Cancer, physiological development, and retinal disorders

Van Der Woude syndrome (LDS); Retinitis pigmentosa 67 (RP67); Leber congenital amaurosis (CRB)

Van Der Woude Syndrome (LDS) is a development disease affecting the structure of the face, often characterized by cleft lip and, or a cleft palate. LDS can affec the testis, brain, and salivary glands. Retinitis Pigmentosa 67 (RP67) is normally expressed in the cells at the back of the eye. RP67 is typically characterized by loss of rod photoreceptor cells followed by loss of cone cells, leading to night vision blindness, and loss of the midperipheral vision field. Leber Congenital Amaurosis (CRB) is a rare condition characterized by vision impairment during early infancy, photophobia, nystagmus (uncontrolled eye movement), far-sightedness, night blindness, abnormal pupil reactivity, and abnormal scaring. CRB affects the retina, but can also affect the eye and testis tissues.
 

Plexiform Neurofibromas; Polyploidy; Breast cancer

NEK2 is linked to Plexiform Neurofibromas, which are related to the disorders neurofibroma and neurofibromatosis disorders, and can affect skin, salivary gland, and bone tissues. Polyploidy is the abnormal duplication of chromosomes above the typical diploid level. Polyploidy is linked to breast cancer and melanoma, and most often affects smooth muscle, liver, and breast tissues. NEK2 has been associated with both primary and secondary breast tumours.
 

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= +162, p<0.013); Breast epithelial carcinomas (%CFC= +309, p<0.068); Breast non-basal-like cancer (BLC) (%CFC= +76, p<0.0001); Breast sporadic basal-like cancer (BLC) (%CFC= +102, p<0.0001); Cervical cancer (%CFC= -79, p<0.0001); Colon mucosal cell adenomas (%CFC= +147, p<0.0001); Oral squamous cell carcinomas (OSCC) (%CFC= +227, p<0.006); Ovary adenocarcinomas (%CFC= +428, p<0.0009); Prostate cancer (%CFC= -58, p<0.025); and Vulvar intraepithelial neoplasia (%CFC= +307, p<0.0004). The COSMIC website notes an up-regulated expression score for NEK2 in diverse human cancers of 878, which is 1.9-fold of the average score of 462 for the human protein kinases. The down-regulated expression score of 11 for this protein kinase in human cancers was 0.2-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. The ability for NEK2 to activate NEK11 is lost with a K37R mutation. The autophosphorylation of NEK2 can be inhibited with a D141A mutation. NEK2 kinase phosphotransferase activity can be increased 2-fold with a T170E, or S171D or T175E mutation, while the phosphotransferase activity can be decreased two-fold with a T175A mutation. Complete kinase phosphotransferase activity can be lost with a T179A, T179E, S241A or S241D mutation.

Percent mutation rates per 100 amino acids length in human cancers: 0.05 % in 25158 diverse cancer specimens. This rate is only -38 % lower 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: 0.29 % in 864 skin cancers tested; 0.22 % in 603 endometrium cancers tested; 0.1 % in 1512 liver cancers tested; 0.09 % in 238 bone cancers tested; 0.09 % in 1270 large intestine cancers tested; 0.08 % in 273 cervix cancers tested; 0.08 % in 1490 breast cancers tested; 0.05 % in 1768 lung cancers tested.

Most frequent mutations with the number of reports indicated in brackets: S296L (4).

Only 1 deletion, and no insertions or complex mutations are noted on the COSMIC website.