The a chain contains an N terminal hair pin loop followed by four kringle cdk1 inhibitor domains. The b chain is homologous to serine proteases in the blood clotting cascade, but lacks proteolytic action. Physiologically, c MET is responsible to the cell scattering phenotype, as first demonstrated with MDCK cells treated with HGF.
Through embryogenesis, cdk1 inhibitor this motility func tion of c MET is crucial for the long range migration of skeletal muscle progenitor cells. Ablation of the MET or Hgf gene in mice results in the complete absence of all muscle groups derived from these cells. During development, c MET and HGF provide essential signals for survival and proliferation of hepatocytes and placental trophoblast cells, con sequently, MET or Hgf knockout embryos show markedly reduced liver size. As well, altered pla cental development in Hgf and MET knockout mice is responsible for the death of these animals in utero. The complex phenotype that results from c MET signaling involves a number of molecular events, which have been described in detail in previous reviews.
In addition, unique to c MET is its association with the NSCLC adaptor protein GRB2 associated binding protein 1, a multi adaptor protein that, once bound to and phosphorylated by c MET, creates binding sites for more downstream adaptors. GAB1 can bind either directly to c MET or indi rectly, through GRB2. Additional tyrosines can also contribute to c MET signaling. When Y1313 is phosphorylated, it binds and activates PI3K, which probably promotes cell viability and motility. In addition, Y1365 regulates cell morphogenesis when phosphorylated. The downstream response to c MET activation relies on stereotypical signaling modulators common to many RTKs. These pathways have been reviewed in detail, and are summarized in Figure 2.
The other major arm of c MET signaling is the PI3K/Akt signaling axis. The p85 subunit of PI3K can bind either directly to c MET or indi rectly through GAB1, which then signals through AKT/protein Cell Cycle inhibitor kinase B. This axis is primarily responsible for the cell survival response to c MET signaling .
Wednesday, February 20, 2013
The Interpretation Of cdk1 inhibitor Cell Cycle inhibitor
Subscribe to:
Post Comments (Atom)
No comments:
Post a Comment