Cancer

ALK-negative anaplastic large cell lymphomas; ALK-positive anaplastic large cell lymphomas; ALK-related neuroblastomas susceptibility; ALK-positive large B-cell lymphomas; ALK+ histiocytosis; neuroblastomas; Anaplastic large cell lymphomas (ALCL); Inflammatory myofibroblastic tumours (IMTs); lung cancer; neuroblastomas 3; Reticulosarcomas; neuroblastomas; Susceptibility; Primary cutaneous anaplastic large cell lymphomas; Follicular dendritic Cell tumours; Tracheal lymphomas

ALK is a known oncoprotein (OP). Cancer-related mutations in human tumours point to a gain of function of the protein kinase. The active form of the protein kinase normally acts to promote tumour cell proliferation. Chromosomal rearrangments (most common), mutations, and amplifications with the ALK gene are associated with numerous tumours including: anaplastic large cell lymphomas, neuroblastomas, and non-small cell lung cancer. These fusion proteins, as well as other mutations and amplifications, likely confer heightened (possibly consititutive) phosphotransferase activity and promote cell growth and anti-apoptotic pathways such as the Akt and MAPK pathways. In Neuroblastoma 3 (NBLST3), there was constitutive activation, and Endoplasmic Reticulum or Golgi Apparatus localization when ALK had gain of function mutations with F1174I or F1174V (located in the kinase catalytic subdomain III) or R1275Q (located just before the kinase catalytic Subdomain VII). NBLST3 is a common neoplasm of early childhood resulting from the embryonic cells that form the primitive neural crest and generate the adrenal medulla and the sympathetic nervous system. Large-cell lymphomas make up 25% of non-Hodgkin lymphomas. Non-Hodgkin lymphomas are cancers beginning in the lymphatic system, and they arise from B- or T- cells. Non-Hodgkin lymphomas spread in an unpredictable way (distinguishing it from Hodgkin lymphomas), and manifests in at least 30 forms of cancer. Translocations of the ALK gene resulting in fusion proteins with NPM1 are observed in 5-10% of non-Hodgkin lymphomas, with CARS and SEC31A in inflammatory myofibroblastic tumours (IMTs) and ALO17 in anaplastic large-cell lymphoma (ALCL). The genes C/EBPB, and BCL2A1 are essential for ALCL growth and transcriptionally induced by ALK.
 

TranscriptoNET (www.transcriptonet.ca) analysis with mRNA expression data retrieved from the National Center for Biotechnology Information's Gene Expression Omnibus (GEO) database, which was normalized against 60 abundantly and commonly found proteins, indicated altered expression for this protein kinase as shown here as the percent change from normal tissue controls (%CFC) as supported with the Student T-test in the following types of human cancers: Bladder carcinomas (%CFC= -53, p<0.0001); Breast epithelial cell carcinomas (%CFC= -47, p<0.061); and Ovary adenocarcinomas (%CFC= +169, p<0.096). The COSMIC website notes an up-regulated expression score for ALK in diverse human cancers of 353, which is 0.8-fold of the average score of 462 for the human protein kinases. The down-regulated expression score of 0 for this protein kinase in human cancers was 100% lower than the average score of 60 for the human protein kinases.

Insertional mutagenesis studies in mice have not yet revealed a role for this protein kinase in mouse cancer oncogenesis.

Percent mutation rates per 100 amino acids length in human cancers: 0.16 % in 32013 diverse cancer specimens. This rate is 2.2-fold higher than the average rate of 0.075 % calculated for human protein kinases in general.

Highest percent mutation rates per 100 amino acids length in human cancers: 0.57 % in 1279 large intestine cancers tested; 0.55 % in 2710 autonomic ganglia cancers tested; 0.52 % in 994 skin cancers tested; 0.27 % in 2128 lung cancers tested; 0.25 % in 619 stomach cancers tested; 0.2 % in 603 endometrium cancers tested; 0.17 % in 607 oesophagus cancers tested; 0.11 % in 694 thyroid cancers tested; 0.1 % in 930 upper aerodigestive tract cancers tested; 0.08 % in 968 ovary cancers tested; 0.06 % in 2042 haematopoietic and lymphoid cancers tested; 0.06 % in 1271 liver cancers tested; 0.05 % in 2315 breast cancers tested.

Most frequent mutations with the number of reports indicated in brackets: F1174L (146); F1174C (13); F1174V (7); F1174I (6); R1275Q (87); F125V (11); F125C (9); F125I (6).

Only 7 deletions, 2 insertions and 2 complex mutations are noted on the COSMIC website.