO:2000767	positive regulation of cytoplasmic translation	11051545

AS Summary

Information of the canonical protein with experimentally identified structure from PDB (2023).

UniProt Acc	File name	PDB ID	Method	Resolution	Chain	Start	End
Q14103-1	Q14103-1_5im0_B.pdb	5IM0	X-ray	1.7	B	96	174

ASpdb's canonical and alternatively spliced isoform information.

accession_id

gene_name

canonical_id

alternative_id

canonical_length

alternative_length

canonical_start

canonical_end

type

originalSEQ

variationSEQ

alternative_start

alternative_end

Q14103

HNRNPD

Q14103-1

Q14103-2

355

336

Deletion

none

Q14103

HNRNPD

Q14103-1

Q14103-3

355

306

285

334

Substitution

GPSQNWNQGYSNYWNQGYGNYGYNSQGYGGYGGYDYTGYNNYYGYGDYSN

285

Q14103

HNRNPD

Q14103-1

Q14103-4

355

287

Deletion

none

Q14103

HNRNPD

Q14103-1

Q14103-4

355

287

285

334

Substitution

GPSQNWNQGYSNYWNQGYGNYGYNSQGYGGYGGYDYTGYNNYYGYGDYSN

266

Multiple sequence alignment of our canonical and alternatively spliced HNRNPD

Matched gene isoform IDs with Ensembl and RefSeq of our canonical and alternative spliced genes of HNRNPD

UniProt-id	ENSG	ENST	ENSP
Q14103-1	ENSG00000138668.20	ENST00000313899.12	ENSP00000313199.7
Q14103-1	ENSG00000138668.20	ENST00000507010.6	ENSP00000421952.2
Q14103-2	ENSG00000138668.20	ENST00000352301.8	ENSP00000305860.6
Q14103-2	ENSG00000138668.20	ENST00000703971.1	ENSP00000515597.1
Q14103-3	ENSG00000138668.20	ENST00000353341.8	ENSP00000313327.6
Q14103-4	ENSG00000138668.20	ENST00000503822.2	ENSP00000422615.2

UniProt-id	NM ID	NP ID
Q14103-1	NM_031370.2	NP_112738.1
Q14103-2	NM_031369.2	NP_112737.1
Q14103-3	NM_002138.3	NP_002129.2
Q14103-4	NM_001003810.1	NP_001003810.1

Amino acid sequences of our canonical and alternatively spliced HNRNPD

accession_id	Protein sequence
Q14103-1	MSEEQFGGDGAAAAATAAVGGSAGEQEGAMVAATQGAAAAAGSGAGTGGGTASGGTEGGSAESEGAKIDASKNEEDEGHSNSSPRHSEAA TAQREEWKMFIGGLSWDTTKKDLKDYFSKFGEVVDCTLKLDPITGRSRGFGFVLFKESESVDKVMDQKEHKLNGKVIDPKRAKAMKTKEP VKKIFVGGLSPDTPEEKIREYFGGFGEVESIELPMDNKTNKRRGFCFITFKEEEPVKKIMEKKYHNVGLSKCEIKVAMSKEQYQQQQQWG
Q14103-2	MSEEQFGGDGAAAAATAAVGGSAGEQEGAMVAATQGAAAAAGSGAGTGGGTASGGTEGGSAESEGAKIDASKNEEDEGKMFIGGLSWDTT KKDLKDYFSKFGEVVDCTLKLDPITGRSRGFGFVLFKESESVDKVMDQKEHKLNGKVIDPKRAKAMKTKEPVKKIFVGGLSPDTPEEKIR EYFGGFGEVESIELPMDNKTNKRRGFCFITFKEEEPVKKIMEKKYHNVGLSKCEIKVAMSKEQYQQQQQWGSRGGFAGRARGRGGGPSQN
Q14103-3	MSEEQFGGDGAAAAATAAVGGSAGEQEGAMVAATQGAAAAAGSGAGTGGGTASGGTEGGSAESEGAKIDASKNEEDEGHSNSSPRHSEAA TAQREEWKMFIGGLSWDTTKKDLKDYFSKFGEVVDCTLKLDPITGRSRGFGFVLFKESESVDKVMDQKEHKLNGKVIDPKRAKAMKTKEP VKKIFVGGLSPDTPEEKIREYFGGFGEVESIELPMDNKTNKRRGFCFITFKEEEPVKKIMEKKYHNVGLSKCEIKVAMSKEQYQQQQQWG
Q14103-4	MSEEQFGGDGAAAAATAAVGGSAGEQEGAMVAATQGAAAAAGSGAGTGGGTASGGTEGGSAESEGAKIDASKNEEDEGKMFIGGLSWDTT KKDLKDYFSKFGEVVDCTLKLDPITGRSRGFGFVLFKESESVDKVMDQKEHKLNGKVIDPKRAKAMKTKEPVKKIFVGGLSPDTPEEKIR EYFGGFGEVESIELPMDNKTNKRRGFCFITFKEEEPVKKIMEKKYHNVGLSKCEIKVAMSKEQYQQQQQWGSRGGFAGRARGRGGDQQSG

Protein Functional Features

Main function of this protein. (from UniProt)

HNRNPD (go to UniProt):Q14103

Retention analysis result of 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.

- Retained protein feature among the 13 regional features.

Accession_id	Subsection	Start	End	Funcitonal feature	Splicing information
Q14103	Domain	97	179	Note=RRM 1;Ontology_term=ECO:0000255;evidence=ECO:0000255\|PROSITE-ProRule:PRU00176	Type=Deletion;Start=79;End=97
Q14103	Domain	97	179	Note=RRM 1;Ontology_term=ECO:0000255;evidence=ECO:0000255\|PROSITE-ProRule:PRU00176	Type=Deletion;Start=79;End=97
Q14103	Region	1	92	Note=Disordered;Ontology_term=ECO:0000256;evidence=ECO:0000256\|SAM:MobiDB-lite	Type=Deletion;Start=79;End=97
Q14103	Region	1	92	Note=Disordered;Ontology_term=ECO:0000256;evidence=ECO:0000256\|SAM:MobiDB-lite	Type=Deletion;Start=79;End=97
Q14103	Compositional bias	67	92	Note=Basic and acidic residues;Ontology_term=ECO:0000256;evidence=ECO:0000256\|SAM:MobiDB-lite	Type=Deletion;Start=79;End=97
Q14103	Compositional bias	67	92	Note=Basic and acidic residues;Ontology_term=ECO:0000256;evidence=ECO:0000256\|SAM:MobiDB-lite	Type=Deletion;Start=79;End=97

Gene Isoform Structures and Expression Levels for HNRNPD

Gene structures of our canonical and alternative spliced genes of HNRNPD
* Click on the image to open the UCSC genome browser with custom track showing this image in a new window.

Expression levels of gene isoforms across GTEx.

Expression levels of gene isoforms across TCGA.

Protein Structures

PDB and CIF files of the predicted protein structures
* Here we show the 3D structure of the proteins using Mol*. AlphaFold produces a per-residue confidence score (pLDDT) between 0 and 100. Model confidence is shown from the pLDDT values per residue. pLDDT corresponds to the model’s prediction of its score on the local Distance Difference Test. It is a measure of local accuracy (from AlphfaFold website). To color code individual residues, we transformed individual PDB files into CIF format.

3D view using mol* of Q14103-1

3D view using mol* of Q14103-2

3D view using mol* of Q14103-3

3D view using mol* of Q14103-4

pLDDT Score Distribution

pLDDT score distribution of the predicted protein structures from AlphaFold2
* AlphaFold produces a per-residue confidence score (pLDDT) between 0 and 100.

pLDDT distribution across the protein length of Q14103-1

pLDDT distribution across the protein length of Q14103-2

pLDDT distribution across the protein length of Q14103-3

pLDDT distribution across the protein length of Q14103-4

Ramachandran Plot of Protein Structures

Ramachandran plot of the torsional angles - phi (φ)and psi (ψ) - of the residues (amino acids) contained in this protein peptide.

Ramachandran plot of Q14103-1

Ramachandran plot of Q14103-2

Ramachandran plot of Q14103-3

Ramachandran plot of Q14103-4

Potential Active Site Information

The potential binding sites of these proteins were identified using SiteMap, a module of the Schrodinger suite.

UniProt-id	Site score	Size	D score	Volume	Exposure	Enclosure	Contact	Phobic	Philic	Balance	Don/Acc	Residues
Q14103-1	0.942	90	0.959	226.037	0.548	0.656	0.947	0.586	0.999	0.586	0.519	176,178,179,181,182,183,185,227,255,256,257,258,25 9,260,262,263
Q14103-2	0.878	74	0.896	227.066	0.662	0.62	0.854	0.526	0.871	0.604	0.599	159,160,162,163,164,166,208,236,237,238,239,240,24 1,243,244
Q14103-3	0.978	95	1.04	266.854	0.683	0.603	0.792	0.645	0.73	0.884	1.105	176,177,178,179,180,181,183,185,227,233,236,237,24 0,255,256,257,258,259,260,262,263
Q14103-4	0.909	80	0.949	204.771	0.661	0.601	0.854	0.507	0.774	0.655	1.244	68,69,72,74,75,76,77,79,81,110,123,129,132,151,152 ,153,154,155,156

Protein Structure and Feature Comparision

Protein Structure Comparision Using Template Modeling Scores (TM-score).

Protein Structure Comparision Visualization with mol*. between Canonical predicted structure (AF2)(orange) vs Canonical validated structure (PDB)(green)

3D view using mol* of Q14103-1_Q14103-1_5im0_B.pdb

Protein Structure Comparision Visualization with mol*. between Canonical validated structure (PDB)(orange) vs Alternative predicted structure (AF2)(green)

3D view using mol* of Q14103-1_5im0_B_Q14103-2.pdb

3D view using mol* of Q14103-1_5im0_B_Q14103-3.pdb

3D view using mol* of Q14103-1_5im0_B_Q14103-4.pdb

Protein Structure Comparision Visualization with mol*. between Canonical predicted structure (AF2)(orange) vs Alternative predicted structure (AF2)(green)

3D view using mol* of Q14103-1_Q14103-2.pdb

3D view using mol* of Q14103-1_Q14103-3.pdb

3D view using mol* of Q14103-1_Q14103-4.pdb

Protein Feature Comparison of the protein sequendary structures among the protiens.

./stats/secondary_structure/figure/Q14103-1_vs_Q14103-2.png

./stats/secondary_structure/figure/Q14103-1_vs_Q14103-3.png

./stats/secondary_structure/figure/Q14103-1_vs_Q14103-4.png

Protein Feature Comparison of the relative accessible surface area (ASA) among the protiens.

./stats/relative_asa/Q14103-1_vs_Q14103-2.png

./stats/relative_asa/Q14103-1_vs_Q14103-3.png

./stats/relative_asa/Q14103-1_vs_Q14103-4.png

Protein-Protein Interaction

Interactors from UniProt.

Accession_id

Subsection

Start

End

Funcitonal feature

Splicing information

Interactors from STRING.

Gene name

Interactors

Related Drugs to HNRNPD

Drugs targeting this gene/protein.
(DrugBank)

UniProt accession	Gene name	DrugBank ID	Drug name	Drug group	Actions
Q14103	HNRNPD	DB11638	Artenimol	approved, experimental, investigational	ligand

Related Diseases to HNRNPD

Previous studies relating to the alternative splicing of HNRNPD and disease information from the MeSH term (PubMed)

Gene	PMID	Title	Abstract	MeSH ID	MeSH term
HNRNPD	24711643	Identifying biological pathways that underlie primordial short stature using network analysis.	Mutations in CUL7, OBSL1 and CCDC8, leading to disordered ubiquitination, cause one of the commonest primordial growth disorders, 3-M syndrome. This condition is associated with i) abnormal p53 function, ii) GH and/or IGF1 resistance, which may relate to failure to recycle signalling molecules, and iii) cellular IGF2 deficiency. However the exact molecular mechanisms that may link these abnormalities generating growth restriction remain undefined. In this study, we have used immunoprecipitation/mass spectrometry and transcriptomic studies to generate a 3-M 'interactome', to define key cellular pathways and biological functions associated with growth failure seen in 3-M. We identified 189 proteins which interacted with CUL7, OBSL1 and CCDC8, from which a network including 176 of these proteins was generated. To strengthen the association to 3-M syndrome, these proteins were compared with an inferred network generated from the genes that were differentially expressed in 3-M fibroblasts compared with controls. This resulted in a final 3-M network of 131 proteins, with the most significant biological pathway within the network being mRNA splicing/processing. We have shown using an exogenous insulin receptor (INSR) minigene system that alternative splicing of exon 11 is significantly changed in HEK293 cells with altered expression of CUL7, OBSL1 and CCDC8 and in 3-M fibroblasts. The net result is a reduction in the expression of the mitogenic INSR isoform in 3-M syndrome. From these preliminary data, we hypothesise that disordered ubiquitination could result in aberrant mRNA splicing in 3-M; however, further investigation is required to determine whether this contributes to growth failure.	D004392	Dwarfism
HNRNPD	24711643	Identifying biological pathways that underlie primordial short stature using network analysis.	Mutations in CUL7, OBSL1 and CCDC8, leading to disordered ubiquitination, cause one of the commonest primordial growth disorders, 3-M syndrome. This condition is associated with i) abnormal p53 function, ii) GH and/or IGF1 resistance, which may relate to failure to recycle signalling molecules, and iii) cellular IGF2 deficiency. However the exact molecular mechanisms that may link these abnormalities generating growth restriction remain undefined. In this study, we have used immunoprecipitation/mass spectrometry and transcriptomic studies to generate a 3-M 'interactome', to define key cellular pathways and biological functions associated with growth failure seen in 3-M. We identified 189 proteins which interacted with CUL7, OBSL1 and CCDC8, from which a network including 176 of these proteins was generated. To strengthen the association to 3-M syndrome, these proteins were compared with an inferred network generated from the genes that were differentially expressed in 3-M fibroblasts compared with controls. This resulted in a final 3-M network of 131 proteins, with the most significant biological pathway within the network being mRNA splicing/processing. We have shown using an exogenous insulin receptor (INSR) minigene system that alternative splicing of exon 11 is significantly changed in HEK293 cells with altered expression of CUL7, OBSL1 and CCDC8 and in 3-M fibroblasts. The net result is a reduction in the expression of the mitogenic INSR isoform in 3-M syndrome. From these preliminary data, we hypothesise that disordered ubiquitination could result in aberrant mRNA splicing in 3-M; however, further investigation is required to determine whether this contributes to growth failure.	D006130	Growth Disorders
HNRNPD	24711643	Identifying biological pathways that underlie primordial short stature using network analysis.	Mutations in CUL7, OBSL1 and CCDC8, leading to disordered ubiquitination, cause one of the commonest primordial growth disorders, 3-M syndrome. This condition is associated with i) abnormal p53 function, ii) GH and/or IGF1 resistance, which may relate to failure to recycle signalling molecules, and iii) cellular IGF2 deficiency. However the exact molecular mechanisms that may link these abnormalities generating growth restriction remain undefined. In this study, we have used immunoprecipitation/mass spectrometry and transcriptomic studies to generate a 3-M 'interactome', to define key cellular pathways and biological functions associated with growth failure seen in 3-M. We identified 189 proteins which interacted with CUL7, OBSL1 and CCDC8, from which a network including 176 of these proteins was generated. To strengthen the association to 3-M syndrome, these proteins were compared with an inferred network generated from the genes that were differentially expressed in 3-M fibroblasts compared with controls. This resulted in a final 3-M network of 131 proteins, with the most significant biological pathway within the network being mRNA splicing/processing. We have shown using an exogenous insulin receptor (INSR) minigene system that alternative splicing of exon 11 is significantly changed in HEK293 cells with altered expression of CUL7, OBSL1 and CCDC8 and in 3-M fibroblasts. The net result is a reduction in the expression of the mitogenic INSR isoform in 3-M syndrome. From these preliminary data, we hypothesise that disordered ubiquitination could result in aberrant mRNA splicing in 3-M; however, further investigation is required to determine whether this contributes to growth failure.	D009123	Muscle Hypotonia

Clinically important variants in HNRNPD

(ClinVar, 04/20/2024)

accession_id

uniprot_id

gene_name

Type

Variant

Clinical_significance