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ALK (anaplastic lymphoma kinase)

Identity

HGNC (Hugo) ALK
Location 2p23
Location_base_pair Starts at 29269144 and ends at 29997936 bp from pter ( according to hg18-Mar_2006)  [Mapping]
 
  ALK (2p23) - Courtesy Mariano Rocchi, Resources for Molecular Cytogenetics. Laboratories willing to validate the probes are welcome : contact rocchi@biologia.uniba.it

DNA/RNA

Transcription 6226 bp cDNA; coding sequence: 4.9 kb

Protein

Description 1620 amino acids; 177 kDa; after glycosylation, produces a 200 kDa mature glycoprotein; composed of an extracellular domain, a transmembrane domain, a tyrosine kinase domain, and an intracytoplasmic domain in C-term; dimerization
Expression is tissue specific; mainly in: brain, gut and testis; not in the lymphocytes
Localisation cell membrane
Function membrane associated tyrosine kinase receptor; probable role in the nervous system development and maintenance
Homology homologies with the insulin receptor super family: LTK (leucocyte tyrosine kinase), TRKA, ROS (homolog of the drosophila Sevenless), IGF1-R, IRb

Implicated in

Entity Anaplasic large cell lymphoma (ALCL) with t(2;5)(p23;q35) --> NPM1-ALK
Disease ALCL are high grade non Hodgkin lymphomas; ALK+ ALCL are ALCL where ALK is involved in a fusion gene; ALK+ ALCL represent 50 to 60 % of ALCL cases (they are CD30+, ALK+;); 70 to 80% of ALK+ ALCL cases bear a t(2;5); the remaining ALK+ ALCL cases bear variant translocations described below and are called "cytoplasmic ALK+" cases, of which is the t(1;2) TPM3/ALK, found in 20% of ALK+ ALCL.
Prognosis althouth presenting as a high grade tumour, a 80% five yr survival is associated with this anomaly
Cytogenetics additional anomalies and complex karyotypes are most often found
Hybrid/Mutated Gene 5' NPM1-3' ALK on the der(5)
Abnormal Protein 680 amino acids, 80 kDa; N-term 116 amino acids from NPM1 fused to the 562 C-term aminoacids of ALK (i.e. composed of the oligomerization domain and the metal binding site of NPM1, and the entire cytoplasmic portion of ALK); no apparent expression of the ALK/NPM1 counterpart. Characteristic localisation both in the cytoplasm and in the nucleus, due to heterooligomerization of NPM-ALK and normal NPM whereas the normal NPM protein is confined to the nucleus; constitutive activation of the catalytic domain of ALK.
Oncogenesis via the kinase function activated by oligomerization of NPM1-ALK mediated by the NPM1 part
  
Entity Cytoplasmic ALK+ anaplasic large cell lymphoma
Prognosis present a favourable prognosis comparable to the one found in t(2;5) ALK+ ALCL.
Cytogenetics Either <t(X;2)(q11;p23), t(1;2)(q25;p23), inv(2)(p23q35), t(2;3)(p23;q21), t(2;17)(p23;q23), t(2;17)(p23;q25) or t(2;22)(p23;q11.2); hidden translocation is frequently found.
Hybrid/Mutated Gene 5' MSN, TPM3, ATIC TFG, CLTC, ALO17 or MYH9 - 3' ALK
Abnormal Protein N-term amino acids from the partner gene fused to the 562 C-term amino acids (in the great majority of cases) from ALK (i.e. the entire cytoplasmic portion of ALK with the tyrosine kinase domain); cytoplasmic/membraneous localisation only.
Oncogenesis the partner gene seems to provoke the dimerization of the fused-ALK, which should lead to constitutive autophosphorylation and activation of the ALK tyrosine kinase, as for NPM1-ALK (see t(2;5)(p23;q35) ).
  
Entity Inflammatory myofibroblastic tumours with 2p23 rearrangements
Disease rare soft tissue tumour found in children and young adults about one third to half of inflammatory myofibroblastic tumour cases present with a 2p23 rearrangement involving ALK.
Prognosis good prognosis
Cytogenetics t(1;2)(q25;p23), t(2;2)(p23;q13), t(2;11)(p23;p15), t(2;17)(p23;q23) , or t(2;19)(p23;p13.1) so far
Hybrid/Mutated Gene 5' TPM3 in the t(1;2), RANBP2 in the t(2;2), CARS in the t(2;11), 5' CLTC in the t(2;17), or 5' TPM4 in the t(2;19)- 3' ALK
Abnormal Protein N-term amino acids from the partner gene fused to the 562 C-term amino acids from ALK (i.e. the entire cytoplasmic portion of ALK with the tyrosine kinase domain); homodimerization of the fusion protein is known or suspected.
Oncogenesis fused-ALK is contitutively activated
  

Breakpoints

 
Note Most of the breakpoints occur in the same intron of ALK, whichever partner is involved in the fusion protein

To be noted

ALK and some of the above ALK partners, or closely related genes, are found implicated both in anaplasic large cell lymphoma and in Inflammatory myofibroblastic tumours; this is a new concept, that 2 different types of tumour may result from the same chromosomal/genes rearrangement.

External links

Nomenclature
HGNC (Hugo)ALK   427
Entrez_Gene (NCBI)ALK  238  anaplastic lymphoma receptor tyrosine kinase
Cards
AtlasALK
GeneCards (Weizmann)ALK
Ensembl (Hinxton)ENSG00000171094 [Gene_View]  ALK [Vega]
AceView (NCBI)ALK
Genatlas (Paris)ALK
euGene (Indiana)238
SOURCE (Stanford)NM_004304
Gene Expression (Array Express) ENSG00000171094
Genomic and cartography
GoldenPath (UCSC)ALK  -  2p23   chr2:29269144-29997936 -  2p23   [Description]    (hg18-Mar_2006)
EnsemblALK - 2p23 [CytoView]
Mapping of homologs : NCBIALK [Mapview]
OMIM105590   256700   613014   
Gene and transcription
Gene : Genbank (Entrez)AB209477 AB374361 AB374362 AF125093 AK296218
Reference sequence (RefSeq transcript) :SRSNM_004304
Reference transcript : EntrezNM_004304
RefSeq genomic : SRSAC_000045 AC_000134 NC_000002 NG_009445 NT_022184 NW_001838768 NW_927719
RefSeq genomic : EntrezAC_000045 AC_000134 NC_000002 NG_009445 NT_022184 NW_001838768 NW_927719
Consensus coding sequences : CCDS NCBIALK
Cluster EST : UnigeneHs.654469 [ SRS ] Hs.654469 [ NCBI ]
Alternative Splicing : Fast-db (Paris)3569
Protein : pattern, domain, 3D structure
Protein : UniProt/SwissProtQ9UM73 (SRS) Q9UM73 (Expasy) Q9UM73 (Uniprot)
With graphics : InterProQ9UM73
Splice isoforms : VarSplice FASTAQ9UM73(VarSplice FASTA)
Domaine pattern : Prosite (SRS)LDLRA_1 (PS01209)    LDLRA_2 (PS50068)    MAM_1 (PS00740)    MAM_2 (PS50060)    PROTEIN_KINASE_ATP (PS00107)    PROTEIN_KINASE_DOM (PS50011)    PROTEIN_KINASE_TYR (PS00109)    RECEPTOR_TYR_KIN_II (PS00239)   
Domain pattern : Prosite (Expaxy)LDLRA_1 (PS01209)    LDLRA_2 (PS50068)    MAM_1 (PS00740)    MAM_2 (PS50060)    PROTEIN_KINASE_ATP (PS00107)    PROTEIN_KINASE_DOM (PS50011)    PROTEIN_KINASE_TYR (PS00109)    RECEPTOR_TYR_KIN_II (PS00239)   
Domains : Interpro (SRS)Kinase-like_dom    LDL_rcpt_classA_cys-rich_rpt    MAM    Prot_kinase_cat_dom    Protein_kinase_ATP_BS    Tyr_prot_kinase    Tyr_prot_kinase_AS    Tyr_prot_kinase_cat_dom    Tyr_prot_kinase_rcpt_2_CS    Tyr_prot_kinase_subgr_cat_dom   
Domains : Interpro (EBI)Kinase-like_dom    LDL_rcpt_classA_cys-rich_rpt    MAM    Prot_kinase_cat_dom    Protein_kinase_ATP_BS    Tyr_prot_kinase    Tyr_prot_kinase_AS    Tyr_prot_kinase_cat_dom    Tyr_prot_kinase_rcpt_2_CS    Tyr_prot_kinase_subgr_cat_dom   
Related proteins : CluSTrQ9UM73
Domain families : Pfam SRSMAM (PF00629)    Pkinase_Tyr (PF07714)   
Domain families : Pfam SangerMAM (PF00629)    Pkinase_Tyr (PF07714)   
Domain families : Pfam NCBIpfam00629    pfam07714   
Domain families : Smart EMBLLDLa (SM00192)  TyrKc (SM00219)  
Blocks (Seattle)Q9UM73
Crystal structure of protein : PDB SRS2YS5    2YT2   
Crystal structure of protein : PDBSum2YS5    2YT2   
Crystal structure of protein : IMB2YS5    2YT2   
Crystal structure of protein : PDB RSDB2YS5    2YT2   
HPRD00104
Protein Interaction databases
DIP (DOE-UCLA)Q9UM73
IntAct (EBI)Q9UM73
Polymorphism : SNP, mutations, diseases
Single Nucleotide Polymorphism (SNP) : dbSNP NCBIALK
SNP : GeneSNP UtahALK
SNP : HGBaseALK
Genetic variants : HAPMAPALK
Somatic Mutations in Cancer : COSMICALK 
Rearrangement : COSMICALK 2p23.2  -  MSN Xq11.1
Rearrangement : COSMICCLTC 17q23.1  -  ALK 2p23.2
Rearrangement : COSMICEML4 2p21  -  ALK 2p23.2
Rearrangement : COSMICMSN Xq11.1  -  ALK 2p23.2
Rearrangement : COSMICNPM1 5q35.1  -  ALK 2p23.2
Rearrangement : COSMICRANBP2 2q13  -  ALK 2p23.2
Rearrangement : COSMICSEC31A 4q21.22  -  ALK 2p23.2
Translocation Breakpoints in Cancer : TICdbALK 
Mutations and Diseases : HGMDALK
Hereditary diseases : OMIM105590    256700    613014   
Hereditary diseases : GENETests105590    256700    613014   
Diseases : Genetic AssociationALK
General knowledge
Homologs : HomoloGeneALK
Homology/Alignments : Family Browser UCSCALK
Phylogenetic Trees/Animal Genes : TreeFamALK
Catalytic activity : Enzyme2.7.10.1 [ Enzyme-Expasy ]   2.7.10.1 [ Enzyme-SRS ]   2.7.10.1 [ IntEnz-EBI ]   2.7.10.1 [ BRENDA ]   2.7.10.1 [ KEGG ]   
Chemical/Protein Interactions : CTD238
Keywords Ontology : AmiGOnucleotide binding  transmembrane receptor protein tyrosine kinase activity  receptor signaling protein tyrosine kinase activity  receptor activity  protein binding  ATP binding  integral to plasma membrane  protein amino acid phosphorylation  protein amino acid N-linked glycosylation  transmembrane receptor protein tyrosine kinase signaling pathway  nervous system development  brain development  membrane  transferase activity  
Keywords Ontology : EGO-EBInucleotide binding  transmembrane receptor protein tyrosine kinase activity  receptor signaling protein tyrosine kinase activity  receptor activity  protein binding  ATP binding  integral to plasma membrane  protein amino acid phosphorylation  protein amino acid N-linked glycosylation  transmembrane receptor protein tyrosine kinase signaling pathway  nervous system development  brain development  membrane  transferase activity  
Pathways : BIOCARTA
Pathways : KEGG
Other databases
Probes
ProbeCancer Cytogenetics (Bari)
Probes : ImagenesALK Related clones (RZPD - Berlin)
Literature
PubMed107 Pubmed reference(s) in Entrez
PubGeneALK

Bibliography

Fusion of a kinase gene, ALK, to a nucleolar protein gene, NPM, in non-Hodgkin's lymphoma.
Morris SW, Kirstein MN, Valentine MB, Dittmer KG, Shapiro DN, Saltman DL, Look AT
Science (New York, N.Y.). 1994 ; 263 (5151) : 1281-1284.
PMID 8122112
 
Molecular characterization of ALK, a receptor tyrosine kinase expressed specifically in the nervous system.
Iwahara T, Fujimoto J, Wen D, Cupples R, Bucay N, Arakawa T, Mori S, Ratzkin B, Yamamoto T
Oncogene. 1997 ; 14 (4) : 439-449.
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ALK, the chromosome 2 gene locus altered by the t(2;5) in non-Hodgkin's lymphoma, encodes a novel neural receptor tyrosine kinase that is highly related to leukocyte tyrosine kinase (LTK)
Morris SW, Naeve C, Mathew P, James PL, Kirstein MN, Cui X, Witte DP
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PMID 9174053
 
Role of the nucleophosmin (NPM) portion of the non-Hodgkin's lymphoma-associated NPM-anaplastic lymphoma kinase fusion protein in oncogenesis.
Bischof D, Pulford K, Mason DY, Morris SW
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Recurrent involvement of 2p23 in inflammatory myofibroblastic tumors.
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TRK-fused gene (TFG) is a new partner of ALK in anaplastic large cell lymphoma producing two structurally different TFG-ALK translocations.
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A new fusion gene TPM3-ALK in anaplastic large cell lymphoma created by a (1;2)(q25;p23) translocation.
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Complex variant translocation t(1;2) with TPM3-ALK fusion due to cryptic ALK gene rearrangement in anaplastic large-cell lymphoma.
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TPM3-ALK and TPM4-ALK oncogenes in inflammatory myofibroblastic tumors.
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ATIC-ALK: A novel variant ALK gene fusion in anaplastic large cell lymphoma resulting from the recurrent cryptic chromosomal inversion, inv(2)(p23q35).
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PMID 10702393
 
Inv(2)(p23q35) in anaplastic large-cell lymphoma induces constitutive anaplastic lymphoma kinase (ALK) tyrosine kinase activation by fusion to ATIC, an enzyme involved in purine nucleotide biosynthesis.
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A new variant anaplastic lymphoma kinase (ALK)-fusion protein (ATIC-ALK) in a case of ALK-positive anaplastic large cell lymphoma.
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CD30(+) anaplastic large cell lymphoma: a review of its histopathologic, genetic, and clinical features.
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PMID 11090048
 
Further demonstration of the diversity of chromosomal changes involving 2p23 in ALK-positive lymphoma: 2 cases expressing ALK kinase fused to CLTCL (clathrin chain polypeptide-like).
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PMID 10807789
 
Pathobiology of NPM-ALK and variant fusion genes in anaplastic large cell lymphoma and other lymphomas.
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Fusion of the ALK gene to the clathrin heavy chain gene, CLTC, in inflammatory myofibroblastic tumor.
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Molecular characterization of a new ALK translocation involving moesin (MSN-ALK) in anaplastic large cell lymphoma.
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Identification of novel fusion partners of ALK, the anaplastic lymphoma kinase, in anaplastic large-cell lymphoma and inflammatory myofibroblastic tumor.
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Fusion of ALK to the Ran-binding protein 2 (RANBP2) gene in inflammatory myofibroblastic tumor.
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PMID 12661011
 
Non-muscle myosin heavy chain (MYH9): a new partner fused to ALK in anaplastic large cell lymphoma.
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REVIEW articlesautomatic search in PubMed
Last year publicationsautomatic search in PubMed

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Contributor(s)

Written09-1997Jean-Loup Huret
Updated08-2001Jean-Loup Huret
Updated08-2003Jean-Loup Huret, Sylvie Senon

Citation

This paper should be referenced as such :
Huret JL . ALK (anaplastic lymphoma kinase). Atlas Genet Cytogenet Oncol Haematol. September 1997 .
URL : http://AtlasGeneticsOncology.org/Genes/ALK.html
Huret JL . ALK (anaplastic lymphoma kinase). Atlas Genet Cytogenet Oncol Haematol. August 2001 .
URL : http://AtlasGeneticsOncology.org/Genes/ALK.html
Huret JL, Senon S . ALK (anaplastic lymphoma kinase). Atlas Genet Cytogenet Oncol Haematol. August 2003 .
URL : http://AtlasGeneticsOncology.org/Genes/ALK.html

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indexed on : Sat Feb 6 13:41:36 CET 2010

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