DDR1 (discoidin domain receptor tyrosine kinase 1)

2011-05-01 Barbara Roig , Elisabet Vilella Affiliation

Hospital Psiquiatic Universitari Institut Pere Mata, IISPV, Universitat Rovira i Virgili, C\\\/Sant Llorenc 21, 43201 REUS, Spain

Identity

HGNC

DDR1

LOCATION

6p21.33

LOCUSID

780

ALIAS

CAK,CD167,DDR,EDDR1,HGK2,MCK10,NEP,NTRK4,PTK3,PTK3A,RTK6,TRKE

FUSION GENES

Show Gene Fusions

DNA/RNA

Genomic organisation of the DDR1 gene on chromosome 6. Exons that are implicated in the alternative splicing process of the DDR1 gene are represented by open boxes. The alternative splicing process of exon 10 to exon 14 generates 5 DDR1 isoforms, which are affixed a-e.

Description

The DDR1 gene comprises 17 exons and spans 12 kb of the genomic sequence on chromosome 6 (from position 30851861 bp to 30867933 bp in the positive strand orientation).

Transcription

The 3840-bp mRNA is transcribed in a centromeric to telomeric orientation. Alternative splicing can occur, and 5 named isoforms (DDR1a-e) are recognised.

Pseudogene

No pseudogene has been described.

Proteins

Schematic diagram of the DDR1 protein and localization of the DDR1 Tyrosine phosphorylated sites at intracellular domain.

Description

DDR1 belongs to the DDRs subfamily of tyrosine kinase receptors. This subfamily is composed of only two members, DDR1 and DDR2, and it is distinguished by an extracellular domain that is homologous to the carbohydrate-binding lectin discoidin-I in Dictyostelium discoideum. The Discoidin domain is essential for the ability of DDRs to bind ligands. To-date, collagen is the only unique DDR1 ligand that has been identified. Five isoforms of DDR1 that are generated by alternative splicing have been described. The longest DDR1 transcript codes for the full-length receptor (DDR1c isoform) and is composed of 919 amino acids. DDR1a and DDR1b isoforms lack 37 amino acids in the juxtamembrane domain or 6 amino acids in the kinase domain. DDR1d and DDR1e isoforms are C-terminally truncated receptors. DDR1d lacks exons 11 and 12 causing a frame-shift mutation that generates a stop codon and premature termination of transcription. Finally, DDR1e lacks exons 11 and 12 as well as the first half of exon 10 (Alves et al., 1995).

Expression

DDR1 is ubiquitously expressed in a variety of epithelial tissues (Alves et al., 1995; Curat and Vogel, 2002; Ferri et al., 2004; Hou et al., 2001; Mohan et al., 2001; Sakamoto et al., 2001; Tanaka et al., 1998). DDR1 is also expressed in endothelial blood capillary cells and oligodendrocytes in the human brain (Franco-Pons et al., 2009; Roig et al., 2010). DDR1 is significantly overexpressed in several human cancers (Barker et al., 1995; Colas et al., 2011; Ford et al., 2007; Hajdu et al., 2010; Heinzelmann-Schwarz et al., 2004; Laval et al., 1994; Nemoto et al., 1997; Park et al., 2007; Tun et al., 2011; Weiner et al., 1996; Weiner et al., 2000; Yamanaka et al., 2006; Yoshida et al., 2007) and carcinoma cell lines (Alves et al., 1995; Gu et al., 2011; Park et al., 2007; Sakuma et al., 1996).

Localisation

Transmembrane.

Function

Receptor tyrosine kinases are key components of several signal transduction pathways. These kinases control multiple cellular processes, including motility, proliferation, differentiation, metabolism and survival.
DDR1 is actively involved in tumorigenesis and promotes the proliferation of neoplasic cells. The interaction of DDR1 and Notch1 displays a prosurvival effect (Kim et al., 2011). DDR1 participates in the collective migration of cancer cells by coordinating the cell polarity regulators Par3 and Par6 (Hidalgo-Carcedo et al., 2011).

Homology

- P. troglodytes, discoidin domain receptor tyrosine kinase 1, DDR1
- C. lupus, discoidin domain receptor tyrosine kinase 1, DDR1
- M. musculus, discoidin domain receptor family member 1, Ddr1
- R. norvegicus, discoidin domain receptor tyrosine kinase 1

Mutations

Note

Few somatic mutations have been described. Four mutations (G1486T, A496S, CC2469/2470TT, R824W) have been identified in a cohort of 26 primary lung neoplasms (Davies et al., 2005). One somatic mutation (A803V) was found in 4 acute myeloid leukaemia patients (Tomasson et al., 2008).

Implicated in

Entity name

Breast cancer

Note

DDR1 overexpression was observed in human primary breast tumours samples compared to that in normal breast tissues (Barker et al., 1995). In addition, invasive ductal and lobular carcinomas showed differential expression of DDR1. DDR1 was downregulated in lobular carcinomas (Turashvili et al., 2007a; Turashvili et al., 2007b).

Entity name

Osteosarcoma

Note

The DDR1 promoter presents a potential p53 binding-site. A previous study has shown that p53 expression upregulated the mRNA expression levels of DDR1 in human osteosarcoma cells (Sakuma et al., 1996).

Entity name

Oesophageal cancer

Note

The overexpression of DDR1 was reported in 12 carcinomatous oesophageal tissues compared to that in normal tissues. Furthermore, a positive correlation was identified between DDR1 mRNA expression and the proliferative activity of the tumoural cells (Nemoto et al., 1997).

Entity name

Ovarian cancer

Note

DDR1 was highly expressed in 158 histological subtypes of primary epithelial ovarian cancers (EOC) compared to that in normal ovarian surface epithelium samples (Heinzelmann-Schwarz et al., 2004).

Entity name

Endometrial cancer

Note

DDR1 has been implicated as a potential molecular marker of endometrial cancer (Colas et al., 2011; Domenyuk et al., 2007). A gene expression screening of 52 carcinomas samples showed differential expression of several genes, including the DDR1 gene. These data were also demonstrated in 50 tumoural and non-tumoural uterine aspirates (Colas et al., 2011).

Entity name

Brain tumours

Note

DDR1 was originally isolated in malignant childhood brain tumours, which overexpressed DDR1 (Weiner et al., 1996). Replicable findings were found in metastatic brain neoplasms and glioma cells (Yamanaka et al., 2006; Weiner et al., 2000). In glioma cells, DDR1 was involved in cell proliferation and invasion via cell interactions with the extracellular matrix (Ram et al., 2005; Yamanaka et al., 2006). Moreover, a study on DDR1a and DDR1b isoforms overexpression in glioma cells has identified distinct roles for each DDR1 isoforms in the cell attachment process, which is mediated by collagen I (Ram et al., 2005). The analysis of the expression profile in mice that had PDGF-induced glioma showed overexpression of DDR1 (Johansson et al., 2005).

Entity name

Primary central nervous system lymphoma (PCNSL)

Note

A PCNSL pathway analysis revealed upregulation of DDR1 expression in the extracellular matrix and the adhesion-related pathways (Tun et al., 2011).

Entity name

Pituitary adenoma

Note

In different subtypes of pituitary adenoma, DDR1 expression was related to the hormonal background. DDR1 was more highly expressed in macroadenomas, compared to microadenomas, and in PRL- and GH-producing adenomas (Yoshida et al., 2007).

Entity name

Lung cancer

Note

DDR1 was upregulated in tumour lung tissue compared to that in normal tissue and was an independent favourable predictor for prognosis (Ford et al., 2007). Similarly, DDR1 was highly phosphorylated in non-small cell lung cancer (NSCLC) (Rikova et al., 2007).
One study described the presence of DDR1 somatic mutations in lung cancer (Davies et al., 2005). However, no mutations were detected in another lung cancer study (Ford et al., 2007).

Entity name

Liver cancer

Note

DDR1a and DDR1b isoforms were overexpressed in hepatocellular carcinoma cell lines HLE and Huh-7. DDR1 isoform overexpression enhanced the migration and invasion of the hepatocellular carcinoma cell lines in association with the matrix metalloproteinases MMP2 and MMP9 (Park et al., 2007).
The downregulation of miR-199a-5p, which is a direct target of DDR1, deregulated DDR1 functionality and increased cell invasion in human hepatocellular carcinoma (HCC) (Shen et al., 2010).
Finally, a profiling study on receptor tyrosine kinase phosphorylation in cholangiocarcinoma patients showed high levels of phosphorylation of DDR1 and other tyrosine kinases in tumour tissues in comparison to para-tumour tissues (Gu et al., 2011).

Entity name

Mesenchymal neoplasm

Note

Solitary fibrous tumour (SFT) expression profiling of 23 samples showed an over-expression of several receptor tyrosine kinase genes, including DDR1. However, no mutations were identified using cDNA sequencing (Hajdu et al., 2010).

Article Bibliography

Pubmed ID	Last Year	Title	Authors
11344127	2001	Identification of two novel, kinase-deficient variants of discoidin domain receptor 1: differential expression in human colon cancer cell lines.	Alves F et al
7845687	1995	Distinct structural characteristics of discoidin I subfamily receptor tyrosine kinases and complementary expression in human cancer.	Alves F et al
7845682	1995	Expression patterns of the novel receptor-like tyrosine kinase, DDR, in human breast tumours.	Barker KT et al
21207424	2011	Molecular markers of endometrial carcinoma detected in uterine aspirates.	Colas E et al
12397034	2002	Discoidin domain receptor 1 controls growth and adhesion of mesangial cells.	Curat CA et al
16140923	2005	Somatic mutations of the protein kinase gene family in human lung cancer.	Davies H et al
17704737	2007	Identification of new DNA markers of endometrial cancer in patients from the Ukrainian population.	Domenyuk VP et al
15111304	2004	Role of discoidin domain receptors 1 and 2 in human smooth muscle cell-mediated collagen remodeling: potential implications in atherosclerosis and lymphangioleiomyomatosis.	Ferri N et al
17299390	2007	Expression and mutation analysis of the discoidin domain receptors 1 and 2 in non-small cell lung carcinoma.	Ford CE et al
18836851	2009	Discoidin domain receptor 1, a tyrosine kinase receptor, is upregulated in an experimental model of remyelination and during oligodendrocyte differentiation in vitro.	Franco-Pons N et al
21253578	2011	Survey of tyrosine kinase signaling reveals ROS kinase fusions in human cholangiocarcinoma.	Gu TL et al
20527023	2010	IGF2 over-expression in solitary fibrous tumours is independent of anatomical location and is related to loss of imprinting.	Hajdu M et al
15240533	2004	Overexpression of the cell adhesion molecules DDR1, Claudin 3, and Ep-CAM in metaplastic ovarian epithelium and ovarian cancer.	Heinzelmann-Schwarz VA et al
21170030	2011	Collective cell migration requires suppression of actomyosin at cell-cell contacts mediated by DDR1 and the cell polarity regulators Par3 and Par6.	Hidalgo-Carcedo C et al
15750623	2005	Expression analysis of genes involved in brain tumor progression driven by retroviral insertional mutagenesis in mice.	Johansson FK et al
21398698	2011	DDR1 receptor tyrosine kinase promotes prosurvival pathway through Notch1 activation.	Kim HG et al
9396043	1997	Overexpression of protein tyrosine kinases in human esophageal cancer.	Nemoto T et al
17982627	2007	Overexpression of discoidin domain receptor 1 increases the migration and invasion of hepatocellular carcinoma cells in association with matrix metalloproteinase.	Park HS et al
8622863	1996	Identification of two isoforms of the Cak receptor kinase that are coexpressed in breast tumor cell lines.	Perez JL et al
16234985	2006	Discoidin domain receptor-1a (DDR1a) promotes glioma cell invasion and adhesion in association with matrix metalloproteinase-2.	Ram R et al
18083107	2007	Global survey of phosphotyrosine signaling identifies oncogenic kinases in lung cancer.	Rikova K et al
8977099	1996	Receptor protein tyrosine kinase DDR is up-regulated by p53 protein.	Sakuma S et al
20799954	2010	Role of microRNA-199a-5p and discoidin domain receptor 1 in human hepatocellular carcinoma invasion.	Shen Q et al
18270328	2008	Somatic mutations and germline sequence variants in the expressed tyrosine kinase genes of patients with de novo acute myeloid leukemia.	Tomasson MH et al
18184868	2008	Pathway analysis of primary central nervous system lymphoma.	Tun HW et al
17690741	2007	Novel immunohistochemical markers for the differentiation of lobular and ductal invasive breast carcinomas.	Turashvili G et al
11126911	2000	Consistent and selective expression of the discoidin domain receptor-1 tyrosine kinase in human brain tumors.	Weiner HL et al
9075249	1996	Pediatric brain tumors express multiple receptor tyrosine kinases including novel cell adhesion kinases.	Weiner HL et al
16652150	2006	Identification of expressed genes characterizing long-term survival in malignant glioma patients.	Yamanaka R et al
17001518	2007	Enhancement of pituitary adenoma cell invasion and adhesion is mediated by discoidin domain receptor-1.	Yoshida D et al

Other Information

Locus ID:

NCBI: 780
MIM: 600408
HGNC: 2730
Ensembl: ENSG00000204580

Variants:

dbSNP: 780
ClinVar: 780
TCGA: ENSG00000204580
COSMIC: DDR1

RNA/Proteins

Gene ID	Transcript ID	Uniprot
ENSG00000204580	ENST00000324771	Q08345
ENSG00000204580	ENST00000324771	A0A024RCL1
ENSG00000204580	ENST00000376567	Q08345
ENSG00000204580	ENST00000376567	A0A024RCQ1
ENSG00000204580	ENST00000376568	Q08345
ENSG00000204580	ENST00000376568	A0A024RCL1
ENSG00000204580	ENST00000376569	Q08345
ENSG00000204580	ENST00000376569	A0A024RCQ1
ENSG00000204580	ENST00000376570	Q08345
ENSG00000204580	ENST00000376570	A0A024RCQ1
ENSG00000204580	ENST00000376575	Q08345
ENSG00000204580	ENST00000396342	A2ABL0
ENSG00000204580	ENST00000412274	D6RBU7
ENSG00000204580	ENST00000417521	A2ABM8
ENSG00000204580	ENST00000418800	Q08345
ENSG00000204580	ENST00000418800	A0A024RCQ1
ENSG00000204580	ENST00000421124	A2ABL2
ENSG00000204580	ENST00000424544	H0Y717
ENSG00000204580	ENST00000428153	E7EQ30
ENSG00000204580	ENST00000437124	E7ERI6
ENSG00000204580	ENST00000446312	A0A0A0MSX3
ENSG00000204580	ENST00000452441	Q08345
ENSG00000204580	ENST00000452441	A0A024RCL1
ENSG00000204580	ENST00000454612	Q08345
ENSG00000204580	ENST00000454612	A0A024RCQ1
ENSG00000204580	ENST00000460944	E7EPH4
ENSG00000204580	ENST00000482873	Q08345
ENSG00000204580	ENST00000484556	H0Y9F4
ENSG00000204580	ENST00000502955	D6RB82
ENSG00000204580	ENST00000503180	D6RB35
ENSG00000204580	ENST00000503495	E7EUP7
ENSG00000204580	ENST00000503628	D6RAJ3
ENSG00000204580	ENST00000503670	D6R9C4
ENSG00000204580	ENST00000504651	E7EX99
ENSG00000204580	ENST00000504679	E7ETX3
ENSG00000204580	ENST00000504927	E7ETI3
ENSG00000204580	ENST00000505066	E7EVW6
ENSG00000204580	ENST00000505534	E7EN94
ENSG00000204580	ENST00000507046	E7EQ23
ENSG00000204580	ENST00000507901	E7EXB0
ENSG00000204580	ENST00000508312	Q08345
ENSG00000204580	ENST00000508317	E7EUD5
ENSG00000204580	ENST00000509639	E7ES06
ENSG00000204580	ENST00000511510	E7ESR9
ENSG00000204580	ENST00000512336	E7EVT1
ENSG00000204580	ENST00000512694	E7EPN2
ENSG00000204580	ENST00000512725	E7ERN0
ENSG00000204580	ENST00000513043	D6RB35
ENSG00000204580	ENST00000513240	Q08345
ENSG00000204580	ENST00000513240	A0A024RCJ0
ENSG00000204580	ENST00000513749	D6RAJ3
ENSG00000204580	ENST00000514434	H0YAH6
ENSG00000204580	ENST00000515219	D6RGW5
ENSG00000204580	ENST00000515233	E7ERN0
ENSG00000204580	ENST00000515881	E7ENJ2

Expression (GTEx)

100

150

Adipose - Subcutaneous

Adipose - Visceral

Adrenal Gland

Artery - Aorta

Artery - Tibial

Bladder

Brain - Amygdala

Brain - Anterior cingulate cortex

Brain - Caudate

Brain - Cerebellar Hemisphere

Brain - Cerebellum

Brain - Cortex

Brain - Frontal Cortex

Brain - Hippocampus

Brain - Hypothalamus

Brain - Nucleus accumbens

Brain - Putamen

Brain - Spinal cord

Brain - Substantia nigra

Breast - Mammary Tissue

Cells - Cultured fibroblasts

Cells - EBV - transformed lymphocytes

Cervix - Ectocervix

Cervix - Endocervix

Colon - Sigmoid

Colon - Transverse

Esophagus - Gastroesophageal Junction

Esophagus - Mucosa

Esophagus - Muscularis

Fallopian Tube

Heart - Atrial Appendage

Heart - Left Ventricle

Kidney - Cortex

Kidney - Medulla

Liver

Lung

Minor Salivary Gland

Muscle - Skeletal

Nerve - Tibial

Ovary

Pancreas

Pituitary

Prostate

Skin - Not Sun Exposed

Skin - Sun Exposed

Small Intestine - Terminal Ileum

Spleen

Stomach

Testis

Thyroid

Uterus

Vagina

Whole Blood

Pathways

Pathway	Source	External ID
Extracellular matrix organization	REACTOME	R-HSA-1474244
Non-integrin membrane-ECM interactions	REACTOME	R-HSA-3000171

Protein levels (Protein atlas)

Not detected

Low

Medium

High

References

Pubmed ID	Year	Title	Citations
36809965	2024	DDR1-Induced Paracrine Factors of Hepatocytes Promote HSC Activation and Fibrosis Development.	0
38395959	2024	Coexpression network analysis of the adult brain sheds light on the pathogenic mechanism of DDR1 in schizophrenia and bipolar disorder.	0
38570692	2024	Inactivation of kindlin-3 increases human melanoma aggressiveness through the collagen-activated tyrosine kinase receptor DDR1.	0
36809965	2024	DDR1-Induced Paracrine Factors of Hepatocytes Promote HSC Activation and Fibrosis Development.	0
38395959	2024	Coexpression network analysis of the adult brain sheds light on the pathogenic mechanism of DDR1 in schizophrenia and bipolar disorder.	0
38570692	2024	Inactivation of kindlin-3 increases human melanoma aggressiveness through the collagen-activated tyrosine kinase receptor DDR1.	0
36675255	2023	DDR1 and Its Ligand, Collagen IV, Are Involved in In Vitro Oligodendrocyte Maturation.	1
37117273	2023	Collagen I-DDR1 signaling promotes hepatocellular carcinoma cell stemness via Hippo signaling repression.	2
37201403	2023	Collagen-induced DDR1 upregulates CXCL5 to promote neutrophil extracellular traps formation and Treg infiltration in breast cancer.	4
37768856	2023	Discoidin Domain Receptor Tyrosine Kinase 1 (DDR1) Is a Novel Therapeutic Target in Liposarcoma: A Tissue Microarray Study.	0
36675255	2023	DDR1 and Its Ligand, Collagen IV, Are Involved in In Vitro Oligodendrocyte Maturation.	1
37117273	2023	Collagen I-DDR1 signaling promotes hepatocellular carcinoma cell stemness via Hippo signaling repression.	2
37201403	2023	Collagen-induced DDR1 upregulates CXCL5 to promote neutrophil extracellular traps formation and Treg infiltration in breast cancer.	4
37768856	2023	Discoidin Domain Receptor Tyrosine Kinase 1 (DDR1) Is a Novel Therapeutic Target in Liposarcoma: A Tissue Microarray Study.	0
35032738	2022	Identification of novel discoidin domain receptor 1 (DDR1) inhibitors using E-pharmacophore modeling, structure-based virtual screening, molecular dynamics simulation and MM-GBSA approaches.	13

Citation

Barbara Roig ; Elisabet Vilella

DDR1 (discoidin domain receptor tyrosine kinase 1)

Atlas Genet Cytogenet Oncol Haematol. 2011-05-01

Online version: http://atlasgeneticsoncology.org/gene/40280/case-report-explorer/js/gene-explorer/