Cancer, immune, respiratory, bone, and skin disorders

Protein-tyrosine kinase 2 deficiency (TYK2 deficiency); Hyper Ige syndrome (HIES); Venezuelan equine encephalitis; Subacute cutaneous lupus erythematosus (SCLE); Polyarticular onset juvenile Idiopathic arthritis; Oligoarticular juvenile arthritis; Familial atypical mycobacteriosis, Tyk2-related

Protein-tyrosine kinase 2 deficiency (TYK2 deficiency) is a disorder consisting of a defective immune system and is characterized by pneumonia, skin abscesses, and high levels of IgE in serum. Hyper Ige Syndrome (HIES) is a rare immunodeficiency disorder where serum IgE may be elevated, and the skin may be inflamed. One form of HIES, AD-HIES, is characterized by connective tissue issues, skeletal deformations, distinct facial structure, and dental abnormalities. The AR-HIES form of the disease is characterized by extreme hypereosinophilia, viral infection susceptibility, an abnormal central nervous system, and T-cell defects. Venezuelan Equine Encephalitis is a rare infectious disorder which is characterized by inflammation of the brain in humans or horses. Subacute Cutaneous Lupus Erythematosus (SCLE) is a rare immune and skin disorder that results in scaled lesions on skin. SCLE can affect skin, T cells, and lung tissues. Polyarticular Onset Juvenile Idiopathic Arthritis is a rare respiratory and bone disorder which has been related to Juvenile Rheumatoid Arthritis and Rheumatoid Arthritis. Some symptoms of Polyarticular Onset Juvenile Idiopathic Arthritis include biological inflammatory syndrome, upregulated erythrocyte sedimentation rate, and autoimmunity. Oligoarticular Juvenile Arthritis is characterized by joint pain, hydrarthrosis, and autoimmunity. Oligoarticular Juvenile Arthritis can affect the eye, bone, and T cells.
 

Polycythemia vera (PV); Gallbladder adenocarcinomas

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: Barrett's esophagus epithelial metaplasia (%CFC= +98, p<0.025); Bladder carcinomas (%CFC= +59, p<0.002); Brain glioblastomas (%CFC= -97, p<0.0001); Brain oligodendrogliomas (%CFC= -90, p<0.0001); Breast epithelial cell carcinomas (%CFC= +60, p<0.003); Cervical cancer (%CFC= -59, p<0.0001); Classical Hodgkin lymphomas (%CFC= +66, p<0.0005); Large B-cell lymphomas (%CFC= +136, p<0.0004); Ovary adenocarcinomas (%CFC= +65, p<0.032); Skin fibrosarcomas (%CFC= +65); and Skin melanomas - malignant (%CFC= +86, p<0.0001). The COSMIC website notes an up-regulated expression score for TYK2 in diverse human cancers of 544, which is 1.2-fold of the average score of 462 for the human protein kinases. The down-regulated expression score of 151 for this protein kinase in human cancers was 2.5-fold of 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: 0.08 % in 25688 diverse cancer specimens. This rate is very similar (+ 3% higher) to 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: 0.29 % in 805 skin cancers tested; 0.29 % in 1093 large intestine cancers tested; 0.22 % in 602 endometrium cancers tested; 0.19 % in 589 stomach cancers tested; 0.19 % in 500 urinary tract cancers tested; 0.14 % in 605 oesophagus cancers tested; 0.1 % in 1941 lung cancers tested; 0.09 % in 904 ovary cancers tested; 0.06 % in 1522 breast cancers tested; 0.05 % in 2228 haematopoietic and lymphoid cancers tested.

Most frequent mutations with the number of reports indicated in brackets: N346T (4); G422S (4).

Only 1 deletion, 3 insertions and 1 complex mutations are noted on the COSMIC website.