Cancer

Glioblastoma multiforme (GBM); Non-small cell lung cancer (NSCLC)

ROS1 appears to be an 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. ROS is linked to Glioblastoma Multiforme, in which this protein-tyrosine kinase can be constitutively active. This activity can arise either from ROS fusion with the FIG protein or a deletion (q21q21) leading to GOPC-ROS1. Glioblastoma Multiforme is related to astrocytoma and anaplastic astrocytoma, with regions of anaplastic cells surrounding necrotizing tissue. Glioblastoma Multiforme affects brain, endothelial, and bone tissues. Non-small cell lung carcinoma can arise from a SLC34A2-ROS1 fusion expressing the chimeric CD74-ROS1 protein. In non-small cell lung cancer a gain of function has been observed with MLK1 (MAP3K9), activating ERK downstream.
 

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: Uterine leiomyosarcomas (%CFC= +101, p<0.057). The COSMIC website notes an up-regulated expression score for ROS1 in diverse human cancers of 234, which is 0.5-fold of the average score of 462 for the human protein kinases. The down-regulated expression score of 1 for this protein kinase in human cancers was 98% 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. A K1980M mutation can lead to impaired phosphotransferase activity, while the mutations Y2274F or Y2334F can lead to loss of phosphorylation and reduced complex formation with PTPN11.

Percent mutation rates per 100 amino acids length in human cancers: 0.09 % in 25640 diverse cancer specimens. This rate is only 24 % 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: 0.65 % in 805 skin cancers tested; 0.32 % in 1243 large intestine cancers tested; 0.22 % in 629 stomach cancers tested; 0.17 % in 602 endometrium cancers tested; 0.15 % in 1756 lung cancers tested; 0.13 % in 500 urinary tract cancers tested; 0.07 % in 950 upper aerodigestive tract cancers tested; 0.07 % in 904 ovary cancers tested; 0.07 % in 605 oesophagus cancers tested; 0.06 % in 1466 breast cancers tested; 0.06 % in 1314 kidney cancers tested; 0.04 % in 1962 central nervous system cancers tested; 0.04 % in 1942 haematopoietic and lymphoid cancers tested; 0.04 % in 1270 liver cancers tested.

None > 5 in 20,733 cancer specimens

Broad distribution of mutation sites with many point mutations, deletions, and insertions noted on the COSMIC website.