Gastrointestinal disorder

Crohn's disease

The pathogenesis of Crohn's disease has been associated with an aberrant autophagic response through an association with the ATG16L1 and IRGM genes, which are involved in autophagic regulation. ULK1 is a downstream effector and negative regulator of both mTOR (via interaction with RPTOR) and AMPK, thus the protein is a key component of the regulatory feedback loops present in autophagy. Crohn's disease is a gastrointestinal disease characterized by excessive and inappropriate inflammation in the gastrointestinal tract. Primary symptoms of the disease include diarrhea, abdominal pain, fever, and weight loss, which can be accompanied by anemia, skin irritation, eye inflammation, and general tiredness. Due to its role in regulating autophagy, ULK1 has been hypothesized to be a suceptibility gene for Crohn's disease. A significantly higher frequency of a particular single nucleotide polymorphism (SNP), the rs12303764(T) allele, was observed in patients with Crohn's disease as compared to controls, indicating that genetic variation in ULK1 may contribute to Crohn's disease suceptibility.
 

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: Colorectal adenocarcinomas (early onset) (%CFC= +81, p<0.004); Oral squamous cell carcinomas (OSCC) (%CFC= +79, p<0.015); Pituitary adenomas (ACTH-secreting) (%CFC= +337); Prostate cancer (%CFC= +49, p<0.015); and Skin squamous cell carcinomas (%CFC= +67, p<0.053). The COSMIC website notes an up-regulated expression score for ULK1 in diverse human cancers of 471, which is close to the average score of 462 for the human protein kinases. The down-regulated expression score of 34 for this protein kinase in human cancers was 0.6-fold of the average score of 60 for the human protein kinases.

Insertional mutagenesis studies in mice support a role for this protein kinase in mouse cancer oncogenesis.

Percent mutation rates per 100 amino acids length in human cancers: 0.07 % in 24726 diverse cancer specimens. This rate is only -1 % lower and is very similar 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: 0.37 % in 864 skin cancers tested; 0.33 % in 1270 large intestine cancers tested; 0.26 % in 589 stomach cancers tested; 0.17 % in 603 endometrium cancers tested; 0.15 % in 1634 lung cancers tested; 0.14 % in 548 urinary tract cancers tested; 0.11 % in 710 oesophagus cancers tested; 0.07 % in 1512 liver cancers tested; 0.07 % in 127 biliary tract cancers tested; 0.05 % in 833 ovary cancers tested; 0.04 % in 1316 breast cancers tested; 0.04 % in 1276 kidney cancers tested; 0.03 % in 558 thyroid cancers tested; 0.03 % in 273 cervix cancers tested; 0.03 % in 1459 pancreas cancers tested; 0.02 % in 881 prostate cancers tested; 0.02 % in 2082 central nervous system cancers tested; 0.01 % in 942 upper aerodigestive tract cancers tested.

Most frequent mutations with the number of reports indicated in brackets: A125T (3).

Thirteen deletions, no insertions and 1 complex mutation are noted on the COSMIC website.