LZTR1

Based on its role in several tumor types, the LZTR1 protein is thought to act as a tumor suppressor. Tumor suppressors are proteins that keep cells from growing and dividing too rapidly or in an uncontrolled way. The LZTR1 is a non-specific protein that is found in all cells inside the body. It is believed to be a transcriptional regulator that is typically degraded on apoptotic cells. The protein will be phosphorylated at its tyrosine receptors that will target it for degradation. Intracellularly, LZTR proteins will be found in the Golgi apparatus. Studies suggest that the LZTR1 protein may help stabilize this structure. LTZR1 protein could possibly be associated with the CUL3 ubiquitin ligase (Cullin-Based Ubiquitin Ligase 3) complex that helps function to destroy unneeded proteins in the cell. It has also been observed that LZTR protein will inhibit Ras signaling in the membrane by reducing the affinity of Ras to the membrane. Ras belongs to the family of GTPases that are involved in transcription regulation and activation of Raf enzymes. Raf molecules will cascade phosphorylate other molecules in the body to have a wide impact on a cell. Studies using immunoprecipitation of endogenous LZTR1 followed by Western blotting were used to find the function of the LZTR gene. By trapping LZTR1 complexes from intact mammalian cells, Steklov et al. (2018) identified the guanosine triphosphatase RAS as a substrate for the LZTR1-CUL3 complex. == Gene ==

The LZTR 1 gene is located on Chromosome 22: more specifically on the long arm at 22q11.21. The gene is approximately 16,768 base pairs long. == Mutations ==

Studies have found that mutations in the LZTR1 gene were found in malignant cancerous cells in the tumors of patients with glioblastoma. These mutations were found to be somatic, typically caused by environmental factors, and the loss of the LZTR1 gene are seen in the cells that are divided uncontrollably. == DiGeorge Syndrome ==

DiGeorge syndrome == Noonan syndrome ==

Noonan syndrome is an autosomal dominant multisystem disorder characterized by a wide phenotypic spectrum including distinctive facial dysmorphism, postnatal growth retardation, short stature, ectodermal and skeletal defects, congenital heart anomalies, renal anomalies, lymphatic malformations, bleeding difficulties and variable cognitive deficits. Studies have shown that in 29 genes there were 163 variants in patients with Noonan Syndrome. In the study, using In Silco software, the heterozygous missense mutation of the LZTR1 gene at exon 4 was the most pathogenic. This missense mutation will lead to a substitution of an alanine to valine in the primary structure of amino acid for the LZTR protein. == Schwannomatosis ==

In patients with schwannomatosis, more than fifty different mutations in the LZTR1 gene are observed. These mutations themselves are not sufficient to cause the disorder, but are typically associated with it. The somatic changes from environmental factors are also seen in patients with schwannomatosis. When the gene is altered, the LTZR protein cannot function properly to regulate the cell cycle by controlling the growth division. This unregulated growth will lead to non-cancerous (benign) tumors along the peripheral nerves. These tumors are known as Schwannomas. ==References==